Neurogenic orthostatic hypotension, postprandial hypotension and exercise-induced hypotension are common features of cardiovascular autonomic failure. Despite the serious impact on patient’s quality of life, evidence-based guidelines for non-pharmacological and pharmacological management are lacking at present. Here, we provide a systematic review of the literature on therapeutic options for neurogenic orthostatic hypotension and related symptoms with evidence-based recommendations according to the Grading of Recommendations Assessment, Development and Evaluation (GRADE). Patient’s education and non-pharmacological measures remain essential, with strong recommendation for use of abdominal binders. Based on quality of evidence and safety issues, midodrine and droxidopa reach a strong recommendation level for pharmacological treatment of neurogenic orthostatic hypotension. In selected cases, a range of alternative agents can be considered (fludrocortisone, pyridostigmine, yohimbine, atomoxetine, fluoxetine, ergot alkaloids, ephedrine, phenylpropanolamine, octreotide, indomethacin, ibuprofen, caffeine, methylphenidate and desmopressin), though recommendation strength is weak and quality of evidence is low (atomoxetine, octreotide) or very low (fludrocortisone, pyridostigmine, yohimbine, fluoxetine, ergot alkaloids, ephedrine, phenylpropanolamine, indomethacin, ibuprofen, caffeine, methylphenidate and desmopressin). In case of severe postprandial hypotension, acarbose and octreotide are recommended (strong recommendation, moderate level of evidence). Alternatively, voglibose or caffeine, for which a weak recommendation is available, may be useful.
Neurogenic orthostatic hypotension (nOH) is a key feature of cardiovascular autonomic failure, defined by a sustained blood pressure (BP) fall ≥ 20 mmHg systolic and/or ≥ 10 mmHg diastolic within the 3 min of active standing or head-up tilt.
Prevalence of nOH is 30% above 65 years of age (Tilvis et al. 1996) and rises up to 70% in institutionalized patients (Freeman et al. 2011). nOH occurs in up to 80% of patients with multiple system atrophy (MSA) (Ha et al. 2011; Köllensperger et al. 2010; Fanciulli and Wenning 2015), 30% of patients with Parkinson’s disease (PD) (Velseboer et al. 2011) and 100% of patients with pure autonomic failure (PAF) (Goldstein et al. 2015). nOH may also develop in one-third of patients suffering from diabetes mellitus, amyloidosis or spinal cord injury (Low et al. 2004; Wang et al. 2008; Cariga et al. 2002; Illman et al. 2000).
In patients with cardiovascular autonomic failure, a profound and rapid BP fall occurs following food ingestion, due to inability of the sympathetic nervous system to counteract postprandial splanchnic hyperemia, and frequently leads to exacerbation of orthostatic hypotension (Onrot et al. 1985; Mathias et al. 1989, 1991). Post-prandial hypotension, that is a systolic BP drop > 20 mmHg within 2 h from food ingestion, may accompany nOH in up to 50% of patients (Frongillo et al. 1995; Senard et al. 1992).
Symptoms of nOH, including recurrent syncope, dizziness, weakness, nausea, tremulousness, headache or “coat-hanger pain” (pain in the neck and shoulder region) upon standing, may be exacerbated in the early morning, by exercise, heat exposure, dehydration and alcohol consumption. Symptomatic nOH can be severely disabling and poses at higher risk for injurious falls (Rascol et al. 2015). Development of cardiovascular autonomic failure has been also associated with shorter survival, cognitive impairment, as well as higher incidence of cardio- and cerebrovascular events on the long term (Fanciulli et al. 2013).
Management of cardiovascular autonomic failure may result challenging in clinical practice, relying on a combination of non-pharmacological and pharmacological measures, in which the underlying etiology, severity of symptoms and the individual risk–benefit ratio need to be taken into account.
Aim and methods
In the present paper, we provide an evidence-based overview of non-pharmacological and pharmacological treatment options for nOH and related symptoms of cardiovascular autonomic failure, i.e., post-prandial hypotension and exercise-induced hypotension.
A systematic keyword-based literature search was performed. Articles published in PubMed between January 1985 and March 2017 were screened. Keyword terms comprised: ‘neurogenic orthostatic hypotension’, ‘postural hypotension’, ‘postprandial hypotension’, ‘exercise-induced hypotension’ and ‘syncope’. These terms were searched alone and in combination with ‘non-pharmacological treatment’, ‘pharmacological treatment’, ‘therapy’ and ‘treatment’.
Following selection criteria were adopted:
Study cohorts: Patients with idiopathic nOH (e.g., pure autonomic failure, multiple system atrophy, Parkinson’s disease) and, with the exception of spinal cord injury, nOH secondary to other diseases [e.g., diabetes mellitus, amyloidosis—for classification of primary and secondary nOH, see also Fig. 1 Primary and secondary causes of nOH according to the site of lesion (Low 2008)].
Allowed study design: randomized controlled trials, open-label trials, case series and case reports.
Additional data were collected by hand-searching references of selected articles according to the abovementioned criteria.
The Grading of Recommendations Assessment, Development and Evaluation (GRADE) approach has been applied for classification of quality of evidence and recommendation level (Leone et al. 2013). The GRADEpro GDT software, provided by the GRADE working group to support grading of quality of evidence and strength of recommendation, has been used for this purpose (“https://gradepro.org”).
Treatment of nOH and related symptoms: classification of evidence
Effects of water drinking on orthostatic, postprandial and exercise-induced hypotension
The short-term effect of rapid water drinking on orthostatic hypotension has been investigated in studies with sample sizes ranging from 5 to 47 patients with autonomic failure. Nine open-label studies, using different study protocols and outcomes, that investigated the hemodynamic effect of 300–500 ml water have been identified. Six studies reported a significant pressor effect of water drinking that lasted approximately 35 min after ingestion of water (Jordan et al. 1999, 2000; Cariga and Mathias 2001; Shannon et al. 2002; Young and Mathias 2004; Deguchi et al. 2007). In contrast, Mathias et al. 1991 reported that 300 ml water drinking did not have an effect on BP when measured 45 min after water ingestion in patients with MSA and PAF (Mathias et al. 1991). Similar findings were also reported in patients with PD and nOH: ingestion of 500 ml water did not change orthostatic BP when measured 60 min after fluid intake (Senard et al. 1999).
