Investigating the regulation of long-chain fatty acid metabolism by the Cpx envelope stress response in Escherichia coli

dc.contributor.authorMEGHA
dc.date.accessioned2025-12-17T04:46:51Z
dc.date.issued2025-03-01
dc.description.abstractLong-chain fatty acids (LCFAs) represent a tremendous energy source for bacteria including many pathogens; however, their utilization confers stress in bacteria. Using Escherichia coli as a model, previous work from our lab showed that the oxidation of a large number of reduced cofactors generated during LCFA metabolism increases electron flow towards ubiquinone, a lipid-soluble electron carrier in the electron transport chain (ETC). Because ubiquinone also re-oxidizes the disulfide bond (DSB)-forming machinery that performs oxidative protein folding in the envelope, the outermost multi-layered compartment critical for cellular growth and viability, increased electron flow during LCFA metabolism hampers the essential process of DSB formation, thereby compromising envelope redox balance. Notably, E. coli induces the CpxAR two-component system to counteract stress. The upregulation of envelope-localized chaperones and proteases is a well-recognized remedial mechanism by which Cpx restores cellular integrity. However, my work has identified Cpx as a global regulator of LCFA metabolism that uses a preventive measure to maintain envelope homeostasis in LCFA-grown cells; it facilitates DSB formation by downregulating LCFA metabolism and increasing the oxidizing power of ETC. Interestingly, contrary to its conventional mode of imparting regulation via CpxR working mainly as a transcriptional regulator, during LCFA metabolism, Cpx uses its non-coding arm to counteract envelope redox stress. The Cpx-regulated small RNA (sRNA) CpxQ i) represses fad genes involved in LCFA transport and -oxidation, ii) downregulates components of the glyoxylate shunt, gluconeogenesis, and ETC, and iii) stabilizes another sRNA OmrA, and both these sRNAs increase ubiquinone content. My work in E. coli revealing the interconnection between LCFA metabolism, redox stress, and envelope stress response provides the rationale for investigating similar networks in other LCFA utilizing bacteria.
dc.description.provenanceSubmitted by Gaurav Singh (gsgauravsingh476@gmail.com) on 2025-12-17T04:46:51Z No. of bitstreams: 1 Thesis final_Megha_PH18006_IISER Mohali.pdf: 4317125 bytes, checksum: 06081149acc6a004344d1a379e666247 (MD5)en
dc.description.provenanceMade available in DSpace on 2025-12-17T04:46:51Z (GMT). No. of bitstreams: 1 Thesis final_Megha_PH18006_IISER Mohali.pdf: 4317125 bytes, checksum: 06081149acc6a004344d1a379e666247 (MD5) Previous issue date: 2025-03-01en
dc.guideRachna Chaba
dc.guideRachna Chaba
dc.identifier.urihttp://210.212.36.82:4000/handle/123456789/6019
dc.language.isoen
dc.subjectmetabolism
dc.subjectEscherichia coli
dc.titleInvestigating the regulation of long-chain fatty acid metabolism by the Cpx envelope stress response in Escherichia coli
dc.typeThesis

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