Motifs of Three HLA-DQ Amino Acid Residues (α44, β57, β135) Capture Full Association With the Risk of Type 1 Diabetes in DQ2 and DQ8 Children

Zhao, Lue Ping; Papadopoulos, George K; Kwok, William W; Moustakas, Antonis K; Bondinas, George P; Larsson, Helena Elding; Ludvigsson, Johnny; Marcus, Claude; Samuelsson, Ulf; Wang, Ruihan; Pyo, Chul-Woo; Nelson, Wyatt C; Geraghty, Daniel E; Lernmark, Åke

Motifs of Three HLA-DQ Amino Acid Residues (α44, β57, β135) Capture Full Association With the Risk of Type 1 Diabetes in DQ2 and DQ8 Children

Mark

Zhao, Lue Ping ; Papadopoulos, George K ; Kwok, William W ; Moustakas, Antonis K ; Bondinas, George P ; Larsson, Helena Elding ^LU ; Ludvigsson, Johnny ; Marcus, Claude ; Samuelsson, Ulf and Wang, Ruihan , et al. (2020) In Diabetes 69(7). p.1573-1587

Abstract: HLA-DQA1 and -DQB1 are strongly associated with type 1 diabetes (T1D), and DQ8.1 and DQ2.5 are major risk haplotypes. Next-generation targeted sequencing of HLA-DQA1 and -DQB1 in Swedish newly diagnosed 1- to 18 year-old patients (n = 962) and control subjects (n = 636) was used to construct abbreviated DQ haplotypes, converted into amino acid (AA) residues, and assessed for their associations with T1D. A hierarchically organized haplotype (HOH) association analysis allowed 45 unique DQ haplotypes to be categorized into seven clusters. The DQ8/9 cluster included two DQ8.1 risk and the DQ9 resistant haplotypes, and the DQ2 cluster included the DQ2.5 risk and DQ2.2 resistant haplotypes. Within each cluster, HOH found residues α44Q (odds... (More); HLA-DQA1 and -DQB1 are strongly associated with type 1 diabetes (T1D), and DQ8.1 and DQ2.5 are major risk haplotypes. Next-generation targeted sequencing of HLA-DQA1 and -DQB1 in Swedish newly diagnosed 1- to 18 year-old patients (n = 962) and control subjects (n = 636) was used to construct abbreviated DQ haplotypes, converted into amino acid (AA) residues, and assessed for their associations with T1D. A hierarchically organized haplotype (HOH) association analysis allowed 45 unique DQ haplotypes to be categorized into seven clusters. The DQ8/9 cluster included two DQ8.1 risk and the DQ9 resistant haplotypes, and the DQ2 cluster included the DQ2.5 risk and DQ2.2 resistant haplotypes. Within each cluster, HOH found residues α44Q (odds ratio [OR] 3.29, P = 2.38 * 10-85) and β57A (OR 3.44, P = 3.80 * 10-84) to be associated with T1D in the DQ8/9 cluster representing all ten residues (α22, α23, α44, α49, α51, α53, α54, α73, α184, β57) due to complete linkage disequilibrium (LD) of α44 with eight such residues. Within the DQ2 cluster and due to LD, HOH analysis found α44C and β135D to share the risk for T1D (OR 2.10, P = 1.96 * 10-20). The motif "QAD" of α44, β57, and β135 captured the T1D risk association of DQ8.1 (OR 3.44, P = 3.80 * 10-84), and the corresponding motif "CAD" captured the risk association of DQ2.5 (OR 2.10, P = 1.96 * 10-20). Two risk associations were related to GAD65 autoantibody (GADA) and IA-2 autoantibody (IA-2A) but in opposite directions. CAD was positively associated with GADA (OR 1.56, P = 6.35 * 10-8) but negatively with IA-2A (OR 0.59, P = 6.55 * 10-11). QAD was negatively associated with GADA (OR 0.88; P = 3.70 * 10-3) but positively with IA-2A (OR 1.64; P = 2.40 * 10-14), despite a single difference at α44. The residues are found in and around anchor pockets 1 and 9, as potential T-cell receptor contacts, in the areas for CD4 binding and putative homodimer formation. The identification of three HLA-DQ AAs (α44, β57, β135) conferring T1D risk should sharpen functional and translational studies.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/16049245-1600-4ea6-959d-42f82160e936

author

Zhao, Lue Ping ; Papadopoulos, George K ; Kwok, William W ; Moustakas, Antonis K ; Bondinas, George P ; Larsson, Helena Elding ^LU ; Ludvigsson, Johnny ; Marcus, Claude ; Samuelsson, Ulf and Wang, Ruihan , et al. (More)

