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ASSOCIATION AND LINKAGE ANALYSES OF RESTRICTION-FRAGMENT-LENGTH-POLYMORPHISMS FOR THE HUMAN RENIN AND ANTITHROMBIN-III GENES IN ESSENTIAL-HYPERTENSION

被引:54
作者
ZEE, RYL [1 ]
YING, LH [1 ]
MORRIS, BJ [1 ]
GRIFFITHS, LR [1 ]
机构
[1] UNIV SYDNEY, DEPT PHYSIOL, MOLEC BIOL & HYPERTENS LAB, BLDG F13, SYDNEY, NSW 2006, AUSTRALIA
来源
JOURNAL OF HYPERTENSION | 1991年 / 9卷 / 09期
关键词
ESSENTIAL HYPERTENSION; GENETICS; CHROMOSOME-1; RESTRICTION FRAGMENT LENGTH POLYMORPHISM; RENIN; ANTITHROMBIN-III; ASSOCIATION AND LINKAGE ANALYSES;
D O I
10.1097/00004872-199109000-00009
中图分类号
R6 [外科学];
学科分类号
1002 ; 100210 ;
摘要
Essential hypertension is a highly hereditable disorder in which genetic influences predominate over environmental factors. The molecular genetic profiles which predispose to essential hypertension are not known. In rats with genetic hypertension, there is some recent evidence pointing to linkage of renin gene alleles with blood pressure. The genes for renin and antithrombin III belong to a conserved synteny group which, in humans, spans the q2l.3-32.3 region of chromosome I and, in rats, is linkage group X on chromosome 13. The present study examined the association of particular human renin gene (REN) and antithrombin III gene (AT3) polymorphisms with essential hypertension by comparing the frequency of specific alleles for each of these genes in 50 hypertensive off spring of hypertensive parents and 91 normotensive off spring of normotensive parents. In addition, linkage relationships were examined in hypertensive pedigrees with multiple affected individuals. Alleles of a REN HindIII restriction fragment length polymorphism (RFLP) were detected using a genomic clone, lambda-HR5, to probe Southern blots of HindIII-cut leucocyte DNA, and those for an AT3 Pstl RFLP were detected by phATIII 113 complementary DNA probe. The frequencies of each REN allele in the hypertensive group were 0.76 and 0.24 compared with 0.74 and 0.26 in the normotensive group. For AT3, hypertensive allele frequencies were 0.49 and 0.51 compared with normotensive values of 0.54 and 0.46. These differences were not significant by chi-2 analysis (P > 0.2). Linkage analysis of a family (data from 16 family members, 10 of whom were hypertensive), informative for both markers, without an age-of-onset correction, and assuming dominant inheritance of hypertension, complete penetrance and a disease frequency of 20%, did not indicate linkage of REN with hypertension, but gave a positive, although not significant, logarithm of the odds for linkage score of 0.784 at a recombination fraction of 0 for AT3 linkage to hypertension. In conclusion, the present study could find no evidence for an association of a REN HindIII RFLP with essential hypertension or for a linkage of the locus defined by this RFLP in a family segregating for hypertension. In the case of an AT3 Pstl RFLP, although association analysis was negative, linkage analysis suggested possible involvement (odds of 6:1 in favour) of a gene located near the 1q23 locus with hypertension in one informative family.
引用
收藏
页码:825 / 830
页数:6
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