MICROSATELLITE ALTERATIONS AS CLONAL MARKERS FOR THE DETECTION OF HUMAN CANCER

被引：425

作者：

MAO, L

LEE, DJ

TOCKMAN, MS

EROZAN, YS

ASKIN, F

SIDRANSKY, D

机构：

[1] JOHNS HOPKINS UNIV,SCH MED,DEPT OTOLARYNGOL HEAD & NECK SURG,DIV HEAD & NECK CANC RES,BALTIMORE,MD 21205

[2] JOHNS HOPKINS UNIV,SCH HYG,DEPT ENVIRONM HLTH SCI,BALTIMORE,MD 21205

[3] JOHNS HOPKINS UNIV HOSP,DEPT PATHOL,BALTIMORE,MD 21287

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1994年 / 91卷 / 21期

关键词：

D O I：

10.1073/pnas.91.21.9871

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

Microsatellite instability has been reported to be an important feature of tumors from hereditary nonpolyposis colorectal carcinoma (HNPCC) patients. The recent discovery of genetic instability in small cell lung carcinoma, a neoplasm not associated with HNPCC, led us to investigate the possible presence of microsatellite alterations in other tumor types. We examined 52 microsatellite repeat sequences in the DNA of normal and tumor pairs from 100 head and neck, bladder, and lung cancer patients by the polymerase chain reaction. Although alterations were rare in dinucleotide repeats, larger (tri- or tetranucleotide) repeats were found to be more pi one to expansion or deletion. We screened 100 tumors with a panel of nine tri- and tetranucleotide repeat markers and identified 26 (26%) that displayed alterations in at least one locus. This observation prompted us to examine the possibility of using microsatellite alterations as markers to detect clonal tumor-derived cell populations in pathologic samples. The identical microsatellite alterations detected in the primary tumors were successfully identified in corresponding urine, sputum, and surgical margins from affected patients. This study demonstrates that appropriately selected microsatellite loci are commonly altered in many cancers and can serve as clonal markers for their detection.

引用

页码：9871 / 9875

页数：5

共 43 条

[1] ANALYSIS OF SOMATIC MUTATIONS AT HUMAN MINISATELLITE LOCI IN TUMORS AND CELL-LINES
ARMOUR, JAL
PATEL, I
THEIN, SL
FEY, MF
JEFFREYS, AJ
[J]. GENOMICS, 1989, 4 (03) : 328 - 334
[2] Biancalana V., 1992, Human Molecular Genetics, V1, P255, DOI 10.1093/hmg/1.4.255
[3] CANCER STATISTICS, 1994
BORING, CC
SQUIRES, TS
TONG, T
MONTGOMERY, S
[J]. CA-A CANCER JOURNAL FOR CLINICIANS, 1994, 44 (01) : 7 - 26
[4] BRENNAN JA, 1994, 85TH P ANN M AM ASS, V35, P221
[5] MUTATION IN THE DNA MISMATCH REPAIR GENE HOMOLOG HMLH1 IS ASSOCIATED WITH HEREDITARY NONPOLYPOSIS COLON-CANCER
BRONNER, CE
BAKER, SM
MORRISON, PT
WARREN, G
SMITH, LG
LESCOE, MK
KANE, M
EARABINO, C
LIPFORD, J
LINDBLOM, A
TANNERGARD, P
BOLLAG, RJ
GODWIN, AR
WARD, DC
NORDENSKJOLD, M
FISHEL, R
KOLODNER, R
LISKAY, RM
[J]. NATURE, 1994, 368 (6468) : 258 - 261
[6] CAIRNS P, 1994, CANCER RES, V54, P1422
[7] EVIDENCE FOR A MECHANISM PREDISPOSING TO INTERGENERATIONAL CAG REPEAT INSTABILITY IN SPINOCEREBELLAR ATAXIA TYPE-I
CHUNG, MY
RANUM, LPW
DUVICK, LA
SERVADIO, A
ZOGHBI, HY
ORR, HT
[J]. NATURE GENETICS, 1993, 5 (03) : 254 - 258
[8] FEARON ER, 1990, CELL, V61, P709
[9] CLONAL ORIGIN OF HUMAN TUMORS
FIALKOW, PJ
[J]. BIOCHIMICA ET BIOPHYSICA ACTA, 1976, 458 (03) : 283 - 321
[10] THE HUMAN MUTATOR GENE HOMOLOG MSH2 AND ITS ASSOCIATION WITH HEREDITARY NONPOLYPOSIS COLON-CANCER
FISHEL, R
LESCOE, MK
RAO, MRS
COPELAND, NG
JENKINS, NA
GARBER, J
KANE, M
KOLODNER, R
[J]. CELL, 1993, 75 (05) : 1027 - 1038

← 1 2 3 4 5 →