RETINITIS-PIGMENTOSA FAMILIES SHOWING APPARENT X-LINKED INHERITANCE BUT UNLINKED TO THE RP2 OR RP3 LOCI

被引:6
作者
ALDRED, MA
TEAGUE, PW
JAY, M
BUNDEY, S
REDMOND, RM
JAY, B
BIRD, AC
BHATTACHARYA, SS
WRIGHT, AF
机构
[1] WESTERN GEN HOSP, MRC, HUMAN GENET UNIT, EDINBURGH EH4 2XU, MIDLOTHIAN, SCOTLAND
[2] UNIV LONDON, MOORFIELDS EYE HOSP, DEPT CLIN OPHTHALMOL, LONDON EC1V 2PD, ENGLAND
[3] BIRMINGHAM MATERNITY HOSP, CLIN GENET UNIT, BIRMINGHAM B15 2TG, W MIDLANDS, ENGLAND
[4] QUEENS UNIV BELFAST, BELFAST CITY HOSP, DEPT OPHTHALMOL, BELFAST BT9 7AB, ANTRIM, NORTH IRELAND
[5] QUEENS UNIV BELFAST, BELFAST CITY HOSP, DEPT MED GENET, BELFAST BT9 7AB, ANTRIM, NORTH IRELAND
[6] INST OPHTHALMOL, DEPT MOLEC GENET, LONDON EC1V 9EL, ENGLAND
来源
JOURNAL OF MEDICAL GENETICS | 1994年 / 31卷 / 11期
关键词
D O I
10.1136/jmg.31.11.848
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Three families with retinitis pigmentosa (RP) are described in which the disorder shows apparent X linked inheritance but does not show linkage to the RP2 and RP3 regions of the short arm of the X chromosome. The families are also inconsistent with a localisation of the disease gene between DXS164 and DXS28. In one case, reassessment of the family in the light of these results suggested that the family may have an autosomal dominant form of RP. The remaining two families are consistent with X linkage and suggest the possibility of a new X Linked RP (XLRP) locus. These families highlight the difficulties in determining the mode of inheritance on the basis of pedigree structure and clinical data alone. Molecular genetics plays an important role in confirming the mode of inheritance and in detecting potential misclassifications, particularly in a group of disorders as heterogeneous as RP. They emphasise that caution is required in genetic counselling of RP families, particularly in the absence of any molecular genetic analysis.
引用
收藏
页码:848 / 852
页数:5
相关论文
共 24 条
  • [1] LINKAGE ANALYSIS IN X-LINKED CONGENITAL STATIONARY NIGHT BLINDNESS
    ALDRED, MA
    DRY, KL
    SHARP, DM
    VANDORP, DB
    BROWN, J
    HARDWICK, LJ
    LESTER, DH
    PRYDE, FE
    TEAGUE, PW
    JAY, M
    BIRD, AC
    JAY, B
    WRIGHT, AF
    [J]. GENOMICS, 1992, 14 (01) : 99 - 104
  • [2] ARVEILER B, 1990, AM J HUM GENET, V46, P906
  • [3] GERMLINE MOSAICISM AND DUCHENNE MUSCULAR-DYSTROPHY MUTATIONS
    BAKKER, E
    VAN BROECKHOVEN, C
    BONTEN, EJ
    VANDEVOOREN, MJ
    VEENEMA, H
    VANHUL, W
    VANOMMEN, GJB
    VANDENBERGHE, A
    PEARSON, PL
    [J]. NATURE, 1987, 329 (6139) : 554 - 556
  • [4] A STUDY OF RETINITIS PIGMENTOSA IN THE CITY OF BIRMINGHAM .2. CLINICAL AND GENETIC-HETEROGENEITY
    BUNDEY, S
    CREWS, SJ
    [J]. JOURNAL OF MEDICAL GENETICS, 1984, 21 (06) : 421 - 428
  • [5] DUCHENNE MUSCULAR-DYSTROPHY WITH ADRENAL INSUFFICIENCY AND GLYCEROL KINASE-DEFICIENCY - HIGH-RESOLUTION CYTOGENETIC ANALYSIS WITH MOLECULAR, BIOCHEMICAL, AND CLINICAL-STUDIES
    CLARKE, A
    ROBERTS, SH
    THOMAS, NST
    WHITFIELD, A
    WILLIAMS, J
    HARPER, PS
    [J]. JOURNAL OF MEDICAL GENETICS, 1986, 23 (06) : 501 - 508
  • [6] COLEMAN M, 1990, AM J HUM GENET, V47, P935
  • [7] A PARTIAL DELETION OF THE MUSCULAR-DYSTROPHY GENE TRANSMITTED TWICE BY AN UNAFFECTED MALE
    DARRAS, BT
    FRANCKE, U
    [J]. NATURE, 1987, 329 (6139) : 556 - 558
  • [8] ANALYSIS OF LINKAGE RELATIONSHIPS OF X-LINKED RETINITIS PIGMENTOSA WITH THE FOLLOWING XP LOCI - L1.28, OTC, 754, XJ-1.1, PERT87, AND C7
    DENTON, MJ
    CHEN, JD
    SERRAVALLE, S
    COLLEY, P
    HALLIDAY, FB
    DONALD, J
    [J]. HUMAN GENETICS, 1988, 78 (01) : 60 - 64
  • [9] XP21 DNA MICRODELETION IN A PATIENT WITH CHRONIC GRANULOMATOUS-DISEASE, RETINITIS PIGMENTOSA, AND MCLEOD PHENOTYPE
    DESTBASILE, G
    BOHLER, MC
    FISCHER, A
    CARTRON, J
    DUFIER, JL
    GRISCELLI, C
    ORKIN, SH
    [J]. HUMAN GENETICS, 1988, 80 (01) : 85 - 89
  • [10] FRANCKE U, 1985, AM J HUM GENET, V37, P250
123