pISSN 1738-6586   eISSN 2005-5013
Open Access, Peer-reviewed
    J Clin Neurol. 2013 Jan;9(1):1-8. English.
    Published online Jan 03, 2013.
    https://doi.org/10.3988/jcn.2013.9.1.1
    Copyright © 2013 Korean Neurological Association
    Review

    Autonomic Function Tests: Some Clinical Applications

    Phillip A. Low,a Victoria A. Tomalia,a and Ki-Jong Parkb
      • aDepartment of Neurology, Mayo Clinic, Rochester, MN, USA.
      • bDepartment of Neurology, Gyeongsang Institute of Health Science, School of Medicine, Gyeongsang National University, Jinju, Korea.
    • Correspondence: Phillip A. Low, MD. Department of Neurology, Mayo Clinic, 200 First Street SW Rochester, MN 55905, USA. Tel +1-507-284-3375, Fax +1-507-284-3133, Email: low@mayo.edu
    Received September 11, 2012; Revised September 28, 2012; Accepted September 28, 2012.

    This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

    Abstract

    Modern autonomic function tests can non-invasively evaluate the severity and distribution of autonomic failure. They have sufficient sensitivity to detect even subclinical dysautonomia. Standard laboratory testing evaluates cardiovagal, sudomotor and adrenergic autonomic functions. Cardiovagal function is typically evaluated by testing heart rate response to deep breathing at a defined rate and to the Valsalva maneuver. Sudomotor function can be evaluated with the quantitative sudomotor axon reflex test and the thermoregulatory sweat test. Adrenergic function is evaluated by the blood pressure and heart rate responses to the Valsalva maneuver and to head-up tilt. Tests are useful in defining the presence of autonomic failure, their natural history, and response to treatment. They can also define patterns of dysautonomia that are useful in helping the clinician diagnose certain autonomic conditions. For example, the tests are useful in the diagnosis of the autonomic neuropathies and distal small fiber neuropathy. The autonomic neuropathies (such as those due to diabetes or amyloidosis) are characterized by severe generalized autonomic failure. Distal small fiber neuropathy is characterized by an absence of autonomic failure except for distal sudomotor failure. Selective autonomic failure (which only one system is affected) can be diagnosed by autonomic testing. An example is chronic idiopathic anhidrosis, where only sudomotor function is affected. Among the synucleinopathies, autonomic function tests can distinguish Parkinson's disease (PD) from multiple system atrophy (MSA). There is a gradation of autonomic failure. PD is characterized by mild autonomic failure and a length-dependent pattern of sudomotor involvement. MSA and pure autonomic failure have severe generalized autonomic failure while DLB is intermediate.

    Keywords
    cardiovagal; sudomotor; adrenergic; dysautonomia

    Introduction

    The autonomic nervous system regulates such important functions as blood pressure (BP), heart rate, thermoregulation, respiration, gastrointestinal, bladder, and sexual function. Autonomic dysfunction can occur as a result of many diseases that affect autonomic pathways. The clinician's role is to seek out symptoms of dysautonomia, but it is then necessary to determine if these symptoms are really due to involvement of autonomic systems. In the past, methods to evaluate autonomic function has been unavailable or too invasive. Recent advances in technology and the development/selection of autonomic function tests have resulted in the availability of quantitative, non-invasive, and reproducible tests and have made autonomic function testing accessible to the clinician. The focus of this review is to briefly describe a number of tests that are available to the clinician and how they might help in clinical situations.

    Autonomic Function Tests

    The goals of autonomic function tests are summarized in Table 1. In clinical terms, they help the clinician diagnose the presence of dysautonomia, its distribution and severity, and since they are quantitative, whether it is getting better or worse. Goal #1 is to evaluate the severity and distribution of sudomotor, cardiovagal, and adrenergic function using non-invasive quantitative tests (described below). Goal #2 is to diagnose limited or restricted autonomic failure. When autonomic testing first began, the goal was to diagnose generalized autonomic failure alone. With increasing sophistication, we can now diagnose dysautonomia confined to a single system or area. One example is distal small fiber neuropathy (DSFN), where unmyelinated fibers to the toes and feet are affected, causing loss of sweating and pain. Another example is chronic idiopathic anhidrosis,1 where widespread sudomotor failure occurs and adrenergic and cardiovagal functions remain intact. Goal #3 is to diagnose and evaluate orthostatic intolerance. Head-up tilt (HUT) will allow the laboratory to diagnose orthostatic hypotension (OH). It now is recognized that more subtle alterations, such as the postural tachycardia syndrome (POTS), can be diagnosed on HUT by an excessive heart rate response. Goal #4 is to monitor the course of dysautonomia. The laboratory permits the clinician to quantitatively determine if the condition is getting better or worse and the rate of change. For instance, the rate of change is quite slow in Parkinson's disease and much more rapid in multiple system atrophy (MSA). Goal #5 is to monitor response to treatment either clinically or in research (Goal #6). Autonomic testing is very useful when incorporated into clinical trials. It is possible to provide a quantity of autonomic failure and determine whether treatment is making this number get better or worse. We have used this approach in evaluating if IVIG will work in treatment of autoimmune autonomic ganglionopathy.

