Disruption of <i>SMIM1</i> causes the Vel− blood type

Ballif, Bryan A.; Helias, Virginie; Peyrard, Thierry; Ménanteau, Cècile; Saison, Carole; Lucien, Nicole; Bourgouin, Sébastien; Gall, Maude Le; Cartron, Jean‐Pierre; Arnaud, Lionel

doi:10.1002/emmm.201302466

Cited by 47 publications

(89 citation statements)

References 32 publications

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“…Nine of the 53 non-Alu SVs were found in the GYPA and GYPB genes, known to have a high rate of recombination and gene conversions. However, we noted that neither the 37-bp insertion characteristic of the RHD pseudogene 31 nor the 17-bp deletion in SMIM1 underlying the Vel-negative phenotype [32][33][34] were called in 1000G. While the former allele was still detected because of a downstream stop codon (p.Tyr269Ter), the latter remained invisible.…”

Section: Structural Variants and Indelsmentioning

confidence: 94%

Erythrogene: a database for in-depth analysis of the extensive variation in 36 blood group systems in the 1000 Genomes Project

et al. 2016

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Section: Structural Variants and Indelsmentioning

confidence: 94%

Erythrogene: a database for in-depth analysis of the extensive variation in 36 blood group systems in the 1000 Genomes Project

et al. 2016

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“…Encouraged by our recent success in elucidating the molecular bases of 3 other long-sought-after blood group antigens, [6][7][8] we decided to reinvestigate the case of this French woman.…”

Section: Introductionmentioning

confidence: 99%

Lack of the nucleoside transporter ENT1 results in the Augustine-null blood type and ectopic mineralization

Daniels

Ballif

Helias

et al. 2015

Blood

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“…In 2013 different groups reported the genetic basis of the Vel- blood type [4,5,6]. A 17 bp frame-shift deletion (64-80del) in the coding region of the SMIM1 gene was homozygous in all Vel- samples.…”

Section: Introductionmentioning

confidence: 99%

“…A 17 bp frame-shift deletion (64-80del) in the coding region of the SMIM1 gene was homozygous in all Vel- samples. The reduced or weak expression of the Vel antigen was associated with a heterozygous 64-80del genotype [4,5]. The International Society of Blood Transfusion (ISBT) Working Party for Red Cell Immunogenetics and Blood Group Terminology assigned the blood group system name VEL and number 034 and promoted Vel from a genetically unresolved blood group antigen (ISBT number 212001) to the new system defined by the SMIM1 locus (antigen number 034001).…”

Section: Introductionmentioning

confidence: 99%

Molecular Screening for Vel- Blood Donors in Southwestern Germany

Wieckhusen

Rink

Scharberg

et al. 2015

Transfus Med Hemother

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Background: The SMIM1 protein carries the Vel blood group antigen, and homozygosity for a 17 bp deletion in the coding region of the SMIM1 gene represents the molecular basis of the Vel- blood group phenotype. We developed PCR-based methods for typing the SMIM1 17 bp (64-80del) gene deletion and performed a molecular screening for the Vel- blood type in German blood donors. Methods: For SMIM1 genotyping, TaqMan-PCR and PCR-SSP methods were developed and validated using reference samples. Both methods were used for screening of donors with blood group O from southwestern Germany. Heterozygotes and homozygotes for the SMIM1 64-80del allele were serologically typed for the Vel blood group antigen. In addition, the rs1175550 SNP in SMIM1 was typed and correlated to the results of the phenotyping. Results: Both genotyping methods, TaqMan-PCR and PCR-SSP, represent reliable methods for the detection of the SMIM1 64-80del allele. Screening of 10,598 blood group O donors revealed 5 individuals homozygous for the deletional allele. They were confirmed Vel- by serological typing. Heterozygotes for the 64-80del allele showed different antigen expressions ranging from very weak to regular positive. Conclusion: Molecular screening of blood donors for the Vel- blood type is feasible and avoids the limitations of serological typing which might show false-negative results with heterozygous individuals. The identification of Vel- blood donors significantly contributes to the adequate blood supply of patients with anti-Vel.

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Disruption of SMIM1 causes the Vel− blood type

Cited by 47 publications

References 32 publications

Erythrogene: a database for in-depth analysis of the extensive variation in 36 blood group systems in the 1000 Genomes Project

Erythrogene: a database for in-depth analysis of the extensive variation in 36 blood group systems in the 1000 Genomes Project

Lack of the nucleoside transporter ENT1 results in the Augustine-null blood type and ectopic mineralization

Molecular Screening for Vel- Blood Donors in Southwestern Germany

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