The effect of rapid water drinking on postprandial hypotension has been evaluated in two studies. In seven patients with PAF, rapid water drinking (480 ml, < 5 min before test meal) significantly decreased postprandial BP fall (Shannon et al. 2002). A similar effect was also observed in five patients with MSA (350 ml, < 5 min before test meal) (Deguchi et al. 2007). The effect of water drinking (480 ml distilled water within 5 min) on exercise-induced OH has further been evaluated in a small study in 8 patients with PAF. Although water drinking had an effect on post-exercise OH, no benefit has been demonstrated on BP fall during supine exercise (Humm et al. 2008). Although none of the abovementioned studies reported any adverse event, Jordan et al. 1999 commented that water ingestion may cause supine systolic BP increase more than 100 mm Hg in some patients with underlying cardiovascular autonomic failure (Jordan et al. 1999).
Quality of evidence The quality of evidence for water drinking to reduce postural BP drop is very low.
Safety issues None.
Recommendation The recommendation for water to stabilize BP in patients with autonomic failure is weak.
Few data are available on the effect of salt intake on BP in patients with nOH. Lipp et al. (2005) studied the response to water (500 ml) or to normal saline (500 ml NaCl 0.9%) administered through nasogastric tube in 10 patients with MSA. Results of this single-blinded crossover study demonstrated that ingestion of water increased systolic BP, whereas normal saline hardly showed any pressor response (Lipp et al. 2005).
Raj et al. (2006) evaluated the benefit of water and salt intake in nine patients with nOH of unspecified origin in a randomized, crossover trial. Although both water alone (473 ml) and in combination with salt (2 g NaCl) increased BP, salt intake attenuated global pressor effect (Raj et al. 2006). One further study investigated the effect of water and salt intake in seven patients with MSA: whereas water intake (450 ml) significantly increased BP values, clear soup intake (450 ml soup containing 1.7 g salt) reversed this effect (Z’Graggen et al. 2010).
Quality of evidence Based on available data, the quality of evidence for salt intake to reduce orthostatic BP fall is low.
Safety issues None.
Recommendation The recommendation for increased salt intake to stabilize BP in patients with autonomic failure is weak.
The intake of smaller meals may improve postprandial hypotension, since food volume and caloric load play an essential role in determining the degree of postprandial splanchnic hyperemia.
The effect of meal size on postprandial hypotension has been studied in one study by Puvi-Rajasingham and Mathias (1996) in seven patients with autonomic failure due to MSA or PAF. Patients were randomized to start either with three meals per day or six meals per day, providing identical daily caloric intake: larger meals resulted in significant lower BP levels in all positions and aggravation of postprandial orthostatic symptoms compared to small meals. However, the mean orthostatic BP fall was unaffected by meal size (Puvi-Rajasingham and Mathias 1996).
Quality of evidence The quality of evidence of smaller meals to reduce orthostatic BP drop is very low.
Safety issues None.
Recommendation Based on limited data, the recommendation for reduction of meal size is weak.
Sleeping with head-up tilt
Nocturnal head-up tilt is aimed at reducing nocturnal pressure natriuresis and, therefore, preventing exacerbation of nOH in the early morning.
Two small-sized, open-label studies have been conducted to investigate the effect of nocturnal head-up tilt (12°) on orthostatic BP in patients with nOH. Ten Harkel et al. (1992) reported that nocturnal head-up tilt alone or in combination with fludrocortisone (0.1–0.2 mg) significantly reduced orthostatic BP fall and improved orthostatic symptoms in six patients with nOH. Study period for each intervention was 1 week, including an average follow-up of 14 months (Ten Harkel et al. 1992). Latter findings were replicated by Van Lieshout et al. (1999) in a 3-week open-label study in patients with PAF (n = 8): combination of nocturnal head-up sleep and fludrocortisone led to a significant increase in upright BP and minimally improved orthostatic tolerance (van Lieshout et al. 1999). Both studies reported that supine BP remained uninfluenced by treatment. Similar results have been reported in one further patient, where chronic volume expansion due to nocturnal head-up sleep and fludrocortisone administration improved symptoms of orthostatic intolerance (van Lieshout et al. 1991).
Quality of evidence Based on limited data, the quality of evidence for nocturnal head-up tilt is very low.
Safety issues None.
Recommendation The recommendation for sleeping with head-up tilt position during night is weak.
Physical countermaneuvers may stabilize orthostatic BP through enhancement of peripheral vasoconstriction during orthostatic stress.
The effect of several countermaneuvers has been investigated in a cohort of 17 patients with familial dysautonomia by Tutaj et al. (2006) in an open-label, randomized crossover trial: bending forward, squatting and abdominal compression (20 mmHg), but not leg crossing, significantly ameliorated orthostatic BP fall in this cohort (Tutaj et al. 2006).
In contrast, leg crossing, but not tiptoeing, was able to combat orthostatic BP fall in patients with nOH due to PAF (Ten Harkel et al. 1994). Two further open-label studies and one case report are available confirming that a range of physical countermaneuvers attenuate nOH in chronic autonomic failure (Bouvette et al. 1996; van Lieshout et al. 1992; Wieling et al. 1993). In addition, Smit et al. (2004) evaluated the combination of legs crossing and abdominal compression in an open-label, randomized study. The combination of leg crossing and abdominal compression (20–40 mmHg) was more effective than abdominal compression alone in stabilizing orthostatic BP. Leg crossing alone also improved standing BP in 12 patients with nOH due to PAF, MSA and diabetes mellitus (Smit et al. 2004).
Quality of evidence The quality of evidence of physical countermaneuvers to reduce orthostatic BP drop in patients with autonomic failure is very low.
Safety issues None.
Recommendation Based on available data, there is a weak recommendation for use of physical countermaneuvers.
Abdominal binders and compression stockings
The efficacy of compression garments applied to different parts of the body to reduce venous pooling has been assessed in several small-sized studies.
