The Perils of Standing: Orthostatic Intolerance in Chronic Fatigue Syndrome (ME/CFS) II
- Types by Cort Johnson (Feb 2005)
New! Treating Orthostatic
Intolerance - Click here.
The
evidence indicates that many CFS patients display symptoms and laboratory
findings associated with orthostatic dysfunction. There are several
different kinds of orthostatic dysfunction. Stewart (2003a) reports that three
abnormal responses to tilt testing have been identified; vasovagal faint,
dysautonomia and postural tachycardia syndrome (POTS). The first two occur
in CFS but are not common. The orthostatic intolerance that is most commonly
occurring in CFS is called postural tachycardia syndrome or POTS.
Vasovagal faint or Neurocardiogenic
Syncope
– is a delayed response (7-20 minutes) to a TILT test that culminates in a
fainting episode.
Vasovagal faint appears to be the technical name for a
‘fainting spell’. In these patients peripheral vasoconstriction occurs
upon standing but slow decreases in vasoconstriction eventually result in a
precipitous fall in blood pressure and heart rate and a fainting spell. CFS
patients often faint during tilt tests but rarely do so otherwise.
Dysautonomia Induced Orthostatic Intolerance
- occurs when peripheral (i.e. outside the CNS) nerve failure or
central nerve atrophy results in rapidly reduced blood pressure
(systolic and diastolic) during the TILT test. Interestingly transient forms of dysautonomia induced OI can occur during infections or inflammatory
episodes. These patients typically experience other symptoms of dysautonomia
such as abnormal papillary activity, gastrointestinal symptoms and
sweating episodes. While tests indicate that some CFS patients do
exhibit a degree of autonomic instability they are not thought to
display this kind of braod sweeping dysautonomia (Stewart 2003a)
Postural Tachycardia Syndrome
(POTS) – While
the name is relatively new POTS has been referred in the medical literature
for many years. The many synonyms that still exist for POTS (a table lists
13 recent ones!) illustrates how fluid the field of orthostatic research is.
POTS is characterized by rapidly
increased heart beat upon standing caused by low blood flows to the heart.
The symptoms found in POTS appear to arise from decreased blood flows to the
brain, increased cerebrovascular resistance, and (an unexplained)
hyperventilation associated with low carbon dioxide levels.
Low blood pressure and high
resting heart beat can be persent. Low blood pressure (neurally mediated
hypotension (NMH) is not a requirement for POTS. The only overt autonomic
abnormality in POTS is increased heart beat upon standing.
Symptoms:
POTS symptoms are manifold; they include: dizziness,
lightheadedness, shortness of breath upon standing, fatigue, exercise
intolerance, frequent urination, headache, flu-like symptoms, tingling
and/or numbness in the extremities, poor sleep, abdominal discomfort,
irritable bowel syndrome, poor balance and coordination, visual disturbances
(floaters), allergies and chemical sensitivities, chest pain, neurocognitive
disorders, anxiety, palpitations (sound familiar?).
In contrast to those people who simply experience
fainting upon standing people with POTS are often disabled, and unable to
attend school or hold a job. POTS effects up to a million Americans.
A Window
Into Chronic Fatigue Syndrome (ME/CFS)?
– While OI has been a subject of interest in CFS since
1995, Rowe (2002) points out that as early as 1940 Maclean and Allen
suggested orthostatic tachycardia resulting from impaired venous blood flows
to the heart upon standing (i.e. POTS) contributed to diseases (effort
syndrome, neuro-circulatory asthenia, irritable heart) now believed to be
synonymous with CFS. They recommended two treatments (increased fluid and
sodium intake) now commonly prescribed in CFS.
Stewart states the clinical findings for the orthostatic
intolerance found in POTS and pediatric CFS patients show great similarity.
