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Control of Mycobacterium tuberculosis protein secretion by ESX-4 and the outer membrane EsxUT-EsxEF complex

Nature Communications. 2025-11; 
Rashmi Ravindran Nair, Virginia Meikle, Swati Dubey, Mikhail Pavlenok, Anna D Tischler, Michael Niederweis Department of Microbiology, University of Alabama at Birmingham
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Polyclonal Antibody Services Similarly, the antigenic peptide sequences of EsxF and EsxU were selected (Table S1), synthesized, and the respective polyclonal antibodies were obtained (GenScript). The primary antibodies were used in the following dilutions: rabbit polyclonal anti-TNT (1:100, ProMab), rabbit polyclonal anti-EsxU (1:300, GenScript), rabbit polyclonal anti-EsxF (1:10, GenScript). The primary antibodies were used in the following dilutions: rabbit polyclonal anti-TNT (1:150, ProMab), rabbit polyclonal anti-EsxF (1:50, GenScript), rabbit polyclonal anti-EsxU (1:300, GenScript) The primary antibody was used in the following dilutions: rabbit polyclonal anti-EsxU (1:500, GenScript) Get A Quote

Abstract

Mycobacterium tuberculosis uses five ESX systems to secrete effector proteins with distinct functions essential for the pathogen’s growth and virulence. The current paradigm assumes that each ESX system secretes a distinct set of effector proteins. Here, we show that the EsxU-EsxT proteins, associated with the ESX-4 system, and the EsxE-EsxF proteins, encoded in the toxin operon cpnT, form a supercomplex that is required not only for toxin secretion, but also for outer membrane localization and for secretion of all Esx proteins into the cytosol of infected macrophages. Secretion of non-Esx proteins such as EspB, proteins involved in iron uptake, and PPE62, which are dependent on ESX-1, ESX-3 and ESX-5, respec... More

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