Warning: this case is complicated and the medical stuff is hard to follow if you do not have a science or medical background.
I recently met a 50 year-old female who came into my office
in a wheelchair seeking help for Lyme disease. She had been under the care of
another “Lyme” doctor for 3 years. She suffered with a neurological disease
causing progressive weakness. The illness started more than 15 years ago but
has rapidly progressed over the last three years. Until 3 years ago she had
been a patient at Johns Hopkins. At this point she states that she had a bad
experience there, mostly within the department of neurology. Doctors had
bandied her about and been unable to diagnose her. She feels that no one ever
listed to her. According to various consulting physicians things did not fit
together in her case. One physician told her he had finally figured out what
was wrong with her: she had chronic fatigue syndrome and fibromyalgia! One of
her S, reluctantly, prescribed IVIG which she stopped 3 years ago because it
wasn’t helping.
For the past three years she had been under the care of a “Lyme
doctor” who had treated her with a steady diet of supplements and antibiotics
while her condition continued to worsen.
It is at this point she came to see me. Searching through
the morass of medical records from “the Johns” I found a copy of an EMG/NCV
performed several years ago. It showed a demyelinating peripheral neuropathy.
She additionally informed me that she had a small fiber biopsy which was abnormal
as well. Some of the puzzle pieces which did not fit together were: a diagnosis
of neutrally mediated hypotension per tilt table test without POTS and other evidence
of autoimmune disease. Of particular interest was the presence of elevated
anti-GAD antibodies. She recalled that several years ago she was prescribed
Klonopin which initially helped some of her symptoms but the effects were
not durable. At Hopkins a Lyme test (ELISA only) was negative and this
possibility was dismissed.
When she saw the Lyme doctor he ordered a test for Lyme from
IgeneX which showed a weak positive response with two positive, specific IgG
bands present. This was the sole basis for the Lyme diagnosis. When she took
antibiotics she frequently experienced chills, sweats and low grade fevers
followed by worsening of weakness which did not recover with continued therapy
or with cessation of therapy.
My examination showed an ill appearing female seated in a wheelchair.
She had a resting heart rate of 100 and a blood pressure of 150/80. (These
vital signs were “normal” for her). The examination was remarkable for some
muscle wasting in her upper extremities. Moderate weakness of both upper and
lower extremities was present. An absence of deep tendon reflexes globally was
present. The sensory exam was completely normal. The remainder of the
neurological exam and the general physical exam was within normal limits.
Lab findings: Lyme Western Blots were sent to two reference
laboratories, MDL and Stony Brook. The MDL strip showed a positive IgG 41 band
only. The Stony Brook test showed a few non-specific IgG and IgM bands. The remainder of the test series was positive
for an elevated anti-GAD antibody and otherwise unremarkable.
So what’s going on?
Discussion of case: This patient has a CIDP-like illness
affecting only motor neurons. The diagnosis may be something called multifocal motor
neuropathy. Features that favor the diagnosis are: demyelinating neuropathy,
progressive nature of illness and the absence of deep tendon reflexes. Lyme is
not the primary issue here. Lyme is known to cause primarily axonal neuropathy
although I have seen both types of neuropathy in patients with Lyme disease. Which
is which? Slowing with nerve conduction
testing (the shock test) shows axonal dysfunction and reduced amplitude of wave
on EMG (needle test) shows demyelinating neuropathy. CIDP is thought of as a
chronic form of Guillain-Barre syndrome and MMN (multifocal motor neuropathy)
is related to CIDP which stands for: chronic inflammatory demyelinating
polyneuropathy. Neutrally mediated hypotension is a disorder of the central
nervous system and should not be seen in any of these diseases which only
involved the peripheral nervous system. At any rate, the peripheral neuropathy
component is due to an autoimmune disease and IVIG is the appropriate
therapy. Lyme on another infection may
have incited the disease in someone with a genetic predisposition as is likely
in this case. It certainly sounds like this is the case as she experiences classic Herxheimer
reactions when she takes antibiotics. A worsening of symptoms in this scenario
sometimes called a neurological Herxheimer reaction. The inflammation which ensues when the
offending germs are killed causes a worsening of disease which does not improve even with cessation of therapy. In other words, the cure may be worse than the illness. The elevated anti-GAD antibodies is something
of a red herring; it is evidence of a second, unrelated, autoimmune disorder and
something which may respond to a different kind of therapy. Centrally mediated
hypertension is another red herring as noted above, but this finding makes sense within the
context of multisystem disease, especially Lyme disease.
Patient Lyme disease have weird symptoms and syndromes which
cannot easily be connected in a linear fashion.
Symptoms and syndromes which forgot to read the textbook followed by
academic specialist.
The presence of anti-GAD antibodies is something seen in
disorder called stiff man syndrome.
These antibodies block the GABAergic system and drugs like Klonopin are
the appropriate therapy.
One Lesson is: Do not be a hammer and see everything as a
nail. Another is: if a treatment is
making the patient worse, step back and take another look. If you are a Lyme
doctor you have to be an expert in everything. Other medical
specialists will not help since they do not believe in Lyme disease. Other physicians
will give up when everything does not fit together and seem to inevitably reach
into their bag of tricks and pull out the “go see a shrink” card. I have seen the same scenario unfurl repeatedly in multiple patients
whereas many neurologist are unfamiliar with the disorders. There are some knowledgeable
specialist who can be helpful out there – somewhere.
My recommendations: Do not take antibiotics at this time.
Restart IVIG and do not stop, consider the treatment as indefinite (then
consider antibiotic therapy) and start hyperbaric oxygen therapy and get a home
unit: this will be a very long term form of therapy. Other supplemental
therapies may be helpful but this is my core recommendation. I recommend the
patient start low doses of drugs like Klonopin and /or Neurontin which may also
help with neuropathy symptoms.
The idea that killing germs will fix everything is not only
wrong but may be detrimental as well.
Keep in mind that hyperbaric oxygen heals nerves and also kills germs. Herxheimer responses are likely to occur.
A repeat EMG/NCV is needed to determine disease progression and
other studies.
I think this patient will get better but it is going to take
some time.
dear Dr Jaller, i understand there will be many Lyme patients in this unenviable position soon. please could you keep us updated on the outcomes of the therapy you are doing with seronegative Lyme patients.
ReplyDeleteRegards
Fiona
Why do you think she did not respond to earlier IVIG treatment? ..."One of her S, reluctantly, prescribed IVIG which she stopped 3 years ago because it wasn’t helping. "
ReplyDeleteDid you take a vaccine history? I bet her symptoms started after a vaccine. This really looks like adult vaccine injury to me.
ReplyDeleteSpirochick i was thinking the same thing.
ReplyDeleteSpirochick i was thinking the same thing.
ReplyDeleteDr. Jaller, I see utmost logic in your recommendation to this patient. Her resting HR of 100 and hypertension indicate autonomic nervous system involvement, likely being affected by toxin release. I see perfectly well why you would not want another "hammer" (ABX) to go down on the proverbial "lyme nail" at this time. Klonopin and Gabapentin are great drug choices that would help settle the nervous system response. Of the two, Gabapentin (Neurontin) makes better sense as it has better effect on the quality of sleep where as klonazepam disrupts delta-wave in the brain which affects slow wave sleep making it a poorer choice.
ReplyDeleteGreat post, I enjoyed reading about this case - thank you!
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