Dimerization of small integral membrane protein 1 promotes cell surface presentation of the Vel blood group epitope

Liam P. Kelley; Anja Nylander; Lionel Arnaud; Anna M. Schmoker; Riley M. St. Clair; Lindsey A. Gleason; Jessica M. Souza; Jill R. Storry; Martin L. Olsson; Bryan A. Ballif

doi:10.1002/1873-3468.13726

Dimerization of small integral membrane protein 1 promotes cell surface presentation of the Vel blood group epitope

Liam P. Kelley, Anja Nylander, Lionel Arnaud, Anna M. Schmoker, Riley M. St. Clair, Lindsey A. Gleason, Jessica M. Souza, Jill R. Storry, Martin L. Olsson, Bryan A. Ballif

Forskningsoutput: Tidskriftsbidrag › Artikel i vetenskaplig tidskrift › Peer review

Sammanfattning

The Vel blood group antigen is carried on the short extracellular segment of the 78-amino-acid-long, type II transmembrane protein SMIM1 of unknown function. Here, using biochemical analysis and flow cytometry of cells expressing wild-type and mutant alleles of SMIM1, we demonstrate that dimerization of SMIM1 promotes cell surface display of the Vel epitope. We show that SMIM1 dimerization is mediated both by an extracellular Cys77-dependent, homomeric disulfide linkage and via a GxxxG helix–helix interaction motif in the transmembrane domain. These results provide important context for the observed variability in reactivity patterns of clinically important anti-Vel identified in patient sera.

Originalspråk	engelska
Sidor (från-till)	1261-1270
Antal sidor	10
Tidskrift	FEBS Letters
Volym	594
Nummer	8
Tidigt onlinedatum	2019
DOI	https://doi.org/10.1002/1873-3468.13726
Status	Published - 2020 apr.

Ämnesklassifikation (UKÄ)

Immunologi inom det medicinska området

Tillgång till dokument

10.1002/1873-3468.13726

Further investigation into the structure and function of SMIM1, a newly discovered erythroid transmembrane protein
Nylander, A., Olsson, M. L., Flygare, J. & Allhorn, M.
2016/05/01 → …
Projekt: Avhandling

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title = "Dimerization of small integral membrane protein 1 promotes cell surface presentation of the Vel blood group epitope",

abstract = "The Vel blood group antigen is carried on the short extracellular segment of the 78-amino-acid-long, type II transmembrane protein SMIM1 of unknown function. Here, using biochemical analysis and flow cytometry of cells expressing wild-type and mutant alleles of SMIM1, we demonstrate that dimerization of SMIM1 promotes cell surface display of the Vel epitope. We show that SMIM1 dimerization is mediated both by an extracellular Cys77-dependent, homomeric disulfide linkage and via a GxxxG helix–helix interaction motif in the transmembrane domain. These results provide important context for the observed variability in reactivity patterns of clinically important anti-Vel identified in patient sera.",

keywords = "disulfide bond, GxxxG, SMIM1, transfusion medicine, Vel blood group system",

author = "Kelley, {Liam P.} and Anja Nylander and Lionel Arnaud and Schmoker, {Anna M.} and {St. Clair}, {Riley M.} and Gleason, {Lindsey A.} and Souza, {Jessica M.} and Storry, {Jill R.} and Olsson, {Martin L.} and Ballif, {Bryan A.}",

year = "2020",

month = apr,

doi = "10.1002/1873-3468.13726",

language = "English",

volume = "594",

pages = "1261--1270",

journal = "FEBS Letters",

issn = "1873-3468",

publisher = "Wiley-Blackwell",

number = "8",

}

TY - JOUR

T1 - Dimerization of small integral membrane protein 1 promotes cell surface presentation of the Vel blood group epitope

AU - Kelley, Liam P.

AU - Nylander, Anja

AU - Arnaud, Lionel

AU - Schmoker, Anna M.

AU - St. Clair, Riley M.

AU - Gleason, Lindsey A.

AU - Souza, Jessica M.

AU - Storry, Jill R.

AU - Olsson, Martin L.

AU - Ballif, Bryan A.

PY - 2020/4

Y1 - 2020/4

N2 - The Vel blood group antigen is carried on the short extracellular segment of the 78-amino-acid-long, type II transmembrane protein SMIM1 of unknown function. Here, using biochemical analysis and flow cytometry of cells expressing wild-type and mutant alleles of SMIM1, we demonstrate that dimerization of SMIM1 promotes cell surface display of the Vel epitope. We show that SMIM1 dimerization is mediated both by an extracellular Cys77-dependent, homomeric disulfide linkage and via a GxxxG helix–helix interaction motif in the transmembrane domain. These results provide important context for the observed variability in reactivity patterns of clinically important anti-Vel identified in patient sera.

AB - The Vel blood group antigen is carried on the short extracellular segment of the 78-amino-acid-long, type II transmembrane protein SMIM1 of unknown function. Here, using biochemical analysis and flow cytometry of cells expressing wild-type and mutant alleles of SMIM1, we demonstrate that dimerization of SMIM1 promotes cell surface display of the Vel epitope. We show that SMIM1 dimerization is mediated both by an extracellular Cys77-dependent, homomeric disulfide linkage and via a GxxxG helix–helix interaction motif in the transmembrane domain. These results provide important context for the observed variability in reactivity patterns of clinically important anti-Vel identified in patient sera.

KW - disulfide bond

KW - GxxxG

KW - SMIM1

KW - transfusion medicine

KW - Vel blood group system

U2 - 10.1002/1873-3468.13726

DO - 10.1002/1873-3468.13726

M3 - Article

C2 - 31879955

AN - SCOPUS:85078602210

SN - 1873-3468

VL - 594

SP - 1261

EP - 1270

JO - FEBS Letters

JF - FEBS Letters

IS - 8

ER -

Dimerization of small integral membrane protein 1 promotes cell surface presentation of the Vel blood group epitope

Sammanfattning

Ämnesklassifikation (UKÄ)

Tillgång till dokument

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Projekt

Further investigation into the structure and function of SMIM1, a newly discovered erythroid transmembrane protein

Citera det här