Mode of Action of Kanglemycin A, an Ansamycin Natural Product that Is Active against Rifampicin-Resistant Mycobacterium tuberculosis

康格霉素A(一种对利福平耐药结核分枝杆菌有效的安沙霉素天然产物)的作用机制

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作者:Hamed Mosaei ,Vadim Molodtsov ,Bernhard Kepplinger ,John Harbottle ,Christopher William Moon ,Rose Elizabeth Jeeves ,Lucia Ceccaroni ,Yeonoh Shin ,Stephanie Morton-Laing ,Emma Claire Louise Marrs ,Corinne Wills ,William Clegg ,Yulia Yuzenkova ,John David Perry ,Joanna Bacon ,Jeff Errington ,Nicholas Edward Ellis Allenby ,Michael John Hall ,Katsuhiko S Murakami ,Nikolay Zenkin

Abstract

Antibiotic-resistant bacterial pathogens pose an urgent healthcare threat, prompting a demand for new medicines. We report the mode of action of the natural ansamycin antibiotic kanglemycin A (KglA). KglA binds bacterial RNA polymerase at the rifampicin-binding pocket but maintains potency against RNA polymerases containing rifampicin-resistant mutations. KglA has antibiotic activity against rifampicin-resistant Gram-positive bacteria and multidrug-resistant Mycobacterium tuberculosis (MDR-M. tuberculosis). The X-ray crystal structures of KglA with the Escherichia coli RNA polymerase holoenzyme and Thermus thermophilus RNA polymerase-promoter complex reveal an altered-compared with rifampicin-conformation of KglA within the rifampicin-binding pocket. Unique deoxysugar and succinate ansa bridge substituents make additional contacts with a separate, hydrophobic pocket of RNA polymerase and preclude the formation of initial dinucleotides, respectively. Previous ansa-chain modifications in the rifamycin series have proven unsuccessful. Thus, KglA represents a key starting point for the development of a new class of ansa-chain derivatized ansamycins to tackle rifampicin resistance. Keywords: MDR-TB; RNA polymerase; antibiotic resistance; antibiotics; holo-enzyme crystal structure; kanglemycin A; multidrug-resistant Mycobacterium tuberculosis; promoter complex crystal structure; rifampicin; rifamycin.

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