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FhaA plays a key role in mycobacterial polar elongation and asymmetric growth
Resumen
Mycobacteria, including pathogens like Mycobacterium tuberculosis, exhibit unique growth patterns and cell envelope structures that challenge our understanding of bacterial physiology. This study sheds light on FhaA, a conserved protein in Mycobacteriales, revealing its pivotal role in coordinating cell envelope biogenesis and asymmetric growth. The elucidation of the FhaA interactome in living mycobacterial cells reveals its participation in the protein
[ver mas...]
Mycobacteria, including pathogens like Mycobacterium tuberculosis, exhibit unique growth patterns and cell envelope structures that challenge our understanding of bacterial physiology. This study sheds light on FhaA, a conserved protein in Mycobacteriales, revealing its pivotal role in coordinating cell envelope biogenesis and asymmetric growth. The elucidation of the FhaA interactome in living mycobacterial cells reveals its participation in the protein network orchestrating cell envelope biogenesis and cell elongation/division. By manipulating FhaA levels, we uncovered its influence on cell morphology, cell envelope organization, and the localization of peptidoglycan biosynthesis machinery. Notably, fhaA deletion disrupted the characteristic asymmetric growth of mycobacteria, highlighting its importance in maintaining this distinctive feature. Our findings position FhaA as a key regulator in a complex protein network, orchestrating the asymmetric distribution and activity of cell envelope biosynthetic machinery. This work not only advances our understanding of mycobacterial growth mechanisms but also identifies FhaA as a potential target for future studies on cell envelope biogenesis and bacterial growth regulation. These insights into the fundamental biology of mycobacteria may pave the way for novel approaches to combat mycobacterial infections addressing the ongoing challenge of diseases like tuberculosis in global health.
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Autor
Rossello, Jessica;
Rivera, Bernardina;
Anzibar Fialho, Maximiliano;
Augusto, Ingrid;
Gil, Magdalena;
Forrellad, Marina Andrea;
Bigi, Fabiana;
Rodríguez Taño, Azalia;
Urdániz, Estefanía;
Piuri, Mariana;
Miranda, Kildare;
Wehenkel, Anne Marie;
Alzari, Pedro M.;
Malacrida, Leonel;
Durán, Rosario;
Fuente
mBio 16 (3) : e02526-24 (March 2025)
Fecha
2025-03
Editorial
American Society for Microbiology
ISSN
2161-2129
Formato
pdf
Tipo de documento
artículo
Palabras Claves
Derechos de acceso
Abierto
