MOLECULAR-BASIS AND EXPRESSION OF THE LW(A)/LW(B) BLOOD-GROUP POLYMORPHISM

被引：31

作者：

HERMAND, P

GANE, P

MATTEI, MG

SISTONEN, P

CARTRON, JP

BAILLY, P

机构：

[1] INST NATL TRANSFUS SANGUINE,INSERM,U76,F-75015 PARIS,FRANCE

[2] HOP ENFANTS LA TIMONE,INSERM,U242,F-13385 MARSEILLE,FRANCE

[3] FINNISH RED CROSS & BLOOD TRANSFUS SERV,SF-00310 HELSINKI,FINLAND

来源：

BLOOD | 1995年 / 86卷 / 04期

关键词：

D O I：

10.1182/blood.V86.4.1590.bloodjournal8641590

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

The Landsteiner-Wiener (LW) blood group antigens reside on a 42-kD erythrocyte membrane glycoprotein that has recently been cloned. Here, we found that the molecular basis for the LW(a)/LW(b) polymorphism is determined by a single base pair mutation (A308G) that correlates with a Pvu II restriction site and results in a Gln70Arg amino acid substitution. COS-7 cells transfected with LW(a) or LW(b) cDNAs reacted with human anti-LM(a) and anti-LW(b) sera, respectively, as well as with a murine monoclonal anti-LW(ab) antibody, as shown by flow cytometry analysis. Moreover, a 42-kD protein was immunoprecipitated from the transfected cells with the monoclonal anti-LW(ab) antibody. These findings indicate that LW(a) and LW(b) are alleles of the LW blood group locus as defined also by a monoclonal anti-LW(ab) of nonhuman origin, in addition, the LW locus has been assigned to chromosome 19p13.3 by in situ hybridization. Study by Southern blot analysis indicated also that the LW locus is composed of a single gene that was not grossly rearranged in rare LW(a-b-) and Rh-null individuals deficient for LW antigens. In addition, Pvu II restriction fragment-length polymorphism analysis indicated that these variants were all homozygous for a phenotypically silent LM(a) allele. (C) 1995 by The American Society of Hematology.

引用

页码：1590 / 1594

页数：5

共 50 条

[1] GENETIC-POLYMORPHISM OF THE LW BLOOD-GROUP SYSTEM
SISTONEN, P
GREEN, CA
LOMAS, CG
TIPPETT, P
ANNALS OF HUMAN GENETICS, 1983, 47 (OCT) : 277 - 284
[2] THE LW BLOOD-GROUP - A REVIEW
GILES, CM
IMMUNOLOGICAL COMMUNICATIONS, 1980, 9 (02): : 225 - 242
[3] MOLECULAR-BASIS AND PCR-DNA TYPING OF THE FYA/FYB BLOOD-GROUP POLYMORPHISM
TOURNAMILLE, C
KIM, CLV
GANE, P
CARTRON, JP
COLIN, Y
HUMAN GENETICS, 1995, 95 (04) : 407 - 410
[4] LINKAGE OF THE LW BLOOD-GROUP LOCUS WITH THE COMPLEMENT C-3 AND LUTHERAN BLOOD-GROUP LOCI
SISTONEN, P
ANNALS OF HUMAN GENETICS, 1984, 48 (JUL) : 239 - 242
[5] IMMUNOCHEMISTRY OF THE LEWIS BLOOD-GROUP SYSTEM .3. STUDIES ON THE MOLECULAR-BASIS OF THE LEX BLOOD-GROUP PROPERTY
HANFLAND, P
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[6] A NEW ALLELE GIVING FURTHER INSIGHT INTO THE LW BLOOD-GROUP SYSTEM
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TIPPETT, P
VOX SANGUINIS, 1982, 42 (05) : 252 - 255
[7] THE LW BLOOD-GROUP GLYCOPROTEIN IS HOMOLOGOUS TO INTERCELLULAR-ADHESION MOLECULES
BAILLY, P
HERMAND, P
CALLEBAUT, I
SONNEBORN, HH
KHAMLICHI, S
MORNON, JP
CARTRON, JP
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (12) : 5306 - 5310
[8] A NEW ALLELE GIVING FURTHER INSIGHT INTO THE LW BLOOD-GROUP SYSTEM
SISTONEN, P
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TRANSFUSION, 1982, 22 (05) : 425 - 425
[9] PROPERTIES OF THE BLOOD-GROUP LW GLYCOPROTEIN AND PRELIMINARY COMPARISON WITH RH PROTEINS
BLOY, C
BLANCHARD, D
HERMAND, P
KORDOWICZ, M
SONNEBORN, HH
CARTRON, JP
MOLECULAR IMMUNOLOGY, 1989, 26 (11) : 1013 - 1019
[10] Characterization of the gene encoding the human LW blood group protein in LW(+) and LW(-) phenotypes
Hermand, P
LePennec, PY
Rouger, P
Cartron, JP
Bailly, P
BLOOD, 1996, 87 (07) : 2962 - 2967

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