Evaluation of candidate tumour suppressor genes on chromosome 18 in colorectal cancers

被引：525

作者：

Thiagalingam, S

Lengauer, C

Leach, FS

Schutte, M

Hahn, SA

Overhauser, J

Willson, JKV

Markowitz, S

Hamilton, SR

Kern, SE

Kinzler, KW

Vogelstein, B

机构：

[1] JOHNS HOPKINS ONCOL CTR,BALTIMORE,MD 21231

[2] JOHNS HOPKINS UNIV,SCH MED,DEPT PATHOL,BALTIMORE,MD 21205

[3] THOMAS JEFFERSON UNIV,DEPT BIOCHEM & MOLEC BIOL,PHILADELPHIA,PA 19107

[4] CASE WESTERN RESERVE UNIV HOSP,DEPT MED,CLEVELAND,OH 44106

[5] CASE WESTERN RESERVE UNIV HOSP,IRELAND CANC CTR,CLEVELAND,OH 44106

[6] JOHNS HOPKINS ONCOL CTR,HOWARD HUGHES MED INST,BALTIMORE,MD 21231

来源：

NATURE GENETICS | 1996年 / 13卷 / 03期

关键词：

D O I：

10.1038/ng0796-343

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Chromosome deletions are the most common genetic events observed in cancer. These deletions are generally thought to reflect the existence of a tumour suppressor gene within the lost region. However, when the lost region does not precisely coincide with a hereditary cancer locus, identification of the putative tumour suppressor gene (target of the deletion) can be problematic. For example, previous studies have demonstrated that chromosome 18q is lost in over 60% of colorectal as well as in other cancers, but the lost region could not be precisely determined. Here we present a rigorous strategy for mapping and evaluating allelic deletions in sporadic tumours, and apply it to the evaluation of chromosome 18 in colorectal cancers. Using this approach, we define a minimally lost region (MLR) on chromosome 18q21, which contains at least two candidate tumour suppressor genes, DPC4 and DCC. The analysis further suggested genetic heterogeneity, with DPC4 the deletion target in up to a third of the cases and DCC or a neighbouring gene the target in the remaining tumours.

引用

页码：343 / 346

页数：4

共 32 条

[1] CLUES TO THE PATHOGENESIS OF FAMILIAL COLORECTAL-CANCER
AALTONEN, LA
PELTOMAKI, P
LEACH, FS
SISTONEN, P
PYLKKANEN, L
MECKLIN, JP
JARVINEN, H
POWELL, SM
JEN, J
HAMILTON, SR
PETERSEN, GM
KINZLER, KW
VOGELSTEIN, B
DELACHAPELLE, A
[J]. SCIENCE, 1993, 260 (5109) : 812 - 816
[2] MUTATION FREQUENCY IN HUMAN BLOOD-CELLS INCREASES WITH AGE
AKIYAMA, M
KYOIZUMI, S
HIRAI, Y
KUSUNOKI, Y
IWAMOTO, KS
NAKAMURA, N
[J]. MUTATION RESEARCH-DNAGING GENETIC INSTABILITY AND AGING, 1995, 338 (1-6): : 141 - 149
[3] THE GENETIC-BASIS OF CANCER
CAVENEE, WK
WHITE, RL
[J]. SCIENTIFIC AMERICAN, 1995, 272 (03) : 72 - 79
[4] THE DCC GENE - STRUCTURAL-ANALYSIS AND MUTATIONS IN COLORECTAL CARCINOMAS
CHO, KR
OLINER, JD
SIMONS, JW
HEDRICK, L
FEARON, ER
PREISINGER, AC
HEDGE, P
SILVERMAN, GA
VOGELSTEIN, B
[J]. GENOMICS, 1994, 19 (03) : 525 - 531
[5] DCC - LINKING TUMOR-SUPPRESSOR GENES AND ALTERED CELL-SURFACE INTERACTIONS IN CANCER
CHO, KR
FEARON, ER
[J]. CURRENT OPINION IN GENETICS & DEVELOPMENT, 1995, 5 (01) : 72 - 78
[6] SPONTANEOUS LENGTH VARIATION IN MICROSATELLITE DNA FROM HUMAN T-CELL CLONES
HACKMAN, P
GABBANI, G
OSTERHOLM, AM
HELLGREN, D
LAMBERT, B
[J]. GENES CHROMOSOMES & CANCER, 1995, 14 (03) : 215 - 219
[7] DPC4, a candidate tumor suppressor gene at human chromosome 18q21.1
Hahn, SA
Schutte, M
Hoque, ATMS
Moskaluk, CA
daCosta, LT
Rozenblum, E
Weinstein, CL
Fischer, A
Yeo, CJ
Hruban, RH
Kern, SE
[J]. SCIENCE, 1996, 271 (5247) : 350 - 353
[8] UBIQUITOUS SOMATIC MUTATIONS IN SIMPLE REPEATED SEQUENCES REVEAL A NEW MECHANISM FOR COLONIC CARCINOGENESIS
IONOV, Y
PEINADO, MA
MALKHOSYAN, S
SHIBATA, D
PERUCHO, M
[J]. NATURE, 1993, 363 (6429) : 558 - 561
[9] ALLELIC LOSS OF CHROMOSOME 18Q AND PROGNOSIS IN COLORECTAL-CANCER
JEN, J
KIM, HG
PIANTADOSI, S
LIU, ZF
LEVITT, RC
SISTONEN, P
KINZLER, KW
VOGELSTEIN, B
HAMILTON, SR
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1994, 331 (04) : 213 - 221
[10] ANTIONCOGENES AND HUMAN CANCER
KNUDSON, AG
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (23) : 10914 - 10921

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