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Microbiology 154 (2008), 240-248; DOI  10.1099/mic.0.2007/012153-0IMMEDIATE OPEN ACCESS ARTICLE
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Microbiology 154 (2008), 240-248; DOI  10.1099/mic.0.2007/012153-0
© 2008 Society for General Microbiology

EmbA is an essential arabinosyltransferase in Mycobacterium tuberculosis

Anita G. Amin1, Renan Goude2, Libin Shi1, Jian Zhang1, Delphi Chatterjee1 and Tanya Parish2

1 Department of Microbiology, Immunology and Pathology, Colorado State University, CO 80523, USA
2 Centre for Infectious Disease, Barts and the London, Queen Mary's School of Medicine and Dentistry, London E1 2AT, UK

Correspondence
Tanya Parish
t.parish{at}qmul.ac.uk

The Emb proteins (EmbA, EmbB, EmbC) are mycobacterial arabinosyltransferases involved in the biogenesis of the mycobacterial cell wall. EmbA and EmbB are predicted to work in unison as a heterodimer. EmbA and EmbB are involved in the formation of the crucial terminal hexaarabinoside motif [Araβ(1->2)Ara{alpha}(1->5)] [Araβ(1->2)Ara{alpha}(1->3)]Ara{alpha}(1->5)Ara{alpha}1->(Ara6) in the cell wall polysaccharide arabinogalactan. Studies conducted in Mycobacterium smegmatis revealed that mutants with disruptions in embA or embB are viable, although the growth rate was affected. In contrast, we demonstrate here that embA is an essential gene in Mycobacterium tuberculosis, since a deletion of the chromosomal gene could only be achieved when a second functional copy was provided on an integrated vector. Complementation of an embA mutant of M. smegmatis by M. tuberculosis embA confirmed that it encodes a functional arabinosyltransferase. We identified a promoter for M. tuberculosis embA located immediately upstream of the gene, indicating that it is expressed independently from the upstream gene, embC. Promoter activity from PembA(Mtb) was sevenfold lower when assayed in M. smegmatis compared to M. tuberculosis, indicating that the latter is not a good host for genetic analysis of M. tuberculosis embA expression. PembA(Mtb) activity remained constant throughout growth phases and after stress treatment, although it was reduced during hypoxia-induced non-replicating persistence. Ethambutol exposure had no effect on PembA(Mtb) activity. These data demonstrate that M. tuberculosis embA encodes a functional arabinosyltransferase which is constitutively expressed and plays a critical role in M. tuberculosis.


Abbreviations: AG, arabinogalactan; DCO, SCO, double, single cross-over; del-int, one deleted copy and one integrated copy of embA; HPAEC, high-pH anion-exchange chromatography; LAM, lipoarabinomannan; mAGP, mycolyl-AG-peptidoglycan (complex); OADC, oleic acid, albumin, dextrose, catalase




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