SMIM1 underlies the Vel blood group and influences red blood cell traits

Ana Cvejic; Lonneke Haer-Wigman; Jonathan C. Stephens; Myrto Kostadima; Peter A. Smethurst; Mattia Frontini; Emile van den Akker; Paul Bertone; Ewa Bielczyk-Maczyńska; Samantha Farrow; Rudolf S. N. Fehrmann; Alan Gray; Masja de Haas; Vincent G. Haver; Gregory Jordan; Juha Karjalainen; Hindrik H. D. Kerstens; Graham Kiddle; Heather Lloyd-Jones; Malcolm Needs; Joyce Poole; Aicha Ait Soussan; Augusto Rendon; Klaus Rieneck; Jennifer G. Sambrook; Hein Schepers; Herman H. W. Silljé; Botond Sipos; Dorine Swinkels; Asif U. Tamuri; Niek Verweij; Nicholas A. Watkins; Harm-Jan Westra; Derek Stemple; Lude Franke; Nicole Soranzo; Hendrik G. Stunnenberg; Nick Goldman; Pim van der Harst; C. Ellen van der Schoot; Willem H. Ouwehand; Cornelis A. Albers

doi:https://doi.org/10.1038/ng.2603

SMIM1 underlies the Vel blood group and influences red blood cell traits

Ana Cvejic, Lonneke Haer-Wigman, Jonathan C. Stephens, Myrto Kostadima, Peter A. Smethurst, Mattia Frontini, Emile van den Akker, Paul Bertone, Ewa Bielczyk-Maczyńska, Samantha Farrow, Rudolf S. N. Fehrmann, Alan Gray, Masja de Haas, Vincent G. Haver, Gregory Jordan, Juha Karjalainen, Hindrik H. D. Kerstens, Graham Kiddle, Heather Lloyd-Jones, Malcolm NeedsJoyce Poole, Aicha Ait Soussan, Augusto Rendon, Klaus Rieneck, Jennifer G. Sambrook, Hein Schepers, Herman H. W. Silljé, Botond Sipos, Dorine Swinkels, Asif U. Tamuri, Niek Verweij, Nicholas A. Watkins, Harm-Jan Westra, Derek Stemple, Lude Franke, Nicole Soranzo, Hendrik G. Stunnenberg, Nick Goldman, Pim van der Harst, C. Ellen van der Schoot, Willem H. Ouwehand, Cornelis A. Albers

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

The blood group Vel was discovered 60 years ago, but the underlying gene is unknown. Individuals negative for the Vel antigen are rare and are required for the safe transfusion of patients with antibodies to Vel. To identify the responsible gene, we sequenced the exomes of five individuals negative for the Vel antigen and found that four were homozygous and one was heterozygous for a low-frequency 17-nucleotide frameshift deletion in the gene encoding the 78-amino-acid transmembrane protein SMIM1. A follow-up study showing that 59 of 64 Vel-negative individuals were homozygous for the same deletion and expression of the Vel antigen on SMIM1-transfected cells confirm SMIM1 as the gene underlying the Vel blood group. An expression quantitative trait locus (eQTL), the common SNP rs1175550 contributes to variable expression of the Vel antigen (P = 0.003) and influences the mean hemoglobin concentration of red blood cells (RBCs; P = 8.6 × 10(-15)). In vivo, zebrafish with smim1 knockdown showed a mild reduction in the number of RBCs, identifying SMIM1 as a new regulator of RBC formation. Our findings are of immediate relevance, as the homozygous presence of the deletion allows the unequivocal identification of Vel-negative blood donors

Original language	English
Pages (from-to)	542-545
Journal	Nature Genetics
Volume	45
Issue number	5
DOIs	https://doi.org/10.1038/ng.2603
Publication status	Published - 2013

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Cvejic, A., Haer-Wigman, L., Stephens, J. C., Kostadima, M., Smethurst, P. A., Frontini, M., van den Akker, E., Bertone, P., Bielczyk-Maczyńska, E., Farrow, S., Fehrmann, R. S. N., Gray, A., de Haas, M., Haver, V. G., Jordan, G., Karjalainen, J., Kerstens, H. H. D., Kiddle, G., Lloyd-Jones, H., ... Albers, C. A. (2013). SMIM1 underlies the Vel blood group and influences red blood cell traits. Nature Genetics, 45(5), 542-545. https://doi.org/10.1038/ng.2603

