首页> 外文期刊>Archives of Internal Medicine >Progressive preclinical interstitial lung disease in rheumatoid arthritis.
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Progressive preclinical interstitial lung disease in rheumatoid arthritis.

机译:先进的临床前间质性肺病在类风湿性关节炎。

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BACKGROUND: Early detection and treatment for interstitial lung disease (ILD) in patients with rheumatoid arthritis (RA) may ameliorate disease progression. The objective of this study was to identify asymptomatic lung disease and potential therapeutic targets in patients having RA and preclinical ILD (RA-ILD). METHODS: Sixty-four adults with RA and 10 adults with RA and pulmonary fibrosis (RAPF) were referred to the National Institutes of Health, Bethesda, Maryland, and underwent high-resolution computed tomography (HRCT) and pulmonary physiology testing. Proteins capable of modulating fibrosis were quantified in alveolar fluid. RESULTS: Twenty-one of 64 patients (33%) having RA without dyspnea or cough had preclinical ILD identified by HRCT. Compared with patients without lung disease, patients with RA-ILD had statistically significantly longer histories of cigarette smoking (P< .001), increased frequencies of crackles (P= .02), higher alveolar-arterial oxygen gradients (P= .004), and higher HRCT scores (P< .001). The HRCT abnormalities progressed in 12 of 21 patients (57%) with RA-ILD. The alveolar concentrations of platelet-derived growth factor-AB and platelet-derived growth factor-BB were statistically significantly higher in patients having RA-ILD (mean [SE], 497.3 [78.6] and 1473 [264] pg/mL, respectively) than in patients having RA without ILD (mean [SE], 24.9 [42.4] and 792.7 [195.0] pg/mL, respectively) (P< .001 and P=.047, respectively). The concentrations of interferon gamma and transforming growth factor beta(2) were statistically significantly lower in patients having RAPF (mean [SE], 5.59 [1.11] pg/mL and 0.94 [0.46] ng/mL, respectively) than in patients having RA without ILD (mean [SE], 14.1 [1.9] pg/mL and 2.30 [0.39] ng/mL, respectively) (P=.001 and P=.006, respectively) or with preclinical ILD (mean [SD], 11.4 [2.6] pg/mL and 3.63 [0.66] ng/mL, respectively) (P=.04 and P=.007, respectively). Compared with patients having stable RA-ILD, patients having progressive RA-ILD had statistically significantly higher frequencies of treatment using methotrexate and higher alveolar concentrations of interferon gamma and transforming growth factor beta(1) (P=.046, P=.04, and P=.04, respectively). CONCLUSIONS: Asymptomatic preclinical ILD, which is detectable by HRCT, may be prevalent and progressive among patients having RA. Cigarette smoking seems to be associated with preclinical ILD in patients having RA, and treatment using methotrexate may be a risk factor for progression of preclinical ILD. Quantification of alveolar proteins indicates that potential pathogenic mechanisms seem to differ in patients having RA-ILD and symptomatic RAPF.
机译:背景:早期发现和治疗间质性肺病(ILD)的患者类风湿性关节炎(RA)可以改善疾病进展。确定无症状的肺疾病和潜力在RA患者和治疗目标临床前ILD (RA-ILD)。成人RA和10个成年人和RA肺纤维化(RAPF)的引用美国国立卫生研究院的贝塞斯达,马里兰,进行了高分辨率的计算断层扫描(HRCT)和肺生理测试。在肺泡液体量化。21岁的64名患者(33%)有风湿性关节炎呼吸困难或咳嗽临床ILD确认HRCT。疾病,患者RA-ILD统计大大延长历史的香烟吸烟(P <措施),频率的增加陶瓷器皿(P = .02点),alveolar-arterial更高氧梯度(P = 04),和更高的HRCT分数(P <措施)。发展12 21例(57%)RA-ILD。血小板源生长factor-AB和血小板源生长factor-BB是统计上显著更高RA-ILD(平均(SE), 497.3(78.6)和1473年分别为[264]pg / mL)的病人在RA没有ILD(平均(SE), 24.9 (42.4)分别为792.7 (195.0)pg / mL) (P <措施P =。干扰素γ和转化生长因子β(2)在统计学上显著降低病人有RAPF(平均(SE), 5.59 (1.11)pg / mL和0.94 [0.46]ng / mL,分别)无ILD的RA患者(平均(SE),14.1 [1.9] pg / mL和2.30 [0.39]ng / mL,) (P =。或临床前ILD(意味着(SD), 11.4 (2.6)pg / mL和3.63 [0.66]ng / mL,分别)(P = .04点和P =。有稳定RA-ILD,病人有进步RA-ILD有统计上显著提高使用甲氨蝶呤和频率的治疗干扰素的肺泡浓度更高γ和转化生长因子β(1)(P =。结论:无症状的临床前ILD,由HRCT可检测,可能是普遍的和进步的RA患者中。吸烟似乎与临床相关ILD的病人有风湿性关节炎,治疗使用甲氨蝶呤可能进展的危险因素临床前ILD。蛋白质表明潜在的致病性机制似乎不同的病人RA-ILD RAPF症状。

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