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Double-Blinded, Placebo-Controlled Cross-Over Trial to Determine the Effects of Midodrine on Blood Pressure during Cognitive Testing in Persons with SCI

Double-Blinded, Placebo-Controlled Cross-Over Trial to Determine the Effects of Midodrine on... Study Design: Clinical trial. Objectives: Individuals with spinal cord injury (SCI) above T6 experience impaired descending cortical control of the autonomic nervous system which predisposes them to hypotension. However, treatment of hypotension is uncommon in the SCI population because there are few safe and effective pharmacological options available. The primary aim of this investigation was to test Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms Corresponding Author: Jill M. Wecht: James J. Peters VA Medical Center, 130 W Kingsbridge Road, Bronx, NY. Jill.Wecht@va.gov; Phone: 718-584-9000 ext. 3122. Authors Contribution: JMW: oversaw and was primarily responsible for designing the study, participant enrollment, data collection procedures, database management, data analysis, result dissemination and regulation compliance; JPW: was primarily responsible for designing the study, data analysis, and result dissemination; CGK: was primarily responsible for participant enrollment, data collection procedures, database management, and regulation compliance; NDC: oversaw study design pertaining to the cognitive outcomes and was primarily responsible for the cognitive data analyses; SCK: was responsible for monitoring patient safety at the Kessler Foundation; TAD: was responsible for participant enrollment and monitoring patient safety at the Kessler Foundation; EW: was responsible for analysis of the cognitive outcomes; WAB: monitored patient safety at the VA and oversaw data analysis and result dissemination. Data Archiving: The datasets generated and analyzed in the current study are available from the corresponding authors upon request. Statement of Ethics: The authors certify that all applicable institutional and governmental regulations concerning the ethical use of human volunteers were followed during the course of this research. Conflict of Interest Statement: The authors report no financial conflict of interest in association with conducting the current clinical trial. Clinical Trials Registration # NCT02307565 VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 2 the efficacy of a single dose of midodrine (10 mg), compared to placebo, to increase and normalize systolic blood pressure (SBP) between 110–120 mmHg during cognitive testing in hypotensive individuals with SCI. Secondary aims were to determine the effects of midodrine on cerebral blood flow velocity (CBFv) and global cognitive function. Setting: United States clinical research laboratory. Methods: Forty-one healthy hypotensive individuals with chronic (≥ 1-year post-injury) SCI participated in this 2-day study. Seated SBP, CBFv, cognitive performance were monitored before and after administration of identical encapsulated tablets, containing either midodrine or placebo. Results: Compared to placebo, midodrine increased SBP (4±13 vs. 18±24 mmHg, respectively; p<0.05); however, responses varied widely with midodrine (−15.7 to +68.6 mmHg). Further, the proportion of SBP recordings within the normotensive range did not improve during cognitive testing with midodrine compared to placebo. Although higher SBP was associated with higher CBFv (p=0.02), global cognitive function was not improved with midodrine. Conclusions: The findings indicate that midodrine increases SBP and may be beneficial in some hypotensive patients with SCI; however, large heterogeneity of responses to midodrine suggest careful monitoring of patients following administration. Keywords Tetraplegia; Paraplegia; Spinal Cord Injuries; Hypotension; Orthostatic Hypotension; Cognition; Rehabilitation INTRODUCTION Focus on blood pressure in the medical literature is heavily skewed towards hypertension as opposed to hypotension. A recent PubMed search for hypertension yielded 490,320 literature references compared to 65,491 for hypotension over the course of the past century. Moreover, blood pressure threshold(s) used to define hypotension vary extensively, and whereas the diagnosis of hypertension is based solely on blood pressure, the diagnosis of hypotension is usually based on the presence of significant symptomology reflecting cerebral hypoperfusion, which includes dizziness, light-headedness, pre-syncope and syncope, as well as non-specific symptoms of generalized weakness, fatigue, nausea, cognitive slowing, blurry vision, leg buckling or headache (1). However, it should be appreciated that individuals with low blood pressure often remain asymptomatic and are, therefore, not diagnosed or treated. Further, longstanding sentiment argues that low blood pressure is a clinical syndrome unassociated with pathological consequences, and there persists an implicit belief that hypotension may convey significant cardiovascular benefit (2). Yet 13-year all-cause and cardiovascular disease mortality risk was 2.4 to 3.4 times higher, respectively, in males 40 to 49 years with systolic hypotension compared to age-matched males with normal blood pressure (3), and in a recent meta-analysis all-cause mortality was 36% higher in association with orthostatic hypotension (4). Moreover, there is a growing body of evidence that links persistent asymptomatic hypotension and orthostatic hypotension with adverse changes in health-related quality of life, as well as an increased incidence of Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 3 anxiety and depression (2), cognitive deficits (5), hopelessness (5) and dementia (6, 7). Therefore, treatment to increase and normalize low blood pressure, even in asymptomatic patients with SCI, should be considered. Loss of integral descending cortical control of autonomic cardiovascular regulation following spinal cord injury (SCI) results in a variety of measurable abnormalities in blood pressure, most prominently chronic hypotension, orthostatic hypotension and autonomic dysreflexia. As in the general population, chronic hypotension and orthostatic hypotension in the SCI population are associated with cognitive deficits (8), adverse changes in health- related quality of life (9), increased arterial stiffness (10) and a 3–4 fold increased stroke risk (11). Although evidence suggests improved cognitive performance following increases in blood pressure with midodrine (12), because most hypotensive individuals with SCI are asymptomatic there is a wide disparity between the incidence of hypotension and orthostatic hypotension and the diagnoses of these conditions and very few patients are treated for disorders of low blood pressure (13, 14). Additionally, there is a paucity of treatment options for hypotension and orthostatic hypotension that are clinically available and have been proven safe and effective for widespread use in the SCI population. Non-pharmacological remedies for treatment of hypotension and orthostatic hypotension that are often prescribed in hypotensive individuals with SCI include: exercise (15), functional electrical stimulation (16), compression garments (17) and salt and water intake (18); however, there is little supporting evidence for any of these interventions and the data that are available are of poor quality (19). Pharmacological treatment options for hypotension and orthostatic hypotension include: midodrine hydrochloride (20), L-threo-3,4-dihydroxyphenylserine (droxidopa) (21), fludrocortisone and ergotamine (22), and ephedrine (23). In a randomized, placebo- controlled, double-blinded clinical trial in four individuals with SCI, midodrine (10 mg) increased average seated systolic blood pressure to within a normotensive range (i.e., 110 and 120 mmHg), in 1 of the 4 subjects tested; one subject became hypertensive (average systolic blood pressure of 143 mmHg) and 2 remained hypotensive (average systolic blood pressure < 110 mmHg) (20). Despite this limited evidence, midodrine is the most commonly prescribed anti-hypotensive agent used in the SCI population (https://scireproject.com/ evidence/rehabilitation-evidence/orthostatic-hypotension/). Clearly, more data are needed to support the clinical management of hypotension and orthostatic hypotension in the SCI population. The primary aim of this investigation was to test the efficacy of midodrine (10 mg), compared to placebo, to increase seated systolic blood pressure at rest and during a battery of neuropsychological tests in hypotensive individuals with SCI in a randomized, double- blinded, cross-over trial. Our primary hypothesis was that seated systolic blood pressure would be significantly increased from baseline following midodrine administration as compared to placebo. Secondarily, we hypothesized that the proportion and stability of systolic blood pressure recordings within the normotensive range would be significantly increased during cognitive testing following administration of midodrine compared to placebo. Additional study aims were to determine if midodrine administration would be Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 4 associated with increases in cerebral blood flow velocity and improved cognitive function compared to placebo. We hypothesized that cerebral blood flow velocity would be significantly increased and that composite scores on a battery of cognitive tasks would be improved following midodrine administration. METHODS Participants: This trial was conducted at two research facilities under identical study protocols, which were approved by the IRB committees at both facilities. Participants were deemed eligible for an in-person screening visit based on the following criteria: 1) between the ages of 18 and 65 years, 2), non-ventilator dependent, 3) duration of injury more than 12 months, 4) native English speaker and 5) better than 20/60 vision in worst eye with prescription eyewear. Exclusion criteria included: 1) three or more self-reported symptomatic episodes of autonomic dysreflexia per week, 2) current illness or infection, and 3) documented history of hypertension, diabetes, traumatic brain injury, or any neurological condition other than SCI. Eligible participants underwent a screening visit to confirm that they met the World Health Organization definition of hypotension, (i.e., systolic blood pressure ≤ 110 mmHg for males and ≤ 100 mmHg for females) (24). At the screening visit blood pressure was measured at 1- minute intervals for 5-minutes in the seated and supine positions using manual auscultation at the brachial artery. Eligibility for inclusion in the study was based on either: 1) a supine systolic blood pressure ≤ 90 mmHg; 2) seated systolic blood pressure ≤ 110 mmHg for males or ≤ 100 mmHg for females, or 3) a fall in blood pressure ≥ 20/10 mmHg within 5 minutes of assuming a seated upright position. Eligible participants were then scheduled for two testing visits and were issued a participant ID that was associated with the randomized order as either: midodrine/placebo or placebo/midodrine. The study participants, the research staff, and the investigators were blinded as to the order of administration and the randomization scheme was generated by the research pharmacist at the James J Peters VAMC who was responsible for dispensing the study medication. To limit the chance of autonomic dysreflexia during or after testing we scheduled participant visits the day after their bowel-care routine and asked that they void their bladder immediately before testing began on each visit. Procedures: Participants arrived at the testing site between 9am and 2pm and remained