One randomized, single-blind, placebo-controlled, crossover trial in 15 patients with PD and nOH by Fanciulli et al. (2016a) showed that abdominal binders, exerting a compression of 20 mmHg, significantly diminished BP fall upon head-up tilt without influencing supine BP values. In a 4-week open-label follow-up, daily use of abdominal binders also significantly improved nOH-related disability, assessed by means of the Orthostatic Hypotension Questionnaire (OHQ) (Fanciulli et al. 2016a).
One further randomized, crossover trial using an open-label study design has been conducted to evaluate the effect of abdominal compression with conventional and adjustable binders in 13 patients with nOH by Figueroa et al. (2015): mild abdominal compression (10 mmHg) prior to rising proved to ameliorate nOH. Although an increase in abdominal compression upon standing up to maximal tolerance did not further ameliorate nOH, decompression tended to aggravate orthostatic BP fall (Figueroa et al. 2015). The benefit of abdominal compression has been also reported by Smit et al. (2004) and Tutaj et al. (2006) using an abdominal compression that ranged from 20 to 40 mmHg (see description above).
Studies that systematically evaluated the effect of compression stockings are limited. Denq et al. (1997) showed that either contemporary compression of calves, thighs and low abdomen (40 mmHg each) or of the abdomen alone significantly improved nOH 14 patients with MSA, PAF and diabetic neuropathy. In contrast, the sole leg compression (calves and/or thighs) was less effective (Denq et al. 1997). In a young patient with insulin-dependent diabetes mellitus and nOH, symptomatic relief was reported with use of a G-suit (Elizondo et al. 1996).
Quality of evidence The quality of evidence for abdominal binders to reduce orthostatic BP fall is moderate, for compression stockings is very low.
Safety issues None.
Recommendation The recommendation for the use of abdominal binders to improve orthostatic BP fall in patients with autonomic failure is strong, for compression stockings is weak.
Midodrine, a peripheral α1-selective adrenoceptor agonist and prodrug of the active metabolite desglymidodrine, increases blood pressure by inducing vasoconstriction (Pittner et al. 1976).
Three randomized double-blind trials, with either cross-over study design (Wright et al. 1998) or parallel group (Jankovic et al. 1993; Low et al. 1997), that directly compared the effect of midodrine in a dosage of 2.5–30 mg per day versus placebo, have been conducted. The potent pressor effect of midodrine on standing BP was shown in all three studies with sample sizes ranging from 25 to 171 patients with autonomic failure and a study period (randomized, placebo-controlled phase) lasting up to 4 weeks.
Previously, Kaufmann et al. (1988) had investigated midodrine (25–40 mg/day) in combination with fludrocortisone (0.1 mg) or fludrocortisone alone in a randomized controlled trial with seven patients with MSA and PAF, demonstrating that both combination therapy and fludrocortisone alone were effective in only half of the patients. In the non-responder group, midodrine and fludrocortisone even decreased upright BP with respect to placebo.
Two further randomized, placebo-controlled, comparative studies with a cross-over design are available. Fouad-Tarazi et al. (1995) demonstrated that midodrine administered in a dosage of 2.5–10 mg three times a day, but not ephedrine (6–24 mg/day), significantly improved standing BP and the ability to stand in eight patients with MSA and PAF.
More recently, midodrine (5–10 mg/day) was compared to atomoxetine (18 mg/day) in 69 patients with nOH due to PAF, MSA or PD by Ramirez et al. (2014). Although both treatment arms significantly increased upright BP with respect to placebo, atomoxetine led to a higher increase of standing BP than midodrine. Nonetheless, the lack of a wash-out phase limits interpretation of this study, given that plasmatic half-live of atomoxetine may range from 5 h (extensive metabolizers) to 21 h (poor metabolizers) (Sauer et al. 2005).
The effect of midodrine on nOH has been investigated in further small-sized, non-randomized, open-label studies in patients with autonomic failure of different etiologies [familial dysautonomia (Axelrod et al. 1995), idiopathic OH (Axenti et al. 1993) and PAF/autonomic neuropathy (Schrage et al. 2004)] supporting efficacy of midodrine for treatment of nOH.
Quality of evidence The quality of evidence of midodrine to reduce orthostatic BP fall in patients with autonomic failure is high.
Safety issues The main safety concern of midodrine is supine hypertension. Further side effects include urinary retention and uncomfortable reactions such as paresthesia, piloerection, chills, scalp and generalized pruritus.
Recommendation Based on available data, there is a strong recommendation for use midodrine for treatment of nOH. Monitoring for exacerbation of supine hypertension and increase of post-void residual urine volume is required.
The efficacy of droxidopa (l-Dihydroxyphenylserine, l-DOPS), a precursor of norepinephrine, has been investigated in five randomized controlled trials involving more than 600 patients with nOH mainly due to PAF, MSA and PD, in a dosage ranging from 200 to 1800 mg, for a placebo-controlled, randomized period of up to 8 weeks.
Whereas four clinical trials demonstrated a significant difference in diverse outcomes favouring droxidopa over placebo [change in supine and upright systolic and diastolic BP (Freeman et al. 1999); supine and standing BP, HR, orthostatic tolerance (Kaufmann et al. 2003); change in OHQ composite score (Kaufmann et al. 2014); change in item 1 (dizziness/lightheadedness) of the Orthostatic Hypotension Symptoms Assessment (OHSA) scale (Hauser et al. 2015)], two further studies failed to meet the primary endpoint, defined as change in OHSA item 1 (dizziness/lightheadedness) (Biaggioni et al. 2015) and change in OHQ composite score (Hauser et al. 2014).
In details, Biaggioni et al. (2015) administered droxidopa, 100–600 mg three times a day, in 101 patients with autonomic failure. The primary efficacy end-point, defined as mean change of OHSA item 1 from randomization to study end, did not significantly differ from placebo (Biaggioni et al. 2015). Nonetheless, a conducted post hoc analysis showed a significant effect of droxidopa measured by OHQ composite score (Biaggioni et al. 2015). The possibility of a substantial carryover effect, explaining the failure of droxidopa in primary outcome, has been discussed, since patients randomized to placebo reported a sustained relief of the orthostatic dizziness/lightheadedness score and standing systolic BP at the end of the study. Besides, symptomatic improvement simply related to study participation has been hypothesized, possibly due to better adherence to non-pharmacological countermeasures during observation period (Kaufmann et al. 2015).
