Interception of host fatty acid metabolism by mycobacteria under hypoxia to suppress anti-TB immunity

Pathogenic mycobacteria induce the formation of hypoxic granulomas during latent tuberculosis (TB) infection, in which the immune system contains, but fails to eliminate the mycobacteria. Fatty acid metabolism-related genes are relatively overrepresented in the mycobacterial genome and mycobacteria...

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Published inCell discovery Vol. 7; no. 1; p. 90
Main Authors Yang, Hua, Wang, Fei, Guo, Xinya, Liu, Feng, Liu, Zhonghua, Wu, Xiangyang, Zhao, Mengmeng, Ma, Mingtong, Liu, Haipeng, Qin, Lianhua, Wang, Lin, Tang, Tianqi, Sha, Wei, Wang, Yang, Chen, Jianxia, Huang, Xiaochen, Wang, Jie, Peng, Cheng, Zheng, Ruijuan, Tang, Fen, Zhang, Lu, Wu, Chunyan, Oehlers, Stefan H., Song, Zhigang, She, Jialei, Feng, Hua, Xie, Xunwei, Ge, Baoxue
Format Journal Article
LanguageEnglish
Published Singapore Springer Singapore 05.10.2021
Springer Nature B.V
Nature Publishing Group
Subjects
631/250/262
631/337/176
Acetic acid
Acetyltransferase
Biodegradation
Biomedical and Life Sciences
Cell Biology
Cell Culture
Cell Cycle Analysis
Cell Physiology
Fatty acids
Genomes
Granuloma
Granulomas
Hypoxia
Immune system
Inflammation
Interleukin 6
Life Sciences
Metabolism
Nutrient sources
Oxidation
Stem Cells
Supplements
Tuberculosis
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Summary:Pathogenic mycobacteria induce the formation of hypoxic granulomas during latent tuberculosis (TB) infection, in which the immune system contains, but fails to eliminate the mycobacteria. Fatty acid metabolism-related genes are relatively overrepresented in the mycobacterial genome and mycobacteria favor host-derived fatty acids as nutrient sources. However, whether and how mycobacteria modulate host fatty acid metabolism to drive granuloma progression remains unknown. Here, we report that mycobacteria under hypoxia markedly secrete the protein Rv0859/MMAR_4677 (Fatty-acid degradation A, FadA), which is also enriched in tuberculous granulomas. FadA acts as an acetyltransferase that converts host acetyl-CoA to acetoacetyl-CoA. The reduced acetyl-CoA level suppresses H3K9Ac-mediated expression of the host proinflammatory cytokine Il6 , thus promoting granuloma progression. Moreover, supplementation of acetate increases the level of acetyl-CoA and inhibits the formation of granulomas. Our findings suggest an unexpected mechanism of a hypoxia-induced mycobacterial protein suppressing host immunity via modulation of host fatty acid metabolism and raise the possibility of a novel therapeutic strategy for TB infection.
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ISSN:2056-5968
2056-5968
DOI:10.1038/s41421-021-00301-1