    Table 1
    Clinical goals in the evaluation of autonomic function

    Tests of sudomotor function

    The tests are summarized in Table 2, the system evaluated, neural pathways involved, and clinical interpretation. We provide here a brief description of each test.

    Table 2
    Tests of autonomic function

    Quantitative sudomotor axon reflex test (QSART)

    QSART evaluates the functional integrity of the postganglionic sympathetic sudomotor axon. Acetylcholine is iontophoresed into the skin, activating axon terminal. Impulses travel along the postganglionic sudomotor axon, initially antidromically, reaching a branch point, then orthodromically (hence an axon reflex) to release acetylcholine at nerve terminal, releasing acetylcholine, which activates muscarinic receptors on eccrine sweat gland.2 The resulting sweat response is recorded routinely from four sites (forearm, proximal leg, distal leg, and foot). The results are then interpreted by comparison with normative data derived from studies on 223 healthy subjects aged 10-83 years.3

    Thermoregulatory sweat test (TST)

    The TST is a test where sweating is induced by thermoregulatory warming resulting in a rise of core temperature. Sweating occurs when core temperature exceeds thermoregulatory set point at the hypothalamus. This tests the intactness of thermoregulatory sympathetic pathways from the hypothalamus to eventually the eccrine sweat gland. Therefore, this is a test of lesions anywhere from the hypothalamus to the sweat gland. An unclothed subject lies supine and his or her exposed body surface is covered with an indicator powder mixture.4, 5 The body is warmed to a core temperature of 38℃; sweat is recognized by a change in color in the indicator. The sweat distribution is documented by digital photography. The sweat pattern provides a pattern of intact sweating and of anhidrosis. Some patterns are highly characteristic, for instance of neuropathy, ganglionopathy, or of generalized autonomic failure. The digital images are processed by a pixel counter to derive an accumulative value for the area and percentage of anhidrosis. The percent anhidrosis has provided a useful number to follow quantitatively the course of an autonomic disorder.

    Tests of cardiovagal function

    Cardiovagal function can be evaluated by a number of methods. In the time domain, the commonly used and most reliable approach is to quantify heart rate response to deep breathing and to the Valsalva maneuver. The subject breathes at 6 breaths per minute and the magnitude of heart rate variation (maximal heart rate minus minimum heart rate) is averaged and provides an index of cardiovagal function. There are a number of alternative approaches, including mean circular resultant.6

    The Valsalva ratio is derived from the maximum heart rate generated by the Valsalva maneuver divided by the lowest heart rate occurring within 30 seconds of the peak heart rate.2, 4, 7 Our studies suggest that 40 mm Hg for a duration of 15 seconds should be used as the standard since it has yielded the most reproducible results.8

    Cardiovagal function can also be quantified in the frequency domain. Spectral analysis of resting heart rate produces several peaks. The highest frequency peak (>0.15 Hz) reflects oscillations of heart rate due to respiratory sinus arrhythmia and is considered to be a measure of cardiovagal function.6

