Respiratory Medicine Unit, Department of Medicine Solna and Center for Molecular Medicine, Karolinska Institutet, Stockholm, Sweden.
Division of Rheumatology, Department of Medicine Solna and Center for Molecular Medicine, Karolinska Institutet, Stockholm, Sweden.
Respirology. 2023 Oct;28(10):925-933. doi: 10.1111/resp.14543. Epub 2023 Jun 27.
Studies of autoimmunity and anti-citrullinated protein antibodies (ACPA) in idiopathic pulmonary fibrosis (IPF) have been confined to investigations of anti-cyclic citrullinated peptide (anti-CCP) antibodies which utilize synthetic peptides as surrogate markers for in vivo citrullinated antigens. We studied immune activation by analysing the prevalence of in vivo anti-modified protein antibodies (AMPA) in IPF.
We included patients with incident and prevalent IPF (N = 120), sex and smoking-matched healthy controls (HC) (N = 120) and patients with RA (N = 104). Serum (median time: 11 months [Q1-Q3: 1-28 months] from diagnosis) was analysed for presence of antibodies towards native and posttranslational modified (citrullinated [Cit, N = 25]; acetylated [Acet, N = 4] and homocitrullinated [Carb, N = 1]) peptides derived from tenascin (TNC, N = 9), fibrinogen (Fib, N = 11), filaggrin (Fil, N = 5), histone (N = 8), cathelicidin (LL37, N = 4) and vimentin (N = 5) using a custom-made peptide microarray.
AMPA were more frequent and in increased levels in IPF than in HC (44% vs. 27%, p < 0.01), but less than in RA (44% vs. 79%, p < 0.01). We specifically observed AMPA in IPF towards certain citrullinated, acetylated and carbamylated peptides versus HC: tenascin (Cit -TNC ; Cit -TNC ; Cit -TNC ) fibrinogen (Cit -Fibα ; Cit -Fibβ ) and filaggrin (Acet-Fil , Carb-Fil ). No differences in survival (p = 0.13) or disease progression (p = 0.19) between individuals with or without AMPA was observed in IPF. However, patients with incident IPF had better survival if AMPA were present (p = 0.009).
A significant proportion of IPF patients present with specific AMPA in serum. Our results suggest autoimmunity as a possible characteristic for a subgroup of IPF that may affect disease outcome.
特发性肺纤维化(IPF)的自身免疫和抗瓜氨酸化蛋白抗体(ACPA)的研究仅限于对环瓜氨酸肽(抗-CCP)抗体的研究,这些抗体利用合成肽作为体内瓜氨酸化抗原的替代标志物。我们通过分析 IPF 中体内抗修饰蛋白抗体(AMPA)的患病率来研究免疫激活。
我们纳入了 120 例新发和现患 IPF 患者(N=120)、性别和吸烟匹配的健康对照者(HC)(N=120)和类风湿关节炎(RA)患者(N=104)。分析血清(中位数时间:诊断后 11 个月[1-28 个月的第 1 至第 3 个四分位数])中针对源自 tenascin(TNC,N=9)、纤维蛋白原(Fib,N=11)、filaggrin(Fil,N=5)、组蛋白(N=8)、cathelicidin(LL37,N=4)和 vimentin(N=5)的天然和翻译后修饰(瓜氨酸化[Cit,N=25];乙酰化[Acet,N=4]和同型瓜氨酸化[Carb,N=1])肽的抗体存在情况,使用定制的肽微阵列。
与 HC 相比,IPF 中 AMPA 的频率更高且水平更高(44% vs. 27%,p<0.01),但低于 RA(44% vs. 79%,p<0.01)。我们在 IPF 中观察到针对某些瓜氨酸化、乙酰化和氨甲酰化肽的特定 AMPA 与 HC 相比:tenascin(Cit-TNC;Cit-TNC;Cit-TNC)、纤维蛋白原(Cit-Fibα;Cit-Fibβ)和 filaggrin(Acet-Fil,Carb-Fil)。在 IPF 中,未观察到 AMPA 与个体的生存(p=0.13)或疾病进展(p=0.19)之间存在差异。然而,新发 IPF 患者如果存在 AMPA,则生存情况更好(p=0.009)。
相当一部分 IPF 患者的血清中存在特定的 AMPA。我们的结果表明自身免疫可能是 IPF 亚组的一个特征,可能影响疾病结局。
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