No other diseases have as great a symptom overlap with CFS as does POTS. One
research group believes some people with POTS have misdiagnosed as having
CFS. Almost all CFS patients with OI appear to have POTS and some POTS
patients have CFS. Both diseases often occur after an infectious event. As
with CFS the great majority of POTS sufferers are female. Stewart suggests
from 25-50% of CFS sufferers probably have POTS. He believes POTS could be a
milder form of CFS (Stewart 2000)
Some general differences have been noted. Children with
POTS usually have less severe symptoms and recover more quickly than those
with CFS. In addition while POTS can be debilitating, POTS appears not to be
as disabling as CFS. The similarities between the two diseases are
undoubtedly more important than their differences. Research into POTS will
surely spur insights into CFS and vice-versa.
Much of this enquiry into the nature of the orthostatic
dysfunction found in CFS will focus on findings from studies on POTS
patients.
Possible Causes
-
POTS was at first believed to originate in a
dysfunctional cardiac response to standing. In the 90’s Streeten turned this
idea by its head by arguing that the increased heartbeat was an appropriate
response to reduced heart blood flows caused by blood pooling in the
extremities. As heart blood volume dropped the heart beat was increased in
order to ensure sufficient blood flowed to the brain.. Reduced venous heart
flows of blood are now agreed to be the proximate cause of POTS.
The ultimate cause of the reduced cardiac blood flows is
unclear; two theories - low blood volume, blood pooling in the extremities -
both of which may be correct, have garnered most of the interest. The
outcome of increased blood pooling and low blood volume is similar; both
result in increased tachycardia (heart beat) that is sometimes followed by
low blood pressure or fainting or both on tilt.
Low Blood Volume.
In a small study in 1997 Jacob et al.
demonstrated that reduced blood volume was associated with low plasma renin
and a trend towards low aldosterone levels in about half the patients with
OI. In another very small study Streeten and Bell (1998) found CFS patients
demonstrated low red blood cell (RBC) mass but not low mean plasma or blood
volume levels. While mean plasma and blood volume were not significantly
different from controls the range of readings was very high; a subset of CFS
patients clearly did have reduced blood and/or plasma volume. Because
the RBC’s carry oxygen to the tissues and organs of the body Streeten and
Bell argued that low RBC mass and normal blood volume was analogous to have
normal RBC mass and low blood volume. In either case insufficient oxygen was
very likely reaching the brain.
Five possible causes for low blood
volume in CFS have been proposed; dyfunctional renin-angiotensin-aldosterone
system, increased sympathetic nervous system (SNS) activity, extracellular
alkalosis and deconditioning.
Renin converts angiotension into
its active form angiotensin II (see Glossary) which increases blood volume
by (a) inducing water retention in the proximal tubule of the kidney and (b)
by inducing sodium retention through the activation of aldosterone. Both
renin and aldosterone levels were low in Jacob’s study. This was highly
unexpected – renin and aldosterone levels are usually increased in
patients with low blood volume. Given the patients low blood volume it
sounds like even normal renin and aldosterone readings would have probably
been considered abnormal in these patients.
Aldosterone secretion can be
induced by angtiotensin II, potassium and ACTH. Since electrolyte levels
were normal, and ACTH is involved in acute rather than chronic conditions,
it appears low angiotensin levels are the source of the trend towards low
aldosterone in CFS. Jacob's speculated that autonomic denervation (reduced
nerve supply) of the kidneys could also cause reduced low renin production.
It is perhaps notable given the increased symptoms of POTS patients given
beta adrenoreceptor antagonists that the authors note that these agents
decrease plasma renin levels. Some of the symptoms patients taking
these drugs experienced may have been due to further eductions in blood
volume due to low renin levels.
Because a chronic state of
adrenergic activation (i.e. increased SNS activity) can either cause
low blood volume or low blood volume can cause increased SNS activity, it is
hard to tell which causes which (Stewart 2003a).
Dr. Cheney believes
low blood volume may be due to a compensatory response to extracellular
alkalosis (= intracellular acidosis) called ‘contraction alkalosis’. Reduced
blood volume results in less tissue perfusion which in turn increases blood
pH (alkalosis). Since this scenario suggests increasing blood volume would
interfere with this compensatory response it could explain why CFS patients
do not respond well to plasma volume enhancers such as fludrocortisone.
There is evidence for increased SNS activity in CFS. Low
blood volume can also be induced by deconditioning. In one study 15 days of
bed rest resulted in a 15% reduction in plasma volume (Kimberly and
Shoemaker 2002).
