High-Throughput Next-Generation Sequencing of the Kidd Blood Group: Unexpected Antigen Expression Properties of Four Alleles and Detection of Novel Variants

BACKGROUND: The blood supply for patients with foreign ethnic backgrounds can be challenging, as they often have blood group and HPA patterns that differ from the variants prevalent in the German population. In addition, hemoglobinopathies requiring regular blood transfusion may be more common in su...

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Autores principales: Vorholt, Stephanie M., Lenz, Veronika, Just, Burkhard, Enczmann, Jürgen, Fischer, Johannes C., Horn, Peter A., Zeiler, Thomas A., Balz, Vera
Formato: Online Artículo Texto
Lenguaje:English
Publicado: S. Karger AG 2022
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9911998/
https://www.ncbi.nlm.nih.gov/pubmed/36818776
http://dx.doi.org/10.1159/000525326
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author Vorholt, Stephanie M.
Lenz, Veronika
Just, Burkhard
Enczmann, Jürgen
Fischer, Johannes C.
Horn, Peter A.
Zeiler, Thomas A.
Balz, Vera
author_facet Vorholt, Stephanie M.
Lenz, Veronika
Just, Burkhard
Enczmann, Jürgen
Fischer, Johannes C.
Horn, Peter A.
Zeiler, Thomas A.
Balz, Vera
author_sort Vorholt, Stephanie M.
collection PubMed
description BACKGROUND: The blood supply for patients with foreign ethnic backgrounds can be challenging, as they often have blood group and HPA patterns that differ from the variants prevalent in the German population. In addition, hemoglobinopathies requiring regular blood transfusion may be more common in such populations. High-throughput genotyping tests can facilitate the identification of the most compatible blood products, thereby reducing the risk of transfusion reactions. The present study reports the results of a molecular study for the Kidd (JK) blood group. Allele frequencies and antigen prevalence data are presented for >8,000 individuals of various origins. MATERIAL AND METHODS: More than 8,000 blood donors were genotyped for 22 blood group systems and 5 HPA genes using an amplicon-based next-generation sequencing (NGS) approach. As part of the test system, we focused on the JK system in more detail. Double-ARMS PCR analysis was performed for the haplotype phasing of the JK1/JK2 and two more common synonymous polymorphisms. We performed transcript analysis to detect potential alternative splice products. For a subset of samples, a comparison between serotype and red cell genotype was conducted. Allele frequencies were determined for geographically different panels of individuals. RESULTS: We successfully genotyped the JK blood group for 99.6% of the samples. Haplotype phasing revealed 96 different alleles. For several alleles that carry one of the synonymous SNVs c.588A>G and c.810G>A, we could not confirm the reported JK phenotypes. We found a higher frequency of JK:1 alleles for all populations except Iraqis. JK*01W.01 alleles were more common in the Asian groups and sub-Saharan Africans. A variant of the allele JK*02N.01 was present exclusively in Southeast Asians. CONCLUSION: Genotyping for JK antigens with a targeted NGS assay can easily be performed in routine. The interpretation that c.588A>G leads to a weak phenotype and c.810G>A to a null phenotype is questionable. IDs as well as the descriptions of alleles carrying these SNVs should be revised in the ISBT JK table.
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spelling pubmed-99119982023-02-16 High-Throughput Next-Generation Sequencing of the Kidd Blood Group: Unexpected Antigen Expression Properties of Four Alleles and Detection of Novel Variants Vorholt, Stephanie M. Lenz, Veronika Just, Burkhard Enczmann, Jürgen Fischer, Johannes C. Horn, Peter A. Zeiler, Thomas A. Balz, Vera Transfus Med Hemother Research Article BACKGROUND: The blood supply for patients with foreign ethnic backgrounds can be challenging, as they often have blood group and HPA patterns that differ from the variants prevalent in the German population. In addition, hemoglobinopathies requiring regular blood transfusion may be more common in such populations. High-throughput genotyping tests can facilitate the identification of the most compatible blood products, thereby reducing the risk of transfusion reactions. The present study reports the results of a molecular study for the Kidd (JK) blood group. Allele frequencies and antigen prevalence data are presented for >8,000 individuals of various origins. MATERIAL AND METHODS: More than 8,000 blood donors were genotyped for 22 blood group systems and 5 HPA genes using an amplicon-based next-generation sequencing (NGS) approach. As part of the test system, we focused on the JK system in more detail. Double-ARMS PCR analysis was performed for the haplotype phasing of the JK1/JK2 and two more common synonymous polymorphisms. We performed transcript analysis to detect potential alternative splice products. For a subset of samples, a comparison between serotype and red cell genotype was conducted. Allele frequencies were determined for geographically different panels of individuals. RESULTS: We successfully genotyped the JK blood group for 99.6% of the samples. Haplotype phasing revealed 96 different alleles. For several alleles that carry one of the synonymous SNVs c.588A>G and c.810G>A, we could not confirm the reported JK phenotypes. We found a higher frequency of JK:1 alleles for all populations except Iraqis. JK*01W.01 alleles were more common in the Asian groups and sub-Saharan Africans. A variant of the allele JK*02N.01 was present exclusively in Southeast Asians. CONCLUSION: Genotyping for JK antigens with a targeted NGS assay can easily be performed in routine. The interpretation that c.588A>G leads to a weak phenotype and c.810G>A to a null phenotype is questionable. IDs as well as the descriptions of alleles carrying these SNVs should be revised in the ISBT JK table. S. Karger AG 2022-07-26 /pmc/articles/PMC9911998/ /pubmed/36818776 http://dx.doi.org/10.1159/000525326 Text en Copyright © 2022 by The Author(s). Published by S. Karger AG, Basel https://creativecommons.org/licenses/by/4.0/This article is licensed under the Creative Commons Attribution 4.0 International License (CC BY). Usage, derivative works and distribution are permitted provided that proper credit is given to the author and the original publisher.
spellingShingle Research Article
Vorholt, Stephanie M.
Lenz, Veronika
Just, Burkhard
Enczmann, Jürgen
Fischer, Johannes C.
Horn, Peter A.
Zeiler, Thomas A.
Balz, Vera
High-Throughput Next-Generation Sequencing of the Kidd Blood Group: Unexpected Antigen Expression Properties of Four Alleles and Detection of Novel Variants
title High-Throughput Next-Generation Sequencing of the Kidd Blood Group: Unexpected Antigen Expression Properties of Four Alleles and Detection of Novel Variants
title_full High-Throughput Next-Generation Sequencing of the Kidd Blood Group: Unexpected Antigen Expression Properties of Four Alleles and Detection of Novel Variants
title_fullStr High-Throughput Next-Generation Sequencing of the Kidd Blood Group: Unexpected Antigen Expression Properties of Four Alleles and Detection of Novel Variants
title_full_unstemmed High-Throughput Next-Generation Sequencing of the Kidd Blood Group: Unexpected Antigen Expression Properties of Four Alleles and Detection of Novel Variants
title_short High-Throughput Next-Generation Sequencing of the Kidd Blood Group: Unexpected Antigen Expression Properties of Four Alleles and Detection of Novel Variants
title_sort high-throughput next-generation sequencing of the kidd blood group: unexpected antigen expression properties of four alleles and detection of novel variants
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9911998/
https://www.ncbi.nlm.nih.gov/pubmed/36818776
http://dx.doi.org/10.1159/000525326
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