Chemical remodeling of the mycomembrane with chain-truncated lipids sensitizes mycobacteria to rifampicin

利用链截短脂质对分枝杆菌膜进行化学重塑,可使分枝杆菌对利福平敏感。

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Abstract

The outer mycomembrane of Mycobacterium tuberculosis and related pathogens is a robust permeability barrier that protects against antibiotic treatment. Here, we demonstrate that synthetic analogues of the mycomembrane biosynthetic precursor trehalose monomycolate bearing truncated lipid chains increase permeability of Mycobacterium smegmatis cells and sensitize them to treatment with the first-line anti-tubercular drug rifampicin. The reported strategy may be useful for enhancing entry of drugs and other molecules to mycobacterial cells, and represents a new way to study mycomembrane structure and function.

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