    Tests of adrenergic function

    1. BP and heart rate responses to the Valsalva maneuver

    2. Head-up tilt study

    3. Plasma norepinephrine

    4. MIBG, cardiac uptake

    The evaluation of adrenergic function, specifically the vagal and adrenergic components of the baroreflex, can be made by studying dynamic alterations during the Valsalva maneuver.9 There are four main phases in the Valsalva maneuver (Fig. 1). Phase I is a transient rise in BP due to the act of blowing. Early phase II is due to reduced preload (venous return). The baroreflex then results in efferent sympathetic discharge to muscle resulting in a rise in BP. This sustained rise in BP is interrupted by a transient fall in BP, phase III, which like phase I, is mechanical, lasting 1-2 seconds, during which BP falls (because the subject stops the maneuver). This rise in BP is described as phase II_L, BP recovery following phase III and phase IV, reflects the increase in total peripheral resistance (Fig. 1A). Evaluation of the baroreflex can be done non-invasively from the Valsalva maneuver. The vagal component of the baroreflex is evaluated by relating the beat-to-beat BP during phase II_E to the heart period (reciprocal of heart rate) providing baroreflex sensitivity in msec/mm Hg.10 The adrenergic component of the baroreflex can be evaluated by BP recovery time (PRT), which is the time (in seconds) that the BP takes to recover from phase III to baseline.11 Fig. 1B is a Valsalva maneuver from a patient with diabetic autonomic neuropathy. Note that, in contrast with a normal response (IA), heart rate response to the fall in BP (phase II_E) is blunted (indicating impaired vagal baroreflex function). Adrenergic baroreflex function is markedly impaired. This is manifested by the absence of either II_L and IV (absence of reflex vasoconstriction) and prolonged PRT.

    Fig. 1
    Valsalva maneuver from a normal subject (A) and a patient with diabetic autonomic neuropathy (B). The heart rate and beat-to-beat blood pressure responses to the Valsalva maneuver are shown. Expiratory pressure is shown at the bottom. The phases of the Valsalva maneuver (I, II_E, II_L, III, IV) are indicated in the Fig. 1A. Autonomic neuropathy with adrenergic failure is manifested as a loss of phases II_L and IV and delayed blood pressure recovery. Impairment of the vagal component of the baroreflex is manifested as blunting of heart rate response to changes in blood pressure.

    HUT complements the beat-to-beat BP responses to the Valsalva maneuver. HUT provides an evaluation of the BP and heart rate response to tilt. A normal response consists of a modest rise in heart rate (by 5-20 bpm) and BP remains relatively constant (modest fall in systolic BP by <10 mm Hg and modest diastolic rise). HUT is done to detect if OH is present. Fig. 2 are examples of HUT showing a normal response (Fig. 2A), neurogenic OH (Fig. 2B), POTS in Fig. 2C, and syncope (Fig. 2D). In Fig. 2B, there is a marked fall in BP with a blunted heart rate response, typical of neurogenic OH. This was recorded in a patient with MSA. Fig. 2C is a recording from a patient with POTS, showing orthostatic tachycardia without OH. Heart rate increment is >30 bpm and eventually exceeds 120 bpm. Fig. 2D shows a patient with vasodepressor syncope. To HUT (first mark) there was a transient increase in BP (sympathetic surge) followed by abrupt fall in BP.

    Fig. 2
    Head-up tilt (HUT) responses in a normal subject (A), neurogenic OH (B), POTS (C), and syncope (D). Neurogenic OH is manifested as a pronounced fall in blood pressure (BP) with a blunted heart rate (HR) response. POTS (C) is manifested as an exaggerated HR response without OH. D shows vasodepressor syncope manifested as an abrupt fall in BP. OH: orthostatic hypotension, POTS: postural tachycardia syndrome.

    Plasma norepinephrine measured with the subject supine and after a period of standing provides another method of studying adrenergic function.12 A normal response consists of doubling of NE on standing. The patient with generalized postganglionic adrenergic failure, as in pure autonomic failure (PAF), will have low supine NE. The patient with preganglionic lesion, as in MSA, will typically have normal supine values (since the postganglionic fibers are intact) but a failure to increment on standing.13

    The quantitative uptake of the radiopharmaceutical [123I]MIBG (iodine-123 meta-iodobenzylguanidine), a norepinephrine analog, can be measured by single photon emission computed tomography. A newer approach, using 6-[18F]fluorodopamine positron-emission tomography and neurochemical analyses provide better resolution. These approaches provide an index of the functional integrity of presynaptic postganglionic adrenergic sympathetic terminals in the heart. Cardiac adrenergic imaging is reduced in a postganglionic lesion as in PAF or PD and is usually normal in MSA, although not invariably.14

    Applications of Autonomic Testing

    The Mayo Autonomic Laboratory was established in 1983. It now performs autonomic studies on over 4000 patients per year. A number of applications have been well-documented and have stood the test of time. We shall summarize examples of such applications.

