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10.1016/j.molcel.2015.10.016

http://scihub22266oqcxt.onion/10.1016/j.molcel.2015.10.016
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C6051517!6051517!26585386
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suck abstract from ncbi


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pmid26585386      Mol+Cell 2015 ; 60 (4): 637-50
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  • Polyketide Quinones Are Alternate Intermediate Electron Carriers during Mycobacterial Respiration in Oxygen-Deficient Niches #MMPMID26585386
  • Anand A; Verma P; Singh AK; Kaushik S; Pandey R; Shi C; Kaur H; Chawla M; Elechalawar CK; Kumar D; Yang Y; Bhavesh NS; Banerjee R; Dash D; Singh A; Natarajan VT; Ojha AK; Aldrich CC; Gokhale RS
  • Mol Cell 2015[Nov]; 60 (4): 637-50 PMID26585386show ga
  • Mycobacterium tuberculosis (Mtb) adaptation to hypoxia is considered crucial to its prolonged latent persistence in humans. Mtb lesions are known to contain physiologically heterogeneous microenvironments that bring about differential responses from bacteria. Here we exploit metabolic variability within biofilm cells to identify alternate respiratory polyketide quinones (PkQs) from both Mycobacterium smegmatis (Msmeg) and Mtb. PkQs are specifically expressed in biofilms and other oxygen-deficient niches to maintain cellular bioenergetics. Under such conditions, these metabolites function as mobile electron carriers in the respiratory electron transport chain. In the absence of PkQs, mycobacteria escape from the hypoxic core of biofilms and prefer oxygen-rich conditions. Unlike the ubiquitous isoprenoid pathway for the biosynthesis of respiratory quinones, PkQs are produced by type III polyketide synthases using fatty acyl-CoA precursors. The biosynthetic pathway is conserved in several other bacterial genomes, and our study reveals a redox-balancing chemicocellular process in microbial physiology.
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