THE INHERITANCE OF TYPE-I AND TYPE-III VONWILLEBRANDS DISEASE IN ISRAEL - LINKAGE ANALYSIS, CARRIER DETECTION AND PRENATAL-DIAGNOSIS USING 3 INTRAGENIC RESTRICTION-FRAGMENT-LENGTH-POLYMORPHISMS

被引：12

作者：

INBAL, A

KORNBROT, N

ZIVELIN, A

SHAKLAI, M

SELIGSOHN, U

机构：

[1] ICHILOV HOSP, TEL AVIV MED CTR, INST HAEMATOL, IL-64239 TEL AVIV, ISRAEL

[2] TEL AVIV UNIV, SACKLER SCH MED, TEL AVIV, ISRAEL

来源：

BLOOD COAGULATION & FIBRINOLYSIS | 1992年 / 3卷 / 02期

关键词：

VONWILLEBRANDS DISEASE; RLFP; CARRIER DETECTION; PRENATAL DIAGNOSIS;

D O I：

10.1097/00001721-199204000-00005

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Three intragenic restriction fragment length polymorphisms (RFLPs) were used to study linkage and analyse the mode of inheritance in type I and type III von Willebrand's disease (vWD). In two families linkage was established between Sac I RFLPs and the inheritance of type I vWD. RFLP analysis of amniocyte DNA from a potentially affected foetus enabled us to establish a prenatal diagnosis of vWD in a third family with type I vWD. Linkage was also established in four families between the Sac I and two Taq I RFLPs and the inheritance of type III vWD. All type III probands were homozygotes and inherited the same mutant vWF allele from both parents. Heterozygous carriers from one type III family were phenotypically normal and could be detected only by linkage analysis, whereas carriers from the remaining three type III families were asymptomatic but had decreased values of vWF antigen and activity. RFLP-based linkage analysis of vWD alleles provides a way to improve the diagnostic precision, detect carriers, and may be useful for prenatal diagnosis of type III vWD.

引用

页码：167 / 177

页数：11

共 59 条

[1]

ALLAIN JP, 1975, J LAB CLIN MED, V86, P152

[2]

BAHNAK BR, 1988, THROMB HAEMOSTASIS, V60, P178

[3]

BAHOU WF, 1988, BLOOD, V72, P308

[4] POLYMORPHIC DNA REGION ADJACENT TO THE 5'-END OF THE HUMAN INSULIN GENE [J].

BELL, GI ;

KARAM, JH ;

RUTTER, WJ .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1981, 78 (09) :5759-5763

[5]

BENARDI F, 1990, BLOOD, V75, P677

[6]

BENNETT B, 1972, J LAB CLIN MED, V80, P256

[7] A RELATIVELY HIGH-FREQUENCY OF SEVERE (TYPE-III) VONWILLEBRANDS DISEASE IN ISRAEL [J].

BERLINER, SA ;

SELIGSOHN, U ;

ZIVELIN, A ;

ZWANG, E ;

SOFFERMAN, G .

BRITISH JOURNAL OF HAEMATOLOGY, 1986, 62 (03) :535-543

[8] 2 TAQI RFLPS IN THE HUMAN VONWILLEBRAND-FACTOR GENE [J].

BERNARDI, F ;

MARCHETTI, G ;

BERTAGNOLO, V ;

FAGGIOLI, L ;

DELSENNO, L .

NUCLEIC ACIDS RESEARCH, 1987, 15 (03) :1347-1347

[9] CHARACTERIZATION OF POLYMORPHIC MARKERS IN THE VONWILLEBRAND-FACTOR GENE AND PSEUDOGENE [J].

BERNARDI, F ;

MARCHETTI, G ;

CASONATO, A ;

GEMMATI, D ;

PATRACCHINI, P ;

LEGNANI, C ;

DEROSA, V ;

GIROLAMI, A ;

CONCONI, F .

BRITISH JOURNAL OF HAEMATOLOGY, 1990, 74 (03) :282-289

[10] VONWILLEBRAND DISEASE INVESTIGATED BY 2 NOVEL RFLPS [J].

BERNARDI, F ;

GUERRA, S ;

PATRACCHINI, P ;

VOLINIA, S ;

BUZZONI, D ;

BALLERINI, G ;

CASONATO, A ;

MARCHETTI, G .

BRITISH JOURNAL OF HAEMATOLOGY, 1988, 68 (02) :243-248

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