Prevalence in CFS
-
Research has demonstrated that low blood volume ‘almost certainly’ occurs in
a subset of CFS and POTS patients (Stewart 2003a). A trend toward low
blood volume is associated with reduced low VO2 max in CFS patients
(Farquhar et. al. 2002). (Other studies have shown that increased blood
volume is associated with increased endurance in healthy people (Hageberg
et.al. 1998). This, of course, suggests reduced blood volume could
contribute to the fatigue in CFS. Stewart (2003) argues, however,
that low blood volume cannot account for all the circulatory abnormalities
seen in CFS or POTS. In particular low blood volume cannot account for the
increased leg blood flows seen in some POTS patients.
Summary:
The extent, significance and cause of low blood volume in POTS and CFS
patients is unclear. We should be getting some answers ‘soon’, however.
Hurwitz has been engaged in a long term study of red blood cell mass and
blood volume in CFS patients. (See Ongoing Research in Part IV).
Blood Pooling.
Upon standing both CFS and POTS
patients display increased blood pooling in the legs (sometimes manifested
by swelling) that results in increased losses of blood from the upper body
and heart and thus the brain. As mentioned earlier the tachycardia seen in
POTS and CFS is believed to be a compensatory mechanism designed to combat
the low venous flows of blood into the heart during standing. The question
researchers are trying to answer is where does the blood go and why? Stewart
(2003) states that increased blood pooling could be due several factors:
This gets quite complicated.
- An autonomic neuropathy primarily
found in the legs could inhibit vasoconstrictive activity.
Autonomic neuropathy refers to reduced numbers of the nerves
that control blood flows in the legs.
- Similarly a beta receptor
hypersensitivity could cause increased blood vessel dilation in
the legs. Beta receptors cause the blood vessels in the legs
to dilate allowing more blood flow (i.e. pooling) in the veins.
- Altered venoconstriction could result
in increased blood flows in the veins.
- Increased capillary filtration resulting in fluid leakage
into the surrounding tissues could cause blood pooling (i.e.
'leaky' capillaries.)
Autonomic neuropathy (Warning - Extremely Complicated Section) -
The presence of hypersensitive alpha adrenergic nerve
receptors on the veins of some POTS patients suggests that autonomic
denervation (nerve loss) in the lower body is a cause of blood pooling.
Denervated arteries have thinner walls, are smaller and show greater
sensitivity to NE. Instead of clustering at the endpoints of muscles
denervated nerves tend to flow over them.
Apparently the receptors on the
remaining nerves attempt to ‘make up’ for the reduced nerve levels by
increasing their sensitivity. Alpha adrenoreceptors cause the arteries to
vasoconstrict. The cause of the possible nerve loss is unclear. Infections
can cause nerve damage. Autonomic neuropathies that cause orthostatic
intolerance (among other things) rise, for instance, due to reduced
immuno-vigilance during the progression of AIDS. Several researchers believe
CFS is a disease of reduced immuno-vigilance.
Increased sensitivity to phenylephrine – a vasoconstrictor, and
isopreterenol – a vasodilator, and resistance to tyramine - an agent
that enhances NE release, suggests noradrenergic neuronal dysfunction.
Noradrenergic refers to nerves that release noradrenaline,
i.e. norepinephrine (NE). Noradrenergic receptors are activated by NE. Since
NE is the principal vasoconstrictor these findings suggest reduced
vasoconstriction due to reduced NE release is occurring. Short term
improvements following administration of the alpha adrenoreceptor agonist
(enhancer) Midodrine also suggest impaired noradrenergic functioning (Jacob
et. al. 2000). Midodrine enhances norepinephrine release. Reduced NE
release upon tyramine administration suggests either decreased neuronal NE
stores or reduced NE release (Jacob et. al. 1999).
