Granzyme B disrupts central metabolism and protein synthesis in bacteria to promote an immune cell death program
- Autores: Farokh Dotiwala, Sumit Sen Santara, Andres Ariel Binker-Cosen
- Localización: Cell, ISSN 0092-8674, Vol. 171, Nº. 5, 2017, págs. 1125-1137
- Idioma: inglés
- Texto completo no disponible (Saber más ...)
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Resumen
Human cytotoxic lymphocytes kill intracellular microbes. The cytotoxic granule granzyme proteases released by cytotoxic lymphocytes trigger oxidative bacterial death by disrupting electron transport, generating superoxide anion and inactivating bacterial oxidative defenses. However, they also cause non-oxidative cell death because anaerobic bacteria are also killed. Here, we use differential proteomics to identify granzyme B substrates in three unrelated bacteria: Escherichia coli, Listeria monocytogenes, and Mycobacteria tuberculosis. Granzyme B cleaves a highly conserved set of proteins in all three bacteria, which function in vital biosynthetic and metabolic pathways that are critical for bacterial survival under diverse environmental conditions. Key proteins required for protein synthesis, folding, and degradation are also substrates, including multiple aminoacyl tRNA synthetases, ribosomal proteins, protein chaperones, and the Clp system. Because killer cells use a multipronged strategy to target vital pathways, bacteria may not easily become resistant to killer cell attack.
