IG20, in contrast to DENN-SV,(MADD splice variants) suppresses tumor cell survival, and enhances their susceptibility to apoptosis and cancer drugs

EV Efimova, AM Al-Zoubi, O Martinez, S Kaithamana… - Oncogene, 2004 - nature.com
EV Efimova, AM Al-Zoubi, O Martinez, S Kaithamana, S Lu, T Arima, BS Prabhakar
Oncogene, 2004nature.com
We identified seven putative splice variants of the human IG20 gene. Four variants namely,
IG20, MADD, IG20-SV2 and DENN-SV are expressed in human tissues. While DENN-SV is
constitutively expressed in all tissues, expression of IG20 appears to be regulated.
Interestingly, overexpression of DENN-SV enhanced cell replication and resistance to
treatments with TNFα, vinblastine, etoposide and γ-radiation. In contrast, IG20 expression
suppressed cell replication and increased susceptibility to the above treatments. Moreover …
Abstract
We identified seven putative splice variants of the human IG20 gene. Four variants namely, IG20, MADD, IG20-SV2 and DENN-SV are expressed in human tissues. While DENN-SV is constitutively expressed in all tissues, expression of IG20 appears to be regulated. Interestingly, overexpression of DENN-SV enhanced cell replication and resistance to treatments with TNFα, vinblastine, etoposide and γ-radiation. In contrast, IG20 expression suppressed cell replication and increased susceptibility to the above treatments. Moreover, cells that were resistant and susceptible to TNFα-induced apoptosis exclusively expressed endogenous DENN-SV and IG20, respectively. When PA-1 ovarian cancer cells that are devoid of endogenous IG20 variant, but express higher levels of DENN-SV, were transfected with IG20, they showed reduced cell proliferation and increased susceptibility to apoptosis induced by TNFα, TRAIL and γ-radiation. This indicated that overexpression of IG20 can override endogenous DENN-SV function. CrmA reversed the effects of IG20, but not DENN-SV. In contrast, dominant-negative-I-kappa B reversed the effects of DENN-SV, but not IG20, and showed that DENN-SV most likely exerted its effects through NFκB activation. Together, our data show that IG20 gene can play a novel and significant role in regulating cell proliferation, survival and death through alternative mRNA splicing.
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