A pre-planned interim efficacy analysis of study 306 A in 51 patients with PD failed to show a significant difference for droxidopa with respect to placebo in primary endpoint, which was defined as change in OHQ composite score after 8 weeks (Hauser et al. 2014). Primary outcome was, therefore, modified to changes in item 1 of the OHSA score at 1-week-treatment for patients subsequently enrolled in study 306 B. Pooled results from study 306A and B demonstrated significant improvement in the dizziness/lightheadedness OHSA score (item 1) after 1-week-treatment in 171 patients with PD (Hauser et al. 2015).
Several additional small-sized studies (Carvalho et al. 1997; Mathias et al. 2001; Kaufmann et al. 1991; Matsubara et al. 1990; Goldstein and Sharabi 2009) and case reports (Sakoda et al. 1958; Kachi et al. 1988; Man in’t Veld et al. 1987; Biaggioni and Robertson 1987) further report benefit from droxidopa in patients with nOH due to MSA, PAF, PD, familial amyloidotic polyneuropathy and dopamine-beta-hydroxylase deficiency.
Quality of evidence The quality of evidence of droxidopa to reduce nOH-related symptoms is moderate based on missing long-term data.
Safety issues Possible side effects include hypertension, headache, dizziness and nausea. Falls, urinary tract infections, headache, syncope and dizziness have been reported at open-label follow-up, though systematic post-marketing studies to define rate of adverse events in clinical practice are not available yet (Kaufmann et al. 2015).
Recommendation recommendation for droxidopa to treat orthostatic intolerance in patients with cardiovascular autonomic failure is strong. Regular BP monitoring is required, since treatment may exacerbate supine hypertension.
Fludrocortisone, a synthetic mineralocorticoid, increases BP by expanding intravascular volume through sodium and water retention.
Evidence-based data on fludrocortisone for treatment of nOH are limited. Only two randomized, double-blind, crossover studies are available.
Kaufmann et al. (1988) investigated the effect of fludrocortisone in a dosage of 0.1 mg per day in combination with placebo or midodrine (25–40 mg/day) in 7 patients with nOH due to MSA or PAF. Fludrocortisone, administered for a period of 1 week, increased upright BP only in half of patients. The remaining patients did not respond to medication and upright BP even decreased (Kaufmann et al. 1988).
Schoffer et al. (2007) compared the efficacy of fludrocortisone and domperidone in a randomized, double-blind comparative study. In 17 patients it was shown that both fludrocortisone (0.1 mg/day) as well domperidone (30 mg/d) improved primary outcomes measured by Composite Autonomic Symptom Scale (COMPASS) and clinical global impression of change (CGI) within 3 weeks of treatment. In addition, fludrocortisone and domperidone showed a trend, though not significant, towards reduction of BP fall upon tilt-table testing (Schoffer et al. 2007).
The anti-hypotensive effect of fludrocortisone has been further demonstrated in small-sized, open-label studies in patients with MSA, PD, PAF and hypoadrenergic OH). (Ten Harkel et al. 1992; van Lieshout et al. 1991, 1999; Matsubara et al. 1990; Hakamäki et al. 1998).
Quality of evidence The quality of evidence of fludrocortisone to reduce orthostatic BP fall is very low.
Safety issues Main side effect that has been reported is nocturnal hypertension (Hakamäki et al. 1998). Further adverse events include headache, nausea, dizziness as well as generalized or localized edema and hypokalemia (Ricci et al. 2015). Data for long-term administration are limited. Experimental data suggest that long-term use is associated with end-organ damage (Norcliffe-Kaufmann et al. 2013) and increased risk of renal and cardiac fibrosis (Kaufmann 2016, personal communication).
Recommendation Recommendation for use of fludrocortisone for treatment of nOH is weak, based on quality of evidence and safety issues. Monitoring of supine BP and electrolytes is required.
The therapeutic rationale of the cholinesterase-inhibitor pyridostigmine for treatment of nOH relies on enhancement of cholinergic sympathetic ganglionic transmission, secondarily inducing BP rise. Such effect is especially to be expected during sympathetic activation, i.e., when subjects are in the upright position (Biaggioni 2014).
Based on two prospective open-label trials (Singer et al. 2003, 2006a), Singer et al. (2006b) conducted a double-blind, randomized, 4-arms (pyridostigmine 60 mg alone, placebo, pyridostigmine 60 mg in combination with 2.5 or 5 mg midodrine), cross-over study. In 58 patients with nOH (MSA, PAF, diabetic and autoimmune autonomic neuropathy), the authors demonstrated that pyridostigmine significantly improved standing diastolic BP one hour after administration. Importantly, no aggravation of supine hypertension was observed (Singer et al. 2006b). In a follow-up, open-label study pyridostigmine maintained favorable effects, especially in patients with less severe nOH without major side effects (Sandroni et al. 2005).
Shibao et al. (2010) evaluated the effect of pyridostigmine (60 mg) versus yohimbine (5.4 mg) in 31 patients with autonomic failure (MSA, PAF, PD) in a single-blind, randomized, controlled trial. In contrast to Singer et al. (2006b), this study could neither confirm that pyridostigmine increases standing diastolic BP 1 h after drug administration, nor that it improves pre-syncopal symptoms. The authors commented that the study population was more severely affected than in previous studies, partially explaining the conflicting results (Shibao et al. 2010).
Quality of evidence Very low, due to inconsistency of results.
Safety issues Side effects include gastrointestinal symptoms and urinary urgency (Biaggioni 2014).
Recommendation The recommendation for use of pyridostigmine to improve nOH is weak.
Yohimbine, an α2-adrenergic antagonist, leads to augmentation of sympathetic activity at CNS level, thus increasing norepinephrine release from adrenergic nerve terminals (Biaggioni et al. 1994a).
