Erythroid urea transporter deficiency due to novel JK(null) alleles

Wester, Elisabet S; Johnson, Susan T; Copeland, Tama; Malde, Ranjan; Lee, Edmond; Storry, Jill R; Olsson, Martin L

Erythroid urea transporter deficiency due to novel JK(null) alleles

Mark

Wester, Elisabet S ; Johnson, Susan T ; Copeland, Tama ; Malde, Ranjan ; Lee, Edmond ; Storry, Jill R and Olsson, Martin L ^LU

(2008) In Transfusion 48(2). p.365-372

Abstract: BACKGROUND: The Kidd blood group antigens Jk(a) and Jk(b) are encoded by the red blood cell (RBC) urea transporter gene. Homozygosity for silent JK alleles results in the rare Jk(a-b-) phenotype. To date, seven JK(null) alleles have been identified, and of these, two are more frequent in the Polynesians and Finns. This study reports the identification of other JK(null) alleles in Jk(a-b-) individuals of different ethnic or geographic origins. STUDY DESIGN AND METHODS: Nine Jk(a-b-) samples and a sample from a Jk(a-b+) mother of a Jk(a+b-) baby were investigated. Polymerase chain reaction amplification and sequence analysis of the JK gene was performed. Western blotting and urea lysis were used to confirm Jk(a-b-) RBCs. RESULTS: Four novel... (More); BACKGROUND: The Kidd blood group antigens Jk(a) and Jk(b) are encoded by the red blood cell (RBC) urea transporter gene. Homozygosity for silent JK alleles results in the rare Jk(a-b-) phenotype. To date, seven JK(null) alleles have been identified, and of these, two are more frequent in the Polynesians and Finns. This study reports the identification of other JK(null) alleles in Jk(a-b-) individuals of different ethnic or geographic origins. STUDY DESIGN AND METHODS: Nine Jk(a-b-) samples and a sample from a Jk(a-b+) mother of a Jk(a+b-) baby were investigated. Polymerase chain reaction amplification and sequence analysis of the JK gene was performed. Western blotting and urea lysis were used to confirm Jk(a-b-) RBCs. RESULTS: Four novel alleles were identified: two different nonsense mutations, 202C > T (Gln68Stop) and 723delA (Ile262Stop) were identified on otherwise consensus JK*1 and JK*2 alleles, respectively. A missense mutation, 956C > T (Thr319Met), was identified in a JK*1 allele from an African-American and a JK*2 allele in two people of subcontinental Indian descent. Immunoblotting and urea lysis confirmed absence of JK glycoprotein in RBC membranes from a sample carrying the 956C > T mutation. Other previously described JK(null) mutations were found in samples of origins other than in which they were first identified. CONCLUSION: The molecular bases of the Jk(a-b-) phenotype are diverse and this is the first report of JK(null) alleles in individuals of African and subcontinental Indian descent. Although rare, these alleles should be taken into consideration when planning genotyping strategies for blood donors and patients. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1198878

author

Wester, Elisabet S ; Johnson, Susan T ; Copeland, Tama ; Malde, Ranjan ; Lee, Edmond ; Storry, Jill R and Olsson, Martin L ^LU

organization

publishing date

2008

type

Contribution to journal

publication status

published

subject

Hematology

in

Transfusion

volume

48

issue

2

pages

365 - 372

publisher

Wiley-Blackwell

external identifiers

wos:000252589400022
scopus:38349184783
pmid:18028269

ISSN

1537-2995

DOI

10.1111/j.1537-2995.2007.01532.x

language

English

LU publication?

yes

id

36649cf9-a7ce-4ae5-8551-30ee1e97176a (old id 1198878)

date added to LUP

2016-04-01 15:05:52

date last changed

2022-01-28 04:32:02

@article{36649cf9-a7ce-4ae5-8551-30ee1e97176a,
  abstract     = {{BACKGROUND: The Kidd blood group antigens Jk(a) and Jk(b) are encoded by the red blood cell (RBC) urea transporter gene. Homozygosity for silent JK alleles results in the rare Jk(a-b-) phenotype. To date, seven JK(null) alleles have been identified, and of these, two are more frequent in the Polynesians and Finns. This study reports the identification of other JK(null) alleles in Jk(a-b-) individuals of different ethnic or geographic origins. STUDY DESIGN AND METHODS: Nine Jk(a-b-) samples and a sample from a Jk(a-b+) mother of a Jk(a+b-) baby were investigated. Polymerase chain reaction amplification and sequence analysis of the JK gene was performed. Western blotting and urea lysis were used to confirm Jk(a-b-) RBCs. RESULTS: Four novel alleles were identified: two different nonsense mutations, 202C &gt; T (Gln68Stop) and 723delA (Ile262Stop) were identified on otherwise consensus JK*1 and JK*2 alleles, respectively. A missense mutation, 956C &gt; T (Thr319Met), was identified in a JK*1 allele from an African-American and a JK*2 allele in two people of subcontinental Indian descent. Immunoblotting and urea lysis confirmed absence of JK glycoprotein in RBC membranes from a sample carrying the 956C &gt; T mutation. Other previously described JK(null) mutations were found in samples of origins other than in which they were first identified. CONCLUSION: The molecular bases of the Jk(a-b-) phenotype are diverse and this is the first report of JK(null) alleles in individuals of African and subcontinental Indian descent. Although rare, these alleles should be taken into consideration when planning genotyping strategies for blood donors and patients.}},
  author       = {{Wester, Elisabet S and Johnson, Susan T and Copeland, Tama and Malde, Ranjan and Lee, Edmond and Storry, Jill R and Olsson, Martin L}},
  issn         = {{1537-2995}},
  language     = {{eng}},
  number       = {{2}},
  pages        = {{365--372}},
  publisher    = {{Wiley-Blackwell}},
  series       = {{Transfusion}},
  title        = {{Erythroid urea transporter deficiency due to novel JK(null) alleles}},
  url          = {{http://dx.doi.org/10.1111/j.1537-2995.2007.01532.x}},
  doi          = {{10.1111/j.1537-2995.2007.01532.x}},
  volume       = {{48}},
  year         = {{2008}},
}

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Erythroid urea transporter deficiency due to novel JK(null) alleles