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A new SEMA7A variant found in Native Americans with alloantibody
Author(s) -
Richard M.,
StLaurent J.,
Perreault J.,
Long A.,
StLouis M.
Publication year - 2011
Publication title -
vox sanguinis
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.68
H-Index - 83
eISSN - 1423-0410
pISSN - 0042-9007
DOI - 10.1111/j.1423-0410.2010.01413.x
Subject(s) - antibody , biology , exon , recombinant dna , antigen , microbiology and biotechnology , genetics , gene
Background and Objectives  John Milton Hagen (JMH) antigens are carried by Semaphorin 7A that plays important roles in the nervous system and the immune responses. Its role on the erythrocytes is unclear. Over the years, few samples were referred to our Immunohaematology Reference Laboratory to elucidate their JMH status. Materials and Methods  Seven blood samples with antibodies compatible with JMH1‐negative red cells were studied at the molecular level to identify polymorphisms and explain the JMH diversity observed. Four samples were of Native American background and three were Caucasians. Molecular analyses of the SEMA7A were undertaken, and soluble form of recombinant Sema7A proteins was produced to characterize the antibodies. Results  Sequencing of the cDNA showed a polymorphism in SEMA7A exon 9 at position 1040 (G>T) in the four Native American samples. Caucasians had a normal sequence. This polymorphism precludes a change at position 347 where an Arg is replaced by a Leu. Plasma was assayed in ELISA on wild‐type Sema7A Arg347 and variant Sema7A Leu347 proteins. Results clearly indicated a specific recognition of the antibody produced by the Native Americans for the wild‐type Sema7A Arg347 protein and not the variant one. Conclusion  A new SEMA7A variant was identified in this study. The antibody present in the Native American plasma samples should be considered as an alloantibody because it recognizes the wild‐type protein.

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