HLA‐B leader genotypes in a clinical population

The −21 dimorphism in the leader sequences of HLA‐B exon 1 is associated with risk of graft‐versus‐host disease (GVHD), relapse and overall survival after unrelated donor hematopoietic cell transplantation (HCT), haploidentical HCT and cord blood transplantation. Consideration of the leader dimorphi...

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Published inHLA Vol. 102; no. 1; pp. 44 - 51
Main Authors Balgansuren, Gansuvd, Sprague, Maggie, Peterson, Paula, Shenavar, Yasaman, Ng, Ada, Regen, Lois, Shelton, Nakita, Petersdorf, Effie
Format Journal Article
LanguageEnglish
Published Oxford, UK Blackwell Publishing Ltd 01.07.2023
Subjects
Alleles
Epitopes
Genotype
Hematopoietic Stem Cell Transplantation - adverse effects
HLA-B Antigens - genetics
HLA‐B leader sequence
Humans
M‐leader peptide
NGS
Prospective Studies
Receptors, KIR - genetics
rs1050458‐C/T
T‐leader peptide
T-leader peptide
rs1050458-C/T
NGS
M-leader peptide
HLA-B leader sequence
genotype
Online AccessGet full text

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Abstract The −21 dimorphism in the leader sequences of HLA‐B exon 1 is associated with risk of graft‐versus‐host disease (GVHD), relapse and overall survival after unrelated donor hematopoietic cell transplantation (HCT), haploidentical HCT and cord blood transplantation. Consideration of the leader dimorphism in the prospective selection of allogeneic donors for HCT may help to lower risks for patients, but requires understanding of the frequencies of the leader in patients and candidate transplant donors. We defined the frequencies of the HLA‐B leader, and its association to HLA‐B Bw4/Bw6 and C1/C2 KIR epitopes. Sequence variants of rs1050458 of exon 1 position −21 for 11,126 haplotypes were analyzed from high resolution HLA typing of over 5500 study subjects. HLA typing was performed by TruSight/AlloSeq NGS and analyzed using TruSight/AlloSeq Assign software. HLA‐B Bw4/Bw6 and C1/C2 KIR epitopes were defined based on established sequence alignments and nomenclature. Alleles at rs1050458 of HLA‐B exon 1 were validated as dimorphic: rs1050458‐C or ‐T variants encoding threonine (T) or methionine (M) at anchor position 2 (P2) of nonameric HLA‐B leader peptides, respectfully. No additional variants were observed. Among study subjects, 70% of HLA‐B haplotypes encoded T‐leader and 30% encoded M‐leader sequences. The genotype frequencies of TT, MT, and MM were consistent among patient, related, and unrelated donor groups. The associations of M/T leader, Bw4/Bw6, and C1/C2 enhanced understanding of the Class I features involved in the innate immune response. A population of patients and transplant donors confirms the rs1050458 leader dimorphism and its association with HLA‐B Bw4/Bw6 and C1/C2 KIR features.
AbstractList The −21 dimorphism in the leader sequences of HLA‐B exon 1 is associated with risk of graft‐versus‐host disease (GVHD), relapse and overall survival after unrelated donor hematopoietic cell transplantation (HCT), haploidentical HCT and cord blood transplantation. Consideration of the leader dimorphism in the prospective selection of allogeneic donors for HCT may help to lower risks for patients, but requires understanding of the frequencies of the leader in patients and candidate transplant donors. We defined the frequencies of the HLA‐B leader, and its association to HLA‐B Bw4/Bw6 and C1/C2 KIR epitopes. Sequence variants of rs1050458 of exon 1 position −21 for 11,126 haplotypes were analyzed from high resolution HLA typing of over 5500 study subjects. HLA typing was performed by TruSight/AlloSeq NGS and analyzed using TruSight/AlloSeq Assign software. HLA‐B Bw4/Bw6 and C1/C2 KIR epitopes were defined based on established sequence alignments and nomenclature. Alleles at rs1050458 of HLA‐B exon 1 were validated as dimorphic: rs1050458‐C or ‐T variants encoding threonine (T) or methionine (M) at anchor position 2 (P2) of nonameric HLA‐B leader peptides, respectfully. No additional variants were observed. Among study subjects, 70% of HLA‐B haplotypes encoded T‐leader and 30% encoded M‐leader sequences. The genotype frequencies of TT, MT, and MM were consistent among patient, related, and unrelated donor groups. The associations of M/T leader, Bw4/Bw6, and C1/C2 enhanced understanding of the Class I features involved in the innate immune response. A population of patients and transplant donors confirms the rs1050458 leader dimorphism and its association with HLA‐B Bw4/Bw6 and C1/C2 KIR features.
The -21 dimorphism in the leader sequences of HLA-B exon 1 is associated with risk of graft-versus-host disease (GVHD), relapse and overall survival after unrelated donor hematopoietic cell transplantation (HCT), haploidentical HCT and cord blood transplantation. Consideration of the leader dimorphism in the prospective selection of allogeneic donors for HCT may help to lower risks for patients, but requires understanding of the frequencies of the leader in patients and candidate transplant donors. We defined the frequencies of the HLA-B leader, and its association to HLA-B Bw4/Bw6 and C1/C2 KIR epitopes. Sequence variants of rs1050458 of exon 1 position -21 for 11,126 haplotypes were analyzed from high resolution HLA typing of over 5500 study subjects. HLA typing was performed by TruSight/AlloSeq NGS and analyzed using TruSight/AlloSeq Assign software. HLA-B Bw4/Bw6 and C1/C2 KIR epitopes were defined based on established sequence alignments and nomenclature. Alleles at rs1050458 of HLA-B exon 1 were validated as dimorphic: rs1050458-C or -T variants encoding threonine (T) or methionine (M) at anchor position 2 (P2) of nonameric HLA-B leader peptides, respectfully. No additional variants were observed. Among study subjects, 70% of HLA-B haplotypes encoded T-leader and 30% encoded M-leader sequences. The genotype frequencies of TT, MT, and MM were consistent among patient, related, and unrelated donor groups. The associations of M/T leader, Bw4/Bw6, and C1/C2 enhanced understanding of the Class I features involved in the innate immune response. A population of patients and transplant donors confirms the rs1050458 leader dimorphism and its association with HLA-B Bw4/Bw6 and C1/C2 KIR features.
Author Balgansuren, Gansuvd
Peterson, Paula
Ng, Ada
Shelton, Nakita
Regen, Lois
Petersdorf, Effie
Shenavar, Yasaman
Sprague, Maggie
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Copyright 2023 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.
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Issue 1
Keywords T-leader peptide
rs1050458-C/T
NGS
M-leader peptide
HLA-B leader sequence
genotype
Language English
License 2023 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.
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Snippet The −21 dimorphism in the leader sequences of HLA‐B exon 1 is associated with risk of graft‐versus‐host disease (GVHD), relapse and overall survival after...
The -21 dimorphism in the leader sequences of HLA-B exon 1 is associated with risk of graft-versus-host disease (GVHD), relapse and overall survival after...
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SubjectTerms Alleles
Epitopes
Genotype
Hematopoietic Stem Cell Transplantation - adverse effects
HLA-B Antigens - genetics
HLA‐B leader sequence
Humans
M‐leader peptide
NGS
Prospective Studies
Receptors, KIR - genetics
rs1050458‐C/T
T‐leader peptide
Title HLA‐B leader genotypes in a clinical population
URI https://onlinelibrary.wiley.com/doi/abs/10.1111%2Ftan.15022
https://www.ncbi.nlm.nih.gov/pubmed/36929133
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