@article{8e02b1b8077e45e3946dfe106d644cda,

title = "SMIM1 underlies the Vel blood group and influences red blood cell traits",

abstract = "The blood group Vel was discovered 60 years ago, but the underlying gene is unknown. Individuals negative for the Vel antigen are rare and are required for the safe transfusion of patients with antibodies to Vel. To identify the responsible gene, we sequenced the exomes of five individuals negative for the Vel antigen and found that four were homozygous and one was heterozygous for a low-frequency 17-nucleotide frameshift deletion in the gene encoding the 78-amino-acid transmembrane protein SMIM1. A follow-up study showing that 59 of 64 Vel-negative individuals were homozygous for the same deletion and expression of the Vel antigen on SMIM1-transfected cells confirm SMIM1 as the gene underlying the Vel blood group. An expression quantitative trait locus (eQTL), the common SNP rs1175550 contributes to variable expression of the Vel antigen (P = 0.003) and influences the mean hemoglobin concentration of red blood cells (RBCs; P = 8.6 × 10(-15)). In vivo, zebrafish with smim1 knockdown showed a mild reduction in the number of RBCs, identifying SMIM1 as a new regulator of RBC formation. Our findings are of immediate relevance, as the homozygous presence of the deletion allows the unequivocal identification of Vel-negative blood donors",

author = "Ana Cvejic and Lonneke Haer-Wigman and Stephens, {Jonathan C.} and Myrto Kostadima and Smethurst, {Peter A.} and Mattia Frontini and {van den Akker}, Emile and Paul Bertone and Ewa Bielczyk-Maczy{\'n}ska and Samantha Farrow and Fehrmann, {Rudolf S. N.} and Alan Gray and {de Haas}, Masja and Haver, {Vincent G.} and Gregory Jordan and Juha Karjalainen and Kerstens, {Hindrik H. D.} and Graham Kiddle and Heather Lloyd-Jones and Malcolm Needs and Joyce Poole and Soussan, {Aicha Ait} and Augusto Rendon and Klaus Rieneck and Sambrook, {Jennifer G.} and Hein Schepers and Sillj{\'e}, {Herman H. W.} and Botond Sipos and Dorine Swinkels and Tamuri, {Asif U.} and Niek Verweij and Watkins, {Nicholas A.} and Harm-Jan Westra and Derek Stemple and Lude Franke and Nicole Soranzo and Stunnenberg, {Hendrik G.} and Nick Goldman and {van der Harst}, Pim and {van der Schoot}, {C. Ellen} and Ouwehand, {Willem H.} and Albers, {Cornelis A.}",

year = "2013",

doi = "https://doi.org/10.1038/ng.2603",

language = "English",

volume = "45",

pages = "542--545",

journal = "Nature Genetics",

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Cvejic, A, Haer-Wigman, L, Stephens, JC, Kostadima, M, Smethurst, PA, Frontini, M, van den Akker, E, Bertone, P, Bielczyk-Maczyńska, E, Farrow, S, Fehrmann, RSN, Gray, A, de Haas, M, Haver, VG, Jordan, G, Karjalainen, J, Kerstens, HHD, Kiddle, G, Lloyd-Jones, H, Needs, M, Poole, J, Soussan, AA, Rendon, A, Rieneck, K, Sambrook, JG, Schepers, H, Silljé, HHW, Sipos, B, Swinkels, D, Tamuri, AU, Verweij, N, Watkins, NA, Westra, H-J, Stemple, D, Franke, L, Soranzo, N, Stunnenberg, HG, Goldman, N, van der Harst, P, van der Schoot, CE, Ouwehand, WH & Albers, CA 2013, 'SMIM1 underlies the Vel blood group and influences red blood cell traits', Nature Genetics, vol. 45, no. 5, pp. 542-545. https://doi.org/10.1038/ng.2603

TY - JOUR

T1 - SMIM1 underlies the Vel blood group and influences red blood cell traits

AU - Cvejic, Ana

AU - Haer-Wigman, Lonneke

AU - Stephens, Jonathan C.