For yohimbine, three small-sized randomized controlled trials in up to 31 patients with nOH are available, showing inconsistent results.
Shibao et al. (2010) investigated the effect of yohimbine and pyridostigmine on standing diastolic BP one hour after administration in 31 patients with nOH due to MSA, PAF or PD. Only yohimbine (5.4 mg) significantly increased standing diastolic BP, seated systolic and diastolic BP and significantly improved nOH-related symptoms (Shibao et al. 2010). The positive pressor effect of yohimbine has been further reported in small-sized studies (n = 8–35) (Jordan et al. 1998, 2000; Onrot et al. 1987) in patients with autonomic failure.
In contrast to abovementioned findings, Senard et al. (1993) did not observe any BP increase at 24-h ambulatory BP monitoring in 17 patients with PD after 4-week treatment with yohimbine (2 mg three times a day) (Senard et al. 1993).
Similarly, Okamoto et al. (2012) reported negative results in a single-blind, crossover study with 17 patients with nOH due to PAF and PD: neither yohimbine (5.4 mg), nor atomoxetine (18 mg) alone significantly increased seated systolic BP 1 h after drug administration or improved orthostatic symptoms. Only co-administration of both yohimbine and atomoxetine increased seated systolic BP and orthostatic tolerance (Okamoto et al. 2012).
Limits of abovementioned RCTs include lack of a wash-out phase and/or measurement of supine BP.
Quality of evidence The quality of evidence for yohimbine to increase BP and orthostatic tolerance is very low.
Safety issues No side effects reported, effect on supine BP unknown.
Recommendation The recommendation for use of yohimbine is weak, due to very low and inconsistent quality of evidence.
Atomoxetine, which augments norepinephrine concentration in the synaptic gap by selectively blocking norepinephrine transporter, has been evaluated in three randomized, placebo-controlled trials, with a sample size ranging from 21 to 69 subjects.
As mentioned above, Okamoto et al. 2012 showed that neither atomoxetine (18 mg) nor yohimbine (5.4 mg) significantly changed seated systolic BP or orthostatic tolerance 1 h post-treatment in a cohort of 17 patients with nOH due to PAF and PD. Only the combination of both increased seated systolic BP and improved nOH-related symptoms (Okamoto et al. 2012).
In contrast, Shibao et al. (2007a) demonstrated that atomoxetine (18 mg) significantly increases seated and standing systolic BP in patients with central autonomic failure (MSA), but not in patients with peripheral autonomic failure (PAF/PD) (Shibao et al. 2007a).
Ramirez et al. (2014) further reported that both atomoxetine (18 mg, single dose) and midodrine (5–10 mg, single dose) significantly increased seated and upright BP with respect to placebo in a randomized, single-blind, crossover trial with 65 patients with nOH due to MSA, PAF, PD or of undetermined origin. Atomoxetine showed a higher increase in standing systolic BP with respect to midodrine. Atomoxetine, but not midodrine, also improved nOH-related symptoms with respect to placebo (Ramirez et al. 2014).
A possible carry-over effect cannot, however, be excluded in above mentioned studies, since washout-phases were not described in detail. The effect of atomoxetine on supine BP was not mentioned.
Quality of evidence Based on available literature, the quality of evidence for atomoxetine to raise standing BP is low.
Safety issues No side effects reported, effect on supine BP remains unclear.
Recommendation The recommendation for atomoxetine for treatment of nOH is weak, based on quality of evidence and pending safety issues.
The rationale for use of fluoxetine, a selective serotonin reuptake inhibitor, to improve nOH is unknown. One small, open-label study in five patients with nOH of varying etiologies (PAF, renal failure, diabetes mellitus) revealed a positive impact of fluoxetine (20 mg once daily) on nOH after 6–8 weeks of treatment (Grubb et al. 1994). In addition, in an open-label study, Montastruc et al. (1998) demonstrated that chronic administration of fluoxetine (20 mg; 1-month treatment) significantly reduced orthostatic systolic BP fall and provided symptomatic relief in 14 patients with PD (Montastruc et al. 1998).
Quality of evidence The quality of evidence for fluoxetine to improve nOH is very low.
Safety issues Common side effects are gastrointestinal complaints, headache and dizziness (Wernicke 2004).
Recommendation Based on the quality of evidence, the recommendation for fluoxetine for treatment of nOH is weak.
Ergotamine, an ergot alkaloid, and its derivate dihydroergotamine increase BP through α-adrenergic vasoconstriction of arteries and veins (Perrin 1985).
Ergotamine has been investigated in a small-sized (n = 8), placebo-controlled, crossover study. Biaggioni et al. 1990 reported that inhalation of ergotamine (1 puff, 0.36 mg) proved effective compared to placebo in increasing seated and upright BP, as well as prolonging standing time before onset of nOH-related symptoms (Biaggioni et al. 1990). It is, however, unclear whether patients were randomly assigned to begin either with treatment or placebo and if the study included a wash-out phase. In one additional case report (Siminoski et al. 1988) aerosol administration of ergotamine has been described in a patient with multi-domain autonomic failure.
Dihydroergotamine, in a dosage ranging from 6.5 to 13 μg/kg, was investigated in two small-sized, randomized, placebo-controlled studies with a crossover design (Hoeldtke et al. 1989b; Hoeldtke and Israel 1989), in which an increase of upright BP was shown. In both studies, main limitation was represented by the lack or rather unclear description of a wash-out phase.
In addition, one open-label study (Victor and Talman 2002) compared intravenous administration of ergotamine (0.15 mg) versus oral clonidine (0.4 mg) in four patients with severe autonomic failure: whereas both drugs increased supine BP, dihydroergotamine was more effective in contrasting orthostatic BP fall.
Quality of evidence: Based on limited data, the quality of evidence for both ergotamine and dihydroergotamine to reduce orthostatic BP fall in patients with autonomic failure is very low.
Safety issues: common side effects of ergot alkaloids are nausea, vomiting, paresthesias and fatigue. Severe adverse effects include fibrosis (retroperitoneal, cardiac, pleural, pulmonary), peripheral vasoconstriction and ergotism (Schiff 2006).
