NH2-TERMINAL GLOBULAR DOMAIN OF HUMAN PLATELET GLYCOPROTEIN IB-ALPHA HAS A METHIONINE145/THREONINE145 AMINO-ACID POLYMORPHISM, WHICH IS ASSOCIATED WITH THE HPA-2 (KO) ALLOANTIGENS
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KUIJPERS, RWAM
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机构:NETHERLANDS RED CROSS,BLOOD TRANSFUS SERV,CENT LAB,PUBLICAT SECRETARIAT,POB 9406,1006 AK AMSTERDAM,NETHERLANDS
KUIJPERS, RWAM
FABER, NM
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FABER, NM
CUYPERS, HTM
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机构:NETHERLANDS RED CROSS,BLOOD TRANSFUS SERV,CENT LAB,PUBLICAT SECRETARIAT,POB 9406,1006 AK AMSTERDAM,NETHERLANDS
CUYPERS, HTM
OUWEHAND, WH
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OUWEHAND, WH
VONDEMBORNE, AEGK
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VONDEMBORNE, AEGK
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[1] NETHERLANDS RED CROSS,BLOOD TRANSFUS SERV,CENT LAB,PUBLICAT SECRETARIAT,POB 9406,1006 AK AMSTERDAM,NETHERLANDS
[2] UNIV AMSTERDAM,ACAD MED CTR,DEPT HAEMATOL,EXPTL & CLIN IMMUNOL LAB,1006 AK AMSTERDAM,NETHERLANDS
[3] UNIV AMSTERDAM,ACAD MED CTR,CTR BLOOD CELL RES,1006 AK AMSTERDAM,NETHERLANDS
The glycoprotein (GP) Ib/IX complex, a prominent platelet GP complex, is the primary receptor for vWF. Previously, we have established that an antigenic polymorphism of platelets, the HPA-2 or Ko alloantigen system, is located on the 45-kD amino-terminal globular domain of GPIb-alpha. With the polymerase chain reaction, we have amplified two segments of the GPIb-alpha gene coding for the first 382 amino acids of two HPA-2a and two HPA-2b homozygous individuals. Nucleotide sequence analysis revealed as the only difference a C-T polymorphism at position 434 of the coding region for the mature protein. This base change results in a substitution of threonine (ACG) in HPA-2a (Ko(b)) to methionine (ATG) in HPA-2b (Ko(a)) at amino acid position 145. The C-T polymorphism is reflected in a difference in restriction enzyme recognition, resulting in an Aha 2-site in the HPA-2b allele and a SfaN1 site in the HPA-2a allele. Restriction fragment length polymorphism analysis of the amplified DNA of 3 HPA-2(a-,b+), 2 HPA-2(a+,b+), and 11 HPA-2(a+,b-) donors showed that these restriction sites were associated with the HPA-2 alleles. DNA-typing for the HPA-2 alloantigen system on genomic DNA obtained from a small number of cells may be applied for determining the genotype of a fetus from an immunized mother or of severely thrombocytopenic patients.
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页码:381 / 384
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VONDEMBORNE AEG, 1978, BRIT J HAEMATOL, V61, P374