Evolution of the O alleles of the human ABO blood group gene

doi:10.1111/j.1537-2995.2004.03346.x

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Wiley InterScience

Transfusion

Volume 44 Issue 5, Pages 707 - 715

Published Online: 26 Apr 2004

The Journal of AABB

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IMMUNOHEMATOLOGY

Evolution of the O alleles of the human ABO blood group gene

Francis Roubinet , Stéphanie Despiau , Francesc Calafell , Fen Jin , Jaume Bertanpetit , Naruya Saitou , and Antoine Blancher

From the Laboratory of Molecular Immunology, Paul Sabatier University, Rangueil Hospital, 31403 Toulouse Cedex 4, France; the Laboratory of Immunohematology, French Establishment of Transfusion of the Pyrenes-Mediterranean, Toulouse Site, Avenue of Great Britain, BP 3210, 31027 Toulouse Cedex, France; Unit of Evolutionary Biology, Faculty of Health Life Sciences, Pompeu Fabra University, Doctor Aiguader, 80, 08003 Barcelona, Catalonia, Spain; the Institute of Genetics and Developmental Biology, Academia Sinica, Beijing, China; and the Division of Population Genetics, National Institute of Genetics, Mishima, 411-8540, Japan.

Correspondence to Antoine Blancher, MD, PhD, Laboratoire d'Immunogénétique Moléculaire, Université Paul Sabatier, Hôpital Rangueil, Faculte de Medicine Bâtiment A2, 133 Route de Norbonne, 31062 Toulouse Cedex 4, France; e-mail: blancher@easynet.fr.

This work was supported by funds from the Agence Française du Sang (Contract 97002551231) from the Etablissement Français du Sang and from the Ministère des Affaires Etrangères, France (Contract EA 3034).

ABSTRACT

BACKGROUND:

To date, at least 40 different alleles O have been characterized on the basis of exon 6 and exon 7 sequences but not always for intron 6.

STUDY DESIGN AND METHODS:

Among 415 individuals, from four continents (Africa, Europe, South America, and Asia), studied for exon 6 and exon 7 sequences, we selected 46 individuals (of respective phenotypes O [39], AB [3], B [3], or A [1]) for sequencing 1800-bp amplicons spanning exon 6, intron 6, and exon 7. The amplicons were characterized either by direct sequencing or after cloning when required.

RESULTS:

We defined 14 new intron 6 O allele sequences, including four recombinant alleles. Based on sequence comparison, a phylogenetic network was constructed. It confirmed recombinant allele origins and that most O alleles are derived by point mutations from the two worldwide distributed alleles O01 and O02.

CONCLUSION:

Allele O phylogenetic analysis suggests that the most frequent silencing mutation (deletion of a G in exon 6) appeared once in human evolution in the ancient O02 allele lineage and that allele O01 resulted from an interallele exchange between O02 and A101. Assuming constancy of evolutionary rate, diversification of the representative alleles of the three human ABO lineages (A101, B101, and O02) was estimated at 4.5 to 6 million years ago.

Received for publication October 27, 2003; revision received December 20, 2003, and accepted January 8, 2004.

DIGITAL OBJECT IDENTIFIER (DOI)

10.1111/j.1537-2995.2004.03346.x About DOI