Recommendation: in consideration of quality of evidence and safety issues, the recommendation for ergotamine and dihydroergotamine for treatment of nOH is weak.
Erythropoietin is reckoned to combat nOH by stimulating red cell mass production, thus increasing circulating blood volume and tissue oxygenation.
No randomized controlled trials are available for the treatment of nOH with erythropoietin in the setting of autonomic failure. Several small-sized (sample size up to 24 patients), open-label studies and case reports in patients with primary autonomic failure or nOH secondary to diabetes mellitus type 1 or familial amyloidosis reported a beneficial effect of erythropoietin on nOH (Hoeldtke and Streeten 1993; Perera et al. 1995; Biaggioni et al. 1994b; Winkler et al. 2001; Beirão et al. 2008; Kawakami et al. 2003).
Quality of evidence The quality of evidence for erythropoietin to increase orthostatic BP in patients with autonomic failure is very low.
Safety issues Adverse events include flu-like symptoms, allergic reactions, hypertension and increased risk of thrombosis, among others (Eagleton and Littlewood 2003).
Recommendation The recommendation for erythropoietin to treat nOH in patients with autonomic failure is weak.
Available evidence for ephedrine, a nonspecific direct and indirect α- and β-adrenoceptor agonist (Fouad-Tarazi et al. 1995), is scarce.
Efficacy and safety of ephedrine have been compared to midodrine in a randomized, double-blind, placebo-controlled, crossover study in eight patients with PAF and MSA by Fouad-Tarazi et al. (1995): ephedrine neither improved standing BP, nor the ability to stand. In contrast, ephedrine significantly increased supine systolic and diastolic BP (Fouad-Tarazi et al. 1995).
Quality of evidence Based on limited data, the quality of evidence for ephedrine to improve standing BP is very low.
Safety issues Adverse events include exacerbation of supine hypertension, dizziness, lightheadedness, photosensitivity and loss of balance.
Recommendation In consideration of quality of evidence, efficacy and safety profile, the recommendation for ephedrine to treat orthostatic hypotension in patients with autonomic failure is weak.
Other ephedra alkaloids
Phenylpropanolamine was investigated in an open study in 14 patients with nOH of varying etiologies (PAF, MSA, diabetes mellitus). Administration of 12.5 to 25 mg phenylpropanolamine led to a significant increase in seated BP in patients with autonomic failure (Biaggioni et al. 1987).
Jordan et al. (1998) used a single-blinded, placebo-controlled design to administer various pressor agents, including phenylpropanolamine. Phenylpropanolamine in a dosage of 12.5 to 25 mg elicited a significant pressor effect with respect to placebo. Notwithstanding, this study was not primarily designed for therapeutic purposes and presents several limitations: randomization is not mentioned; due to individual contraindications, not every patient received each study medication and no clear description of wash-out phases is provided. The authors further state that the study was carried over a period of several years (Jordan et al. 1998).
Jordan et al. (2004) confirmed in an open-label study in 13 patients with autonomic failure that phenylpropanolamine (12.5 and 25 mg) and pseudoephedrine (a stereoisomer of ephedrine, 30 mg per os) significantly increased BP. The pressor effect was increased by concomitant ingestion of water (Jordan et al. 2004).
Quality of evidence Based on available data, the quality of evidence for phenylpropanolamine and pseudoephedrine to increase BP in the context of cardiovascular autonomic failure is very low.
Safety issues Possible side effects include supine hypertension, anxiety, tremulousness, cerebral and cardiovascular events (Freeman 2008).
Recommendation In consideration of quality of evidence and safety issues, recommendation for phenylpropanolamine and pseudoephedrine for the treatment of nOH is weak.
Various studies have been identified that investigate the efficacy of octreotide, a somatostatin analog, for treatment of nOH.
Although Hoeldtke and Israel 1989 observed a beneficial response to octreotide administration (0.2–26 μg/kg) in 28 patients with PAF, MSA and diabetes mellitus, inconsistency among the different study protocols applied, limits interpretation of results (Hoeldtke and Israel 1989).
Bordet et al. (1995) studied the effect of acute administration of octreotide (100 μg) in nine patients with MSA in an randomized, placebo-controlled, double-blind study. Octreotide increased duration of head-up tilt test and time until minimal BP values was reached. Notably, octreotide also raised supine BP values (Bordet et al. 1995).
The effect of octreotide on exercise-induced hypotension in the supine position was evaluated by Smith et al. (1995), demonstrating no improvement of it. Nonetheless, octreotide improved orthostatic BP fall pre- and post-exercise (Smith et al. 1995).
Data for administration of octreotide on a regular basis are limited. In an open-label study, Bordet et al. 1994 evaluated the effect of a 6-month octreotide administration in 5 patients with MSA, reporting beneficial effects (Bordet et al. 1994).
Quality of evidence The quality of evidence for octreotide to reduce orthostatic BP fall is low.
Safety issues Side effects include gastrointestinal symptoms, in particular nausea and cramps, facial flushing and hyperglycemia. For this reason, use of octreotide is not recommended in patients with diabetes mellitus, especially in case of concomitant gastroparesis diabeticorum. Supine hypertension has been also reported.
Recommendation Recommendation for octreotide to treat nOH is weak.
For a wide range of other compounds, scattered evidence is available. Indomethacin, an inhibitor of prostaglandin synthesis, was studied with different study protocols by Jordan et al. (1998) in 35 patients with nOH of diverse etiologies. Indomethacin (50 mg) elicited a profound pressor effect. In the same study, no significant difference compared to placebo could be demonstrated for ibuprofen, caffeine and methylphenidate (Jordan et al. 1998).
The effect of the vasopressin analog, desmopressin (2–4 μg, intramuscular administration), on nocturnal polyuria was measured in a small cohort of five patients with autonomic failure. Desmopressin reduced nocturnal polyuria and prevented early morning orthostatic BP fall, but also increased supine BP (Mathias et al. 1986). Similarly, Sakakibara et al. (2003) showed that intranasal desmopressin reduced nocturia in three patients with MSA; in this study no hypertension was observed (Sakakibara et al. 2003).
