1998
DOI: 10.1038/32681
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Fas-mediated apoptosis and activation-induced T-cell proliferation are defective in mice lacking FADD/Mort1

Abstract: Programmed cell death, or apoptosis, is important in homeostasis of the immune system: for example, non-functional or autoreactive lymphocytes are eliminated through apoptosis. One member of the tumour necrosis factor receptor (TNFR) family, Fas (also known as CD95 or Apo-1), can trigger cell death and is essential for lymphocyte homeostasis. FADD/Mort1 is a Fas-associated protein that is thought to mediate apoptosis by recruiting the protease caspase-8. A dominant-negative mutant of FADD inhibits apoptosis in… Show more

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Cited by 676 publications
(588 citation statements)
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“…In support of this idea, it is well known that Bid is required in only a subset of cell types and in cell death caused by a certain subset of stimuli. 40 The fact that apoptotic cell death in Bid-deficient mice occurs relatively normally and Biddeficient mice do not have the same severe phenotypes as do knockouts of other members of the extrinsic signaling pathway (such as caspase 8, 41 Fadd, 42,43 or Fas-deficient mice 44 ) also argues for the existence of a compensatory mechanism or molecule in addition to Bid.…”
Section: Discussionmentioning
confidence: 99%
“…In support of this idea, it is well known that Bid is required in only a subset of cell types and in cell death caused by a certain subset of stimuli. 40 The fact that apoptotic cell death in Bid-deficient mice occurs relatively normally and Biddeficient mice do not have the same severe phenotypes as do knockouts of other members of the extrinsic signaling pathway (such as caspase 8, 41 Fadd, 42,43 or Fas-deficient mice 44 ) also argues for the existence of a compensatory mechanism or molecule in addition to Bid.…”
Section: Discussionmentioning
confidence: 99%
“…TNF family receptors use an adaptor system to directly activate caspases and they are subject to complex modulation (Ashkenazi and Dixit, 1998). Ligand binding causes receptor homotrimerization and recruitment on the cytoplasmic face of the membrane of a death-inducing signaling complex (DISC), which includes the adaptors FADD and TRADD and procaspase-8 as crucial physiological death e ectors (Juo et al, 1998;Varfolomeev et al, 1998;Yeh et al, 1998;Zhang et al, 1998). A brief outline of the CD95/ Fas and TNf receptor systems follows since c-Myc has been implied to act both upstream and downstream of each (Janicke et al, 1994;Klefstrom et al, 1994Klefstrom et al, , 1997Hueber et al, 1997;Wang et al, 1998a).…”
Section: Regulatory Connections Between C-myc and Death Receptorsmentioning
confidence: 99%
“…98 FADD-deficient mice die in utero, suggesting that FADD also plays a role in nonlymphoid tissue proliferation. 99 Future studies are required to reveal a more detailed view about the function of HIPKs in death receptor signalling and their role in FADD phosphorylation.…”
Section: Hipksmentioning
confidence: 99%