New p73 variants with altered C-terminal structures have varied transcriptional activities

被引:0
|
作者
Yoshihide Ueda
Makoto Hijikata
Shinji Takagi
Tsutomu Chiba
Kunitada Shimotohno
机构
[1] Institute for Virus Research,Department of Viral Oncology
[2] Kyoto University,Division of Gastroenterology and Hepatology, Department of Internal Medicine
[3] Sakyo-Ku,undefined
[4] Kyoto University,undefined
[5] Sakyo-ku,undefined
来源
Oncogene | 1999年 / 18卷
关键词
p73; splicing variant; p53; transcriptional activity;
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学科分类号
摘要
p73 has been identified as a protein which shares significant homology with the tumor suppressor p53. We found two new types of splicing variant mRNAs for p73 expressed in MCF-7 cells which we named p73γ and ε. Sequence analysis revealed that these mRNAs encode variant p73 proteins bearing distinct carboxy-terminal structures, which are also different from the previously reported variants p73α and β. The mRNAs encoding p73γ and ε as well as α and β were confirmed to be expressed in normal human tissues in varied patterns. All of these splicing variants activated promoter with the p53-binding consensus sequence, but to different degrees. Furthermore, suppressive effects of p73α, γ and ε, but not β, on endogenous p53 activity were observed when transiently expressed in HepG2 and MCF-7 cells. These results suggested that the carboxy-terminal regions of p73 which were altered by alternative splicing affect these transactivation abilities and modulate the functions of p73 molecules.
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页码:4993 / 4998
页数:5
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