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General information | Expression | Regulation | Mutation | Interaction |
Basic Information |
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Gene ID | 91768 |
Name | CABLES1 |
Synonymous | CABL1|CABLES|HsT2563|IK3-1;Cdk5 and Abl enzyme substrate 1;CABLES1;Cdk5 and Abl enzyme substrate 1 |
Definition | CDK5 and ABL1 enzyme substrate 1|interactor with CDK3 1 |
Position | 18q11.2 |
Gene type | protein-coding |
Source | Count: 2; TAG,Generif |
Sentence |
Abstract |
ik3-1/Cables has been identified to be a candidate tumor suppressor for colon and head/neck cancers. | ik3-2 is a close relative to ik3-1/Cables, an associator with cdk3 and cdk5. ik3-1/Cables has been identified to be a candidate tumor suppressor for colon and head/neck cancers. In agreement, it has been pointed out that ik3-1/Cables is a regulator for both p53- and p73-induced apoptosis [J. Biol. Chem. 277 (2002) 2951] although ectopic expression of ik3-1/Cables does not induce apoptosis. Here we show that adenovirus-mediated overexpression of ik3-2 results in apoptosis of p53-intact U2OS cells. ik3-2 binds to p53 in vivo and ectopic coexpression of ik3-2 enhances apoptosis induced by adenovirus-mediated expression of p53. Furthermore, ectopic expression of ik3-2 results in apoptosis of primary p53/Mdm2- and p53/ARF-null mouse embryo fibroblasts, indicating that ik3-2-induced apoptosis is partially p53-independent. Both the highly conserved C-terminal cyclin box-homologous domain (ik3-2-C) and the N-terminal region consisting of 70 amino acids (ik3-2-N) are responsible for ik3-2-mediated enhancement of p53-induced apoptosis. In contrast, ik3-2-induced p53-independent apoptosis is mediated through ik3-2-N. We thus identified ik3-2 as a proapoptotic factor involved in both p53-mediated and p53-independent apoptotic pathways. |
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