in their wheelchair in the seated position for all study procedures, which were identical on both study visits. The 2-study visits were scheduled no less than 2 and no more than 10 days apart and participants were asked to arrive at the laboratory at approximately the same time of day on both visits. Experiments were conducted in a quiet and temperature-controlled room and participants were instructed to avoid consuming caffeine, alcohol and nicotine products for 12 hours prior to testing. Vigorous unaccustomed exercise was also avoided for 24-hours prior to testing. Participants were asked to empty their bladder upon arrival to the testing laboratory, to limit the influence of reflex sympathetic activation on peripheral vascular tone from bladder distension, and medications were stopped for approximately 5 half-lives (at the Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 5 subject’s primary care physicians’ discretion) whenever possible. While resting quietly in the seated position, participants were instrumented with 3 electrocardiogram electrodes, finger and brachial blood pressure monitors and a head harness to secure probe placement for transcranial Doppler ultrasound recording of cerebral blood flow velocity. After instrumentation, a 5-minute continuous baseline assessment of heart rate, blood pressure and cerebral blood flow velocity was recorded while the participant rested quietly prior to administration of the initial neuropsychological battery of tests. After completion of the neuropsychological battery, midodrine or placebo was administered to the study participants in identical encapsulated tablets with a glass of water. Following administration of study medication participants rested quietly in their wheelchairs for 45-minutes. After which, and prior to beginning the second cognitive test battery, a 5-minute continuous assessment of heart rate, blood pressure and cerebral blood flow velocity was recorded. The second neuropsychological battery was then conducted and heart rate, blood pressure and cerebral blood flow velocity were monitored and recorded. The cognitive battery and hemodynamic monitoring occurred between 45 and ~90 minutes after dosing, which corresponds to peak blood pressure effects during a head-up tilt maneuver following administration of midodrine 10 mg. (25) Heart Rate and Blood Pressure: The electrocardiogram recording was performed using a bio-amplifier (Model RESP 1 with ECG: UFI, Morro Bay, CA, USA), with electrodes placed at the right and left mid-axillary lines in the 5th intercostal space and at the right anterior axillary line. Continuous beat-to- beat blood pressure (mmHg) was assessed at the finger using photoplethysmography (Finometer PRO, Finapres Medical Systems B. V., Netherlands) and at 1-minutes intervals at the brachial artery with manual auscultation (Series Wall Mobile Sphygmomanometers, Trimline Medical Products, Raritan, NJ, USA). The beat-to-beat electrocardiogram and photoplethysmography blood pressure signals were sampled at 500 Hz and were continuously monitored in real time on a computer screen. The digitized signals were stored on a computer hard-drive for subsequent analysis using custom data analysis programs written with LabVIEW graphical software for instrumentation (National Instruments, 11500 North Mopac Expressway Austin, TX 78759–3504). Brachial artery blood pressure recordings were used to calibrate the finger blood pressure assessments, to determine the proportion of blood pressure recording within the normotensive range and to calculate the area under the curve (AUC) of the blood pressure recordings during each of the cognitive batteries before and after administration of study drug. The normotensive range was defined as a systolic blood pressure between 110–120 mmHg and a diastolic blood pressure between 70–80 mmHg. Cerebral blood flow velocity: Transcranial Doppler ultrasound technology (Terumo Cardiovascular Systems 1311 Valencia Avenue Tustin, CA 92780–6447) was used to measure cerebral blood flow velocity. The probe was operated at a frequency of 2.0 MHz to visualize the middle cerebral artery and insonation was through the left temporal window. The middle cerebral artery was identified by the target depth (45–55 mm), sound and direction of flow (i.e., towards the probe), the characteristic spectral waveform and relatively faster flow velocity compared to surrounding Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 6 cerebral vessels. Once the middle cerebral artery was visualized, probe placement was secured for the duration of testing using a head-harness. Data output from the transcranial Doppler ultrasound was monitored in real-time and included systolic flow velocity, diastolic flow velocity and mean flow velocities, which were recorded in centimeters per second (cm/s). The beat-to-beat signals were sampled at 500 Hz and were stored on a computer hard-drive for subsequent analysis using custom data analysis programs written with LabVIEW graphical software for instrumentation. Neuropsychological Testing: Participants underwent an abbreviated, non-motor dependent, cognitive battery, to assess global cognitive function. This battery included tests of verbal fluency (Controlled Oral Word Fluency Test), verbal learning and memory (Hopkins Verbal Learning Test-Revised), cognitive inhibition (Stroop), auditory working memory (WAIS-IV Letter-Number Sequencing), cognitive flexibility (Oral Trail Making Test) and processing speed (Symbol Digit Modalities Test). The battery took about ~45 minutes to complete and was performed by the participants before and after administration of study medication on each study visit. A different version of each neuropsychological test was used at each time point to minimize a possible learning effect. Cognitive impairment was defined by a Global Deficit Score (GDS) of at least 0.5, which converts demographically-corrected T-scores to a deficit score, representing the distance each test score is below the normative mean (26). Overall GDS is the average of all converted test scores and a GDS score of 0.5 or higher translates to performance of at least 1 SD below the normative mean on at least half of the cognitive measures. This methodology has demonstrated discriminative validity in detecting individuals with neurological disorders and cognitive impairment, (27) as well as external validity with disease state and everyday functioning outcomes (28). GDS was calculated under each of the 4 test conditions: pre- and post-placebo; pre- and post-midodrine. Statistical Analyses: Repeated measures ANOVA models were constructed to determine significant main and interaction effects for drug (midodrine, placebo) and time (pre- and post-administration) for the systemic and cerebral hemodynamics and for cognitive GDS. Because in these 2×2 models, the interaction effect is equivalent to a paired t-test on the change scores (29), we also calculated effect sizes (Cohen’s dz) (30), 95% confidence intervals, Bayes factors and Bayesian credible intervals from the t-test calculations (31). For the change scores, mean differences were calculated as midodrine minus placebo. Multilevel modeling using the lme4 package in R was used to determine the relationship between changes in systolic blood pressure and changes in mean flow velocity from pre- to post-testing following administration of midodrine compared to placebo. To assess systolic blood pressure stability, we used the serial brachial recordings and set the normotensive systolic range between 110 and 120 mmHg, inclusive. To quantify stability, for the time series of systolic blood pressure values under each time and drug combination, we first calculated the percentage of beats that fell within the desirable range and then expanded the range serially by +/− 10 mmHg, such that the subsequent systolic range was 100 to 130 mmHg, and repeated the percentage calculation until we were inclusive of all Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 7 systolic blood pressure observations (i.e., 40–190 mmHg). The resulting percentage within each range was then plotted against the systolic blood pressure range at each iteration and the area under the curve (AUC) was calculated for each plot. The same method was applied to the serial diastolic blood pressure data, with the desirable range set at 70–80 mmHg. The blood pressure processing and AUC calculations were performed with a custom LabVIEW program. The larger the AUC, the closer the systolic and diastolic blood pressure values were to the respective desirable range, and the more stable were the signals across the recording period. To assess the efficacy of midodrine to normalize blood pressure, the proportion of values that fell within the systolic and diastolic desirable ranges described above was also quantified. As with the hemodynamic data from above, the AUC and proportion in the desirable range data were analyzed with a drug X time repeated measures ANOVA and change score analysis with paired t-tests was used to calculate effect sizes, confidence intervals, Bayes factors and Bayesian credible intervals. All continuous data are presented as mean ± standard deviation and significance was set at an alpha of < 0.05. Statistical calculations were performed using SPSS and JASP (for the Bayesian calculations) and R for the multilevel modeling. RESULTS Characteristics of the Participants: A total of 43 individuals with SCI were consented to participate; however, two withdrew prior to initiation of the study procedures, therefore data are reported in 41 participants (Table 1). The participants were mostly male, with cervical (90%), motor-complete lesions (81%). Self-reported levels of physical activity suggested that most (85%) engaged in at least 1 day of exercise/week at a moderate intensity and that they were otherwise healthy. Twenty participants were randomly assigned to receive midodrine on the first study visit and placebo on the second visit and 21 received placebo first; there were no significant differences for hemodynamics by randomization order. Resting Hemodynamic Responses: Average systemic and cerebral hemodynamic data are presented for 5-minutes in the seated resting position prior to (Table 2a) and following (Table 2b) administration of study medication. Resting hemodynamics did not differ significantly prior to administration of study medication. The drug by time interaction effect was significant for heart rate (all p≤ 0.023) [Figure 1a] (95% CI of mean difference (midodrine minus placebo) = −10.1 to −3.8 bpm), systolic blood pressure [Figure 1b] (95% CI of mean difference = 9.0 to 24.1 mmHg), diastolic blood pressure [Figure 1c] (2.5 to 10.4), mean flow velocity [Figure 1e] (0.3 to 4.4 cm/s) and diastolic flow velocity [Figure 1f] (0.4 to 5.4 cm/s), but was not significant for systolic flow velocity [Figure 1d] (95% CI for mean difference = −3.3 to 6.8 cm/c). Results of the repeated measures ANOVA models are presented (Table 3), which indicate large Bayes Factors (BF ) for heart rate (BF = 390.7), systolic blood pressure (BF = 319.1) 10 10 10 10 and diastolic blood pressure (BF = 15.0) indicating strong evidence that these hemodynamic responses to midodrine differed from placebo. Whereas the BF for mean Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 8 flow velocity (BF =2.01) and diastolic flow velocity (BF = 1.84) were more modest and 10 10 would be considered “anecdotal” evidence of a treatment effect (31). The association between change in systolic blood pressure and change in mean cerebral blood flow velocity is depicted following placebo (Figure 2a) and midodrine (Figure 2b). Results of the multilevel modeling examining