Quality of evidence The quality of evidence for the following compounds to reduce nOH is very low: indomethacin, ibuprofen, caffeine, methylphenidate and desmopressin.
Safety issues Based on limited data, safety issues remain unclear.
Recommendation Recommendation for indomethacin, ibuprofen, caffeine, methylphenidate and desmopressin for treatment of nOH is weak.
Acarbose decreases release of vasodilatory gastrointestinal hormones through inhibition of α-glucosidase in the small intestine (Shibao et al. 2007b).
The effect of acarbose in treatment of postprandial hypotension has been evaluated in two randomized placebo-controlled trials in patients with PAF or PD (Shibao et al. 2007b) and patients with type 2 diabetes mellitus (Madden et al. 2015).
Acarbose (50–100 mg) was shown to significantly improve postprandial systolic BP fall compared to placebo. Limitation of these studies included a small sample size (n = 9–15) and short-term use (single administration) of acarbose.
Favorable effects were also demonstrated in an open-label study in patients with MSA (n = 14) (Fukushima et al. 2013) and case reports (type 1 diabetes mellitus) (Maule et al. 2004) (type 2 diabetes mellitus) (Yamamoto et al. 2006; Sasaki et al. 2001).
Voglibose, another α-glucosidase inhibitor, inhibited postprandial hypotension in a small-sized study (n = 11) with pre-post design in MSA, PD, diabetes mellitus and elderly patients (Maruta et al. 2006).
Quality of evidence The quality of evidence for acarbose to reduce postprandial BP fall is moderate, for voglibose is very low.
Safety issues Most frequent adverse events include gastrointestinal symptoms (e.g. flatulence, diarrhea, stomachache), which have been reported in a meta-analysis, where α-glucosidase inhibitors were administered in patients with type 2 diabetes mellitus for glycemic control (Van de Laar et al. 2005). In abovementioned studies, hypoglycemia was not reported either in patients with or without diabetes mellitus
Recommendation In consideration of quality of evidence, efficacy and safety profile, acarbose is strongly recommended to improve postprandial hypotension in patients with autonomic failure. Based on quality of evidence, the recommendation is weak for voglibose.
Octreotide, a somatostatin analog, combats postprandial hypotension by reducing postprandial splanchnic hyperemia induced by gastrointestinal vasodilatory peptides (Raimbach et al. 1989).
Three randomized controlled trials (Hoeldtke et al. 1986a, 1989a, 1998) have been conducted in patients with autonomic failure (mainly due to PAF, MSA or diabetes mellitus) investigating the effect of octreotide in a dosage ranging from 0.1 to 0.6 μ/kg/day on postprandial hypotension. Although these studies were limited by a small sample size (n = 8–16), a favorable effect of the somatostatin analogue was shown in the short-term.
Hoeldtke et al. (1986a, 1989a, b, 1998) demonstrated in all three studies that somatostatin prevented postprandial BP fall. These findings were replicated in further interventional studies with open-label design (Raimbach et al. 1989; Alam et al. 1995; Armstrong and Mathias 1991) and one case report (Hoeldtke et al. 1986b).
Quality of evidence Based on available data, the quality of evidence for octreotide to reduce postprandial BP fall is moderate.
Safety issues Side effects include gastrointestinal symptoms, in particular nausea and cramps, facial flushing and hyperglycemia. For this reason, use of octreotide is not recommended in patients with diabetes mellitus, especially in case of concomitant gastroparesis diabeticorum. Supine hypertension has been also reported.
Recommendation In consideration of moderate quality of evidence, efficacy and safety profile, recommendation is strong for octreotide to treat postprandial hypotension in patients with autonomic failure, with the exception of diabetes mellitus.
Caffeine inhibits adenosine-induced splanchnic vasodilatation and should therefore diminish BP fall after food ingestion (Onrot et al. 1985).
The effect of caffeine on postprandial hypotension has been evaluated only in one small-sized randomized controlled trial (n = 5) in patients with autonomic failure (diabetes mellitus, PAF, autonomic neuropathy due to alcoholism). Patients were treated with either caffeine 250 mg, subcutaneous dihydroergotamine (10μg/kg), a combination of both or placebo: whereas combination of treatments prevented patients from postprandial hypotension, monotherapy improved postprandial BP fall only partially (Hoeldtke et al. 1989b).
Onrot et al. (1985) further studied the effect of caffeine in a dosage of 250 mg in a small cohort (n = 6) of patients with autonomic failure. In this study, which did not include a placebo arm, caffeine showed a favorable single-dose effect on postprandial hypotension, which was maintained after 7-day administration (Onrot et al. 1985).
Quality of evidence Based on available literature, quality of evidence for caffeine to treat postprandial hypotension is very low.
Safety issues No side effects reported.
Recommendation Based on very low quality of evidence, the recommendation for treating post-prandial hypotension with caffeine is weak.
Remarks on classification of evidence
Tables 1, 2, 3 summarize reviewed studies for non-pharmacological and pharmacological management of nOH and post-prandial hypotension, while Table 4 provides an overview of quality of evidence, recommendation and safety issues.
Three main aspects penalize the quality of evidence for therapeutic interventions: first, studies are mostly small-sized and include populations of patients with nOH of different etiologies, which limits information on safety and efficacy in single diseases; second, for some non-pharmacological interventions (e.g., water, meal size, nocturnal head-up tilting, physical countermaneuvers) it is not possible to achieve a placebo-controlled study design; third, replication in larger placebo-controlled randomized clinical trials are often missing for those pharmacological measures, which showed positive results in pilot studies—such lack of data mirrors the challenges of running clinical trials in orphan diseases, where multi-center, adequately powered studies are hindered by limited commercial interest (Kaufmann et al. 2015).
Approach to nOH and post-prandial hypotension in clinical practice
Cornerstone of therapy includes both non-pharmacological and pharmacological measures applied in a stepwise manner.