    Distal small fiber neuropathy

    One of the most common and distressing neurologic complaints is DSFN. The patient complains of a burning sensation in their feet, especially toes and plantar aspect of their feet. There is typically troublesome allodynia, where a non painful stimulus elicits pain. Sensory examination may demonstrate a loss of sharp/dull or temperature perception at the toes. Motor function is usually normal. Common causes are diabetic and inherited neuropathy, but the most common cause is idiopathic. Nerve conduction studies are often normal since this is a small fiber and not large fiber neuropathy. This condition causes a length-dependent involvement of unmyelinated fibers, both somatic and autonomic. Sympathetic sudomotor fibers are affected, so that QSART will show abnormalities at the feet and normal sweating more proximally (Table 3) in about 3 out of 4 patients tested. Similarly, the thermoregulatory sweat test shows anhidrosis that is confined to the distal feet. Skin biopsy and evaluation of intraepidermal fiber density on the same subjects and the same sites have been studied prospectively in patients with autonomic neuropathy.15 Both skin biopsy and QSART will accurately diagnose DSFN but their agreement is imperfect, since they measure different populations of unmyelinated fibers.15 QSART is also helpful in following the natural history of DSFN and to determine if the neuropathy remains confined or becomes generalized. This capability is of importance since neuropathies due to diabetes or amyloidosis can start with DSFN and progress, while others do not. It is often difficult to make this determination with clinical examination alone. Table 3 provides a summary of experience with autonomic function tests in DSFN. Either TST of QSART will detect distal denervation in >70% of cases and together show an abnormality in 9/10 cases. As expected, adrenergic and cardiovagal abnormalities are less common. EMG is normal in >70% of cases.

    Table 3
    Comparison of current study with earlier studies33

    Generalized autonomic failure

    Physicians have learnt to recognize symptoms of autonomic failure. These include orthostatic lightheadedness, syncope, erectile dysfunction, and symptoms suggestive of neurogenic bladder and bowel. However, it is not possible to quantitate the severity and distribution of such abnormalities to help the physician determine if the patient is getting better or getting worse or if they are responding to therapy. With the availability of autonomic testing, it is possible to determine if generalized autonomic failure is present. Generalized autonomic failure refers to autonomic failure that is diffuse (multiple regions) and involves more than one autonomic system. Examples of generalized autonomic failure are the autonomic neuropathies16 and multiple system atrophy. Examples of autonomic neuropathies are diabetic autonomic neuropathy, amyloid neuropathy,17 and autoimmune autonomic ganglionopathy.18 In severe diabetic autonomic neuropathy,19 there is widespread loss of sweating, cardiovagal failure is present, and OH with impaired baroreflexes is seen. In the synucleinopathies (Parkinson's disease, multiple system atrophy, Lewy body dementia), generalized autonomic failure tends to be present in MSA, mild in PD, and intermediate in DLB.20

    Typically, for a comprehensive evaluation of autonomic function, we undertake an autonomic reflex screen and thermoregulatory sweat test as a routine. We often measure norepinephrine supine and standing to determine if supine values are reduced (indicating widespread postganglionic adrenergic denervation) and if an orthostatic increment (doubling) occurs. We will typically do additional studies to seek a cause. These include fat aspirate or nerve biopsy for amyloidosis17 or an antibody panel seeking especially for presence of ganglionic antibody.21 Detailed descriptions are available for a comprehensive coverage.12

    Selective autonomic failure

    The astute clinician can suspect that autonomic failure may be restricted rather than generalized. This suspicion can be confirmed and quantified with autonomic testing. Autonomic tests can confirm that a specific autonomic function is affected and that other systems are intact. We provide 3 examples. A patient, aged 30 years, feels hot, weak, dizzy and uncomfortable when ambient temperature rises. BP supine and standing is normal. He looks hot and flushed but has dry skin. Orthostatic BP recording is normal without evidence of OH. The clinician may suspect this is restricted autonomic failure but testing is necessary. Autonomic testing demonstrates normal cardiovagal and adrenergic function. However, QSART and TST show global anhidrosis. This is a condition called chronic idiopathic anhidrosis.1 Another example is a patient with gastroparesis. This patient has postprandial bloating and weight loss. He vomits up food that is 3 days old. Autonomic testing shows normal sudomotor and adrenergic function. Gastric transit studies show marked delay in gastric transit. A third patient has Adies pupils. Tests can be done to confirm the entity, but autonomic testing is needed to demonstrate that the deficits are confined and not generalized.