the relationship between systolic blood pressure and mean cerebral blood flow velocity indicate a significant main effect for systolic blood pressure (p=0.02); however, main effects for time (p=0.52) and drug (p=0.34) and the associated interaction effects were not significant (all p > 0.31). This suggests, that regardless of time or drug, higher systolic blood pressure is associated with higher mean blood flow velocity in hypotensive individuals with SCI. Nine of the 41 participants (22%) had an average resting systolic blood pressure within the normotensive range following midodrine administration; however, systolic blood pressure exceeded the normotensive range in 17 (41%) and remained below the desirable range in 15 (37%) participants (Figure 3a). Further, the change in systolic blood pressure (mmHg) following midodrine administration suggested wide variability (delta of −15.7 to +68.6 mmHg) in individual responses to the medication compared to placebo (delta of −15.8 to +38.7 mmHg) (Figure 3b). Normalization and Stability of Blood Pressure: An average of 25±4 brachial systolic blood pressures were collected in participants during each cognitive test battery. The interaction effects for the proportion of systolic or diastolic blood pressures within the desirable ranges were not significant (Table 3), indicating that treatment with midodrine did not “normalize” blood pressure compared to placebo. The AUC of blood pressure “stability” before and after administration of placebo and midodrine is also summarized (Table 3). The interaction effect for AUC was not significant for systolic or diastolic blood pressure, which indicates that the midodrine treatment did not improve blood pressure stability compared to placebo. Corresponding AUC curves for systolic blood pressure are presented for three participants pre- and post-midodrine administration (Figure 4); one participant who remained hypotensive (left panel), one participant who was normotensive (middle panel) and one participant who became hypertensive (right panel) after midodrine administration. Increased AUC (i.e., improved blood pressure stability within or near the desired range), was noted in the participant who had a normotensive response to midodrine (middle panel). Of note, midodrine was effective at stabilizing blood pressure within or near the normotensive range in 6 of the 41 study participants. GDS analyses: Sixty-three percent of the study participants exhibited an average GDS ≥ 0.5 before administration of placebo or midodrine, indicating impaired function in more than half of the cognitive domains tested. There were no significant main or interaction effects for cognitive GDS (interaction p = 0.91, BF = 0.17), suggesting that compared to placebo, midodrine administration did not improve global cognitive function in these 41 hypotensive participants with SCI. However, it might be noted that of the 9 participants with a normal Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 9 systolic blood pressure following midodrine, 3 showed evidence of improved global cognitive function after administration. DISCUSSION Hypotension and orthostatic hypotension are not high on the clinical priority list in patients with SCI, which is due in part to the lack of safe and effective treatment options available for use in the population (19). Yet low resting blood pressure and orthostatic hypotension may be clinically relevant signs to indicate impaired autonomic nervous system control of cardiovascular function and are associated with significant adverse health outcomes. Therefore, treatment of hypotension and orthostatic hypotension should be considered important aspects in the clinical management of individuals with SCI. It was our goal to determine the effectiveness of midodrine, compared to placebo, to increase and maintain systolic blood pressure within a tight normotensive range of 110–120 mmHg in hypotensive participants with SCI. Our findings suggest that, although midodrine did increase blood pressure, large heterogeneity of response was evident such that only a small percentage (22%) of the study participants had systolic blood pressures within the normal range following administration. Furthermore, the proportion and the stability of systolic blood pressures recordings within the normotensive range were not improved with midodrine compared to placebo. There is substantial evidence that demonstrates improved standing blood pressures and reduced symptoms associated with cerebral hypoperfusion following midodrine administration in models of symptomatic neurogenic orthostatic hypotension (32); however, there is limited evidence to support wide spread utility in the SCI population. While it is not our intent to discourage the use of midodrine to treat hypotension and orthostatic hypotension in the SCI population, we sought to 1) increase awareness of the heterogeneity of response, 2) encourage more frequent monitoring of blood pressure following prescription and 3) adjust dose as needed. With that in mind, several points should be considered when interpreting these results in the context of clinical algorithms used to manage hypotension and orthostatic hypotension in the SCI population: 1) lack of a clear consensus regarding the definition of hypotension and normotension, 2) changing guidelines for the management of hypertension, 3) highly prevalent blood pressure instability, and 4) the impact of anti- hypotensive treatment on blood pressure surges during autonomic dysreflexia. There is a lack of clarity regarding the definition of hypotension that contributes to low diagnosis and treatment rates. A recent systematic literature search, that included 63 publications involving over 7000 participants, found 15 different definitions for hypotension (33), and different definitions yielded significantly altered incidence rates (34). Large epidemiological studies tend to define hypotension as the lowest 5–30% of the population (2, 35) while smaller prospective studies use upper limit cut-offs of between 100 and 120 mmHg systole (36). The definition of hypotension in the SCI population as published in the International Standards to Document Remaining Autonomic Function after Spinal Cord Injury is a supine systolic blood pressure < 90 mmHg. (37) However, the World Health Organization defined hypotension as a resting systolic blood pressure of < 110 mmHg for Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 10 males and < 100 mmHg for females without regard to diastolic blood pressure (24), which has been used by our group to define hypotension in persons with chronic SCI (8). The diagnosis of hypotension is usually based on the presence of significant symptomology. Despite views that, in the absence of clinical symptomology, hypotension represents a “non- disease” state, (38) recent evidence suggests that lower baseline systolic blood pressure predicts incident depression at a 2-year follow-up after adjustment for socioeconomic status and relevant clinical factors (cardiovascular disease, chronic illness, frailty) (39). In addition, individuals between the age of 30 and 75 years with asymptomatic hypotension are at increased risk for cognitive and affective disorders, including decreased memory and concentration (40), higher rates of hopelessness, (40) and an increased prevalence of dementia, which includes both Alzheimer’s disease and vascular dementia (7). Therefore, treatment of asymptomatic hypotension in the SCI population should be considered a clinical priority. To our knowledge there are no long-term studies documenting the potential association between hypotension and incident depression or cognitive changes with aging in the SCI population. However, we previously documented higher rates of depressive symptom reporting and deficits in memory and information processing in hypotensive individuals with SCI compared to a normotensive SCI cohort (8). Moreover, although most hypotensive individuals with SCI do not spontaneously report symptoms, when asked directly, they are able to ascribe adverse impacts of hypotension and orthostatic hypotension on their activities of daily living and quality of life (9). Although the results herein do not demonstrate a lessening of cognitive dysfunction following increases in blood pressure with midodrine, the data do suggest that higher blood pressures are associated with higher cerebral blood flow velocities and one-third of participants with normal systolic blood pressure responses to midodrine displayed improved cognitive function. These results suggest that, if higher - more normal - blood pressure is maintained with prolonged anti-hypotensive treatment, improvement in long-term cognitive performance may be evident. There are nearly 200 prescription medications with FDA approval for label and off-label use to treat hypertension, and many patients require combinatorial therapy to maintain optimal blood pressure control. A similar approach to the treatment of hypotension and orthostatic hypotension may be beneficial; however, until a variety of safe and effective agents with different mechanisms of actions are identified, clinical treatment will be inadequate, and individuals will remain un- or under-treated. Further, while prioritizing the treatment of asymptomatic hypertension in clinical practice is well appreciated, lack of acknowledgement that there may be a blood pressure value that is recognized to be too low is noteworthy. Current guidelines used in treatment algorithms for hypertension indicate a normal systolic blood pressure of < 120 mmHg, with systolic pressures between 120–129 mmHg being elevated (41), therefore we chose a desirable range for systolic blood pressure of between 110 and 120 mmHg in this trial. Notwithstanding the lack of clear consensus regarding what constitutes normal blood pressure and the relatively tight normotensive range selected, it is not surprising that we document limited efficacy of midodrine to ‘normalize’ blood pressure following a single 10 mg dose. However, what was surprising is the wide variability in response to midodrine, compared to placebo, in our participants with SCI. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 11 We appreciate that blood pressure instability, which is commonly reported in persons with SCI (42), complicates the clinical management of hypotension and orthostatic hypotension. We recently noted that fluctuations in systolic blood pressure of ≥ 20 mmHg, over a 30-day period were increased with age and duration of injury (43), which may be associated with loss of baroreceptor buffering of blood pressure, similar to the general population (44); therefore, management of hypotension in the SCI population should aim to stabilize, as well as to normalize, blood pressure. The AUC analyses suggest that the stability of the blood pressure, relative to the normotensive range, was not improved with midodrine. In fact, the AUC was lower following midodrine administration compared to following placebo in half of the participants. This finding indicates increased blood pressure instability following midodrine administration, which speaks to the large heterogeneity of responses. However, it should be noted that a few participants did respond to midodrine with a normal and stable systolic blood pressure, as depicted in Figure 3c & 3d. Average brachial systolic blood pressure was within the normotensive range in 9 of the 41 participants tested and these participants tended to be younger and injured fewer years than those with inadequate and excessive responses to midodrine. Given the heterogeneity of response to midodrine and significant blood pressure instability in persons with SCI, increasing the armamentarium of safe and effective clinical strategies is vitally important, particularly in individuals who are prone to autonomic dysreflexia. We did not induce autonomic dysreflexia in this trial and none of the participants reported feeling symptomatic prior to or after administration of study drug. A previous study found that increases in blood pressure during penile vibrator stimulation for sperm retrieval (i.e., a procedure known to induce autonomic dysreflexia), were not worsened with the addition of midodrine (45). However, this response to midodrine was reported during a closely observed clinical procedure; home use of midodrine during life events that may induce autonomic dysreflexia should be studied. Importantly, the practice of ‘boosting’ during athletic competition, should serve as an indicator of the importance of increasing blood pressure – safely – to avoid this dangerous and uncontrolled practice in athletes with SCI. Limitations: There are several study limitations to consider when interpreting the findings reported. Based on prior evidence, we only tested the efficacy of a single 10 mg dose of midodrine, compared to placebo, over a relatively brief observation period; however, higher doses for those who remained hypotensive and lower doses for those in whom blood pressure was elevated above the normotensive range should be tested for efficacy. Additionally, while the 10 mg dose did not improve blood pressure stability, a lower dose (2.5 or 5 mg) administered more frequently throughout the day may be more effective and may provide more clinically relevant information. We did not assess supine blood pressure responses to midodrine and did not investigate the effects on blood pressure during autonomic dysreflexia. We did not record symptom reporting in association with the increase in blood pressure, which in many participants met the definition of autonomic dysreflexia (i.e., systolic increase > 20 mmHg). The range selected to define normotension was narrow and Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 12 arbitrary, because there are currently no guidelines, other than those which define elevated blood pressure and hypertension. Finally, the study sample included a largely homogeneous cohort of participants and extrapolation to the broader SCI population may be inappropriate. Conclusion: Compared to placebo, midodrine, on average, significantly increased systolic blood pressure; however, large heterogeneity of responses among these hypotensive participants with SCI were evident. Furthermore, and perhaps more concerning, was that midodrine appeared to increase blood pressure instability in about half of the participants tested. That said, prescription of midodrine may benefit individual patients, particularly those who are younger and injured for fewer years; this finding requires further study to definitively identify responders from non-responders. Additionally, higher systolic blood pressures were associated with higher cerebral blood flow velocities, which may have beneficial effects on long-term cognitive function. Given the growing body of evidence indicating significant adverse sequela of untreated asymptomatic hypotension and orthostatic hypotension, identifying an armamentarium of safe and effective treatment options for use in the SCI population is needed. Acknowledgement: We would like to thank all the study participants for their involvement in this study and want to acknowledge Beatrice Ugiliweneza, Samineh Mesbah and Susan Harkema for their programming and statistical skills in creating the area-under-the-curve analyses. Sources of Funding: This project was funded by the Craig H Neilsen Foundation (Grant #284196) and the Department of Veterans Affairs, Veterans Health Administration, Rehabilitation Research & Development Service Center for the Medical Consequences of Spinal Cord Injury (Grant #D1382-P, #B2020-C). The authors report no conflict of interest. References: 1. Miller ER 3rd, Appel LJ. High prevalence but uncertain clinical significance of orthostatic hypotension without symptoms. Circulation. 2014;130(20):1772–4. [PubMed: 25278100] 2. Hildrum B, Mykletun A, Stordal E, Bjelland I, Dahl AA, Holmen J. Association of low blood pressure with anxiety and depression: the Nord-Trondelag Health Study. J Epidemiol Community Health. 2007;61(1):53–8. [PubMed: 17183016] 3. LINDHOLM L, LANKE J, BENGTSSON B, EJLERTSSON G, THULIN T, SCHERSTÉN B. Both High and Low Blood Pressures Risk Indicators of Death in Middle‐aged Males: Isotonic Regression of Blood Pressure on Age Applied to Data from a 13‐Year Prospective Study. Acta medica Scandinavica. 1985;218(5):473–80. [PubMed: 4091047] 4. Angelousi A, Girerd N, Benetos A, Frimat L, Gautier S, Weryha G, et al. Association between orthostatic hypotension and cardiovascular risk, cerebrovascular risk, cognitive decline and falls as well as overall mortality: a systematic review and meta-analysis. 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Psychological Bulletin. 1975;82(4):511–8. 30. Calculating Lakens D. and reporting effect sizes to facilitate cumulative science: a practical primer for t-tests and ANOVAs. Front Psychol. 2013;4:863. [PubMed: 24324449] 31. Wagenmakers EJ, Love J, Marsman M, Jamil T, Ly A, Verhagen J, et al. Bayesian inference for psychology. Part II: Example applications with JASP. Psychon Bull Rev. 2018;25(1):58–76. [PubMed: 28685272] 32. Low PA, Gilden JL, Freeman R, Sheng KN, McElligott MA. Efficacy of midodrine vs placebo in neurogenic orthostatic hypotension. A randomized, double-blind multicenter study. Midodrine Study Group. JAMA 1997;277(13):1046–51. 33. Klohr S, Roth R, Hofmann T, Rossaint R, Heesen M. Definitions of hypotension after spinal anaesthesia for caesarean section: literature search and application to parturients. Acta Anaesthesiol Scand. 2010;54(8):909–21. [PubMed: 20455872] 34. Dahlgren G, Irestedt L. The definition of hypotension affects its incidence. Acta Anaesthesiol Scand. 2010;54(8):907–8. [PubMed: 20701595] 35. Kim BS, Bae JN, Cho MJ. Depressive symptoms in elderly adults with hypotension: different associations with positive and negative affect. J Affect Disord. 127(1–3):359–64. [PubMed: 20619901] 36. Pilgrim JA, Stansfeld S, Marmot M. Low blood pressure, low mood? Bmj. 1992;304(6819):75–8. [PubMed: 1737142] 37. Krassioukov A, Biering-Sorensen F, Donovan W, Kennelly M, Kirshblum S, Krogh K, et al. International standards to document remaining autonomic function after spinal cord injury. J Spinal Cord Med. 2012;35(4):201–10. [PubMed: 22925746] 38. Robbins JM, Korda H, Shapiro MF. Treatment for a nondisease: the case of low blood pressure. Soc Sci Med. 1982;16(1):27–33. [PubMed: 7100954] 39. Briggs R, Kenny RA, Kennelly SP. Does baseline hypotension predict incident depression in a cohort of community-dwelling older people? Data from The Irish Longitudinal Study on Ageing (TILDA). Age Ageing. 2017;46(4):648–53. [PubMed: 28338875] 40. Czajkowska J, Ozhog S, Smith E, Perlmuter LC. Cognition and hopelessness in association with subsyndromal orthostatic hypotension. J Gerontol A Biol Sci Med Sci. 65(8):873–9. [PubMed: 20478907] 41. Whelton PK, Carey RM, Aronow WS, Casey DE Jr., Collins KJ, Dennison Himmelfarb C, et al. 2017 ACC/AHA/AAPA/ABC/ACPM/AGS/APhA/ASH/ASPC/NMA/PCNA Guideline for the Prevention, Detection, Evaluation, and Management of High Blood Pressure in Adults: A Report of the American College of Cardiology/American Heart Association Task Force on Clinical Practice Guidelines. J Am Coll Cardiol. 2018;71(19):e127–e248. [PubMed: 29146535] 42. Hubli M, Gee CM, Krassioukov AV. Refined assessment of blood pressure instability after spinal cord injury. Am J Hypertens. 2015;28(2):173–81. [PubMed: 24990527] 43. Katzelnick CG, Weir JP, Jones A, Galea M, Dyson-Hudson TA, Kirshblum SC, et al. Blood Pressure Instability in Persons with SCI: Evidence from a 30-Day Home Monitoring Observation. Am J Hypertens. 2019. 44. Jones PP, Christou DD, Jordan J, Seals DR. Baroreflex buffering is reduced with age in healthy men. Circulation. 2003;107(13):1770–4. [PubMed: 12665501] Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 15 45. Courtois FJ, Charvier KF, Leriche A, Vezina JG, Cote M, Belanger M. Blood pressure changes during sexual stimulation, ejaculation and midodrine treatment in men with spinal cord injury. BJU Int. 2008;101(3):331–7. [PubMed: 17922856] Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 16 Figure 1: Results of the repeated measures ANOVA models for heart rate [a], systolic blood pressure [b], diastolic blood pressure [c], systolic flow velocity [d], mean flow velocity [e] and diastolic flow velocity [f] pre to post placebo (closed circles) and midodrine (open squares). *** p<0.001; ** p<0.01; * p<0.05 for the drug by time interaction effect. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 17 Figure 2: The relationship between change in systolic blood pressure (SBP) and mean cerebral blood flow velocity (FV) following administration of placebo [a] and midodrine [b]. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 18 Figure 3: Average [a] and the change [b] in 5-minute seated resting systolic blood pressure (mmHg) following administration of placebo and midodrine for each participant. The dashed lines represent the upper and lower limits of the normotensive range [a] and the no change [b]. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 19 Figure 4: Systolic blood pressures Pre (closed circles) and Post (open squares) midodrine administration in 3 individual participants (top) and the AUC curves which were generated from these data (bottom). Left panel: the participant is hypotensive Pre and Post midodrine [a] and the AUC indicates a modest improvement in normalizing systolic blood pressure Post midodrine [b]. Middle panel: the participant is hypotensive Pre midodrine and normotensive Post midodrine [c] and the AUC reflects an increased proportion of normal blood pressure Post midodrine [d]. Right panel: the participant is hypotensive Pre midodrine and hypertensive Post midodrine [e] and the AUC reflects a reduced proportion of normal blood pressure Post midodrine [f]. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 20 Table 1. Subject Characteristics Participants (n=41) Age (years) 44 ± 12 Males n (%) 33 (80) Caucasian n (%) 23 (56) African American n (%) 8 (20) Hispanic n (%) 8 (20) Other n (%) 2 (5) American Veteran n (%) 6 (15) BMI (kg/m ) 24 ± 4 Duration of Injury (years) 16 ± 12 Level of Injury C4–T9 AIS A n (%) 18 (44) AIS B n (%) 15 (37) AIS C n (%) 6 (15) AIS D n (%) 2 (5) Data are means ± SD; BMI: body mass index; m: meters; kg: kilograms Other ethnicity = 1 Asian and 1 East Indian Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 21 Table 2a. Average Pre-treatment Hemodynamics Placebo Midodrine Heart Rate (bpm) 68.0±10.2 67.6±10.9 Systolic BP (mmHg) 98.1±14.0 98.6±16.3 Diastolic BP (mmHg) 57.8±9.5 59.6±10.6 Systolic FV (cm/s) 69.4±19.2 70.0±15.9 Mean FV (cm/s) 43.3±13.3 43.5±10.7 Diastolic FV (cm/s) 30.4±8.3 29.7±7.8 Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 22 Table 2b. Average Post-treatment Hemodynamics Placebo Midodrine Heart Rate (bpm) 65.0±10.5 60.0±12.0 Systolic BP (mmHg) 106.3±18.0 115.0±27.1 Diastolic BP (mmHg) 61.4±13.3 66.0±16.5 Systolic FV (cm/s) 70.5±15.6 71.0±16.8 Mean FV (cm/s) 44.6±11.7 46.0±10.5 Diastolic FV (cm/s) 31.3±11.1 32.9±13.2 Hemodynamic data collected during the 5-minutes of seared rest before and after treatment with placebo and midodrine. Dare means ± SD; bpm=beats per minute; BP=blood pressure; FV=flow velocity; cm=centimeters; s=seconds Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 23 Table 3. Hemodynamic Changes and Blood Pressure Instability: Midodrine vs. Placebo Mean 95% CI of mean Bayes Effect Effect Size 95% Variable p value Difference Difference Factor Size Credible Interval Heart Rate (bpm) <0.001 −7.0 −10.1 to −3.8 390.70 −0.93 −1.39 to −0.47 Systolic BP (mmHg) <0.001 16.5 9.0 to 24.1 319.10 0.90 0.44 to 1.37 Diastolic BP (mmHg) <0.001 6.4 2.5 to 10.4 15.00 0.66 0.21 to 1.12 Systolic FV (cm/s) 0.48 1.8 −3.3 to 6.8 0.21 0.13 −0.28 to 0.55 Mean FV (cm/s) 0.023 2.3 0.3 to 4.4 1.84 0.47 0.05 to 0.91 Diastolic FV (cm/s) 0.026 2.9 0.43 to 5.4 2.01 0.46 0.05 to 0.90 Systolic Proportion in 0.86 −0.01 0.14 to 0.11 0.17 −0.04 −.44 to 0.36 Desirable Range Systolic AUC (au) 0.76 159.4 −872.6 to 1191 0.18 0.06 −0.35 to 0.46 Systolic Standard 0.88 −0.2 −2.8 to 2.4 0.17 0.03 −0.43 to 0.37 Deviation (mmHg) Diastolic Proportion in 0.16 −0.1 −0.22 to 0.04 0.44 0.28 0.13 to 0.70 Desirable Range Diastolic AUC (au) 0.13 −385.4 882.6 to 111.9 0.52 −0.30 −0.73 to 0.10 Diastolic Standard 0.48 −0.62 −2.40 to 1.15 0.21 −0.14 −0.55 to 0.26 Deviation (mmHg) Hemodynamics collected during the cognitive assessments following administration of midodrine compared to placebo. p values=drug X time interaction effect, which equals a paired t-test comparing change scores of midodrine minus placebo Mean difference=average difference in change scores (posttest - pretest) between midodrine minus placebo 95% CI of Mean=frequentist confidence interval about the mean difference in change score between midodrine minus placebo Bayes Factor =the likelihood of the data under the alternate hypothesis vs the null hypothesis. Bayes Effect Size=the median Bayesian effect size for the difference in change scores between midodrine minus placebo using an estimate, the population standard deviation as the denominator Bayes Effect Size 95% credible interval=the Bayesian credible interval about the median effect size Spinal Cord. Author manuscript; available in PMC 2020 September 17. http://www.deepdyve.com/assets/images/DeepDyve-Logo-lg.png Spinal Cord Pubmed Central

Double-Blinded, Placebo-Controlled Cross-Over Trial to Determine the Effects of Midodrine on Blood Pressure during Cognitive Testing in Persons with SCI

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1362-4393
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1476-5624
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10.1038/s41393-020-0448-0
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Abstract

Study Design: Clinical trial. Objectives: Individuals with spinal cord injury (SCI) above T6 experience impaired descending cortical control of the autonomic nervous system which predisposes them to hypotension. However, treatment of hypotension is uncommon in the SCI population because there are few safe and effective pharmacological options available. The primary aim of this investigation was to test Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms Corresponding Author: Jill M. Wecht: James J. Peters VA Medical Center, 130 W Kingsbridge Road, Bronx, NY. Jill.Wecht@va.gov; Phone: 718-584-9000 ext. 3122. Authors Contribution: JMW: oversaw and was primarily responsible for designing the study, participant enrollment, data collection procedures, database management, data analysis, result dissemination and regulation compliance; JPW: was primarily responsible for designing the study, data analysis, and result dissemination; CGK: was primarily responsible for participant enrollment, data collection procedures, database management, and regulation compliance; NDC: oversaw study design pertaining to the cognitive outcomes and was primarily responsible for the cognitive data analyses; SCK: was responsible for monitoring patient safety at the Kessler Foundation; TAD: was responsible for participant enrollment and monitoring patient safety at the Kessler Foundation; EW: was responsible for analysis of the cognitive outcomes; WAB: monitored patient safety at the VA and oversaw data analysis and result dissemination. Data Archiving: The datasets generated and analyzed in the current study are available from the corresponding authors upon request. Statement of Ethics: The authors certify that all applicable institutional and governmental regulations concerning the ethical use of human volunteers were followed during the course of this research. Conflict of Interest Statement: The authors report no financial conflict of interest in association with conducting the current clinical trial. Clinical Trials Registration # NCT02307565 VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 2 the efficacy of a single dose of midodrine (10 mg), compared to placebo, to increase and normalize systolic blood pressure (SBP) between 110–120 mmHg during cognitive testing in hypotensive individuals with SCI. Secondary aims were to determine the effects of midodrine on cerebral blood flow velocity (CBFv) and global cognitive function. Setting: United States clinical research laboratory. Methods: Forty-one healthy hypotensive individuals with chronic (≥ 1-year post-injury) SCI participated in this 2-day study. Seated SBP, CBFv, cognitive performance were monitored before and after administration of identical encapsulated tablets, containing either midodrine or placebo. Results: Compared to placebo, midodrine increased SBP (4±13 vs. 18±24 mmHg, respectively; p<0.05); however, responses varied widely with midodrine (−15.7 to +68.6 mmHg). Further, the proportion of SBP recordings within the normotensive range did not improve during cognitive testing with midodrine compared to placebo. Although higher SBP was associated with higher CBFv (p=0.02), global cognitive function was not improved with midodrine. Conclusions: The findings indicate that midodrine increases SBP and may be beneficial in some hypotensive patients with SCI; however, large heterogeneity of responses to midodrine suggest careful monitoring of patients following administration. Keywords Tetraplegia; Paraplegia; Spinal Cord Injuries; Hypotension; Orthostatic Hypotension; Cognition; Rehabilitation INTRODUCTION Focus on blood pressure in the medical literature is heavily skewed towards hypertension as opposed to hypotension. A recent PubMed search for hypertension yielded 490,320 literature references compared to 65,491 for hypotension over the course of the past century. Moreover, blood pressure threshold(s) used to define hypotension vary extensively, and whereas the diagnosis of hypertension is based solely on blood pressure, the diagnosis of hypotension is usually based on the presence of significant symptomology reflecting cerebral hypoperfusion, which includes dizziness, light-headedness, pre-syncope and syncope, as well as non-specific symptoms of generalized weakness, fatigue, nausea, cognitive slowing, blurry vision, leg buckling or headache (1). However, it should be appreciated that individuals with low blood pressure often remain asymptomatic and are, therefore, not diagnosed or treated. Further, longstanding sentiment argues that low blood pressure is a clinical syndrome unassociated with pathological consequences, and there persists an implicit belief that hypotension may convey significant cardiovascular benefit (2). Yet 13-year all-cause and cardiovascular disease mortality risk was 2.4 to 3.4 times higher, respectively, in males 40 to 49 years with systolic hypotension compared to age-matched males with normal blood pressure (3), and in a recent meta-analysis all-cause mortality was 36% higher in association with orthostatic hypotension (4). Moreover, there is a growing body of evidence that links persistent asymptomatic hypotension and orthostatic hypotension with adverse changes in health-related quality of life, as well as an increased incidence of Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 3 anxiety and depression (2), cognitive deficits (5), hopelessness (5) and dementia (6, 7). Therefore, treatment to increase and normalize low blood pressure, even in asymptomatic patients with SCI, should be considered. Loss of integral descending cortical control of autonomic cardiovascular regulation following spinal cord injury (SCI) results in a variety of measurable abnormalities in blood pressure, most prominently chronic hypotension, orthostatic hypotension and autonomic dysreflexia. As in the general population, chronic hypotension and orthostatic hypotension in the SCI population are associated with cognitive deficits (8), adverse changes in health- related quality of life (9), increased arterial stiffness (10) and a 3–4 fold increased stroke risk (11). Although evidence suggests improved cognitive performance following increases in blood pressure with midodrine (12), because most hypotensive individuals with SCI are asymptomatic there is a wide disparity between the incidence of hypotension and orthostatic hypotension and the diagnoses of these conditions and very few patients are treated for disorders of low blood pressure (13, 14). Additionally, there is a paucity of treatment options for hypotension and orthostatic hypotension that are clinically available and have been proven safe and effective for widespread use in the SCI population. Non-pharmacological remedies for treatment of hypotension and orthostatic hypotension that are often prescribed in hypotensive individuals with SCI include: exercise (15), functional electrical stimulation (16), compression garments (17) and salt and water intake (18); however, there is little supporting evidence for any of these interventions and the data that are available are of poor quality (19). Pharmacological treatment options for hypotension and orthostatic hypotension include: midodrine hydrochloride (20), L-threo-3,4-dihydroxyphenylserine (droxidopa) (21), fludrocortisone and ergotamine (22), and ephedrine (23). In a randomized, placebo- controlled, double-blinded clinical trial in four individuals with SCI, midodrine (10 mg) increased average seated systolic blood pressure to within a normotensive range (i.e., 110 and 120 mmHg), in 1 of the 4 subjects tested; one subject became hypertensive (average systolic blood pressure of 143 mmHg) and 2 remained hypotensive (average systolic blood pressure < 110 mmHg) (20). Despite this limited evidence, midodrine is the most commonly prescribed anti-hypotensive agent used in the SCI population (https://scireproject.com/ evidence/rehabilitation-evidence/orthostatic-hypotension/). Clearly, more data are needed to support the clinical management of hypotension and orthostatic hypotension in the SCI population. The primary aim of this investigation was to test the efficacy of midodrine (10 mg), compared to placebo, to increase seated systolic blood pressure at rest and during a battery of neuropsychological tests in hypotensive individuals with SCI in a randomized, double- blinded, cross-over trial. Our primary hypothesis was that seated systolic blood pressure would be significantly increased from baseline following midodrine administration as compared to placebo. Secondarily, we hypothesized that the proportion and stability of systolic blood pressure recordings within the normotensive range would be significantly increased during cognitive testing following administration of midodrine compared to placebo. Additional study aims were to determine if midodrine administration would be Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 4 associated with increases in cerebral blood flow velocity and improved cognitive function compared to placebo. We hypothesized that cerebral blood flow velocity would be significantly increased and that composite scores on a battery of cognitive tasks would be improved following midodrine administration. METHODS Participants: