Structure-function relationship of PE11 esterase ofMycobacterium tuberculosiswith respect to its role in virulence

Author:

Dahiya Priyanka,Banerjee Amit,Saha Abhishek,Nandicoori Vinay Kumar,Ghosh Sudip,Mukhopadhyay Sangita

Abstract

AbstractThe lipolytic enzymes ofMycobacterium tuberculosisplay a critical role in immunomodulation and virulence. Among these proteins, PE11 which also belongs to the PE/PPE family, is the smallest (∼10.8 kDa) and play a significant role in cell wall remodelling and virulence. PE11 is established to be an esterase, but its enzymatic and structural properties are not yet characterized. In this study, using homology modelling we deduced the putative structure which shows the presence of both α-helix and β-sheet structures which is in close agreement with that observed by CD spectra of the purified protein. PE11 was found to contain a GX3SX4G motif homologous to canonical ‘GxSxG’ motif present in many serin hydrolases. The catalytic triad appears to be located within this motif as substitution of Serine26and Glycine31residues abrogated its enzymatic activity. Gel-filtration chromatography data indicate that PE11 possibly exists as dimer and tetramer showing positive cooperativity for binding its substrates. In addition, PE11 esterase activity was found to be critical for cell wall remodelling, antibiotic resistance and conferring survival advantages toM. tuberculosis. Our data suggest that PE11 can be targeted for designing potential therapeutic strategies.

Publisher

Cold Spring Harbor Laboratory

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