    The synucleinopathies

    The term synucleinopathies is used to describe several neurodegenerative disorders characterized by fibrillary aggregates of alpha-synuclein protein in oligodendroglia (in MSA) and in selective population of neurons. These disorders include Parkinson's disease (PD), dementia with Lewy bodies (DLB), PAF, and MSA. Although it is recognized that autonomic failure, manifest as erectile dysfunction, neurogenic bladder, constipation, and OH occur in the synucleinopathies, there has been little emphasis on the use of autonomic function tests in the differential diagnosis of these conditions. Based on our research on the involvement of autonomic structures in brain and spinal cord, we hypothesized that the severity and distribution of autonomic failure was different among synucleinopathies.

    PD and MSA share clinical features of hypomimia, hypertonia, dysarthria, micrographia, and gait impairment. PD is more likely associated with rest tremor and is typically levodopa-responsive. However, MSA can also have rest tremor and levodopa responsiveness, albeit less robust.22 Recent studies indicate that MSA is distinguishable from PD using autonomic tests. PD is characterized by a length-dependent involvement of postganglionic sudomotor fibers, whereas MSA is characterized by widespread, early and preganglionic autonomic failure.23 MIBG or fluorodopa scan of the heart, which images postganglionic adrenergic innervation, is typically defective in PD and normal in MSA.13, 14 However, denervation can occur in 25-30% of MSA patients.14 Another useful test is the TST. TST is either normal or shows very distal anhidrosis, typically affecting the toes (Fig. 3). In Fig. 3, the PD case showed very distal anhidrosis, affecting only parts of the toes, and did not progress over time. In contrast, MSA causes widespread anhidrosis.23 If both QSART and TST are performed, normal QSART volume in an anhidrotic region indicates that the lesion is preganglionic in site (Fig. 3). When the autonomic reflex screen is performed and the aggregate score, the composite autonomic severity score (CASS) calculated, CASS separates MSA from PD with sensitivity and specificity. The autonomic and clinical characteristics of the synucleinopathies are distinctive (Table 4). PAF is characterized by severe OH, without clinical central involvement. Supine plasma norepinephrine is often markedly reduced and CASS is >6 and TST% >40%. PD is associated with normal NE, CASS <6, and TST% <40%. MSA is characterized by CASS >6 and TST% >40%. DLB has intermediate autonomic failure.

    Fig. 3
    Thermoregulatory sweat test (TST) showing characteristic patterns in the synucleinopathies. In Parkinson's disease (top panel), anhidrosis is distal and percent anhidrosis remained <5%. In contrast, in multiple system atrophy (MSA), anhidrosis is regional and percent anhidrosis is greater and progressed more rapidly.

    Table 4
    Autonomic scores in the synucleinopathies

    Orthostatic intolerance

    Orthostatic intolerance refers to the development of symptoms after assuming the standing posture that clears on sitting or lying back down. Typical symptoms are lightheadedness, blurred vision, cognitive difficulties, or tiredness. Some patients also have symptoms of sympathetic activation, such as tremulousness and palpitations. In the category of orthostatic intolerance, we consider OH,9 postural tachycardia syndrome,24 and neurocardiogenic syncope (vasovagal and vasodepressor).25

    Orthostatic hypotension is defined as an orthostatic fall in SBP by >20 mm Hg,26 although in the laboratory, we have routinely required a fall of >30 mm Hg9, 27 and this latter criterion is more robust in the diagnosis of MSA.28 Orthostatic hypotension can occur in the absence of autonomic failure and the role of the laboratory is to determine if it is neurogenic; i.e., if autonomic reflexes, especially the baroreflexes are impaired. Typically in neurogenic OH, the fall in BP is associated with attenuated heart rate increment (Fig. 2B).

    POTS is defined as an increase on tilt of heart rate >30 bpm within 5 minutes in adults and associated with symptoms of orthostatic intolerance.24, 29 Autonomic laboratory testing is essential to make the diagnosis of POTS to demonstrate this heart rate increment and to rule out OH (Fig. 2C).

    Neurocardiogenic syncope typically occurs in subjects who have normal autonomic reflexes. The most common type is vasovagal syncope. There is a sudden fall in BP and heart rate. There is often an antecedent sympathetic surge as might occur in a subject who gets an injection or sees something unpleasant. Hence patients with POTS, who typically have an increased sympathetic tone, are excessively prone to vasovagal syncope. Vasodepressor syncope refers to an event where there is this fall in BP without an associated fall in heart rate (Fig. 2D). The autonomic laboratory will often capture syncope, although most autonomic laboratories do not attempt to provoke syncope.

