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Experimental therapies of Mycobacterium abscessus infections
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Mycobacterium abscessus is a non-tuberculous mycobacteria notoriously known for causing severe, chronic infections. Treatment of these infections is challenging due to either intrinsic or acquired resistance of M. abscessus to multiple antibiotics. Despite prolonged poly-antimicrobial therapy, treatment of M. abscessus infections often fails, leading to progressive morbidity and eventual mortality. Great research efforts are invested in finding new therapeutic options for M. abscessus. Clofazimine and rifabutin are known anti-mycobacterial antibiotics, repurposed for use against M. abscessus. Novel antimicrobials active against M. abscessus include delamanid, pretomanid and PIPD1 and the recently approved beta-lactamase inhibitors avibactam, relebactam and vaborbactam. Previously unused antimicrobial combinations e.g. vancomycin-clarithromycin and dual beta-lactam therapy have been shown to have synergistic effect against M. abscessus in experimental models, suggesting their possible use in multiple-drug regimens. Finally, engineered phage therapy has been reported to be clinically successful in a severe case of disseminated M. abscessus infection. While many of these experimental therapeutics have shown activity against M. abscessus in vitro, as well as intracellular and/or animal models, most have little if any evidence of effect in humans infections. Clinical studies of M. abscesssus treatments are needed in order to reliably determine the value of their incorporation in therapeutic regimens.
Title: Experimental therapies of Mycobacterium abscessus infections
Description:
Mycobacterium abscessus is a non-tuberculous mycobacteria notoriously known for causing severe, chronic infections.
Treatment of these infections is challenging due to either intrinsic or acquired resistance of M.
abscessus to multiple antibiotics.
Despite prolonged poly-antimicrobial therapy, treatment of M.
abscessus infections often fails, leading to progressive morbidity and eventual mortality.
Great research efforts are invested in finding new therapeutic options for M.
abscessus.
Clofazimine and rifabutin are known anti-mycobacterial antibiotics, repurposed for use against M.
abscessus.
Novel antimicrobials active against M.
abscessus include delamanid, pretomanid and PIPD1 and the recently approved beta-lactamase inhibitors avibactam, relebactam and vaborbactam.
Previously unused antimicrobial combinations e.
g.
vancomycin-clarithromycin and dual beta-lactam therapy have been shown to have synergistic effect against M.
abscessus in experimental models, suggesting their possible use in multiple-drug regimens.
Finally, engineered phage therapy has been reported to be clinically successful in a severe case of disseminated M.
abscessus infection.
While many of these experimental therapeutics have shown activity against M.
abscessus in vitro, as well as intracellular and/or animal models, most have little if any evidence of effect in humans infections.
Clinical studies of M.
abscesssus treatments are needed in order to reliably determine the value of their incorporation in therapeutic regimens.
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