Reduced
NE Spillover - Reduced NE 'spillover' also
occurs. After NE is released from the neuron into the synapse much of it
is immediately taken up again. Some of it, however, always spills over into
the blood. By triggering NE release and then measuring NE blood levels
researchers are able to assess NE spillover. To further complicate
matters it turns out that OI patients also display reduced NE
clearance (reuptake). Since reduced NE
clearance should lead to increased NE spillover, this may suggest CFS
patients have really, really low NE spillover (?). It is intriguing that CFS
patients also appear to display reduced uptake of another neurotransmitter,
acetycholine, in the blood vessels of the skin.
Reduced NE spillover suggests one
of three scenarios is occurring; poor NE production or storage, impaired NE
release, or low blood volume. There is evidence for at least three of these
in CFS.
The
presence of hypersensitive adrenergic receptors, as noted above, suggest
autonomic denervation has occurred. Jacob has suggested that damage to the
nerve terminals in the legs could impair the NE reuptake mechanisms and
cause reduced NE clearance (Jacob et. al. 1999). Reduced nerve levels could
result in reduced NE spillover, reduced NE production or storage or impaired
NE release. Because of the reduced circulation it imposes, hypovolemia could
cause the reduced NE spillover. This appears to suggest that in states of
low blood volume there may not be enough blood reaching to the nerve
terminals to carry away normal amounts of NE? McGregor et. al. suggest
increased tyrosine excretions in CFS patients are the result of increased
catabolic activity in CFS. Since tyrosine is the precursor to NE, increased
tyrosine excretions could lead to decreased tyrosine availability and
reduced NE production (see Chap VII CFS ABA).
All of McGregor's amino acid findings have recently
been called into question, however (Chalmers et. al. 2005). This theory no
long appears viable. It appears that reduced spillover is due to both
autonomic denervation and low blood volume.
Another Conundrum
-
Interestingly, despite reduced NE release in response to tyramine OI
patients also display increased plasma NE levels. How to explain decreased
NE secretion and increased NE levels in the blood?
This appears to be due to different types of NE
release. Apparently the hyper alpha adrenoreceptor sensitivity but normal B2
adrenoreceptor sensitivity in OI patients suggests nerve damage in the lower
extremities has resulted in hypersensitive local nerve terminals while
normal humoral norepinephrine production leads to normal B2 receptor
activity. Thus OI patients appear to exhibit reduced local nerve functioning
but intact nerve functioning of the nerves served by the circulation. Jacob
believes this pattern is consistent either with a functional abnormality of
the sympathetic nerves or a disrupted ‘architecture’ of the nerve synapse in
OI patients (Jacob et. al. 2000).
Beta receptor
hypersensitivity
– Because beta adrenoreceptors dilate the blood vessels B AR
hypersensitivity could theoretically result in reduced vasoconstriction and
blood pooling. The importance of beta receptors in the skeletal muscles is,
however, controversial, and Stewart (2003a) discards this explanation. A
2002 study (Stewart and Weldon) which demonstrated that beta adrenoreceptor
blockers (beta blockers) increased the symptomology of POTS patients
argued against excessive beta adrenoreceptor activity in POTS.
Altered venoconstriction
– Stewart states there is little evidence that venoconstriction (as
opposed to arterial vasoconstriction) plays a role in the orthostatic
response anywhere in the body but the abdomen. Reduced venoconstriction may
play a role in the OI experienced by ‘normal-flow’ POTS patients. (See
below)
Increased capillary filtration – Streeten
believed reduced heart blood volume occurs when the peripheral arteries fail
to constrict enough to prevent bloodfrom pooling in the peripheral veins and
capillaries when standing (Streeten and Bell 1998). Since NE is the primary
vasoconstrictive agent in the peripheral arteries the reduced NE ‘spillover’
in the peripheral arteries seen in POTS patients buttresses Streeten’s
theory of reduced arterial vasoconstriction.
In the last five years Stewart has engaged in a series
of studies that indicate a variety of vascular problems in the extremities
lead to the excessive blood pooling in POTS (Stewart 2000, Stewart et. al.
2002, Stewart 2003a). These vascular problems appear to be the greatest
contributor to the orthostatic dysfunction seen in CFS. Of course it’s never
as simple as that…
THE (DREADED) SUBSETS
Any discussion of the cause of the
blood pooling seen in POTS and CFS patients is complicated by the subsets
Stewart has found in a series of studies of adolescent POTS patients.