    Concluding Thoughts

    Clinical management of the dysautonomias depends on good clinical acumen. The role of autonomic testing is to increase sensitivity and specificity in the detection of autonomic failure. The two work hand in glove and each enhances the other. There are limitations of clinical autonomic testing. The non-invasive approach is appropriate but imperfect. For instance, the beat-to-beat BP devices sometimes give erroneous signals, so that judgment is important in the interpretation of autonomic tests. Autonomic testing is a growing and evolving field so that guidelines will and should change over time.

    Notes

    The authors have no financial conflicts of interest.

    Acknowledgements

    This work was supported in part by National Institutes of Health (NS 44233 Pathogenesis and Diagnosis of Multiple System Atrophy, U54 NS065736 Autonomic Rare Disease Clinical Consortium), Mayo CTSA (UL1 TR000135), and Mayo Funds.

    The Autonomic Diseases Consortium is a part of the NIH Rare Diseases Clinical Research Network (RDCRN). Funding and/or programmatic support for this project has been provided by U54 NS065736 from the National Institute of Neurological Diseases and Stroke (NINDS) and the NIH Office of Rare Diseases Research (ORDR).

    The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institute of Neurological Disorders and Stroke or the National Institutes of Health.

    References

      1. Low PA, Fealey RD, Sheps SG, Su WP, Trautmann JC, Kuntz NL. Chronic idiopathic anhidrosis. Ann Neurol 1985;18:344–348.
      1. Low PA. Autonomic nervous system function. J Clin Neurophysiol 1993;10:14–27.
      1. Low PA, Denq JC, Opfer-Gehrking TL, Dyck PJ, O'Brien PC, Slezak JM. Effect of age and gender on sudomotor and cardiovagal function and blood pressure response to tilt in normal subjects. Muscle Nerve 1997;20:1561–1568.
      1. Low PA, Walsh JC, Huang CY, McLeod JG. The sympathetic nervous system in diabetic neuropathy. A clinical and pathological study. Brain 1975;98:341–356.
      1. Fealey RD, Low PA, Thomas JE. Thermoregulatory sweating abnormalities in diabetes mellitus. Mayo Clin Proc 1989;64:617–628.
      1. Freeman RL. Noninvasive evaluation of heart rate: time and frequency domains. In: Low PA, Benarroch EE, editors. Clinical Autonomic Disorders. 3rd ed. Philadelphia: Lippincott Williams & Wilkins; 2008. pp. 185-197.
      1. Low PA, Zimmerman BR, Dyck PJ. Comparison of distal sympathetic with vagal function in diabetic neuropathy. Muscle Nerve 1986;9:592–596.
      1. Benarroch EE, Opfer-Gehrking TL, Low PA. Use of the photoplethysmographic technique to analyze the Valsalva maneuver in normal man. Muscle Nerve 1991;14:1165–1172.
      1. Low PA, Singer W. Management of neurogenic orthostatic hypotension: an update. Lancet Neurol 2008;7:451–458.
      1. Schrezenmaier C, Singer W, Swift NM, Sletten D, Tanabe J, Low PA. Adrenergic and vagal baroreflex sensitivity in autonomic failure. Arch Neurol 2007;64:381–386.
      1. Vogel ER, Sandroni P, Low PA. Blood pressure recovery from Valsalva maneuver in patients with autonomic failure. Neurology 2005;65:1533–1537.
      1. Low PA, Sletten DM. Laboratory evaluation of autonomic failure. In: Low PA, Benarroch EE, editors. Clinical Autonomic Disorders. 3rd ed. Philadelphia: Lippincott Williams & Wilkins; 2008. pp. 130-163.
      1. Goldstein DS, Polinsky RJ, Garty M, Robertson D, Brown RT, Biaggioni I, et al. Patterns of plasma levels of catechols in neurogenic orthostatic hypotension. Ann Neurol 1989;26:558–563.
      1. Kimpinski K, Iodice V, Burton DD, Camilleri M, Mullan BP, Lipp A, et al. The role of autonomic testing in the differentiation of Parkinson's disease from multiple system atrophy. J Neurol Sci 2012;317:92–96.
