EBV II: A Chronic Infection in Chronic Fatigue Syndrome (ME/CFS)? A Laymen's
Guide by Cort Johnson (Oct 09)
The idea that an undiagnosed EBV infection causes or contributes to CFS is controversial.
This type of argument – that inadequate diagnostic procedures prevent researchers
from identifying the pathogens causing or contributin
g to ME/CFS – is frequently made by advocates
of the idea that a chronic infectious state is present in CFS.
It may seem incongruous that researchers in the 21 century might have trouble
determining (a) the identity of a pathogen, and (b) it’s role in causing or contributing
to that illness but such questions can be amongst the most problematic that researchers
and physicians face. In multiple sclerosis, a disease whose locus has been clear,
researchers have been arguing for at least a decade if the damage is caused by a
pathogen and, if so, which one is responsible.
The EBV Chronic Fatigue Syndrome Subset
How many chronic fatigue syndrome patients might be affected by Epstein-Barr
virus activation? Unfortunately given the controversy over how to accurately diagnose
EBV activation and the few studies on the subject it's impossible to tell. Lerner's
finding that serum EBV VCA IgM positive antibody titers were identified in about
60% of 58 patients suggests a significant portion of patients could have EBV activation
(Lerner 2004). Lerner reported he's found two subsets
of ME/CFS patients who contain antibodies to non- structural EBV or HCMV epitopes.
(Lerner et. al. 2002, Lerner et al. 2004b). His findings were buttressed by a study
finding antibodies to non-structural EBV enzyme epitopes in some CFS patients (Glaser
et. al. 2005). The non-structural EBV epitope theory, however, is controversial
(see below).
Missing EBV in CFS?
Two research groups, one headed by the Ronald Glaser and one by Martin Lerner,
assert that the medical establishment has missed evidence of a chronic EBV infection
in ME/CFS patients. (See Appendix for CDC guidelines for diagnosing EBV infection).
Glaser believes that the immune systems of ME/CFS patients are, in fact, largely
effective at inhibiting EBV from replicating but that they are unable to shut it
down early in its life cycle. In this scenario EBV is active but not producing viruses
(virions); instead it’s producing proteins that trigger an immune response which
is causing the symptoms in the disease.
Glaser argues that since the traditional antibody tests measure antibodies produced
to antigens produced later in the infection that while they may catch signs of viral
replication they miss signs of early EBV activation.
Glaser believes that cytokines (IL-1, IL-6, TNF-a) produced in reaction to these
early proteins cause the ‘sickness behavior’ (i.e. lethargy, fatigue, etc.) we call
‘CFS’. He found that adding the dUTPase enzyme to immune cells called monocytes
(but not others) resulted in greatly increased levels of IL-1B, IL-6, 8, 10 and
TNF-a and increased NK cell activity.
The CFS Epstein Barr Virus Pages
Some evidence suggests that early EBV activation is common in individuals with poorly
functioning immune systems. Researchers have found antibodies to early EBV enzymes
in a number of immunosuppressive diseases including HIV. When mice infected with
another herpesvirus (CMV) were subjected to an immune stressor (TNF-a), they were
found to produce only early EBV proteins. This suggests that having multiple herpesvirus
infections could predispose one to early EBV enzyme production. A number of situations
appear then to put one at risk of early EBV activation.
It is not clear though that early activation is necessarily harmful. The CDC states
that patients who have successfully resolved an EBV infection can display high antibody
titers to early EBV antigens for years without being symptomatic.
The early EBV enzyme theory is not new - it’s simply a poorly studied one. Jones
and Glaser first found a relationship between CFS and antibodies to these enzymes
in 1988 (Jones et. al. 1988). A small 1991 study found an early viral protein,
DNase, was expressed in all six ME/CFS patients. A study by another laboratory in
1994 found antibodies to early EBV enzymes in ME/CFS patients (Natelson et. al.
1994). Glaser reported that recent data indicates a large number of ME/CFS patients
(41-83%) do test positive for antibodies to early EBV enzymes. Dr. Glaser recently
received a large NIH grant to study his theories further.
Unclear Cytokine Picture in ME/CFS - Dr. Glaser’s theory
purports that the cytokine cascade triggered by the early EBV enzymes is causing
the symptoms in chronic fatigue syndrome. The cytokine picture in ME/CFS is, however,
unclear. While some studies have provided evidence for increased levels of most
of the cytokines he believes play a role in CFS (Il-1B, IL-6, Il-10, TNF-a) others
have not. Two studies from the Dubbo project – which followed people who came down
with ME/ CFS after being infected with EBV (infectious mononucleosis) - found
no evidence of increased pro-inflammatory cytokines and a Fletcher/Klimas 2009 study
found little evidence of the kind of pro-inflammatory cytokine upregulation Dr.
Glaser proposes. None of these papers, however, have specifically focused on EBV
activated patients.
EBV in the Heart
Dr. Martin Lerner in Michigan has been investigating viral induced cardiac dysfunction
in ME/ CFS for over since 1989. In 1993 Lerner found abnormal T-wave oscillations
that appeared to indicate left ventricular dysfunction in ME/ CFS. MUGA tests
were abnormal in about 13% of patients (Lerner et. al. 1993). Resting ejection fractions
were usually normal but increasing the workload often resulted in what Dr. Lerner
called ‘gross ventricular dysfunction’. This lead Lerner to posit that the fatigue
in CFS is related to a ‘subtle’ cardiac dysfunction (Lerner et. al. 1993).
