SPECIFIC MUTATIONS OF THE RET PROTOONCOGENE ARE RELATED TO DISEASE PHENOTYPE IN MEN 2A AND FMTC

被引:538
作者
MULLIGAN, LM
ENG, C
HEALEY, CS
CLAYTON, D
KWOK, JBJ
GARDNER, E
PONDER, MA
FRILLING, A
JACKSON, CE
LEHNERT, H
NEUMANN, HPH
THIBODEAU, SN
PONDER, BAJ
机构
[1] UNIV CAMBRIDGE,DEPT PATHOL,CANC RES CAMPAIGN,HUMAN CANC GENET RES GRP,CAMBRIDGE CB2 1QP,ENGLAND
[2] UNIV CAMBRIDGE,INST PUBL HLTH,MRC,BIOSTAT UNIT,CAMBRIDGE CB2 2SR,ENGLAND
[3] UNIV HAMBURG KRANKENHAUS,CHIRURG KLIN,W-2000 HAMBURG 20,GERMANY
[4] HENRY FORD HOSP,DEPT MED,DETROIT,MI 48202
[5] UNIV MAINZ,MED KLIN & POLIKLIN,INNERE MED ABT,W-6500 MAINZ,GERMANY
[6] UNIV FREIBURG,INNERE MED ABT 4,D-79106 FREIBURG,GERMANY
[7] MAYO CLIN & MAYO FDN,DEPT LAB MED,ROCHESTER,MN 55905
来源
NATURE GENETICS | 1994年 / 6卷 / 01期
关键词
D O I
10.1038/ng0194-70
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
We have analysed 118 families with inherited medullary thyroid carcinoma (MTC) for mutations of the RET proto-oncogene. These included cases of multiple endocrine neoplasia types 2A (MEN 2A) and 2B (MEN 2B) and familial MTC (FMTC). Mutations at one of 5 cysteines in the extracellular domain were found in 97% of patients with MEN 2A and 86% with FMTC but not in MEN 2B patients or normal controls. 84% of the MEN2A mutations affected codon 634. MEN 2A patients with a Cys634 to Arg substitution had a greater risk of developing parathyroid disease than those with other codon 634 mutations. Our data show a strong correlation between disease phenotype and the nature and position of the RET mutation, suggesting that a simple, constitutive activation of the RET tyrosine kinase is unlikely to explain the events leading to MEN 2A and FMTC.
引用
收藏
页码:70 / 74
页数:5
相关论文
共 22 条
[11]   ANDROGEN RECEPTOR GENE-MUTATIONS IN X-LINKED SPINAL AND BULBAR MUSCULAR-ATROPHY [J].
LASPADA, AR ;
WILSON, EM ;
LUBAHN, DB ;
HARDING, AE ;
FISCHBECK, KH .
NATURE, 1991, 352 (6330) :77-79
[12]   DELETION OF GENES ON CHROMOSOME-1 IN ENDOCRINE NEOPLASIA [J].
MATHEW, CGP ;
SMITH, BA ;
THORPE, K ;
WONG, Z ;
ROYLE, NJ ;
JEFFREYS, AJ ;
PONDER, BAJ .
NATURE, 1987, 328 (6130) :524-526
[13]  
Miya A, 1992, Henry Ford Hosp Med J, V40, P215
[14]   LOCALIZATION OF THE GENE FOR MULTIPLE ENDOCRINE NEOPLASIA TYPE 2A TO A 480-KB REGION IN CHROMOSOME BAND 10Q11.2 [J].
MOLE, SE ;
MULLIGAN, LM ;
HEALEY, CS ;
PONDER, BAJ ;
TUNNACLIFFE, A .
HUMAN MOLECULAR GENETICS, 1993, 2 (03) :247-252
[15]   GERM-LINE MUTATIONS OF THE RET PROTOONCOGENE IN MULTIPLE ENDOCRINE NEOPLASIA TYPE-2A [J].
MULLIGAN, LM ;
KWOK, JBJ ;
HEALEY, CS ;
ELSDON, MJ ;
ENG, C ;
GARDNER, E ;
LOVE, DR ;
MOLE, SE ;
MOORE, JK ;
PAPI, L ;
PONDER, MA ;
TELENIUS, H ;
TUNNACLIFFE, A ;
PONDER, BAJ .
NATURE, 1993, 363 (6428) :458-460
[16]   LINKAGE OF THE MULTIPLE ENDOCRINE NEOPLASIA TYPE-2B GENE (MEN2B) TO CHROMOSOME-10 MARKERS LINKED TO MEN2A [J].
NORUM, RA ;
LAFRENIERE, RG ;
ONEAL, LW ;
NIKOLAI, TF ;
DELANEY, JP ;
SISSON, JC ;
SOBOL, H ;
LENOIR, GM ;
PONDER, BAJ ;
WILLARD, HF ;
JACKSON, CE .
GENOMICS, 1990, 8 (02) :313-317
[17]  
SANTORO M, 1990, ONCOGENE, V5, P1595
[18]   GENETIC-ASPECTS OF MULTIPLE ENDOCRINE NEOPLASIA [J].
SCHIMKE, RN .
ANNUAL REVIEW OF MEDICINE, 1984, 35 :25-31
[19]  
TAKAHASHI M, 1989, ONCOGENE, V4, P805
[20]  
TAKAHASHI M, 1988, ONCOGENE, V3, P571
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