Volume 56, Issue 1 pp. 244-248
BLOOD GROUP GENOMICS

Identification of six new RHCE variant alleles in individuals of diverse racial origin

Mindy Goldman

Mindy Goldman

Canadian Blood Services, Ottawa, Ontario, Canada

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Arantxa Cemborain

Arantxa Cemborain

Banco de Sangre y Tejidos De Navarra, Pamplona, Spain

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Jacqueline Cote

Jacqueline Cote

Canadian Blood Services, Ottawa, Ontario, Canada

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Rachid El Hamss

Rachid El Hamss

Progenika–Grifols, Medford, Massachusetts

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Robert L. Flower

Robert L. Flower

Australian Red Cross Blood Service, Brisbane, Australia

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Adirane Garaizar

Adirane Garaizar

Progenika–Grifols, Medford, Massachusetts

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Felix Garcia-Sanchez

Felix Garcia-Sanchez

Centro de Transfusion de Madrid, Madrid, Spain

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Catherine A. Hyland

Catherine A. Hyland

Australian Red Cross Blood Service, Brisbane, Australia

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Monica Kalvelage

Monica Kalvelage

LifeShare Blood Centers, Shreveport, Louisiana

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Donatella Londero

Donatella Londero

Azienda Ospedaliero Universitaria, Udine, Italy

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Genghis H. Lopez

Genghis H. Lopez

Australian Red Cross Blood Service, Brisbane, Australia

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Nicoletta Revelli

Nicoletta Revelli

Ospedale Maggiore Policlinico Fondazione IRCCS Ca’ Granda, Milano, Italy

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Pablo Rodriguez-Wilhelmi

Pablo Rodriguez-Wilhelmi

Banco de Sangre y Tejidos De Navarra, Pamplona, Spain

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Antonietta Villa

Antonietta Villa

Ospedale Maggiore Policlinico Fondazione IRCCS Ca’ Granda, Milano, Italy

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Gorka Ochoa-Garay

Corresponding Author

Gorka Ochoa-Garay

Grifols Shared Services, San Marcos, Texas

Address correspondence to: Gorka Ochoa-Garay, Grifols Shared Services, 201 Carlson Circle, San Marcos, TX 78666; e-mail: [email protected].Search for more papers by this author
First published: 04 October 2015
Citations: 5

The Australian government funds the Australian Red Cross Blood Service to provide blood, blood products, and services to the Australian community.

Abstract

BACKGROUND

The introduction of molecular methods into routine blood typing is prompting the identification of new blood group alleles. Discrepancies between the results of genotyping and serology or chance events uncovered during genotyping prompted additional investigations, which revealed six new RHCE variant alleles.

STUDY DESIGN AND METHODS

Samples from eight blood donors, two patients (one prenatal), and a patient's relative, all of diverse racial origin, were analyzed by standard serology methods, targeted genotyping arrays, DNA sequencing, and allele-specific polymerase chain reaction.

RESULTS

Six new RHCE alleles were identified, namely, RHCE*cE84A, RHCE*ce202G, RHCE*ce307T, RHCE*Ce377G, RHCE*ce697G,712G,733G,744C, and RHCE*Ce733G.

CONCLUSION

While implementation of new assays in commercial genotyping platforms to detect the polymorphisms reported here may not be justified given their apparent rarity, software interpretative algorithms may benefit from the identification of new alleles for a more accurate determination of genotypes and prediction of phenotypes.

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