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Studies on human low serum IgD phenotype and Gm markers
Author(s) -
Litwin S. D.,
TseEng D.,
Jr V. P. Butler,
Pernis B.
Publication year - 1985
Publication title -
clinical genetics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.543
H-Index - 102
eISSN - 1399-0004
pISSN - 0009-9163
DOI - 10.1111/j.1399-0004.1985.tb00200.x
Subject(s) - immunoglobulin d , phenotype , haplotype , biology , immunoglobulin e , genetics , immunology , microbiology and biotechnology , allele , antibody , gene , b cell
The human “low serum IgD phenotype” was studied by simultaneous Gm typing and IgD immunoassay of several populations. An association between Gm (f+b +) haplotype and low human IgD was confirmed and extended to the “low serum IgD phenotype” ‐ as defined from population distribution and genetic studies by Dunnette et al. 1978. Further, it was shown that Black American sera determined by Gm haplotype, had a similar percentage of “low serum IgD phenotype” samples (16%) although they lacked the “associated” Gm(f+b +) haplotype of White American samples. Sardinian sera showed a low incidence of the “low serum IgD phenotype” which was not correlated with Gm haplotype distribution. Familial aggregation of the “low serum IgD phenotype” was observed. No association was found between “low serum IgD phenotype” and serum IgE values. Age related abiotrophy of IgD could not be attributed to selective survival of “low serum IgD phenotype” persons.