系统性硬化症中的重度限制性肺病。

Severe restrictive lung disease in systemic sclerosis.

作者信息

Steen V D, Conte C, Owens G R, Medsger T A

机构信息

University of Pittsburgh School of Medicine, Pennsylvania.

出版信息

Arthritis Rheum. 1994 Sep;37(9):1283-9. doi: 10.1002/art.1780370903.

DOI:10.1002/art.1780370903

PMID:7945490

Abstract

OBJECTIVE

We sought to identify risk factors for developing severe restrictive lung disease and to determine the time of onset and rate of progression in patients with systemic sclerosis (SSc).

METHODS

Using the University of Pittsburgh Scleroderma Databank, we grouped patients according to their lowest forced vital capacity (FVC) value: > 75% predicted, 50-75% predicted, and < 50% predicted. In patients with severe restrictive disease, we examined serial pulmonary function test (PFT) results to determine the rate of loss of lung volume over time.

RESULTS

Of 890 SSc patients, 60% (n = 531) never had an FVC < or = 75% predicted; 27% (n = 243) had moderate restrictive disease, with an FVC value of 50-75% predicted; and only 13% (n = 116) of the patients had severe restrictive disease, with FVC < or = 50% predicted. Black race, male sex, early disease, and primary cardiac involvement due to SSc were the features most frequently associated with severe restrictive lung disease (by multiple logistic regression). Fifty-five patients with severe restrictive lung disease had their first of at least 2 PFTs during the first 5 years after onset of any SSc (not pulmonary) symptoms. In 30 patients, the FVC declined by 32% per year in the first 2 years of illness, in 16 patients the annual loss was 12% in years 2-4 after disease onset, and in 9 patients annual loss was 3% during years 4-6 of disease (P < 0.005 by 1-way analysis of variance).

CONCLUSION

In SSc patients, black men with early disease who have cardiac involvement are the most likely to have factors associated with the development of severe restrictive lung disease (which is increasingly becoming a major cause of death). Disease subtype (diffuse versus limited cutaneous) and serum anti-topoisomerase I antibody do not differentiate between moderate and severe restrictive disease. Careful monitoring of pulmonary function early in the disease, when the greatest loss of lung function occurs, may help identify patients likely to respond to new therapy.

摘要

目的

我们试图确定系统性硬化症（SSc）患者发生严重限制性肺病的危险因素，并确定发病时间和疾病进展速度。

方法

利用匹兹堡大学硬皮病数据库，我们根据患者的最低用力肺活量（FVC）值对患者进行分组：>预测值的75%、预测值的50%-75%和<预测值的50%。对于患有严重限制性疾病的患者，我们检查了系列肺功能测试（PFT）结果，以确定肺容积随时间的丢失率。

结果

在890例SSc患者中，60%（n = 531）的FVC从未<或=预测值的75%；27%（n = 243）患有中度限制性疾病，FVC值为预测值的50%-75%；只有13%（n = 116）的患者患有严重限制性疾病，FVC<或=预测值的50%。黑人种族、男性、疾病早期以及SSc所致的原发性心脏受累是与严重限制性肺病最常相关的特征（通过多因素逻辑回归分析）。55例患有严重限制性肺病的患者在出现任何SSc（非肺部）症状后的前5年内进行了至少2次PFT中的第一次检查。在30例患者中，疾病最初2年内FVC每年下降32%，在16例患者中，疾病发病后第2-4年每年下降12%，在9例患者中，疾病第4-6年每年下降3%（通过单因素方差分析，P < 0.005）。

结论

在SSc患者中，患有心脏受累的疾病早期黑人男性最有可能具有与严重限制性肺病发生相关的因素（严重限制性肺病正日益成为主要死因）。疾病亚型（弥漫性与局限性皮肤型）和血清抗拓扑异构酶I抗体并不能区分中度和重度限制性疾病。在疾病早期，当肺功能发生最大程度丢失时，仔细监测肺功能可能有助于识别可能对新疗法有反应的患者。