This trial was conducted at two research facilities under identical study protocols, which were approved by the IRB committees at both facilities. Participants were deemed eligible for an in-person screening visit based on the following criteria: 1) between the ages of 18 and 65 years, 2), non-ventilator dependent, 3) duration of injury more than 12 months, 4) native English speaker and 5) better than 20/60 vision in worst eye with prescription eyewear. Exclusion criteria included: 1) three or more self-reported symptomatic episodes of autonomic dysreflexia per week, 2) current illness or infection, and 3) documented history of hypertension, diabetes, traumatic brain injury, or any neurological condition other than SCI. Eligible participants underwent a screening visit to confirm that they met the World Health Organization definition of hypotension, (i.e., systolic blood pressure ≤ 110 mmHg for males and ≤ 100 mmHg for females) (24). At the screening visit blood pressure was measured at 1- minute intervals for 5-minutes in the seated and supine positions using manual auscultation at the brachial artery. Eligibility for inclusion in the study was based on either: 1) a supine systolic blood pressure ≤ 90 mmHg; 2) seated systolic blood pressure ≤ 110 mmHg for males or ≤ 100 mmHg for females, or 3) a fall in blood pressure ≥ 20/10 mmHg within 5 minutes of assuming a seated upright position. Eligible participants were then scheduled for two testing visits and were issued a participant ID that was associated with the randomized order as either: midodrine/placebo or placebo/midodrine. The study participants, the research staff, and the investigators were blinded as to the order of administration and the randomization scheme was generated by the research pharmacist at the James J Peters VAMC who was responsible for dispensing the study medication. To limit the chance of autonomic dysreflexia during or after testing we scheduled participant visits the day after their bowel-care routine and asked that they void their bladder immediately before testing began on each visit. Procedures: Participants arrived at the testing site between 9am and 2pm and remained in their wheelchair in the seated position for all study procedures, which were identical on both study visits. The 2-study visits were scheduled no less than 2 and no more than 10 days apart and participants were asked to arrive at the laboratory at approximately the same time of day on both visits. Experiments were conducted in a quiet and temperature-controlled room and participants were instructed to avoid consuming caffeine, alcohol and nicotine products for 12 hours prior to testing. Vigorous unaccustomed exercise was also avoided for 24-hours prior to testing. Participants were asked to empty their bladder upon arrival to the testing laboratory, to limit the influence of reflex sympathetic activation on peripheral vascular tone from bladder distension, and medications were stopped for approximately 5 half-lives (at the Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 5 subject’s primary care physicians’ discretion) whenever possible. While resting quietly in the seated position, participants were instrumented with 3 electrocardiogram electrodes, finger and brachial blood pressure monitors and a head harness to secure probe placement for transcranial Doppler ultrasound recording of cerebral blood flow velocity. After instrumentation, a 5-minute continuous baseline assessment of heart rate, blood pressure and cerebral blood flow velocity was recorded while the participant rested quietly prior to administration of the initial neuropsychological battery of tests. After completion of the neuropsychological battery, midodrine or placebo was administered to the study participants in identical encapsulated tablets with a glass of water. Following administration of study medication participants rested quietly in their wheelchairs for 45-minutes. After which, and prior to beginning the second cognitive test battery, a 5-minute continuous assessment of heart rate, blood pressure and cerebral blood flow velocity was recorded. The second neuropsychological battery was then conducted and heart rate, blood pressure and cerebral blood flow velocity were monitored and recorded. The cognitive battery and hemodynamic monitoring occurred between 45 and ~90 minutes after dosing, which corresponds to peak blood pressure effects during a head-up tilt maneuver following administration of midodrine 10 mg. (25) Heart Rate and Blood Pressure: The electrocardiogram recording was performed using a bio-amplifier (Model RESP 1 with ECG: UFI, Morro Bay, CA, USA), with electrodes placed at the right and left mid-axillary lines in the 5th intercostal space and at the right anterior axillary line. Continuous beat-to- beat blood pressure (mmHg) was assessed at the finger using photoplethysmography (Finometer PRO, Finapres Medical Systems B. V., Netherlands) and at 1-minutes intervals at the brachial artery with manual auscultation (Series Wall Mobile Sphygmomanometers, Trimline Medical Products, Raritan, NJ, USA). The beat-to-beat electrocardiogram and photoplethysmography blood pressure signals were sampled at 500 Hz and were continuously monitored in real time on a computer screen. The digitized signals were stored on a computer hard-drive for subsequent analysis using custom data analysis programs written with LabVIEW graphical software for instrumentation (National Instruments, 11500 North Mopac Expressway Austin, TX 78759–3504). Brachial artery blood pressure recordings were used to calibrate the finger blood pressure assessments, to determine the proportion of blood pressure recording within the normotensive range and to calculate the area under the curve (AUC) of the blood pressure recordings during each of the cognitive batteries before and after administration of study drug. The normotensive range was defined as a systolic blood pressure between 110–120 mmHg and a diastolic blood pressure between 70–80 mmHg. Cerebral blood flow velocity: Transcranial Doppler ultrasound technology (Terumo Cardiovascular Systems 1311 Valencia Avenue Tustin, CA 92780–6447) was used to measure cerebral blood flow velocity. The probe was operated at a frequency of 2.0 MHz to visualize the middle cerebral artery and insonation was through the left temporal window. The middle cerebral artery was identified by the target depth (45–55 mm), sound and direction of flow (i.e., towards the probe), the characteristic spectral waveform and relatively faster flow velocity compared to surrounding Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 6 cerebral vessels. Once the middle cerebral artery was visualized, probe placement was secured for the duration of testing using a head-harness. Data output from the transcranial Doppler ultrasound was monitored in real-time and included systolic flow velocity, diastolic flow velocity and mean flow velocities, which were recorded in centimeters per second (cm/s). The beat-to-beat signals were sampled at 500 Hz and were stored on a computer hard-drive for subsequent analysis using custom data analysis programs written with LabVIEW graphical software for instrumentation. Neuropsychological Testing: Participants underwent an abbreviated, non-motor dependent, cognitive battery, to assess global cognitive function. This battery included tests of verbal fluency (Controlled Oral Word Fluency Test), verbal learning and memory (Hopkins Verbal Learning Test-Revised), cognitive inhibition (Stroop), auditory working memory (WAIS-IV Letter-Number Sequencing), cognitive flexibility (Oral Trail Making Test) and processing speed (Symbol Digit Modalities Test). The battery took about ~45 minutes to complete and was performed by the participants before and after administration of study medication on each study visit. A different version of each neuropsychological test was used at each time point to minimize a possible learning effect. Cognitive impairment was defined by a Global Deficit Score (GDS) of at least 0.5, which converts demographically-corrected T-scores to a deficit score, representing the distance each test score is below the normative mean (26). Overall GDS is the average of all converted test scores and a GDS score of 0.5 or higher translates to performance of at least 1 SD below the normative mean on at least half of the cognitive measures. This methodology has demonstrated discriminative validity in detecting individuals with neurological disorders and cognitive impairment, (27) as well as external validity with disease state and everyday functioning outcomes (28). GDS was calculated under each of the 4 test conditions: pre- and post-placebo; pre- and post-midodrine. Statistical Analyses: Repeated measures ANOVA models were constructed to determine significant main and interaction effects for drug (midodrine, placebo) and time (pre- and post-administration) for the systemic and cerebral hemodynamics and for cognitive GDS. Because in these 2×2 models, the interaction effect is equivalent to a paired t-test on the change scores (29), we also calculated effect sizes (Cohen’s dz) (30), 95% confidence intervals, Bayes factors and Bayesian credible intervals from the t-test calculations (31). For the change scores, mean differences were calculated as midodrine minus placebo. Multilevel modeling using the lme4 package in R was used to determine the relationship between changes in systolic blood pressure and changes in mean flow velocity from pre- to post-testing following administration of midodrine compared to placebo. To assess systolic blood pressure stability, we used the serial brachial recordings and set the normotensive systolic range between 110 and 120 mmHg, inclusive. To quantify stability, for the time series of systolic blood pressure values under each time and drug combination, we first calculated the percentage of beats that fell within the desirable range and then expanded the range serially by +/− 10 mmHg, such that the subsequent systolic range was 100 to 130 mmHg, and repeated the percentage calculation until we were inclusive of all Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 7 systolic blood pressure observations (i.e., 40–190 mmHg). The resulting percentage within each range was then plotted against the systolic blood pressure range at each iteration and the area under the curve (AUC) was calculated for each plot. The same method was applied to the serial diastolic blood pressure data, with the desirable range set at 70–80 mmHg. The blood pressure processing and AUC calculations were performed with a custom LabVIEW program. The larger the AUC, the closer the systolic and diastolic blood pressure values were to the respective desirable range, and the more stable were the signals across the recording period. To assess the efficacy of midodrine to normalize blood pressure, the proportion of values that fell within the systolic and diastolic desirable ranges described above was also quantified. As with the hemodynamic data from above, the AUC and proportion in the desirable range data were analyzed with a drug X time repeated measures ANOVA and change score analysis with paired t-tests was used to calculate effect sizes, confidence intervals, Bayes factors and Bayesian credible intervals. All continuous data are presented as mean ± standard deviation and significance was set at an alpha of < 0.05. Statistical calculations were performed using SPSS and JASP (for the Bayesian calculations) and R for the multilevel modeling. RESULTS Characteristics of the Participants: A total of 43 individuals with SCI were consented to participate; however, two withdrew prior to initiation of