A MUTATION IN CFTR PRODUCES DIFFERENT PHENOTYPES DEPENDING ON CHROMOSOMAL BACKGROUND

被引:360
作者
KIESEWETTER, S
MACEK, M
DAVIS, C
CURRISTIN, SM
CHU, CS
GRAHAM, C
SHRIMPTON, AE
CASHMAN, SM
TSUI, LC
MICKLE, J
AMOS, J
HIGHSMITH, WE
SHUBER, A
WITT, DR
CRYSTAL, RG
CUTTING, GR
机构
[1] JOHNS HOPKINS UNIV,SCH MED,CTR MED GENET,DEPT PEDIAT & MED,BALTIMORE,MD 21287
[2] HOSP SICK CHILDREN,DEPT GENET,TORONTO M5G 1X8,ONTARIO,CANADA
[3] NHLBI,PULM BRANCH,BETHESDA,MD 20892
[4] UNIV EDINBURGH,HUMAN GENET UNIT,EDINBURGH EH8 9YL,MIDLOTHIAN,SCOTLAND
[5] UNIV DUBLIN TRINITY COLL,DEPT GENET,DUBLIN 2,IRELAND
[6] REG GENET CTR,BELFAST,NORTH IRELAND
[7] BOSTON UNIV,SCH MED,CTR HUMAN GENET,BOSTON,MA 02118
[8] UNIV N CAROLINA,DEPT PATHOL,CHAPEL HILL,NC 27599
[9] INTEGRATED GENET INC,FRAMINGHAM,MA 01701
[10] KAISER PERMANENTE,DEPT GENET,SAN JOSE,CA 95119
[11] JOHNS HOPKINS UNIV HOSP,BALTIMORE,MD 21287
来源
NATURE GENETICS | 1993年 / 5卷 / 03期
关键词
D O I
10.1038/ng1193-274
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Cystic fibrosis (CF) is caused by mutations in the CF transmembrane conductance regulator (CFTR) gene but the association between mutation (genotype) and disease presentation (phenotype) is not straightforward. We have been investigating whether variants in the CFTR gene that alter splicing efficiency of exon 9 can affect the phenotype produced by a mutation. A missense mutation, R117H, which has been observed in three phenotypes, was found to occur on two chromosome backgrounds with intron 8 variants that have profoundly different effects upon splicing efficiency. A close association is shown between chromosome background of the R117H mutation and phenotype. These findings demonstrate that the genetic context in which a mutation occurs can play a significant role in determining the type of illness produced.
引用
收藏
页码:274 / 278
页数:5
相关论文
共 34 条
  • [1] AMOS JA, 1992, PEDIATR PULM S, V8, P142
  • [2] IDENTIFICATION OF 12 NOVEL MUTATIONS IN THE CFTR GENE
    AUDREZET, MP
    MERCIER, B
    GUILLERMIT, H
    QUERE, I
    VERLINGUE, C
    RAULT, G
    FEREC, C
    [J]. HUMAN MOLECULAR GENETICS, 1993, 2 (01) : 51 - 54
  • [3] Boat TF., 1989, CYSTIC FIBROSIS META, V6th, P2649
  • [4] CARROLL TP, IN PRESS CELL PHYSL
  • [5] CHEHAB FF, 1991, AM J HUM GENET, V48, P223
  • [6] VARIABLE DELETION OF EXON-9 CODING SEQUENCES IN CYSTIC-FIBROSIS TRANSMEMBRANE CONDUCTANCE REGULATOR GENE MESSENGER-RNA TRANSCRIPTS IN NORMAL BRONCHIAL EPITHELIUM
    CHU, CS
    TRAPNELL, BC
    MURTAGH, JJ
    MOSS, J
    DALEMANS, W
    JALLAT, S
    MERCENIER, A
    PAVIRANI, A
    LECOCQ, JP
    CUTTING, GR
    GUGGINO, WB
    CRYSTAL, RG
    [J]. EMBO JOURNAL, 1991, 10 (06) : 1355 - 1363
  • [7] GENETIC-BASIS OF VARIABLE EXON-9 SKIPPING IN CYSTIC-FIBROSIS TRANSMEMBRANE CONDUCTANCE REGULATOR MESSENGER-RNA
    CHU, CS
    TRAPNELL, BC
    CURRISTIN, S
    CUTTING, GR
    CRYSTAL, RG
    [J]. NATURE GENETICS, 1993, 3 (02) : 151 - 156
  • [8] A CLUSTER OF CYSTIC-FIBROSIS MUTATIONS IN THE 1ST NUCLEOTIDE-BINDING FOLD OF THE CYSTIC-FIBROSIS CONDUCTANCE REGULATOR PROTEIN
    CUTTING, GR
    KASCH, LM
    ROSENSTEIN, BJ
    ZIELENSKI, J
    TSUI, LC
    ANTONARAKIS, SE
    KAZAZIAN, HH
    [J]. NATURE, 1990, 346 (6282) : 366 - 369
  • [9] MULTIPLE MUTATIONS IN HIGHLY CONSERVED RESIDUES ARE FOUND IN MILDLY AFFECTED CYSTIC-FIBROSIS PATIENTS
    DEAN, M
    WHITE, MB
    AMOS, J
    GERRARD, B
    STEWART, C
    KHAW, KT
    LEPPERT, M
    [J]. CELL, 1990, 61 (05) : 863 - 870
  • [10] DORK T, 1991, HUM GENET, V87, P441
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