Prospects for Treatment of Idiopathic Pulmonary Fibrosis

The Russian Archives of Internal Medicine Pub Date : 2022-07-30 DOI:10.20514/2226-6704-2022-12-4-267-275

R. Mustafin

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Abstract

Idiopathic pulmonary fibrosis (IPF) is a severe, progressive lung disease of unknown etiology with an average worldwide prevalence of 15 per 100,000. According to the etiology, IPF is classified into sporadic, syndromic, and familial cases. Sporadic cases refer to multifactorial diseases and are associated with age, viral infections, smoking and inhalation of dust, contact with chemicals and drugs, gastroesophageal reflux disease. There were revealed an association of sporadic IPF with allelic variants of the genes AKAP13, ATP11A, DPP9, DSP, IVD, IL1RN, FAM13A, MUC5B, SFTPC, SPPL2C, TERC, TERT, TOLLIP. Syndromal IPF develops in German-Pudlak syndrome. Familial cases of the disease are caused by mutations in the genes encoding surfactant (SFTPC), mucin (MUC5B), deadenylation nuclease (PARN), components of telomere functioning (RTEL1, TERC, TERT). In 2000, the American Thoracic Society recommended glucocorticoids and cytostatics for the treatment of ELISA in order to influence the inflammatory process due to the activation of fibroblasts and their accumulation in the extracellular matrix of the lungs. These recommendations are still used by many doctors, despite the publication of reliable data on the increased mortality and hospitalizations of IPF patients taking prednisolone and azathioprine. According to recent meta-analyzes, pirfenidone (an inhibitor of the synthesis of procollagen I and II growth factors) and nintenadib (a tyrosine kinase inhibitor) are the most effective treatments for IPF. Since genetic factors play an important role in the etiopathogenesis of the disease, it is promising to search for methods of targeted therapy for IPF using specific noncoding RNAs as targets, changes in the expression of which are not specific of other bronchopulmonary diseases. These RNAs include miR-9-5p, miR-27b, miR-153, miR-184, miR-326, miR-374, miR-489, miR-630, miR-1343 (decreased expression in IPF); miR-340, miR-424, miR-487b, miR-493, lncRNA AP003419.16, lncRNA AP003419.16 (increased expression in IPF).

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特发性肺纤维化的治疗前景

特发性肺纤维化(IPF)是一种病因不明的严重进行性肺部疾病，全球平均患病率为10万分之15。根据病因，IPF分为散发性、综合征性和家族性病例。散发病例是指多因素疾病，与年龄、病毒感染、吸烟和吸入粉尘、接触化学品和药物、胃食管反流病有关。发现散发性IPF与AKAP13、ATP11A、DPP9、DSP、IVD、IL1RN、FAM13A、MUC5B、SFTPC、SPPL2C、TERC、TERT、TOLLIP等基因等位变异相关。症候群IPF在German-Pudlak综合征中出现。这种疾病的家族性病例是由编码表面活性剂(SFTPC)、粘蛋白(MUC5B)、死基化核酸酶(PARN)、端粒功能成分(RTEL1、TERC、TERT)的基因突变引起的。2000年，美国胸科学会推荐使用糖皮质激素和细胞抑制剂治疗ELISA，以影响因成纤维细胞激活及其在肺细胞外基质中的积累而引起的炎症过程。这些建议仍然被许多医生使用，尽管有可靠的数据表明，服用泼尼松龙和硫唑嘌呤的IPF患者死亡率和住院率增加。根据最近的荟萃分析，吡非尼酮(一种合成前胶原I和前胶原II生长因子的抑制剂)和任天爹(一种酪氨酸激酶抑制剂)是治疗IPF最有效的药物。由于遗传因素在该病的发病机制中起着重要作用，因此寻找以特异性非编码rna为靶点的靶向治疗IPF的方法是有希望的，这些特异性非编码rna的表达变化对其他支气管肺疾病没有特异性。这些rna包括miR-9-5p、miR-27b、miR-153、miR-184、miR-326、miR-374、miR-489、miR-630、miR-1343 (IPF中表达降低);miR-340, miR-424, miR-487b, miR-493, lncRNA AP003419.16, lncRNA AP003419.16(在IPF中表达增加)。

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The Russian Archives of Internal Medicine

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