Loss of ADAM15 prevents necroptosis induction by partial RIPK1 degradation and altered organelle organization.
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ABSTRACT: Death receptor-mediated signaling pathways must be tightly regulated to ensure tissue homeostasis. In a previous study, ADAM15 was identified as a possible TNF-regulated protease. We here unveil ADAM15 as a regulator of TNF-mediated necroptosis, while apoptosis and survival pathways remain unaffected. ADAM15 knockout results in the modulation of death-associated proteins and protein networks. Using a bottom-up proteomics screen to compare human U937 wild-type and ADAM15 knockdown cells enabled us to identify proteins and networks affected by ADAM15 loss, and which may be involved in necroptosis regulation.
ORGANISM(S): Homo Sapiens (human)
SUBMITTER: Jürgen Fritsch
PROVIDER: PXD066056 | JPOST Repository | Sat Jul 11 00:00:00 GMT+01:00 2026
REPOSITORIES: jPOST
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