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Apoptotic signalling targets the post-endocytic sorting machinery of the death receptor Fas/CD95.


ABSTRACT: Fas plays a major role in regulating ligand-induced apoptosis in many cell types. It is well known that several cancers demonstrate reduced cell surface levels of Fas and thus escape a potential control system via ligand-induced apoptosis, although underlying mechanisms are unclear. Here we report that the endosome associated trafficking regulator 1 (ENTR1), controls cell surface levels of Fas and Fas-mediated apoptotic signalling. ENTR1 regulates, via binding to the coiled coil domain protein Dysbindin, the delivery of Fas from endosomes to lysosomes thereby controlling termination of Fas signal transduction. We demonstrate that ENTR1 is cleaved during Fas-induced apoptosis in a caspase-dependent manner revealing an unexpected interplay of apoptotic signalling and regulation of endolysosomal trafficking resulting in a positive feedback signalling-loop. Our data provide insights into the molecular mechanism of Fas post-endocytic trafficking and signalling, opening possible explanations on how cancer cells regulate cell surface levels of death receptors.

SUBMITTER: Sharma S 

PROVIDER: S-EPMC6629679 | biostudies-literature | 2019 Jul

REPOSITORIES: biostudies-literature

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Apoptotic signalling targets the post-endocytic sorting machinery of the death receptor Fas/CD95.

Sharma Shruti S   Carmona Antonio A   Skowronek Agnieszka A   Yu Fangyan F   Collins Mark O MO   Naik Sindhu S   Murzeau Claire M CM   Tseng Pei-Li PL   Erdmann Kai S KS  

Nature communications 20190715 1


Fas plays a major role in regulating ligand-induced apoptosis in many cell types. It is well known that several cancers demonstrate reduced cell surface levels of Fas and thus escape a potential control system via ligand-induced apoptosis, although underlying mechanisms are unclear. Here we report that the endosome associated trafficking regulator 1 (ENTR1), controls cell surface levels of Fas and Fas-mediated apoptotic signalling. ENTR1 regulates, via binding to the coiled coil domain protein D  ...[more]

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