the study procedures, therefore data are reported in 41 participants (Table 1). The participants were mostly male, with cervical (90%), motor-complete lesions (81%). Self-reported levels of physical activity suggested that most (85%) engaged in at least 1 day of exercise/week at a moderate intensity and that they were otherwise healthy. Twenty participants were randomly assigned to receive midodrine on the first study visit and placebo on the second visit and 21 received placebo first; there were no significant differences for hemodynamics by randomization order. Resting Hemodynamic Responses: Average systemic and cerebral hemodynamic data are presented for 5-minutes in the seated resting position prior to (Table 2a) and following (Table 2b) administration of study medication. Resting hemodynamics did not differ significantly prior to administration of study medication. The drug by time interaction effect was significant for heart rate (all p≤ 0.023) [Figure 1a] (95% CI of mean difference (midodrine minus placebo) = −10.1 to −3.8 bpm), systolic blood pressure [Figure 1b] (95% CI of mean difference = 9.0 to 24.1 mmHg), diastolic blood pressure [Figure 1c] (2.5 to 10.4), mean flow velocity [Figure 1e] (0.3 to 4.4 cm/s) and diastolic flow velocity [Figure 1f] (0.4 to 5.4 cm/s), but was not significant for systolic flow velocity [Figure 1d] (95% CI for mean difference = −3.3 to 6.8 cm/c). Results of the repeated measures ANOVA models are presented (Table 3), which indicate large Bayes Factors (BF ) for heart rate (BF = 390.7), systolic blood pressure (BF = 319.1) 10 10 10 10 and diastolic blood pressure (BF = 15.0) indicating strong evidence that these hemodynamic responses to midodrine differed from placebo. Whereas the BF for mean Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 8 flow velocity (BF =2.01) and diastolic flow velocity (BF = 1.84) were more modest and 10 10 would be considered “anecdotal” evidence of a treatment effect (31). The association between change in systolic blood pressure and change in mean cerebral blood flow velocity is depicted following placebo (Figure 2a) and midodrine (Figure 2b). Results of the multilevel modeling examining the relationship between systolic blood pressure and mean cerebral blood flow velocity indicate a significant main effect for systolic blood pressure (p=0.02); however, main effects for time (p=0.52) and drug (p=0.34) and the associated interaction effects were not significant (all p > 0.31). This suggests, that regardless of time or drug, higher systolic blood pressure is associated with higher mean blood flow velocity in hypotensive individuals with SCI. Nine of the 41 participants (22%) had an average resting systolic blood pressure within the normotensive range following midodrine administration; however, systolic blood pressure exceeded the normotensive range in 17 (41%) and remained below the desirable range in 15 (37%) participants (Figure 3a). Further, the change in systolic blood pressure (mmHg) following midodrine administration suggested wide variability (delta of −15.7 to +68.6 mmHg) in individual responses to the medication compared to placebo (delta of −15.8 to +38.7 mmHg) (Figure 3b). Normalization and Stability of Blood Pressure: An average of 25±4 brachial systolic blood pressures were collected in participants during each cognitive test battery. The interaction effects for the proportion of systolic or diastolic blood pressures within the desirable ranges were not significant (Table 3), indicating that treatment with midodrine did not “normalize” blood pressure compared to placebo. The AUC of blood pressure “stability” before and after administration of placebo and midodrine is also summarized (Table 3). The interaction effect for AUC was not significant for systolic or diastolic blood pressure, which indicates that the midodrine treatment did not improve blood pressure stability compared to placebo. Corresponding AUC curves for systolic blood pressure are presented for three participants pre- and post-midodrine administration (Figure 4); one participant who remained hypotensive (left panel), one participant who was normotensive (middle panel) and one participant who became hypertensive (right panel) after midodrine administration. Increased AUC (i.e., improved blood pressure stability within or near the desired range), was noted in the participant who had a normotensive response to midodrine (middle panel). Of note, midodrine was effective at stabilizing blood pressure within or near the normotensive range in 6 of the 41 study participants. GDS analyses: Sixty-three percent of the study participants exhibited an average GDS ≥ 0.5 before administration of placebo or midodrine, indicating impaired function in more than half of the cognitive domains tested. There were no significant main or interaction effects for cognitive GDS (interaction p = 0.91, BF = 0.17), suggesting that compared to placebo, midodrine administration did not improve global cognitive function in these 41 hypotensive participants with SCI. However, it might be noted that of the 9 participants with a normal Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 9 systolic blood pressure following midodrine, 3 showed evidence of improved global cognitive function after administration. DISCUSSION Hypotension and orthostatic hypotension are not high on the clinical priority list in patients with SCI, which is due in part to the lack of safe and effective treatment options available for use in the population (19). Yet low resting blood pressure and orthostatic hypotension may be clinically relevant signs to indicate impaired autonomic nervous system control of cardiovascular function and are associated with significant adverse health outcomes. Therefore, treatment of hypotension and orthostatic hypotension should be considered important aspects in the clinical management of individuals with SCI. It was our goal to determine the effectiveness of midodrine, compared to placebo, to increase and maintain systolic blood pressure within a tight normotensive range of 110–120 mmHg in hypotensive participants with SCI. Our findings suggest that, although midodrine did increase blood pressure, large heterogeneity of response was evident such that only a small percentage (22%) of the study participants had systolic blood pressures within the normal range following administration. Furthermore, the proportion and the stability of systolic blood pressures recordings within the normotensive range were not improved with midodrine compared to placebo. There is substantial evidence that demonstrates improved standing blood pressures and reduced symptoms associated with cerebral hypoperfusion following midodrine administration in models of symptomatic neurogenic orthostatic hypotension (32); however, there is limited evidence to support wide spread utility in the SCI population. While it is not our intent to discourage the use of midodrine to treat hypotension and orthostatic hypotension in the SCI population, we sought to 1) increase awareness of the heterogeneity of response, 2) encourage more frequent monitoring of blood pressure following prescription and 3) adjust dose as needed. With that in mind, several points should be considered when interpreting these results in the context of clinical algorithms used to manage hypotension and orthostatic hypotension in the SCI population: 1) lack of a clear consensus regarding the definition of hypotension and normotension, 2) changing guidelines for the management of hypertension, 3) highly prevalent blood pressure instability, and 4) the impact of anti- hypotensive treatment on blood pressure surges during autonomic dysreflexia. There is a lack of clarity regarding the definition of hypotension that contributes to low diagnosis and treatment rates. A recent systematic literature search, that included 63 publications involving over 7000 participants, found 15 different definitions for hypotension (33), and different definitions yielded significantly altered incidence rates (34). Large epidemiological studies tend to define hypotension as the lowest 5–30% of the population (2, 35) while smaller prospective studies use upper limit cut-offs of between 100 and 120 mmHg systole (36). The definition of hypotension in the SCI population as published in the International Standards to Document Remaining Autonomic Function after Spinal Cord Injury is a supine systolic blood pressure < 90 mmHg. (37) However, the World Health Organization defined hypotension as a resting systolic blood pressure of < 110 mmHg for Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 10 males and < 100 mmHg for females without regard to diastolic blood pressure (24), which has been used by our group to define hypotension in persons with chronic SCI (8). The diagnosis of hypotension is usually based on the presence of significant symptomology. Despite views that, in the absence of clinical symptomology, hypotension represents a “non- disease” state, (38) recent evidence suggests that lower baseline systolic blood pressure predicts incident depression at a 2-year follow-up after adjustment for socioeconomic status and relevant clinical factors (cardiovascular disease, chronic illness, frailty) (39). In addition, individuals between the age of 30 and 75 years with asymptomatic hypotension are at increased risk for cognitive and affective disorders, including decreased memory and concentration (40), higher rates of hopelessness, (40) and an increased prevalence of dementia, which includes both Alzheimer’s disease and vascular dementia (7). Therefore, treatment of asymptomatic hypotension in the SCI population should be considered a clinical priority. To our knowledge there are no long-term studies documenting the potential association between hypotension and incident depression or cognitive changes with aging in the SCI population. However, we previously documented higher rates of depressive symptom reporting and deficits in memory and information processing in hypotensive individuals with SCI compared to a normotensive SCI cohort (8). Moreover, although most hypotensive individuals with SCI do not spontaneously report symptoms, when asked directly, they are able to ascribe adverse impacts of hypotension and orthostatic hypotension on their activities of daily living and quality of life (9). Although the results herein do not demonstrate a lessening of cognitive dysfunction following increases in blood pressure with midodrine, the data do suggest that higher blood pressures are associated with higher cerebral blood flow velocities and one-third of participants with normal systolic blood pressure responses to midodrine displayed improved cognitive function. These results suggest that, if higher - more normal - blood pressure is maintained with prolonged anti-hypotensive treatment, improvement in long-term cognitive performance may be evident. There are nearly 200 prescription medications with FDA approval for label and off-label use to treat hypertension, and many patients require combinatorial therapy to maintain optimal blood pressure control. A similar approach to the treatment of hypotension and orthostatic hypotension may be beneficial; however, until a variety of safe and effective agents with different mechanisms of actions are identified, clinical treatment will be inadequate, and individuals will remain un- or under-treated. Further, while prioritizing the treatment of asymptomatic hypertension in clinical practice is well appreciated, lack of acknowledgement that there may be a blood pressure value that is recognized to be too low is noteworthy. Current guidelines used in treatment algorithms for hypertension indicate a normal systolic blood pressure of < 120 mmHg, with systolic pressures between 120–129 mmHg being elevated (41), therefore we chose a desirable range for systolic blood pressure of between 110 and 120 mmHg in this trial. Notwithstanding the lack of clear consensus regarding what constitutes normal blood pressure and the relatively tight normotensive range selected, it is not surprising that we document limited efficacy of midodrine to ‘normalize’ blood pressure following a single 10 mg dose. However, what was surprising is the wide variability in response to midodrine, compared to placebo, in our participants with SCI. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 11 We appreciate that blood pressure instability, which is commonly reported in persons with SCI (42), complicates the clinical management of hypotension and orthostatic hypotension. We recently noted that fluctuations in systolic blood pressure of ≥ 20 mmHg, over a 30-day period were increased with age and duration of injury (43), which may be associated with loss of baroreceptor buffering of blood pressure, similar to the general population (44); therefore, management of hypotension in the SCI population should aim to stabilize, as well as to normalize, blood pressure. The AUC analyses suggest that the stability of the blood pressure, relative to the normotensive range, was not improved with midodrine. In fact, the AUC was lower following midodrine administration compared to following placebo in half of the participants. This finding indicates increased blood pressure instability following midodrine administration, which speaks to the large heterogeneity of responses. However, it should be noted that a few participants did respond to midodrine with a normal and stable systolic blood pressure, as depicted in Figure 3c & 3d. Average brachial systolic blood pressure was within the normotensive range in 9 of the 41 participants tested and these participants tended to be younger and injured fewer years than those with inadequate and excessive responses to midodrine. Given the heterogeneity of response to midodrine and significant blood pressure instability in persons with SCI, increasing the armamentarium of safe and effective clinical strategies is vitally important, particularly in individuals who are prone to autonomic dysreflexia. We did not induce autonomic dysreflexia in this trial and none of the participants reported feeling symptomatic prior to or after administration of study drug. A previous study found that increases in blood pressure during penile vibrator stimulation for sperm retrieval (i.e., a procedure known to induce autonomic dysreflexia), were not worsened with the addition of midodrine (45). However, this response to midodrine was reported during a closely observed clinical procedure; home use of midodrine during life events that may induce autonomic dysreflexia should be studied. Importantly, the practice of ‘boosting’ during athletic competition, should serve as an indicator of the importance of increasing blood pressure – safely – to avoid this dangerous and uncontrolled practice in athletes with SCI. Limitations: There are several study limitations to consider when interpreting the findings reported. Based on prior evidence, we only tested the efficacy of a single 10 mg dose of midodrine, compared to placebo, over a relatively brief observation period; however, higher doses for those who remained hypotensive and lower doses for those in whom blood pressure was elevated above the normotensive range should be tested for efficacy. Additionally, while the 10 mg dose did not improve blood pressure stability, a lower dose (2.5 or 5 mg) administered more frequently throughout the day may be more effective and may provide more clinically relevant information. We did not assess supine blood pressure responses to midodrine and did not investigate the effects on blood pressure during autonomic dysreflexia. We did not record symptom reporting in association with the increase in blood pressure, which in many participants met the definition of autonomic dysreflexia (i.e., systolic increase > 20 mmHg). The range selected to define normotension was narrow and Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 12 arbitrary, because there are currently no guidelines, other than those which define elevated blood pressure and hypertension. Finally, the study sample included a largely homogeneous cohort of participants and extrapolation to the broader SCI population may be inappropriate. Conclusion: Compared to placebo, midodrine, on average, significantly increased systolic blood pressure; however, large heterogeneity of responses among these hypotensive participants with SCI were evident. Furthermore, and perhaps more concerning, was that midodrine appeared to increase blood pressure instability in about half of the participants tested. That said, prescription of midodrine may benefit individual patients, particularly those who are younger and injured for fewer years; this finding requires further study to definitively identify responders from non-responders. Additionally, higher systolic blood pressures were associated with higher cerebral blood flow velocities, which may have beneficial effects on long-term cognitive function. Given the growing body of evidence indicating significant adverse sequela of untreated asymptomatic hypotension and orthostatic hypotension, identifying an armamentarium of safe and effective treatment options for use in the SCI population is needed. Acknowledgement: We would like to thank all the study participants for their involvement in this study and want to acknowledge Beatrice Ugiliweneza, Samineh Mesbah and Susan Harkema for their programming and statistical skills in creating the area-under-the-curve analyses. Sources of Funding: This project was funded by the Craig H Neilsen Foundation (Grant #284196) and the Department of Veterans Affairs, Veterans Health Administration, Rehabilitation Research & Development Service Center for the Medical Consequences of Spinal Cord Injury (Grant #D1382-P, #B2020-C). The authors report no conflict of interest. References: 1. Miller ER 3rd, Appel LJ. 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Page 16 Figure 1: Results of the repeated measures ANOVA models for heart rate [a], systolic blood pressure [b], diastolic blood pressure [c], systolic flow velocity [d], mean flow velocity [e] and diastolic flow velocity [f] pre to post placebo (closed circles) and midodrine (open squares). *** p<0.001; ** p<0.01; * p<0.05 for the drug by time interaction effect. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 17 Figure 2: The relationship between change in systolic blood pressure (SBP) and mean cerebral blood flow velocity (FV) following administration of placebo [a] and midodrine [b]. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 18 Figure 3: Average [a] and the change [b] in 5-minute seated resting systolic blood pressure (mmHg) following administration of placebo and midodrine for each participant. The dashed lines represent the upper and lower limits of the normotensive range [a] and the no change [b]. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 19 Figure 4: Systolic blood pressures Pre (closed circles) and Post (open squares) midodrine administration in 3 individual participants (top) and the AUC curves which were generated from these data (bottom). Left panel: the participant is hypotensive Pre and Post midodrine [a] and the AUC indicates a modest improvement in normalizing systolic blood pressure Post midodrine [b]. Middle panel: the participant is hypotensive Pre midodrine and normotensive Post midodrine [c] and the AUC reflects an increased proportion of normal blood pressure Post midodrine [d]. Right panel: the participant is hypotensive Pre midodrine and hypertensive Post midodrine [e] and the AUC reflects a reduced proportion of normal blood pressure Post midodrine [f]. Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 20 Table 1. Subject Characteristics Participants (n=41) Age (years) 44 ± 12 Males n (%) 33 (80) Caucasian n (%) 23 (56) African American n (%) 8 (20) Hispanic n (%) 8 (20) Other n (%) 2 (5) American Veteran n (%) 6 (15) BMI (kg/m ) 24 ± 4 Duration of Injury (years) 16 ± 12 Level of Injury C4–T9 AIS A n (%) 18 (44) AIS B n (%) 15 (37) AIS C n (%) 6 (15) AIS D n (%) 2 (5) Data are means ± SD; BMI: body mass index; m: meters; kg: kilograms Other ethnicity = 1 Asian and 1 East Indian Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 21 Table 2a. Average Pre-treatment Hemodynamics Placebo Midodrine Heart Rate (bpm) 68.0±10.2 67.6±10.9 Systolic BP (mmHg) 98.1±14.0 98.6±16.3 Diastolic BP (mmHg) 57.8±9.5 59.6±10.6 Systolic FV (cm/s) 69.4±19.2 70.0±15.9 Mean FV (cm/s) 43.3±13.3 43.5±10.7 Diastolic FV (cm/s) 30.4±8.3 29.7±7.8 Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 22 Table 2b. Average Post-treatment Hemodynamics Placebo Midodrine Heart Rate (bpm) 65.0±10.5 60.0±12.0 Systolic BP (mmHg) 106.3±18.0 115.0±27.1 Diastolic BP (mmHg) 61.4±13.3 66.0±16.5 Systolic FV (cm/s) 70.5±15.6 71.0±16.8 Mean FV (cm/s) 44.6±11.7 46.0±10.5 Diastolic FV (cm/s) 31.3±11.1 32.9±13.2 Hemodynamic data collected during the 5-minutes of seared rest before and after treatment with placebo and midodrine. Dare means ± SD; bpm=beats per minute; BP=blood pressure; FV=flow velocity; cm=centimeters; s=seconds Spinal Cord. Author manuscript; available in PMC 2020 September 17. VA Author Manuscript VA Author Manuscript VA Author Manuscript Wecht et al. Page 23 Table 3. Hemodynamic Changes and Blood Pressure Instability: Midodrine vs. Placebo Mean 95% CI of mean Bayes Effect Effect Size 95% Variable p value Difference Difference Factor Size Credible Interval Heart Rate (bpm) <0.001 −7.0 −10.1 to −3.8 390.70 −0.93 −1.39 to −0.47 Systolic BP (mmHg) <0.001 16.5 9.0 to 24.1 319.10 0.90 0.44 to 1.37 Diastolic BP (mmHg) <0.001 6.4 2.5 to 10.4 15.00 0.66 0.21 to 1.12 Systolic FV (cm/s) 0.48 1.8 −3.3 to 6.8 0.21 0.13 −0.28 to 0.55 Mean FV (cm/s) 0.023 2.3 0.3 to 4.4 1.84 0.47 0.05 to 0.91 Diastolic FV (cm/s) 0.026 2.9 0.43 to 5.4 2.01 0.46 0.05 to 0.90 Systolic Proportion in 0.86 −0.01 0.14 to 0.11 0.17 −0.04 −.44 to 0.36 Desirable Range Systolic AUC (au) 0.76 159.4 −872.6 to 1191 0.18 0.06 −0.35 to 0.46 Systolic Standard 0.88 −0.2 −2.8 to 2.4 0.17 0.03 −0.43 to 0.37 Deviation (mmHg) Diastolic Proportion in 0.16 −0.1 −0.22 to 0.04 0.44 0.28 0.13 to 0.70 Desirable Range Diastolic AUC (au) 0.13 −385.4 882.6 to 111.9 0.52 −0.30 −0.73 to 0.10 Diastolic Standard 0.48 −0.62 −2.40 to 1.15 0.21 −0.14 −0.55 to 0.26 Deviation (mmHg) Hemodynamics collected during the cognitive assessments following administration of midodrine compared to placebo. p values=drug X time interaction effect, which equals a paired t-test comparing change scores of midodrine minus placebo Mean difference=average difference in change scores (posttest - pretest) between midodrine minus placebo 95% CI of Mean=frequentist confidence interval about the mean difference in change score between midodrine minus placebo Bayes Factor =the likelihood of the data under the alternate hypothesis vs the null hypothesis. Bayes Effect Size=the median Bayesian effect size for the difference in change scores between midodrine minus placebo using an estimate, the population standard deviation as the denominator Bayes Effect Size 95% credible interval=the Bayesian credible interval about the median effect size Spinal Cord. Author manuscript; available in PMC 2020 September 17.

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Spinal CordPubmed Central

Published: Mar 17, 2020

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