Lyme disease is caused by Borrelia burgdorferi and other
related species of Borrelia. “Lyme
disease” was coined by Steere in 1977. Microbiologist
Willie Burgdorfer discovered the germ in 1981 -- A thin, elongated spiral shaped
bacteria, or spirochete residing in the gut of ticks.
These bacteria are persistent and frequently cause chronic
disease. The belief that the bacteria
persist has been refuted by the IDSA for decades. The IDSA is wrong. The narrative oft repeated describing the
structure and function of the spirochete by those in my camp, is outdated and
incorrect.
This post is an effort to correct the record.
The following statements are wrong and I explain why.
#1 Lyme bacteria have 3 forms: spirochete, L-form and cyst form.
Lyme does not exist in an L-form. An L form is a cell wall deficient bacterium
derived from a bacterium that ordinarily has a cell wall. Lyme lacks a cell wall to begin with so this
is an impossibility. Lyme bacteria possess a double outer membrane and no cell
wall. Bacterial cysts do no occur. This
is a feature of protozoa. Lyme bacteria are pleomorphic with “phenotypic”
variation. These chameleons of the
bacterial world frequently present as a round bodied forms which are treatment
resistant. In summary: No L-forms, No true
cysts. Yes, spirochetes have shape shifting ability – pleomorphic variation,
commonly observed as round body forms, blebs and many others.
#2 Lyme bacteria persist in large measure because they hide
in cells (are intracellular).
Lyme bacteria primarily exist outside host cells
(extracellular). Intracellular forms
exist but are relatively uncommon. The bacteria adhere to a protein matrix
between cells. Primary mechanisms of
persistence are biofilm formation and pleomorphic variability. The spirochetes are anaerobic (do not require
oxygen) and therefore are able to live in tissues with a poor blood/oxygen
supply, e.g. joint cartilage. These bacteria easily cross the blood brain
barrier which is a safe-haven because immune responses are limited. The
bacteria may survive in other “immune privileged” areas. Intracellular
localization is a relatively minor means of immune evasion.
#3 Treatment must include: cell wall drugs (beta-lactams),
intracellular drugs and “cyst busters.”
Assuming we are talking about the bacterial cells (not host)
With Lyme spirochetes all antibiotics inhibit or kill Lyme
work via an intracellular mechanism. The
molecules that form the bacterial cell wall are called peptidoglycans. Borrelia spirochetes possess strands of peptidoglycans
internally, acting as an internal skeleton.
When beta-lactams kill Lyme, the action is inside the cells. The other
classes of antibiotics generally work inside the cells, disrupting DNA/RNA, metabolic pathways or
protein synthesis. If we are instead
referring to drugs which penetrate host cells, antibiotics from many classes
may penetrate host cells, including beta-lactams.
4# Flagyl is a cyst buster.
If one is referred to round forms of Lyme, Flagyl is no more effective (in a test tube) than doxycycline. Empiric evidence and clinical practice inform us that Flagyl is very effective and may be synergistic with other drugs.
If one is referred to round forms of Lyme, Flagyl is no more effective (in a test tube) than doxycycline. Empiric evidence and clinical practice inform us that Flagyl is very effective and may be synergistic with other drugs.
In summary: No L
forms. No cyst forms. No cyst busters. Ceftin, amoxicillin, others function as
intracellular antibiotics when used against Lyme.
Lyme spirochetes have a developed ability to persist in the
face of adversity. This phenomenon is
not unknown in the world of bacteriology. For example, tuberculosis. TB is treated with a 4-drug combination for 2
months and a 2-drug combination for another 2 months. This complicated formula is the results of
decades of research.
Lyme (chronic) has not had this sort of attention from the
medical community which maintains the persistent delusion the disease does not exist.