Reading Stewart’s latest paper (2004) is like Yogi Berra said ‘Déjà vu all
over again". Once upon a time POTS (and CFS) appeared like a homogeneous
disorder. Although the origin was a mystery at least it was a single
mystery. Ongoing research, however, has indicated the presence of not one or
two and but now three distinct subsets of POTS patients; two of which have
opposite laboratory findings (!). This is obviously quite complicated.
Stewart states all three subsets are found in CFS. The subsets consist of
- Hi-flow POTS patients
– have high blood flows, low arterial resistance
(vasoconstriction) and normal to decreased peripheral venous pressure in
the extremities.
- Low-flow POTS patients
– have low blood flows, increased
arterial resistance and increased peripheral venous pressure in the
extremities (and probably low blood volume).
- Normal flow POTS
– have normal blood flows and arterial resistance but disrupted arterial
and/or venoconstriction in the abdomen.
Hi-flow POTS
– These patients display reduced peripheral arteriole vasoconstriction (a
relative peripheral vasodilation) in combination with increased
microvasculature (capillary) filtration. Thus reduced blood vessel
vasoconstriction results in increased peripheral blood flows and increased
blood volume in the capillaries. The increased capillary filtration does
not, interestingly, appear to be effected by posture – the vasoconstrictive
defects present in these patients are present all the time – they are
simply accentuated by standing. These patients are designated ‘hi-flow’
because they exhibit higher than normal flows of blood in their lower
extremities.
These patients also display
decreased releases of the catecholamine (norepinephrine) responsible for
constricting the arteries. The current theory regarding these patients
posits they have a ‘long axon’ neuropathy that interferes with NE production
in the lower extremities (Stewart 2004). A neuropathy is a disease of the
nerves. These patients appear to have very positive responses to alpha
adrenergic receptor enhancers. Alpha adrenoreceptors cause the smooth
muscles of blood vessels to vasoconstrict. The authors do not speculate
what may be causing this ‘disease’ but do note that many things, including
infection, can cause neuropathies. Stewart (2004) reports that hi-flow POTS
patients often experience infectious events just prior to getting POTS.
Low-flow POTS
– Low flow POTS patients are the most difficult to explain. They exhibit
defective local blood flow regulation, increased peripheral resistance
(vasoconstriction), decreased vein area and probably reduced blood volume of
some degree (Stewart and Montgomery 2004). Thus low-flow POTS patients have
reduced levels of blood to start with plus increased resistance to blood
flow in their legs (and in contrast to hi-flow POTS their arms) and
decreased vein capacity to boot. In contrast to hi-flow POTS patients who
have increased blood flows in their microvasculature, low-flow POTS patients
appear to have reduced microvasculature blood flows. The reduced peripheral
vein capacity seen suggests that either a ‘venous remodeling’ or a
persistent vasoconstriction has taken place. In spite of their reduced
peripheral blood flows, low flow POTS patients still exhibit reduced heart
blood flows during standing.
Stewart suggests their reduced
vein capacity (remodeling) could be due to reduced blood volume. A
laymen like myself could see low blood volume resulting in increased
vasoconstriction (to maintain blood pressure) and reduced heart blood flows
but Stewart does not believe low blood volume is responsible for the
vascular abnormalities in these patients. Stewart believes the main
problem in these patients is not due to damaged nerves due but to a dysfunction
in the small blood vessels in the legs. Some evidence suggests that these
local receptors are responsible for as much as 45% of the orthostatic
response.
Poor Muscle Pump Activity
- As if low-flow POTS patients didn’t have enough problems, a recent study
(Stewart et. al. 2004) found that they exhibit abnormalities in muscle pump
activity as well. The ‘muscle pump’- a major part of the orthostatic
response – consists of a series of very small involuntary muscle
contractions that propel blood upwards during standing.
Since skeletal muscle integrity is dependent upon proper
flows of blood and low-flow POTS patients display low peripheral flows of
blood Stewart examined low-flow POTS patients to determine if they displayed
reduced muscle mass and therefore muscle pump activity (Stewart et. al.