AU - Kostadima, Myrto

AU - Smethurst, Peter A.

AU - Frontini, Mattia

AU - van den Akker, Emile

AU - Bertone, Paul

AU - Bielczyk-Maczyńska, Ewa

AU - Farrow, Samantha

AU - Fehrmann, Rudolf S. N.

AU - Gray, Alan

AU - de Haas, Masja

AU - Haver, Vincent G.

AU - Jordan, Gregory

AU - Karjalainen, Juha

AU - Kerstens, Hindrik H. D.

AU - Kiddle, Graham

AU - Lloyd-Jones, Heather

AU - Needs, Malcolm

AU - Poole, Joyce

AU - Soussan, Aicha Ait

AU - Rendon, Augusto

AU - Rieneck, Klaus

AU - Sambrook, Jennifer G.

AU - Schepers, Hein

AU - Silljé, Herman H. W.

AU - Sipos, Botond

AU - Swinkels, Dorine

AU - Tamuri, Asif U.

AU - Verweij, Niek

AU - Watkins, Nicholas A.

AU - Westra, Harm-Jan

AU - Stemple, Derek

AU - Franke, Lude

AU - Soranzo, Nicole

AU - Stunnenberg, Hendrik G.

AU - Goldman, Nick

AU - van der Harst, Pim

AU - van der Schoot, C. Ellen

AU - Ouwehand, Willem H.

AU - Albers, Cornelis A.

PY - 2013

Y1 - 2013

N2 - The blood group Vel was discovered 60 years ago, but the underlying gene is unknown. Individuals negative for the Vel antigen are rare and are required for the safe transfusion of patients with antibodies to Vel. To identify the responsible gene, we sequenced the exomes of five individuals negative for the Vel antigen and found that four were homozygous and one was heterozygous for a low-frequency 17-nucleotide frameshift deletion in the gene encoding the 78-amino-acid transmembrane protein SMIM1. A follow-up study showing that 59 of 64 Vel-negative individuals were homozygous for the same deletion and expression of the Vel antigen on SMIM1-transfected cells confirm SMIM1 as the gene underlying the Vel blood group. An expression quantitative trait locus (eQTL), the common SNP rs1175550 contributes to variable expression of the Vel antigen (P = 0.003) and influences the mean hemoglobin concentration of red blood cells (RBCs; P = 8.6 × 10(-15)). In vivo, zebrafish with smim1 knockdown showed a mild reduction in the number of RBCs, identifying SMIM1 as a new regulator of RBC formation. Our findings are of immediate relevance, as the homozygous presence of the deletion allows the unequivocal identification of Vel-negative blood donors

AB - The blood group Vel was discovered 60 years ago, but the underlying gene is unknown. Individuals negative for the Vel antigen are rare and are required for the safe transfusion of patients with antibodies to Vel. To identify the responsible gene, we sequenced the exomes of five individuals negative for the Vel antigen and found that four were homozygous and one was heterozygous for a low-frequency 17-nucleotide frameshift deletion in the gene encoding the 78-amino-acid transmembrane protein SMIM1. A follow-up study showing that 59 of 64 Vel-negative individuals were homozygous for the same deletion and expression of the Vel antigen on SMIM1-transfected cells confirm SMIM1 as the gene underlying the Vel blood group. An expression quantitative trait locus (eQTL), the common SNP rs1175550 contributes to variable expression of the Vel antigen (P = 0.003) and influences the mean hemoglobin concentration of red blood cells (RBCs; P = 8.6 × 10(-15)). In vivo, zebrafish with smim1 knockdown showed a mild reduction in the number of RBCs, identifying SMIM1 as a new regulator of RBC formation. Our findings are of immediate relevance, as the homozygous presence of the deletion allows the unequivocal identification of Vel-negative blood donors

U2 - https://doi.org/10.1038/ng.2603

DO - https://doi.org/10.1038/ng.2603

M3 - Article

C2 - 23563608

SN - 1061-4036

VL - 45

SP - 542

EP - 545

JO - Nature Genetics

JF - Nature Genetics

IS - 5

ER -