A larger study (n=87) found abnormal cardiac wall motion (AWCM) in 11% and 21% of
CFS patients with positive EBV tests at rest and under stress respectively. Cardiac
biopsies showed a cardiomyopathy was present in 3 patients (Lerner et. al. 2004).
While cardiac biopsies of 15 ME/CFS patients with high titers for the HCMV antibody
were negative for cytomegalovirus (HCMV) a morphological examination of their heart
tissues revealed heart fiber disarray, dissolution, ‘dropout’ and occasional hypertrophy.The
cardiac biopsies had to be stopped after some patients developed extensive bleeding.
Ultimately Lerner and his
group developed a theory similar to Dr. Glaser's that posits that immune
system breakdowns in ME/CFS lead to incomplete/complete herpesvirus (EBV/HCMV/HHV6)
multiplication in the hearts of ME/CFS patients. Lerner, like Glaser, points out
that viral studies rarely test for non-structural viral epitopes that can be released
during incomplete viral replication. He asserts these early viral gene products
interfer with cell metabolism weakening the heart and causing many of the symptoms
present in CFS.
Completely replicated viruses (virions) consist of a ‘capsid’ (which contains the
DNA) that is surrounded by a viral tegument (containing the factors necessary for
viral synthesis), which in turn, is surrounded by a viral coat (lipid bilayer).
The viral coat contains the proteins that are typically recognized by the immune
system. If viral replication is somehow thwarted in mid-step then proteins in the
capsid or tegument may be released that the immune system could be is poorly adapted
to deal with.
Could CFS patients be particularly vulnerable to EBV? The authors of the Dubbo studies
suggested a Th2 cytokine shift allowed the virus to strike faster and deeper in
ME/CFS patients. Glaser and others suggest that stress could be involved. Interestingly
there is a connection between stress, the Th2 cytokine response and EBV activity.
The EBV Stress Connection
Stress and EBV. Stress has long
been known to increase the risk of herpesvirus (EBV, HHV-6, CMV, etc.) reactivation
in humans. About ten studies have indicated that psychological stressors can reactivate
EBV. Poor academic performance in combination with high internal demands of perfection
was associated with an increased tendency of ‘seroconversion’ to EBV in
West Point
cadets. Stressors have also been shown to induce the production of the early
EBV proteins (enzymes) Dr. Glaser believes is present in chronic fatigue syndrome
(ME/CFS).
Seroconversion
occurs when antibodies to a virus can be detected in the blood stream. This means
the virus is active. After replicating inside cells the virion moves into the blood
stream to find new cells to infect.
Several studies have indicated chronic fatigue syndrome (ME/CFS)
patients have a higher than normal incidence of stressful events in the months preceding
their illness (White et. al. 2001). One study found that being female, having family
support (?) and having more stressful life events prior to having CFS was
associated with poor recovery from infectious mononucleosis (Buchwald et. al. 2000).
A recent study which suggested chronic fatigue syndrome (ME/CFS)
patients were more physically active than normal prior to their illness implicated
physical stress as a possible contributing factor.
This suggests that chronic stress may increase the risk for herpesvirus reactivation
and/or chronic fatigue syndrome (ME/CFS)
by impacting immune functioning. But how? The two stress response systems,
the autonomic nervous system and HPA axis, also regulate immune function. When these
systems are chronically activated they appear to thrust the immune system into an
a state of Th2 cytokine dominance; a situation we have seen EBV appears to be particularly
well adapted to and which some studies suggest is present in chronic fatigue syndrome
(ME/CFS). Thus chronic stress may be
able to produce an immune state which allows some viruses to proliferate.
Dig Deeper! See EBV Part III for
intriguing findings that suggest some ME/CFS patients are at high risk of EBV reactivation.
The Phoenix Rising website and most of the articles in it are created by a layman.
It is not a substitute for a physician and is for informational uses only.
REFERENCES
Glaser R, Padgett DA, Litsky ML, Baiocchi RA, Yang EV, Chen M, Yeh
PE, Klimas NG, Marshall GD, Whiteside T, Herberman R, Kiecolt-Glaser J, Williams
MV.. 2005. Stress-associated changes in the steady-state expression of latent
Epstein-Barr virus: implications for chronic fatigue syndrome and cancer. Brain
Behav Immun. 2005 Mar;19(2):91-103
Lerner AM, Beqaj SH, Deeter RG, Fitzgerald JT. 2002b. IgM serum antibodies
to human cytomegalovirus nonstructural gene products p52 and CM2(UL44 and UL57)
are uniquely present in a subset of patients with chronic fatigue syndrome. In Vivo.
2002 16 (3):153-9.
Lerner AM, Dworkin HJ, Sayyed T, Chang CH, Fitzgerald JT, Beqaj S, Deeter RG, Goldstein
J, Gottipolu P, O'Neill W. 2004a. Prevalence of abnormal cardiac wall motion
in the cardiomyopathy associated with incomplete multiplication of Epstein-Barr
Virus and/or cytomegalovirus in patients with chronic fatigue syndrome.In Vivo.
18(4):417-24
Lerner AM, Beqaj SH, Deeter RG, Fitzgerald JT., 2004b. IgM serum antibodies to Epstein-Barr
virus are uniquely present in a subset of patients with the chronic fatigue syndrome.
In Vivo. 2004 Mar-Apr;18(2):101-6.