Genetic determinants of risk in autoimmune pulmonary alveolar proteinosis

Saori Sakaue(Broad Institute), Etsuro Yamaguchi(Aichi Medical University), Yoshikazu Inoue(NHO Kinki Chuo Chest Medical Center), Meiko Takahashi(Kyoto University), Jun Hirata(Teijin (Japan)), Ken Suzuki(The University of Osaka), Satoru Ito(Aichi Medical University), Toru Arai(NHO Kinki Chuo Chest Medical Center), Masaki Hirose(NHO Kinki Chuo Chest Medical Center), Yoshinori Tanino(Fukushima Medical University), Takefumi Nikaido(Fukushima Medical University), Toshio Ichiwata(Tokyo Medical University), Shinya Ohkouchi(Tohoku University), Taizou Hirano(Tohoku University), Toshinori Takada(Niigata University Medical and Dental Hospital), Satoru Miyawaki(The University of Tokyo), Shogo Dofuku(The University of Tokyo), Yuichi Maeda(The University of Osaka), Takuro Nii(The University of Osaka), Toshihiro Kishikawa(The University of Osaka), Kotaro Ogawa(The University of Osaka), Tatsuo Masuda(The University of Osaka), Kenichi Yamamoto(The University of Osaka), Kyuto Sonehara(The University of Osaka), Ryushi Tazawa(Tokyo Medical and Dental University), Konosuke Morimoto(Nagasaki University), Masahiro Takaki(Nagasaki University Hospital), Satoshi Konno(Hokkaido University), Masaru Suzuki(Hokkaido University), Keisuke Tomii(Kobe City Medical Center General Hospital), Atsushi Nakagawa(Kobe City Medical Center General Hospital), Tomohiro Handa(Kyoto University), Kiminobu Tanizawa(Kyoto University), Haruyuki Ishii(Kyorin University), Manabu Ishida(Kyorin University), Toshiyuki Kato(Kariya Toyota General Hospital), Naoya Takeda(Kariya Toyota General Hospital), Koshi Yokomura(Seirei Mikatabara General Hospital), Takashi Matsui(Seirei Mikatabara General Hospital), Masaki Watanabe(Kagoshima University), Hiromasa Inoue(Kagoshima University), Kazuyoshi Imaizumi(Fujita Health University), Yasuhiro Gotô(Fujita Health University), Hiroshi Kida(Toneyama National Hospital), Tomoyuki Fujisawa(Hamamatsu University School of Medicine), Takafumi Suda(Hamamatsu University School of Medicine), Takashi Yamada(Shizuoka City Hospital), Yasuomi Satake(Shizuoka City Hospital), Hidenori Ibata(Mie Chuo Medical Center), Nobuyuki Hizawa(University of Tsukuba), Hideki Mochizuki(The University of Osaka), Atsushi Kumanogoh(Osaka International University), Fumihiko Matsuda(Kyoto University), Koh Nakata(Niigata University Medical and Dental Hospital), Tomomitsu Hirota(Jikei University School of Medicine), Mayumi Tamari(Jikei University School of Medicine), Yukinori Okada(Osaka International University)
Nature Communications
February 15, 2021
10.1038/s41467-021-21011-y
Cited by 41Open Access
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Abstract

Abstract Pulmonary alveolar proteinosis (PAP) is a devastating lung disease caused by abnormal surfactant homeostasis, with a prevalence of 6–7 cases per million population worldwide. While mutations causing hereditary PAP have been reported, the genetic basis contributing to autoimmune PAP (aPAP) has not been thoroughly investigated. Here, we conducted a genome-wide association study of aPAP in 198 patients and 395 control participants of Japanese ancestry. The common genetic variant, rs138024423 at 6p21, in the major-histocompatibility-complex (MHC) region was significantly associated with disease risk (Odds ratio [OR] = 5.2; P = 2.4 × 10 −12 ). HLA fine-mapping revealed that the common HLA class II allele, HLA-DRB1*08:03, strongly drove this signal (OR = 4.8; P = 4.8 × 10 −12 ), followed by an additional independent risk allele at HLA-DPβ1 amino acid position 8 (OR = 0.28; P = 3.4 × 10 −7 ). HLA-DRB1*08:03 was also associated with an increased level of anti-GM-CSF antibody, a key driver of the disease (β = 0.32; P = 0.035). Our study demonstrated a heritable component of aPAP, suggesting an underlying genetic predisposition toward an abnormal antibody production.

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