Role of Deleterious Rare Alleles for Acute-Onset Diffuse Interstitial Lung Disease in Collagen Diseases

Author:

Furukawa Hiroshi123ORCID,Oka Shomi123,Shimada Kota45,Hashimoto Atsushi4,Komiya Akiko16,Matsui Toshihiro14,Tohma Shigeto13

Affiliation:

1. Clinical Research Center for Allergy and Rheumatology, National Hospital Organization Sagamihara National Hospital, Sagamihara, Japan

2. Molecular and Genetic Epidemiology Laboratory, Faculty of Medicine, University of Tsukuba, Tsukuba, Japan

3. Department of Rheumatology, National Hospital Organization Tokyo National Hospital, Kiyose, Japan

4. Department of Rheumatology, National Hospital Organization Sagamihara National Hospital, Sagamihara, Japan

5. Department of Rheumatic Diseases, Tokyo Metropolitan Tama Medical Center, Fuchu, Japan

6. Department of Clinical Laboratory, National Hospital Organization Sagamihara National Hospital, Sagamihara, Japan

Abstract

Objective: Acute-onset diffuse interstitial lung disease (AoDILD) includes acute exacerbation of interstitial lung disease (ILD), drug-induced ILD, and Pneumocystis pneumonia in collagen diseases patients. As AoDILD causes a poor prognosis in collagen disease patients, the pathogenesis of AoDILD should be investigated. Exome sequencing studies revealed that rare variants were detected to be causative in some diseases. Recently reported upregulated genes in acute exacerbation of idiopathic pulmonary fibrosis could provide candidate genes for restricted exome analysis of AoDILD in collagen disease. Here, we investigated rare variants in the coding and boundary regions of these candidate genes in AoDILD. Methods: Deleterious rare variants in the coding and boundary regions of the candidate genes were analyzed by exome sequencing and the deleterious rare allele frequencies in AoDILD were compared with those of controls. Results: A significant association was detected for deleterious rare alleles in NPL ( P = .0044, Pc = .0399, odds ratio [OR] = 10.05, 95% confidence interval [CI] = 3.01-33.55). A deleterious rare allele frequency in the 9 candidate genes ( P = .0011, OR = 7.17, 95% CI = 2.80-18.33) was also increased in AoDILD in multigene panel analysis. The Krebs von den Lungen–6 (KL-6) levels in AoDILD patients with deleterious rare alleles were tended to be lower than those without ( P = .0168, Pc = .1509). Conclusions: The deleterious rare alleles in NPL were associated with AoDILD. In addition, the deleterious rare allele frequency in the 9 candidate genes was also increased in AoDILD. The deleterious rare alleles might contribute to the pathogenesis of AoDILD.

Funder

takeda pharmaceutical company

Japan Research Foundation for Clinical Pharmacology

Mitsui Sumitomo Insurance Welfare Foundation

bristol-myers squibb

Merck Sharp and Dohme

national hospital organization

Pfizer Japan

Daiwa Securities Health Foundation

Japan Agency for Medical Research and Development

Chugai Pharmaceutical

teijin pharma

Takeda Science Foundation

Abbott Japan

Japan Society for the Promotion of Science

Astellas Pharma

ministry of health, labour and welfare

Nakatomi Foundation

Eisai

mitsubishi tanabe pharma corporation

Publisher

SAGE Publications

Subject

Cardiology and Cardiovascular Medicine,Pulmonary and Respiratory Medicine

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