Identification of an HLA class I allele closely involved in the autoantigen presentation in acquired aplastic anemia

Zaimoku, Yoshitaka; Takamatsu, Hiroyuki; Hosomichi, Kazuyoshi; Ozawa, Tatsuhiko; Nakagawa, Noboru; Imi, Tatsuya; Muto, Hiroyuki; Katagiri, Takamasa; Kishi, Hiroyuki; Tajima, Atsushi; Muraguchi, Atsushi; Kashiwase, Koichi; Nakao, Shinji

doi:10.1182/blood-2016-11-752378

Cited by 70 publications

(70 citation statements)

References 40 publications

(50 reference statements)

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“…Indeed, while our manuscript was in preparation, Zaimoku and colleagues used flow cytometric methods to identify recurrent HLA-B *40:02 mutations in 28 Japanese aAA patients carrying HLA-B *40:02 allele 53 , pointing to the involvement of HLA-B *40:02 allele in aAA in Japan, which has a more restricted HLA pool and a significantly higher frequency of HLA-B *40:02 (Figure 5). Interestingly, the incidence of aAA is also 2–3-fold higher in East Asia 54 .…”

Section: Discussionmentioning

confidence: 99%

Somatic HLA mutations expose the role of class I–mediated autoimmunity in aplastic anemia and its clonal complications

et al. 2017

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Acquired aplastic anemia (aAA) is an acquired deficiency of early hematopoietic cells, characterized by inadequate blood production, and a predisposition to myelodysplastic syndrome (MDS) and leukemia. Although its exact pathogenesis is unknown, aAA is thought to be driven by Human Leukocyte Antigen (HLA)-restricted T cell immunity, with earlier studies favoring HLA class II-mediated pathways. Using whole exome sequencing (WES), we recently identified two aAA patients with somatic mutations in HLA class I genes. We hypothesized that HLA class I mutations are pathognomonic for autoimmunity in aAA, but were previously underappreciated because the Major Histocompatibility Complex (MHC) region is notoriously difficult to analyze by WES. Using a combination of targeted deep sequencing of HLA class I genes and single nucleotide polymorphism array (SNP-A) genotyping we screened 66 aAA patients for somatic HLA class I loss. We found somatic HLA loss in eleven patients (17%), with thirteen loss-of-function mutations in HLA-A*33:03, HLA-A*68:01, HLA-B*14:02 and HLA-B*40:02 alleles. Three patients had more than one mutation targeting the same HLA allele. Interestingly, HLA-B*14:02 and HLA-B*40:02 were significantly overrepresented in aAA patients, compared to ethnicity-matched controls. Patients who inherited the targeted HLA alleles, regardless of HLA mutation status, had a more severe disease course with more frequent clonal complications as assessed by WES, SNP-A, and metaphase cytogenetics, and more frequent secondary MDS. The finding of recurrent HLA class I mutations provides compelling evidence for a predominant HLA class I-driven autoimmunity in aAA, and establishes a novel link between aAA patients’ immunogenetics and clonal evolution.

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Section: Discussionmentioning

confidence: 99%

Somatic HLA mutations expose the role of class I–mediated autoimmunity in aplastic anemia and its clonal complications

et al. 2017

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“…10 Although the hematopoiesis derived from iCD34 1 cells may be primitive rather than definitive hematopoiesis, the CTL line was able to discriminate WT iCD34 1 cells from B4002-lacking iCD34 1 cells in vitro, suggesting that our xenograft model can serve as an AA model in which antigen-specific T cells may selectively eliminate WT HSPCs in vivo. This study thus added a new piece of evidence to support the immune-mediated destruction of HSCs as a central pathogenic mechanism in this disease and opens new venues for the identification of autoantigens that trigger the autoimmune attack.…”

Section: Bloodadvancesorg Frommentioning

confidence: 99%

Hematopoiesis by iPSC-derived hematopoietic stem cells of aplastic anemia that escape cytotoxic T-cell attack

et al. 2018

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“…These recent findings further strengthen the role of HLA class I‐mediated autoimmunity in AA pathogenesis. Among the many identified HLA risk alleles, a version of the HLA‐B gene called HLA‐B*‐ 40:02 plays a critical role in AA pathogenesis . Lack of allele expression of HLA‐B* 40:02, either by loss of heterozygosity of 6p chromosome (6pLOH) or due to various SMs, allows for the escape of HSCs from the attack of cytotoxic T cells that are specific to autoantigens presented by the lacked HLA class I alleles.…”

Section: Immunogenetics Of Immune Dysregulationmentioning

confidence: 99%

Molecular pathogenesis of acquired aplastic anemia

Boddu

Kadia

2018

European J of Haematology

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The application of next‐generation sequencing (NGS) has enhanced our understanding of the genetic landscape in acquired aplastic anemia (AA). Parallel progress has been in addressing aspects underlying immune dysregulation in disease pathogenesis. Novel insights into the molecular and biologic mechanisms have led to a shift in the paradigm of AA, from a solely autoimmune pathogenic concept toward its recognition as a multifaceted pathophysiology characterized by cytogenetic abnormalities, recurrent somatic mutations, telomere attrition, and immune dysregulation. The detection of recurrent driver mutations disrupting myelodysplastic syndrome (MDS)/acute myeloid leukemia (AML)‐associated genes has suggested a pathophysiologic link between clonal hematopoiesis in AA and the later development of these clonal disorders. Further, certain AA‐related somatic genetic alterations may have clinical implications on treatment response, disease progression, and survival following immunosuppressive therapy. Going forward, wider validation of these genetic abnormalities will allow for their incorporation into a more informative risk stratification system that does not rely solely on clinical factors.

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Identification of an HLA class I allele closely involved in the autoantigen presentation in acquired aplastic anemia

Cited by 70 publications

References 40 publications

Somatic HLA mutations expose the role of class I–mediated autoimmunity in aplastic anemia and its clonal complications

Somatic HLA mutations expose the role of class I–mediated autoimmunity in aplastic anemia and its clonal complications

Hematopoiesis by iPSC-derived hematopoietic stem cells of aplastic anemia that escape cytotoxic T-cell attack

Molecular pathogenesis of acquired aplastic anemia

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