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Death receptor 5-recruited raft components contributes to the sensitivity of Jurkat leukemia cell lines to TRAIL-induced cell death

✍ Scribed by Yifan Min; Juan Shi; Yaxi Zhang; Shilian Liu; Yanxin Liu; Dexian Zheng

Book ID
102280737
Publisher
John Wiley and Sons
Year
2009
Tongue
English
Weight
205 KB
Volume
61
Category
Article
ISSN
1521-6543

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✦ Synopsis

Abstract

In the present study we demonstrated Jurkat leukemia cell lines of TIB152 and TIB153 with different sensitivities to recombinant soluble TRAIL cytotoxicity. TRAIL receptor death receptor 5 (DR5) was constitutively localized in the rafts in both cell lines. FADD, caspase‐8, and PI3K‐p85 subunit were recruited into DR5 lipid rafts of TIB152 but not in TIB153 cells. The expression and enzyme activity of acid sphingomyelinase, which digests sphingomyeline to produce ceramide and plays an essential role in lipid raft assembling, were higher in the rafts of TIB152 than in TIB153. These data provide evidences that DR5‐recruited raft components contribute to the different sensitivity of Jurkat leukemia cell lines to TRAIL‐induced cell death and may throw some light on the development of better therapeutic strategies for the cancer cells resistant to TRAIL treatment. © 2009 IUBMB IUBMB Life, 61(3): 261–267, 2009

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