MUTATIONS OF A MUTS HOMOLOG IN HEREDITARY NONPOLYPOSIS COLORECTAL-CANCER

被引：2077

作者：

LEACH, FS

NICOLAIDES, NC

PAPADOPOULOS, N

LIU, B

JEN, J

PARSONS, R

PELTOMAKI, P

SISTONEN, P

AALTONEN, LA

NYSTROMLAHTI, M

GUAN, XY

ZHANG, J

MELTZER, PS

YU, JW

KAO, FT

CHEN, DJ

CEROSALETTI, KM

FOURNIER, REK

TODD, S

LEWIS, T

LEACH, RJ

NAYLOR, SL

WEISSENBACH, J

MECKLIN, JP

JARVINEN, H

PETERSEN, GM

HAMILTON, SR

GREEN, J

JASS, J

WATSON, P

LYNCH, HT

TRENT, JM

DELACHAPELLE, A

KINZLER, KW

VOGELSTEIN, B

机构：

[1] UNIV HELSINKI, DEPT MED GENET, SF-00290 HELSINKI 29, FINLAND

[2] JOHNS HOPKINS ONCOL CTR, BALTIMORE, MD 21231 USA

[3] NATL CTR HUMAN GENOME RES, BETHESDA, MD 20892 USA

[4] ELEANOR ROOSEVELT INST CANC RES, DENVER, CO 80206 USA

[5] LOS ALAMOS NATL LAB, DIV LIFE SCI, LOS ALAMOS, NM 87545 USA

[6] FRED HUTCHINSON CANC RES CTR, SEATTLE, WA 98104 USA

[7] UNIV TEXAS, HLTH SCI CTR, SAN ANTONIO, TX 78284 USA

[8] GENETHON, EVRY, FRANCE

[9] INST PASTEUR, CNRS, URA 1445, UNITE GENET MOLEC HUMAINE, F-75724 PARIS 15, FRANCE

[10] JOHNS HOPKINS UNIV, SCH PUBL HLTH & HYG, BALTIMORE, MD 21205 USA

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

[12] MEM UNIV NEWFOUNDLAND, ST JOHNS A1B 3V6, NEWFOUNDLAND, CANADA

[13] UNIV AUCKLAND, SCH MED, DEPT PATHOL, 92019 AUCKLAND, NEW ZEALAND

来源：

CELL | 1993年 / 75卷 / 06期

关键词：

D O I：

10.1016/0092-8674(93)90330-S

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Recent studies have shown that a locus responsible for hereditary nonpolyposis colorectal cancer (HNPCC) is on chromosome 2p and that tumors developing in these patients contain alterations in microsatellite sequences (RER+ phenotype). We have used chromosome microdissection to obtain highly polymorphic markers from chromosome 2p16. These and other markers were ordered in a panel of somatic cell hybrids and used to define a 0.8 Mb interval containing the HNPCC locus. Candidate genes were then mapped, and one was found to lie within the 0.8 Mb interval. We identified this candidate by virtue of its homology to mutS mismatch repair genes. cDNA clones were obtained and the sequence used to detect germline mutations, including those producing termination codons, in HNPCC kindreds. Somatic as well as germline mutations of the gene were identified in RER+ tumor cells. This mutS homolog is therefore likely to be responsible for HNPCC.

引用

页码：1215 / 1225

页数：11

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