2004). Not only did low-flow POTS patients exhibit reduced muscle pump
activity but that they also had decreased muscle mass and venous capacity.
The authors speculated low-flow POTS patients could be immersed in vicious
circle (reduced muscle pump activity = reduced blood flow = reduced muscle
mass = reduced muscle pump activity, etc.) leading to progressively lower
and lower muscle pump activity. Since neither sedentary people nor those
with congestive heart failure nor other types of POTS patients display
decreased muscle pump activity, it does not appear to be the result of
deconditioning.
Local blood vessel dysfunction
- While the phenomena of local
vasoconstriction is a rich field of study, just how blood vessel walls
initiate vasoconstriction in response to increased pressure is unknown.
As noted
earlier local blood vessels respond to the increased blood pressure caused
by blood pooling by constricting. This vasoconstriction stops blood from
pooling in the capillaries and veins. It appears that in low blood flow POTS
patients these blood vessels are too constricted. This, of course,
inhibits blood flow to the veins (venous remodeling), reduced muscle mass
and muscle pump activity.
The
abnormalities in calf blood flow seen in low-flow POTS patients appear to
originate in defects in the myogenic response or the
venoarteriolar response. The myogenic response occurs when the smooth
muscles constrict the arteries in response to increased blood pressure.
Calcium channel activity is believed to play a key role in the myogenic
response. The venoarteriolar response is believed to occur when
increased blood volume in the small veins triggers stretch receptors to
constrict the arterioles upstream of that vein. As blood begins to pool
in the veins and enlarge them the stretch receptors activate causing the
arterioles at the head of the veins to constrict.
A large number of local vasoactive
agents could effect local blood flow regulation. They include
-
endothelial vasoactive
products – NO, PG1-2, endothelin, EDHF
-
metabolites – adenosine, Ca2+, CO2, H+ ions, lactate
-
autacoids – histamine,
bradykinin, 5-HT (serotonin), PAF, prostaglandins
-
local neurogenic mechanisms
such as the axon reflex
-
neurogenic inflammation – CGRP, substance P
Endothelial
agents with vasodilatory properties such
as nitric oxide, histamine and acetylcholine appear to be responsible for
the venoarteriolar response. These two responses have been held to be
distinct but a recent report indicates that NO, a venoarteriolar agent, is
able to modify the myogenic response by altering the sensitivity of the Ca
receptors on smooth muscles.
These
patients often display acrocyanosis – mottled looking blue and pink skin in
the lower extremities - and the skin is generally cool to the touch. These
are both due to reduced peripheral flows of blood. They also often exhibit
pallor.
Summary:
Overactive
local myogenic or venoarteriolar responses and/or low blood volume in the
low-flow POTS patients appear to cause either increased vasoconstriction in
the periphery and/or a venous remodeling that results in reduced vein area
in the lower extremities. Disrupted local blood flows could be due to
impaired calcium channel functioning (myogenic) or improper endothelial cell
functioning. While increased peripheral vasoconstriction is accompanied by
reduced blood volume, low blood volume is unlikely to account for all the
abnormalities found in low-flow POTS patients.
Normal-flow
POTS patients
– display normal peripheral blood flows but impaired
vasoconstriction and blood pooling in the abdominal (splanchnic) area.
Whether the impaired vasoconstriction is due to reduced veno or arteriole
constriction is unknown. Either a partial dysautonomia (i.e. limited to the
abdomen) or a local regulatory dysfunction is likely responsible.
Summary:
these studies suggest several subsets of POTS
exist in CFS. Depending on which subset is involved, the central factors
appear to be nerve damage (long-axon neuropathy – hi-flow POTS); local blood
flow constrictions due to a disruption in the small blood vessels (low-flow
POTS), low blood volume (low-flow POTS) and impaired vasoconstriction in the
abdominal area (normal-flow POTS). At this point, therefore, both nervous
system and vascular components to the orthostatic dysfunctions found in CFS
patients. Aside from infection in hi-flow POTS patients there is little
speculation as to the ultimate cause of these disruption.
To Part Three - The Source of POTS?