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Identification and differential expression of novel human cervical cancer oncogene HCCR-2 in human cancers and its involvement in p53 stabilization

Authors
Ko, JesangLee, Young HanHwang, Seung YongLee, Youn SooShin, Seung MinHwang, Jae HoonKim, JinKim, Yong WookJang, Sung-WukRyoo, Zae YoungKim, In-KyungNamkoong, Sung EunKim, Jin Woo
Issue Date
Jul-2003
Publisher
Nature Publishing Group
Keywords
HCCR-2; cervical cancer; p53; oncogene
Citation
Oncogene, v.22, no.30, pp.4679 - 4689
Indexed
SCIE
SCOPUS
Journal Title
Oncogene
Volume
22
Number
30
Start Page
4679
End Page
4689
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/46673
DOI
10.1038/sj.onc.1206624
ISSN
0950-9232
Abstract
Basic studies of oncogenesis have demonstrated that either the elevated production of particular oncogene proteins or the occurrence of qualitative abnormalities in oncogenes can contribute to neoplastic cellular transformation. The purpose of this study was to identify unique oncogenes that are differentially expressed in human cancers and characterize their functions in tumorigenesis. To discover new putative oncogenes, the differential display RT-PCR method was applied using normal cervical tissues, cervical cancer cell lines, cervical cancer tissues, and metastatic tissues. We identified a new human cervical cancer oncogene HCCR-2 that was overexpressed in various human tumors including leukemia, lymphoma, and carcinomas of the breast, kidney, ovary, stomach, colon, and uterine cervix. Ectopic expression of HCCR-2 resulted in direct tumorigenic conversions of NIH/3T3 and Rat1 fibroblasts. Nude mice injected with NIH/3T3 cells stably transfected with HCCR-2 formed tumors in 4 weeks. The resultant tumors display characteristics of an epithelial carcinoma. In HCCR-2 transfected NCI-H460 cells and RKO cells, stabilization of the p53 tumor suppressor occurred without genetic mutation and correlated with functional impairment, as indicated by the defective induction of p53-induced p21(WAF1), MDM2, and bax. These results indicate. that HCCR-2 probably represents a new oncogene that is related to tumorigenesis, functioning as a negative regulator of the p53 tumor suppressor.
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ERICA 과학기술융합대학 (ERICA 의약생명과학과)
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