There is a lot of confusion about biofilms and Lyme
disease. I have frequently heard from
patients that a “biofilm-buster” is needed. Biofilms consistent of colonies of
microorganisms who live within the confines of a protective membrane made of
mucopolysaccharides with odd pieces of DNA. These molecules are long chain
sugars. We know that biofilms provide a protective niche permitting the
survival of Lyme spirochetes and many other bacteria. Most of what we know
about biofilms is derived from in-vitro, test tube studies which focus on
surface infections, for example, diabetic wounds and cytstic fibrosis. Most of
this research has focused on Pseudomonas, a notoriously stubborn pathogen
associated with these diseases. We have precious little information about Lyme
biofilms.
Biofilms comprised of Pseudmonas aeruginosa have
experimentally been treated with a number of topical agents, like xylitol, with
some success. Ammons found that lactoferrin has biofilm activity for surface
Pseudomonas. How well does this translate? One mechanism of action is the
chelation of iron. While this may work with Pseudomonas it may not work with
Lyme (even topically), because these spirochetes use manganese in lieu of iron.
Other agents, like stevia, have had some success treating Lyme biofilm-like
colonies but these finding are from test tube studies and likely do not apply
to systemic infection.
Proteolytic enzymes have been widely touted as
‘biofilm-busters.” This has never made sense to me since biofilms do not
contain protein.
Yeast have biofilms. Cremer et al, current Antimicrobial
Agents Chemotherapy, screened 1600 drugs/agents and found that Artemisinins
were synergistic with miconazole for the treatment of Candida albicans biofilm
related infection. This synergy did not occur with several other anti-fungal
drugs studied. I am sure many readers have personal experience with stubborn
Candida biofilms on their tongues. This highlights the fact that drugs used for
a single purpose (artemisinin for Babesia) may help in unexpected ways (Candida).
The recent study from Hopkins about Lyme persisters and the
original studies of Sapi are at odds with one another. The Hopkins study lumps
cysts or round bodied forms together with biofilm-like colonies calling them
stationary phase bacteria. Sapi considers cyst or round body forms and biofilm
forms to be two separate entities. Hopkins reports that doxycycline,
amoxicillin and Flagyl have no effect on stationary forms. Sapi found amoxicillin
and Flagyl have anti-cyst effects and that Tindamax works well against cysts
and also kills spirochetes within biofilms. More study is needed.
An explanation of Tindamax’s greater effect against biofilms
may be due to disruption of quorum sensing: a process by which bacteria within
the biofilm communicate with each other by molecular signaling (very
complicated stuff). In Pseudomonas models a number of antibiotics have been
shown to interfere with quorum sensing and associated virulence factors.
Experimentally, these have included: Zithromax, Flagyl,
Tindamax and Cipro.
The take-away point is that the best biofilm-buster might be a specific antibiotic or combination of antibiotics.
Cyst forms, round body forms, L-forms, biofilms forms: now
we have a new buzz word to add to the list, quorum sensing (QS).
I think parsing ‘Lyme” into these parts and trying to tailor
therapy for each one is generally not helpful. These notions are helpful in a
general sense only; patients respond differently, unpredictably. Experience
remains our best teacher. Theory is no substitute for that which is tried and true.
what about eva sapi and atomic force microscopy?
ReplyDeletehere u can read dr. eva sapi's presentation from strasbourg conference (8 june 2014- conference ' Journées Internationales D’Information sur les Maladies Vectorielles à Tiques (JID’IMVT)'.
http://wlp-lyme.blogspot.ro/2014/10/provocari-clinice-ale-bolii-lyme.html
I am wondering if the enzymes you mention might actually be working on something else instead of biofilm. Since infections can cause hypercoagulation, possibly the fibrin and other components of this are the target instead?
ReplyDeleteNew Research on how nanobacteria cause calcification in tissues that prevents antibiotics and other treatments from working.
ReplyDeleteThis nanobacteria commonly called Bartonella infection is very hard to detect and can only be detected using advanced methods.
There is a newly developed method to overcome this nanobacteria calcification and once that is done treatments become much more effective.
Curing Lyme and Morgellons;
https://www.youtube.com/watch?v=spjzJEME6kI
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