p16INK4andp15INK4BAlterations in Primary Gynecologic Malignancy

Chromosome 9 abnormalities have been found in primary tumors and cell lines from human gynecologic malignancy. Alterations ofp16INK4andp15INK4Bgenes mapped on the band p21 of chromosome 9 have been detected in various human tumors, but the role of these genes as tumor suppressorsin vivoappear to be...

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Published inGynecologic oncology Vol. 65; no. 2; pp. 319 - 324
Main Authors Wong, Y.F., Chung, T.K.H., Cheung, T.H., Nobori, T., Yim, S.F., Lai, K.W.H., Yu, A.L., Diccianni, M.B., Li, T.Z., Chang, A.M.Z.
Format Journal Article
LanguageEnglish
Published Elsevier Inc 01.05.1997
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Summary:Chromosome 9 abnormalities have been found in primary tumors and cell lines from human gynecologic malignancy. Alterations ofp16INK4andp15INK4Bgenes mapped on the band p21 of chromosome 9 have been detected in various human tumors, but the role of these genes as tumor suppressorsin vivoappear to be dependent on tumor type. Polymerase chain reaction (PCR)-based analysis was performed to search for lesions of these genes in 202 primary gynecologic malignancies. Homozygous deletions ofp16INK4were detected in 7 of 128 (5%) cervical, 1 of 41 (2%) endometrial, 2 of 27 (7%) ovarian, and 3 of 6 (50%) vulvar carcinomas, while homozygous deletions ofp15INK4Bwere detected in 19 of 128 (15%) cervical, 1 of 41 (2%) endometrial, 9 of 27 (33%) ovarian, and 3 of 6 (50%) vulvar carcinomas, respectively. No mutations were found in exon 2 ofp16INK4from 161 cases of gynecologic malignancy without deletion ofp16INK4. All 3 cases of vulvar carcinoma showing homozygous deletions ofp16INK4andp15INK4Bwere at advanced clinical stage (stage III–IV), while all 7 cases of cervical carcinoma and 2 cases of ovarian carcinoma showing homozygous deletion ofp16INK4were at early stage (stage I–II). The results indicate that homozygous deletions ofp16INK4and/orp15INK4Bgenes may play a role in a subset of primary gynecologic malignancy.
ISSN:0090-8258
1095-6859
DOI:10.1006/gyno.1997.4669