Upadhyay Vaibhav, Yoon Young Me, Vazquez Sara E, Velez Tania E, Jones Kirk D, Lee Cathryn T, Law Christopher S, Wolters Paul J, Lee Seoyeon, Yang Monica M, Farrand Erica, Noth Imre, Strek Mary E, Anderson Mark S, DeRisi Joseph L, Sperling Anne I, Shum Anthony K
University of California San Francisco.
University of Chicago, Illinois.
ACR Open Rheumatol. 2024 Sep;6(9):568-580. doi: 10.1002/acr2.11696. Epub 2024 Jul 1.
Interstitial lung diseases (ILDs) are a heterogeneous group of disorders that can develop in patients with connective tissue diseases. Establishing autoimmunity in ILD impacts prognosis and treatment. Patients with ILD are screened for autoimmunity by measuring antinuclear autoantibodies, rheumatoid factors, and other nonspecific tests. However, this approach may miss autoimmunity that manifests as autoantibodies to tissue antigens not previously defined in ILD.
We use Phage Immunoprecipitation-Sequencing (PhIP-Seq) to conduct an autoantibody discovery screen of patients with ILD and controls. We screened for novel autoantigen candidates using PhIP-Seq. We next developed a radio-labeled binding assay and validated the leading candidate in 398 patients with ILD recruited from two academic medical centers and 138 blood bank individuals that formed our reference cohort.
PhIP-Seq identified 17 novel autoreactive targets, and machine learning classifiers derived from these targets discriminated ILD serum from controls. Among the 17 candidates, we validated CDHR5 and found CDHR5 autoantibodies in patients with rheumatologic disorders and importantly, patients not previously diagnosed with autoimmunity. Using survival and transplant free-survival data available from one of the two centers, patients with CDHR5 autoantibodies showed worse survival compared with other patients with connective tissue disease ILD.
We used PhIP-Seq to define a novel CDHR5 autoantibody in a subset of select patients with ILD. Our data complement a recent study showing polymorphisms in the CDHR5-IRF7 gene locus strongly associated with titer of anticentromere antibodies in systemic sclerosis, creating a growing body of evidence suggesting a link between CDHR5 and autoimmunity.
间质性肺疾病(ILDs)是一组异质性疾病,可发生于结缔组织病患者。在ILD中确立自身免疫性会影响预后和治疗。通过检测抗核自身抗体、类风湿因子及其他非特异性检测对ILD患者进行自身免疫性筛查。然而,这种方法可能会遗漏表现为针对ILD中以前未定义的组织抗原的自身抗体的自身免疫性。
我们使用噬菌体免疫沉淀测序(PhIP-Seq)对ILD患者和对照进行自身抗体发现筛查。我们使用PhIP-Seq筛选新的自身抗原候选物。接下来,我们开发了一种放射性标记结合试验,并在从两个学术医学中心招募的398例ILD患者和138例血库个体(构成我们的参考队列)中验证了主要候选物。
PhIP-Seq鉴定出17个新的自身反应性靶点,从这些靶点衍生的机器学习分类器可区分ILD血清和对照血清。在这17个候选物中,我们验证了CDHR5,并在风湿性疾病患者中发现了CDHR5自身抗体,重要的是,在以前未诊断为自身免疫性疾病的患者中也发现了该抗体。利用两个中心之一提供的生存和无移植生存数据,与其他结缔组织病ILD患者相比,有CDHR5自身抗体的患者生存率较差。
我们使用PhIP-Seq在一部分特定的ILD患者中定义了一种新的CDHR5自身抗体。我们的数据补充了最近一项研究,该研究表明CDHR5-IRF7基因座的多态性与系统性硬化症中抗着丝粒抗体的滴度密切相关,越来越多的证据表明CDHR5与自身免疫性之间存在联系。
