The mycobacterial glycoside hydrolase LamH enables capsular arabinomannan release and stimulates growth

分枝杆菌糖苷水解酶 LamH 能够促进荚膜阿拉伯甘露聚糖的释放,并刺激生长

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作者:Aaron Franklin, Vivian C Salgueiro, Abigail J Layton, Rudi Sullivan, Todd Mize, Lucía Vázquez-Iniesta, Samuel T Benedict, Sudagar S Gurcha, Itxaso Anso, Gurdyal S Besra, Manuel Banzhaf, Andrew L Lovering, Spencer J Williams, Marcelo E Guerin, Nichollas E Scott, Rafael Prados-Rosales, Elisabeth C Low

Abstract

Mycobacterial glycolipids are important cell envelope structures that drive host-pathogen interactions. Arguably, the most important are lipoarabinomannan (LAM) and its precursor, lipomannan (LM), which are trafficked from the bacterium to the host via unknown mechanisms. Arabinomannan is thought to be a capsular derivative of these molecules, lacking a lipid anchor. However, the mechanism by which this material is generated has yet to be elucidated. Here, we describe the identification of a glycoside hydrolase family 76 enzyme that we term LamH (Rv0365c in Mycobacterium tuberculosis) which specifically cleaves α-1,6-mannoside linkages within LM and LAM, driving its export to the capsule releasing its phosphatidyl-myo-inositol mannoside lipid anchor. Unexpectedly, we found that the catalytic activity of this enzyme is important for efficient exit from stationary phase cultures, potentially implicating arabinomannan as a signal for growth phase transition. Finally, we demonstrate that LamH is important for M. tuberculosis survival in macrophages.

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