Guest guest Posted April 29, 2005 Report Share Posted April 29, 2005 I'm pretty sure, tho not certain, that no virus can infect both prokaryotes and eukaryotes. The 3-d tissue model is cool, but can it reflect whats really up in the body, where immunity is partly endocrinely and neurally marshalled? And I dont think you can have the adaptive branch of the immune system really working in that model... can you? Antimicrobial efficacy is another matter - I dont remember it doing so, but does that model show failure of antimicrobials? That would be fascinating. This paper illustrated that endothelial cells, as well as fibroblasts, were able to protect Bb from ceftriaxone and also penicillin - but doxy and erythromycin still killed well: http://www.pubmedcentral.nih.gov/picrender.fcgi?artid=163368 & blobtype=pdf I have a sort of intuitive suspicion that the blebs/gemmae probably contain the whole genome and are viable. But theres no " good " reason they should resist amx drugs. I dont know much about the privaleged site ideas. Tho there arent really answers about its immunoevasion, theres more deep study out there on syphilis than I thought, it just takes alot of time to find it. PMID 6191721 is a case report, finding that many spirochetes and " a large amount of diffuse indistinct fluorescent " material were present in an immunofluorescent-stained lesion apparantly representing tertiary syphilis - interesting because tertiary syphilis has a lyme-like reputation for extreme paucity of organisms. This biopsy was negative by silver staining, which could call into question the precision of histologic findings in both lyme and syphilis using silver stains. The latter are not all the same, but most of them seem to have pretty shabby specificity. Probably the craziest thing about syphilis is the incubations of 10, 20, 30 years before tertiary syphilis becomes symptomatic. <jenbooks13@h...> wrote: > Very good thinking. > To make a cyst the spirochete literally curls up on itself. I can't > imagine it is impermeable as you said or how would it maintain > itself? I do imagine the granules, seen in the 50's when syphilis > shook itself and all kinds of seeds or spores shook loose, could be > almost inert--comlpletely dormant. The cyst doesn't have obvious > antigens. How could it make you sick? Only if it were active, or > shedding blebs (fake pieces that have antigens to make you sick), but > it has never been described that way, more as a kind of semi dormant > form that degrades over time but if properly stimulated can produce > daughter spirochetes. > > That 3-D work at the NIH showed massive #'s of spirochetes. I think > its an active infection with active spirochetes actively causing > illness but they are indeed in protected niches that antibiotics > can't release, or else there's something else going on if > bioweaponized, maybe viruses live inside them and are released when > they die, who knows. Quote Link to comment Share on other sites More sharing options...
Guest guest Posted April 29, 2005 Report Share Posted April 29, 2005 ERic, just curious why do you use " amx " for antibiotics? I guess we should go with horses not zebras. Thus I think active infection is responsible for symptoms. Thus we have to find novel approaches to kill it, or stop it. One easy way is to stop its ability to adhere to cells. Then over time, the infection will wane and die out. So maybe those glyconutrients are one possibility, so let me know. Another possibility is to get something into the cell that kills it. That's how ICHT worked--within the actual cell itself, shedding heat, and making the antibiotics far more effective. As I said, I'm working on a product--or rather, got some companies to work on one, we'll see if it works, if it does, that would be great but I'm assuming tho the idea is good that something will not work about it in vivo. (Hope for the best, expect the worst) Quote Link to comment Share on other sites More sharing options...
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