Identification of human minor histocompatibility antigens based on genetic association with highly parallel genotyping of pooled DNA

Kawase, Takakazu; Nannya, Yasuhito; Torikai, Hiroki; Yamamoto, Go; Onizuka, Makoto; Morishima, Satoko; Tsujimura, Kunio; Miyamura, Koichi; Kodera, Yoshihisa; Morishima, Yasuo; Takahashi, Toshitada; Kuzushima, Kiyotaka; Ogawa, Seishi; Akatsuka, Yoshiki

doi:10.1182/blood-2007-10-118950

Cited by 45 publications

(44 citation statements)

References 34 publications

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“…30,31 Most of these techniques did not allow or were difficult to adapt for identification of HLA-class IIrestricted mHags. By screening a recombinant bacteria cDNA library, 32 we could now identify 4 unknown CD4 ϩ T-cell specificities.…”

Section: Discussionmentioning

confidence: 99%

“…A 15-mer peptide comprising amino acids shared by the 2 19-mer peptides also stimulated IFN-␥ release, whereas a 15-mer peptide containing the donor variant H at position 39 was not recognized ( Figure 3A). Serial truncations of the 15-mer peptide at the N and C termini led to the identification of a minimal 12-mer YFRLGVSDPIRG peptide (amino acids [29][30][31][32][33][34][35][36][37][38][39][40], designated LB-MR1-1R ( Figure 3A). …”

Section: Lb-mr1-1rmentioning

confidence: 99%

“…[23][24][25][26] Because under noninflammatory or low-inflammatory conditions HLA-class II molecules are predominantly expressed on hematopoietic cells, stimulating CD4 ϩ T-cell immunity late after alloSCT may be another promising strategy to selectively target residual leukemia without inducing severe GVHD. [27][28][29] Although several HLA-class I-restricted mHags have been identified by various methods, [5][6][7][8]10,11,[13][14][15][16][17]30,31 the discovery of HLA-class II-restricted mHags proved to be more difficult and was hampered by technical limitations. We developed a method by which recombinant bacteria cDNA expression libraries were used to identify antigens as targets for CD4 ϩ T cells.…”

Section: Introductionmentioning

confidence: 99%

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Identification of 4 new HLA-DR–restricted minor histocompatibility antigens as hematopoietic targets in antitumor immunity

Stumpf

Meijden

Bergen

et al. 2009

Blood

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Section: Discussionmentioning

confidence: 99%

Section: Lb-mr1-1rmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Identification of 4 new HLA-DR–restricted minor histocompatibility antigens as hematopoietic targets in antitumor immunity

Stumpf

Meijden

Bergen

et al. 2009

Blood

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“…Several HLA class I-restricted minor H Ags have been identified in humans by screening of plasmid cDNA libraries, elution of HLA-bound peptides, and genetic linkage analysis (13)(14)(15)(16). Recently, a novel strategy using whole-genome association scanning reported characterization of 10 new HLA class I-restricted minor H Ags (17).…”

mentioning

confidence: 99%

Isolation of Human CD4/CD8 Double-Positive, Graft-Versus-Host Disease–Protective, Minor Histocompatibility Antigen–Specific Regulatory T Cells and of a Novel HLA-DR7–Restricted HY-Specific CD4 Clone

Eljaafari

Yuruker

Ferrand

et al. 2013

The Journal of Immunology

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Minor histocompatibility (H) Ags are classically described as self-peptides derived from intracellular proteins that are expressed at the cell surface by MHC class I and class II molecules and that induce T cell alloresponses. We have isolated three different T cell populations from a skin biopsy of a patient suffering from acute graft-versus-host disease following sex-mismatched HLA-identical bone marrow transplantation. The first population was: 1) CD4+/CD8+ double-positive; 2) specific for an HLA class I–restricted autosomal Ag; 3) expressed a Tr1 profile with high levels of IL-10, but low IL-2 and IFN-γ; and 4) exerted regulatory function in the presence of recipient APCs. The second was CD8 positive, specific for an HLA class I–restricted autosomally encoded minor H Ag, but was only weakly cytotoxic. The third was CD4 single positive, specific for an HLA-DR7–restricted HY epitope and exerted both proliferative and cytotoxic functions. Identification of the peptide recognized by these latter cells revealed a new human HY epitope, TGKIINFIKFDTGNL, encoded by RPS4Y and restricted by HLA-DR7. In this paper, we show human CD4/CD8 double-positive, acute graft-versus-host disease–protective, minor H Ag–specific regulatory T cells and identify a novel HLA-DR7/ HY T cell epitope, encoded by RPS4Y, a potential new therapeutic target.

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“…Over the years, increasing numbers of MiHA have been identified by cDNA library screening (10)(11)(12), genetic linkage analysis (13)(14)(15), peptide elution from HLA (16)(17)(18), and genome-wide association analysis (19)(20)(21). Collectively, these methods use a forward immunology approach characterized by the isolation of activated T cells from patients demonstrating a clinical response to DLI after allo-SCT and subsequent elucidation of the Ags recognized.…”

mentioning

confidence: 99%

Discovery of T Cell Epitopes Implementing HLA-Peptidomics into a Reverse Immunology Approach

Hombrink

Hassan

Kester

et al. 2013

The Journal of Immunology

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T cell recognition of minor histocompatibility Ags (MiHA) plays an important role in the graft-versus-tumor effect of allogeneic stem cell transplantation. Selective infusion of T cells reactive for hematopoiesis-restricted MiHA presented in the context of HLA class I or II molecules may help to separate the graft-versus-tumor effects from graft-versus-host disease effects after allogeneic stem cell transplantation. Over the years, increasing numbers of MiHA have been identified by forward immunology approaches, and the relevance of these MiHA has been illustrated by correlation with clinical outcome. As the tissue distribution of MiHA affects the clinical outcome of T cell responses against these Ags, it would be beneficial to identify additional predefined MiHA that are exclusively expressed on hematopoietic cells. Therefore, several reverse immunology approaches have been explored for the prediction of MiHA. Thus far, these approaches frequently resulted in the identification of T cells directed against epitopes that are not naturally processed and presented. In this study we established a method for the identification of biologically relevant MiHA, implementing mass spectrometry–based HLA-peptidomics into a reverse immunology approach. For this purpose, HLA class I binding peptides were eluted from transformed B cells, analyzed by mass spectrometry, and matched with a database dedicated to identifying polymorphic peptides. This process resulted in a set of 40 MiHA candidates that were evaluated in multiple selection steps. The identification of LB-NISCH-1A demonstrated the technical feasibility of our approach. On the basis of these results, we present an approach that can be of value for the efficient identification of MiHA or other T cell epitopes.

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Identification of human minor histocompatibility antigens based on genetic association with highly parallel genotyping of pooled DNA

Cited by 45 publications

References 34 publications

Identification of 4 new HLA-DR–restricted minor histocompatibility antigens as hematopoietic targets in antitumor immunity

Identification of 4 new HLA-DR–restricted minor histocompatibility antigens as hematopoietic targets in antitumor immunity

Isolation of Human CD4/CD8 Double-Positive, Graft-Versus-Host Disease–Protective, Minor Histocompatibility Antigen–Specific Regulatory T Cells and of a Novel HLA-DR7–Restricted HY-Specific CD4 Clone

Discovery of T Cell Epitopes Implementing HLA-Peptidomics into a Reverse Immunology Approach

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