Zhao, Lue Ping ; Papadopoulos, George K ; Kwok, William W ; Moustakas, Antonis K ; Bondinas, George P ; Larsson, Helena Elding ^LU ; Ludvigsson, Johnny ; Marcus, Claude ; Samuelsson, Ulf ; Wang, Ruihan ; Pyo, Chul-Woo ; Nelson, Wyatt C ; Geraghty, Daniel E and Lernmark, Åke ^LU

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organization

publishing date

2020-07-01

type

Contribution to journal

publication status

published

subject

Endocrinology and Diabetes

in

Diabetes

volume

69

issue

7

pages

15 pages

publisher

American Diabetes Association Inc.

external identifiers

scopus:85086790348
pmid:32245799
pmid:32245799

ISSN

1939-327X

DOI

10.2337/db20-0075

language

English

LU publication?

yes

id

16049245-1600-4ea6-959d-42f82160e936

date added to LUP

2020-04-10 16:43:32

date last changed

2024-05-15 09:15:23

@article{16049245-1600-4ea6-959d-42f82160e936,
  abstract     = {{<p>HLA-DQA1 and -DQB1 are strongly associated with type 1 diabetes (T1D), and DQ8.1 and DQ2.5 are major risk haplotypes. Next-generation targeted sequencing of HLA-DQA1 and -DQB1 in Swedish newly diagnosed 1- to 18 year-old patients (n = 962) and control subjects (n = 636) was used to construct abbreviated DQ haplotypes, converted into amino acid (AA) residues, and assessed for their associations with T1D. A hierarchically organized haplotype (HOH) association analysis allowed 45 unique DQ haplotypes to be categorized into seven clusters. The DQ8/9 cluster included two DQ8.1 risk and the DQ9 resistant haplotypes, and the DQ2 cluster included the DQ2.5 risk and DQ2.2 resistant haplotypes. Within each cluster, HOH found residues α44Q (odds ratio [OR] 3.29, P = 2.38 * 10-85) and β57A (OR 3.44, P = 3.80 * 10-84) to be associated with T1D in the DQ8/9 cluster representing all ten residues (α22, α23, α44, α49, α51, α53, α54, α73, α184, β57) due to complete linkage disequilibrium (LD) of α44 with eight such residues. Within the DQ2 cluster and due to LD, HOH analysis found α44C and β135D to share the risk for T1D (OR 2.10, P = 1.96 * 10-20). The motif "QAD" of α44, β57, and β135 captured the T1D risk association of DQ8.1 (OR 3.44, P = 3.80 * 10-84), and the corresponding motif "CAD" captured the risk association of DQ2.5 (OR 2.10, P = 1.96 * 10-20). Two risk associations were related to GAD65 autoantibody (GADA) and IA-2 autoantibody (IA-2A) but in opposite directions. CAD was positively associated with GADA (OR 1.56, P = 6.35 * 10-8) but negatively with IA-2A (OR 0.59, P = 6.55 * 10-11). QAD was negatively associated with GADA (OR 0.88; P = 3.70 * 10-3) but positively with IA-2A (OR 1.64; P = 2.40 * 10-14), despite a single difference at α44. The residues are found in and around anchor pockets 1 and 9, as potential T-cell receptor contacts, in the areas for CD4 binding and putative homodimer formation. The identification of three HLA-DQ AAs (α44, β57, β135) conferring T1D risk should sharpen functional and translational studies.</p>}},
  author       = {{Zhao, Lue Ping and Papadopoulos, George K and Kwok, William W and Moustakas, Antonis K and Bondinas, George P and Larsson, Helena Elding and Ludvigsson, Johnny and Marcus, Claude and Samuelsson, Ulf and Wang, Ruihan and Pyo, Chul-Woo and Nelson, Wyatt C and Geraghty, Daniel E and Lernmark, Åke}},
  issn         = {{1939-327X}},
  language     = {{eng}},
  month        = {{07}},
  number       = {{7}},
  pages        = {{1573--1587}},
  publisher    = {{American Diabetes Association Inc.}},
  series       = {{Diabetes}},
  title        = {{Motifs of Three HLA-DQ Amino Acid Residues (α44, β57, β135) Capture Full Association With the Risk of Type 1 Diabetes in DQ2 and DQ8 Children}},
  url          = {{http://dx.doi.org/10.2337/db20-0075}},
  doi          = {{10.2337/db20-0075}},
  volume       = {{69}},
  year         = {{2020}},
}

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Motifs of Three HLA-DQ Amino Acid Residues (α44, β57, β135) Capture Full Association With the Risk of Type 1 Diabetes in DQ2 and DQ8 Children