2014
DOI: 10.1038/cdd.2014.126
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RIP kinases: key decision makers in cell death and innate immunity

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Cited by 216 publications
(206 citation statements)
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References 194 publications
(219 reference statements)
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“…Though no direct apoptotic assays were done in this study, the morphological characteristics indicated that the cell death could partly be due to apoptosis. However, in the present study the TNF-α gene expression was increased with both PM2.5 and PM10, and interestingly, RIP is reported to interact either with TNF receptor signalling or with FADD to bring about apoptosis [35].…”
Section: Discussioncontrasting
confidence: 46%
See 1 more Smart Citation
“…Though no direct apoptotic assays were done in this study, the morphological characteristics indicated that the cell death could partly be due to apoptosis. However, in the present study the TNF-α gene expression was increased with both PM2.5 and PM10, and interestingly, RIP is reported to interact either with TNF receptor signalling or with FADD to bring about apoptosis [35].…”
Section: Discussioncontrasting
confidence: 46%
“…However, the expression of BCL2, BAX and P53 genes in our study did not support apoptotic pattern of cell death indicating a role for other mediators of cell death. Although, interaction with TNF receptor with RIP and FADD is reported to cause apoptosis [35], it is indeed necessary to undertake either an early time point of study for apoptosis or screen for additional pathways of cell death in our subsequent studies.…”
Section: Discussionmentioning
confidence: 99%
“…TNF␣-induced activation of pro-survival (MAPK and NF-B) and apoptotic signaling pathways has been extensively studied and well elucidated (1,6,7,16,70). TNFR1 internalization and the formation of distinct TNFR1 signaling complexes or receptosomes provide the structural basis for spatial compartmentalization of TNFR1-mediated pro-and anti-apoptotic signaling pathways.…”
Section: Discussionmentioning
confidence: 99%
“…The serine-threonine kinase receptorinteracting protein (RIP) 1 is targeted by necrostatin-1 (Nec-1) a specific inhibitor of necroptosis, which depends on RIP1/3 complex activation (15,16). Necroptosis controls normal embryonic organic evolution, T-cell propagation and chronic intestinal inflammation (17). In addition, the discovery of Nec-1, a small molecule that inhibits non-apoptotic programmed cell death-inducing substances, has provided a useful pharmacological tool for the study of necroptosis.…”
Section: Introductionmentioning
confidence: 99%