Your search keyword '"Asparagine genetics"' showing total 2 results

1. Hb Nancy and Hb Osler: two distinct genetic variants with identical clinical and hemoglobin phenotype.

Author

Préhu C, Godart C, Vigneron C, and Wajcman H

Subjects

Asparagine genetics, Aspartic Acid genetics, Base Sequence, Black People genetics, Codon, France, Globins genetics, Hemoglobins, Abnormal chemistry, Humans, Phenotype, Polymerase Chain Reaction, Tyrosine genetics, United States, White People genetics, Black or African American, Hemoglobins, Abnormal genetics

Abstract

Three hemoglobin variants (Hb Nancy, Osler and Fort Gordon), carrying the same Tyr-->Asp substitution at position beta 145 (HC2), have been independently described in 1975 in patients with marked polycythemia. The first one was found in a French caucasian family from Lorraine, and the two others in African Americans. Two unrelated individuals with Hb Osler have been recently reinvestigated at the DNA level and surprisingly, in their beta gene, codon 145 was found to be AAT which encodes for asparagine and not for aspartic acid, the aspartate at the protein level resulting, thus, from a very efficient posttranslational event. We reinvestigated a patient from the family of Hb Nancy and found that codon 145 was GAT, encoding for aspartate. This demonstrates that Hb Nancy is genetically distinct from Hb Osler despite an almost identical phenotype.

Published

1998

2. Assessment of French patients with LPL deficiency for French Canadian mutations.

Author

Foubert L, De Gennes JL, Lagarde JP, Ehrenborg E, Raisonnier A, Girardet JP, Hayden MR, and Benlian P

Subjects

Alleles, Asparagine genetics, Aspartic Acid genetics, Canada, Female, France ethnology, Glycine genetics, Humans, Male, Pedigree, Lipoprotein Lipase genetics, Point Mutation

Abstract

Mutations in the LPL gene show high levels of allelic heterogeneity between and within different populations. Complete LPL deficiency has a very high prevalence in French Canadians, where only three missense mutations account for > 97% of cases, most consistent with founder mutations introduced early in Quebec by French immigrants. In order to determine whether these mutations were present in France, 12 unrelated French families with defined LPL deficiency were investigated for the presence of the mutations found in French Canadians. Of the 24 expected alleles, six (25%) represented mutations in French Canadians (Gly188Glu four alleles, Asp250Asn and Pro207Leu one allele each). Comparison of French Canadian and French alleles identified the same haplotype in all carriers of the Gly188Glu and of the Asp250Asn, suggesting a common origin. In contrast, the Pro207Leu occurred on different haplotypes in France and Quebec, compatible with a different ancestral origin.

Published

1997