Non-pharmacological treatment options remain pivotal for the treatment of autonomic failure (see Table 5). With exception of abdominal binders (high quality of evidence, strong recommendation) the quality of evidence for all other non-pharmacological interventions is low to very low, and recommendation therefore weak. However, given the favorable safety profile of non-pharmacological interventions, patients should be advised and motivated to apply such strategies on a regular basis. Conservative interventions include adequate fluid (1.5–2 l/day) and salt (6–10 g/day) intake (Biaggioni 2014), as well as abdominal binders, alone or in combination with compression stockings to reduce venous pooling. Bolus ingestion of 500 ml water may diminish BP fall in the following 30 min, and can be therefore purposely applied by the patient based on planned activities. Patients should be advised to stand up slowly and to perform physical countermaneuvers (leg crossing, squat position, bending forward) in case of dizziness. Sleeping in a head-up tilt position should be recommended to prevent supine hypertension and reduce nocturnal pressure natriuresis (Fanciulli et al. 2016b). Patients should be also educated to avoid trigger factors such as alcohol, heat exposure and large carbohydrate- or fat-rich meals and be aware that Valsalva-like maneuvers (e.g., micturition and defecation) may precipitate hypotensive episodes.
When aforementioned measures have been implemented and do not provide satisfactory relief, pharmacological therapy is required in addition. Pharmacological options are summarized in Table 6. As a general rule, drug choice should be tailored on the basis of expected benefit, relevant comorbidities, and potential adverse events. In younger, mobile patients, one may treat nOH more vigorously to warrant autonomy and symptoms’ control in daily life. To the contrary, treatment of nOH may be less relevant than limiting polypharmacy in older, wheel-chair bound patients.
At present only midodrine and droxidopa (the latter in the US and Japan only) have been approved for treatment of nOH, while the remaining substances are prescribed in an off-label regimen.
Based on available literature, the quality of evidence is high and recommendation level is strong for midodrine. Starting dose is 2.5 mg two to three times a day, which can be increased up to 10 mg 3 times a day. Midodrine can be administered in mono- or combined therapy with plasma volume expanders, such as fludrocortisone (Lahrmann et al. 2006). Use of midodrine is contraindicated in patients with severe cardiac disease, renal failure and urinary retention (McClellan et al. 1998).
Quality of evidence is moderate for droxidopa and the level of recommendation strong. Droxidopa should be initiated with a dosage of 100 mg three times a day and could be titrated up to a maximum dosage of 600 mg three times a day (Ricci et al. 2015). Notably, long-term data on safety and efficacy of droxidopa are still missing, limiting its use as first line therapy in clinical practice.
Fludrocortisone (quality of evidence very low, weak recommendation strength) can be considered as second-line agent, either as monotherapy (0.1–0.2 mg daily) or in combination with midodrine, if supine hypertension has been excluded (Freeman 2008). Importantly, fludrocortisone is contraindicated in patients with heart failure, kidney failure and hypertension (Ricci et al. 2015) and electrolyte monitoring is recommended to rule out hypokalemia.
Atomoxetine (18 mg, single dose) showed promising results in recent studies and may be considered in selected patients with refractory nOH, proven they have no cerebrovascular or cardiac comorbidities and are not on treatment with monoamine oxidase inhibitors. Data on long-term efficacy and safety are missing for atomoxetine, determining a low quality of evidence and a weak recommendation level.
Quality of evidence is very low and recommendation weak for ephedrine (25–50 mg three times a day) (Freeman 2008). Erythropoietin in combination with iron supplementation may have a positive impact on symptoms of nOH, especially in anemic patients, but risk of supine hypertension and polycythemia have to be considered (Kaufmann et al. 2015; Freeman 2008). For pyridostigmine, yohimbine, ergotamine, dihydroergotamine, ephedra alkaloids, desmopressin, indomethacin and fluoxetine the quality of evidence is very low, for octreotide low. Based on inconsistent results implications for clinical practice for all these treatment options remain investigational and therefore, recommendations are weak. Considering individual risk–benefit ratio, abovementioned supplementary agents might be evaluated in selected cases.
It has to be emphasized that, although anti-hypotensive agents are frequently prescribed in combination in clinical practice, there is little evidence on this approach, especially regarding long-term benefits and safety.
Hypertensive BP fluctuations in the supine position are a common problem in patients with cardiovascular autonomic failure and limit management of nOH. Patients taking any anti-hypotensive medication should be educated to avoid the recumbent position during daytime (Friedrich et al. 2010) and sleep with a head-up position overnight (Ten Harkel et al. 1992). All anti-hypotensive agents should not be taken < 4 h before bedtime and BP in the supine position should be monitored regularly.
In severe postprandial hypotension with limited response to conservative management (avoidance of large fat- or carbohydrate-rich meals and alcohol, increase in fluid and salt intake), acarbose in a dosage of 100 mg can be used in selected cases (quality of evidence is moderate, recommendation strong). Alternatively, subcutaneous octreotide (quality of evidence moderate, recommendation strong, 1 μg/kg) may be helpful (Wenning et al. 2005). Octreotide is contraindicated in patients with diabetes mellitus, given the risk of causing post-prandial hyperglycemia.
Although the quality of evidence is low and recommendation weak, caffeine in a dosage of 250 mg may be considered as further alternative, given its favorable safety profile.
The target of nOH management is improvement of patient’s quality of life by warranting mobility and preventing injurious falls due to syncope and pre-syncope. Although nOH has a high prevalence in the aging population, evidence-based data are limited. The mainstay of clinical management is, therefore, an individually tailored therapy, based on both non-pharmacological and pharmacological measures, which needs to be regularly evaluated and adapted over time, especially if the case of dynamic clinical scenarios, like in neurodegenerative diseases.
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A correction to this article is available online at https://doi.org/10.1007/s00702-017-1814-8.
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Eschlböck, S., Wenning, G. & Fanciulli, A. Evidence-based treatment of neurogenic orthostatic hypotension and related symptoms. J Neural Transm 124, 1567–1605 (2017). https://doi.org/10.1007/s00702-017-1791-y
- Neurogenic orthostatic hypotension
- Postprandial hypotension
- Evidence-based treatment