Abstract
Twenty-one tumors from 18 patients (two independent tumors were obtained from each of three patients) with hepatocellular carcinomas were examined for loss of heterozygosity (LOH) at loci on chromosome 13q, using 15 polymorphic nucleotide sequences of microsatellites as genetic markers. The results revealed LOH in a common region between the centromeric D13S127 locus (13q12.2–q14.1) and the telomeric D13S137 (13q14.3) locus, including the RB1 locus, in nine of 21 tumors. Immunohistochemical staining of paraffin-embedded tumor sections indicated loss of retinoblastoma (RB) protein expression in all tumors showing LOH except one. Absence of RB protein expression was also observed in three of 12 tumors without LOH. Single-strand conformation polymorphism analysis of polymerase chain reaction products using primers flanking all 27 exons of the RB1 gene, as well as nucleotide sequencing, revealed tumor-specific small deletions of the RB1 coding region in the remaining RB1 allele of two tumors having LOH at the RB1 locus with concomitant loss of RB protein expression. Our results indicate that the loss of a region of chromosome 13q including the RB1 locus significantly (P < 0.006) correlates with loss of RB protein in hepatocellular carcinomas. However, tumor-specific mutations of the RB1 gene were detected in only two of 13 tumors with LOH and/or lack of RB protein expression, indicating that analysis of the RB1 status at the protein level in these tumors may be more sensitive than the actual mutational analysis.
Footnotes
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↵1 Supported by a grant-in-aid from the Ministry of Health and Welfare for a Comprehensive 10-Year Strategy for Cancer Control (Japan), a Research Grant on Aging and Health from the Ministry of Health and Welfare, a grant from the Special Coordination Fund of the Science and Technology Agency of Japan, a grant from the Princess Takamatsu Cancer Research Fund, and Grant CA54672 from the National Cancer Institute, NIH (to W. F. B.). X. Z. is a Research Fellow aided by the Sasagawa Foundation for Public Health and Welfare and a recipient of support from the Scientific Fund for Young Investigators from the Ministry of Public Health (People's Republic of China). R. S. is the recipient of a research fellowship under the Program for Invitation of Foreign Scientists to Japanese Institutes from the Foundation for Promotion of Cancer Research (Tokyo, Japan).
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↵4 To whom requests for reprints should be addressed.
- Received February 14, 1994.
- Accepted May 23, 1994.
- ©1994 American Association for Cancer Research.