      1. Singer W, Spies JM, McArthur J, Low J, Griffin JW, Nickander KK, et al. Prospective evaluation of somatic and autonomic small fibers in selected autonomic neuropathies. Neurology 2004;62:612–618.
      1. Low PA. Autonomic neuropathies. Curr Opin Neurol 2002;15:605–609.
      1. Wang AK, Fealey RD, Gehrking TL, Low PA. Patterns of neuropathy and autonomic failure in patients with amyloidosis. Mayo Clin Proc 2008;83:1226–1230.
      1. Klein CM, Vernino S, Lennon VA, Sandroni P, Fealey RD, Benrud-Larson L, et al. The spectrum of autoimmune autonomic neuropathies. Ann Neurol 2003;53:752–758.
      1. Low PA. Diabetic autonomic neuropathy. Semin Neurol 1996;16:143–151.
      1. Thaisetthawatkul P, Boeve BF, Benarroch EE, Sandroni P, Ferman TJ, Petersen R, et al. Autonomic dysfunction in dementia with Lewy bodies. Neurology 2004;62:1804–1809.
      1. Vernino S, Low PA, Fealey RD, Stewart JD, Farrugia G, Lennon VA. Autoantibodies to ganglionic acetylcholine receptors in autoimmune autonomic neuropathies. N Engl J Med 2000;343:847–855.
      1. Iodice V, Lipp A, Ahlskog JE, Sandroni P, Fealey RD, Parisi JE, et al. Autopsy confirmed multiple system atrophy cases: Mayo experience and role of autonomic function tests. J Neurol Neurosurg Psychiatry 2012;83:453–459.
      1. Lipp A, Sandroni P, Ahlskog JE, Fealey RD, Kimpinski K, Iodice V, et al. Prospective differentiation of multiple system atrophy from Parkinson disease, with and without autonomic failure. Arch Neurol 2009;66:742–750.
      1. Thieben MJ, Sandroni P, Sletten DM, Benrud-Larson LM, Fealey RD, Vernino S, et al. Postural orthostatic tachycardia syndrome: the Mayo clinic experience. Mayo Clin Proc 2007;82:308–313.
      1. Shen WK, Low PA, Rea RF, Lohse CM, Hodge DO, Hammill SC. Distinct hemodynamic profiles in patients with vasovagal syncope: a heterogeneous population. J Am Coll Cardiol 2000;35:1470–1477.
      1. The Consensus Committee of the American Autonomic Society and the American Academy of Neurology. Consensus statement on the definition of orthostatic hypotension, pure autonomic failure, and multiple system atrophy. Neurology 1996;46:1470.
      1. Schrezenmaier C, Gehrking JA, Hines SM, Low PA, Benrud-Larson LM, Sandroni P. Evaluation of orthostatic hypotension: relationship of a new self-report instrument to laboratory-based measures. Mayo Clin Proc 2005;80:330–334.
      1. Gilman S, Low PA, Quinn N, Albanese A, Ben-Shlomo Y, Fowler CJ, et al. Consensus statement on the diagnosis of multiple system atrophy. J Neurol Sci 1999;163:94–98.
      1. Schondorf R, Low PA. Idiopathic postural orthostatic tachycardia syndrome: an attenuated form of acute pandysautonomia? Neurology 1993;43:132–137.
      1. Stewart JD, Low PA, Fealey RD. Distal small fiber neuropathy: results of tests of sweating and autonomic cardiovascular reflexes. Muscle Nerve 1992;15:661–665.
      1. Tobin K, Giuliani MJ, Lacomis D. Comparison of different modalities for detection of small fiber neuropathy. Clin Neurophysiol 1999;110:1909–1912.
      1. Novak V, Freimer ML, Kissel JT, Sahenk Z, Periquet IM, Nash SM, et al. Autonomic impairment in painful neuropathy. Neurology 2001;56:861–868.
      1. Low VA, Sandroni P, Fealey RD, Low PA. Detection of small-fiber neuropathy by sudomotor testing. Muscle Nerve 2006;34:57–61.
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    MeSH Terms
    Axons
    Blood Pressure
    Heart Rate
    Hypohidrosis
    Multiple System Atrophy
    Natural History
    Parkinson Disease
    Primary Dysautonomias
    Pure Autonomic Failure
    Reflex
    Respiration
    Sweat
    Valsalva Maneuver
    Metrics
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