EBV III: HERV's, Treatment Studies, Summary - A Laymen's Guide
by Cort Johnson (Oct 09)
Since EBV reactivation commonly occurs in healthy people but
rarely produces symptoms a finding of EBV reactivation is not necessarily a
cause for alarm. But could EBV reactivation be more likely to cause harm in ME/ CFS
patients than others?
Some researchers suggest that while many of the pathogens found in ME/
CFS patients do not cause ME/
CFS they may make its underlying problems worse. A recent
study indicates EBV could possibly accelerate disease pathology in some people
by activating retroviral elements in our DNA
(Sutkowski et. al. 2004). It turns
out that a significant portion of our
DNA (up to 8%) is composed of old degraded
and mutated retroviruses that have managed to insert themselves into our genome.
Although most are inactive some may not be…… Could the EBV reactivation present
in some chronic fatigue syndrome (ME/
CFS) patient’s be turning on the retroviral elements in
their DNA?
The EBV/Endogenous Retrovirus (HERV) Connection?
The Sutkowski study found that EBV produces proteins
which are able
to reactivate a portion of a human endogenous retrovirus K18 (HERV-K18) that
produces a ‘superantigen’. Superantigens are proteins produced by viruses or bacteria that are able, by
binding to a certain spot on T-cells, to provoke unusually large T-cell
responses. The herpesvirus family is one of three viral families (hesperviridae,
retroviridae, rhadboviridae) able to produce superantigens.
Dr. De Meirleir has suggested that
the RNase L fragmentation and immune system activation in
CFS could be due to HERV activation.
Since the proteins (LMP-2A, LMP-1) that activate the superantigen are
associated with EBV’s latent phase they are presumably, since EBV is in the body
for life, always present. This was a laboratory study – we don’t know under what
conditions EBV is able to do this is the body – but it presents the potential
for a great deal of immune disruption. .
Since the HHV-6 herpesvirus is also able to reactivate EBV one could envision
the following chain reaction; HHV-6 reactivates EBV which reactivates HERV
(which causes T/NK cell suppression, immune dysfunction, etc. Some researchers
believe an undiagnosed HHV-6A infection could cause many of the problems in CFS.
Dig Deeper! The Pathogens in
CFS, Part I -HHV-6
As yet here is no evidence it is happening in ME/ CFS.
We should know more about HERV-K18 and CFS
pretty soon – both the NIH and the CFIDS Association of America are funding
studies examining HERV – K18 activity in ME/ CFS
Treatment Studies
Treatment studies and reports provide the most convincing evidence that
EBV infection plays a significant role for at least some chronic fatigue syndrome patients.
The Epstein Barr Virus Pages
An antiviral therapy trial that resulted in much decreased symptoms and
increased energy and improved ventricular functioning for about 2/3rds of ME/
CFS patients at 18 months suggests an EBV associated cardiomyopathy may be
important
in some patients (Lerner et. al. 2002a).
A 2007 study
by Dr. Lerner found that long-term use of Valacyclovir (> 1year) in EBV positive patients
resulted in reduced EBV VCA IgM antibodies, significantly improved
heart functioning (sinus tachycardias,abnormal cardiac wall motion) and progressive improvement functioning overall. Dr. Lerner reported that
'patients resumed normal activities'.
A small 2006 valganciclovir study of patients with increased IgG titers to EBV and HHV-6
found that nine of 12 patients with severe long-term disability returned to normal functioning.
A follow-up larger trial - which has not been published - did not have markedly
positive effects. The trial has reportedly been extended to 12 months to determine if
longer antiviral treatment will show results. Several doctors including Dr. Peterson and Dr. Lerner
have indicated that long-term antiviral treatments are often necessary to show significant
results.
A recent study may explain why long time antiviral therapy may be
necessary (Hoshino 2009). It found that Valacyclovir reduces cell to cell
reinfection but does not effect EBV infected cells. Since cell to cell
reinfection is the chief means EBV has of maintaining itself in the body very
long term antiviral therapy could reduce EBV infection rates simply by allowing
infected B cells to die off over time without being replaced.
Rituximab and EBV
A 2009 case study featuring an B-cell depleting anticancer drug
called methotrexate stirred the EBV pot considerably (Fluge and Mella 2009). A
chronic fatigue syndrome patient had developed severe fatigue, headaches, sleep
disturbances, concentration problems, and severe muscle and skin pain. etc.
after coming down with infectious mononucleosis 10 years earlier. Following
chemotherapy for Hodgkin's lymphoma she unexpectedly demonstrated a significant
improvement from her chronic fatigue syndrome symptoms. For four to five months
she was able to walk for long distances pain free, etc.after which her pain and
symptoms gradually recurred. Stem cell therapy successfully treated me
recurrence of the Hodgkins lymphoma but did not positively affect her chronic
fatigue syndrome symptoms.
She and two other ME/CFS patients with infectious mononucleosis
onset were later treated with the B-cell depleting drug Rituximab. Interestingly
none of the patients tested positive for active EBV infection using standard
serological or PCR techniques. All had high IgG titers and zero IgM titers.
Two experienced dramatic improvement six weeks (and one 26
weeks) after a single Rituximab injection after which their symptoms slowly
returned. Follow up injections produced a similar result. The authors of the
study postulated that reduced antibody or auto-antibody production was
responsible for their improvements - suggesting that ME/CFS may have an
autoimmune component that is possibly driven by a chronic B-cell infection (eg
EBV or another virus). No problematic side effects were reported. The
authors are reportedly engaging in further studies.
The Rituximab case study suggests a possible duo treatment regime
for post infectious mononucleosis ME/CFS patients.
Summary
It
appears that we are not nearly done examining EBV’s role in
ME/ CFS. The Dubbo studies (and others) have indicated that about 10% of
patients with infectious mononucleosis come down with ME/CFS. Why this happens
is still unclear but may have to do with a slightly slower immune response that
enables EBV to strike more quickly and virulently.
The
Dubbo researchers believe the initial EBV infection is resolved but others
disagree.
Both Dr. Glaser and Dr. Lerner believe that the immune system is able to
stop EBV replication but is unable to shut it down completely. Dr. Glaser believes
the chronic production of enzymes produced early in EBV’s life cycle triggers an
immune response that is the symptoms present in ME/
CFS. Dr. Lerner believes a chronic herpesvirus infection is
damaging the hearts of a subset of"ME/CFS patients.
Dr. Lerner's treatment trials suggest long term antiviral therapy may be very
helpful for a subset of patients. A small but successful trial of the
B-cell depleting drug Rituximab in infectious mononucleosis onset ME/CFS
patients potentially adds an intriguing tool to physician toolkit's.
EBV may be well adapted to
attack ME/CFS patients. Several studies indicate that ME/ CFS patients often experience increased stress levels prior to their
becoming ill, and EBV targets a part of the immune system (B lymphocytes) that
are activated during periods of chronic stress. EBV also appears adapted to
thrive during a pronounced Th2 cytokine (anti-inflammatory) response which
some researchers believe is prevalent in chronic fatigue syndrome.
The ongoing Dubbo studies, an NIH funded study by Dr. Taylor, Dr. Montoya’s and Dr. Lerner’s
research and the exciting Rituximab study should keep the EBV/ME/
CFS interaction in the news.
Dig Deeper! Diagnosing EBV
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.
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