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特发性隐源性纤维化肺泡炎及与系统性硬化症相关的纤维化肺泡炎的功能损害:一项比较研究

Functional impairment in lone cryptogenic fibrosing alveolitis and fibrosing alveolitis associated with systemic sclerosis: a comparison.

作者信息

Wells A U, Hansell D M, Rubens M B, Cailes J B, Black C M, du Bois R M

机构信息

Department of Radiology, Royal Brompton Hospital, London, United Kingdom.

出版信息

Am J Respir Crit Care Med. 1997 May;155(5):1657-64. doi: 10.1164/ajrccm.155.5.9154872.

Abstract

Lone cryptogenic fibrosing alveolitis (CFA) is histologically identical to fibrosing alveolitis associated with systemic sclerosis (FASSc), but it has a much worse prognosis after matching for disease severity at presentation. Thin-section CT scanning (CT) provides a reproducible method of quantifying the morphologic extent of fibrosing alveolitis. The aim of this study was to gain insights into contrasting pathophysiologic mechanisms in the two diseases by comparing patterns of functional impairment after matching for extent of disease on CT, demographic factors, smoking history, and concurrent treatment. Patients with emphysema on CT (n = 16) and patients with FASSc with overt pulmonary hypertension (n = 5) were excluded; 111 patients were studied (CFA, n = 54; FASSc, n = 57). Patients with CFA were distinguished by more severe functional impairment and more extensive disease on CT (40.1 versus 22.1%, p < 0.00005). On multivariate analysis, patients with CFA had greater reduction in arterial P(O2) (p < 0.0005), wider AaP(O2) (p < 0.0005), greater oxygen desaturation on maximal exercise (p < 0.03), and higher dyspnea scores (p < 0.02) than did patients with FASSc after controlling for extent of disease on CT and other covariates. Measures of lung volume and gas transfer did not differ independently between CFA and FASSc. These findings persisted in subanalyses of patients with limited disease, extensive disease, histologic confirmation of fibrosing alveolitis, and with the reinclusion of patients with emphysema and pulmonary hypertension. The patterns of functional impairment were indicative of more severe ventilation-perfusion mismatch or anatomic shunting in CFA after adjustment for disease extent; we speculate that perfusion of poorly ventilated lung parenchyma in CFA occurs through new vessels formed in areas of intense inflammation. This mechanism may contribute to the greater mortality of patients with CFA than of patients with FASSc because of the deleterious effects of hypoxia on concurrent cardiac disease.

摘要

特发性隐源性纤维性肺泡炎(CFA)在组织学上与系统性硬化症相关的纤维性肺泡炎(FASSc)相同,但在根据就诊时疾病严重程度进行匹配后,其预后要差得多。薄层CT扫描(CT)提供了一种可重复的方法来量化纤维性肺泡炎的形态学范围。本研究的目的是通过比较在CT上疾病范围、人口统计学因素、吸烟史和同时进行的治疗相匹配后的功能损害模式,深入了解这两种疾病不同的病理生理机制。CT显示有肺气肿的患者(n = 16)和有明显肺动脉高压的FASSc患者(n = 5)被排除;共研究了111例患者(CFA,n = 54;FASSc,n = 57)。CFA患者的特点是功能损害更严重,CT上疾病范围更广(40.1%对22.1%,p < 0.00005)。多因素分析显示,在控制CT上的疾病范围和其他协变量后,CFA患者的动脉血氧分压(P(O2))下降幅度更大(p < 0.0005),肺泡-动脉血氧分压差(AaP(O2))更宽(p < 0.0005),最大运动时氧饱和度下降更明显(p < 0.03),呼吸困难评分更高(p < 0.02)。CFA和FASSc之间肺容积和气体交换的指标没有独立差异。这些发现在对疾病局限、广泛、纤维性肺泡炎组织学确诊的患者进行亚分析时以及重新纳入肺气肿和肺动脉高压患者后仍然存在。功能损害模式表明,在调整疾病范围后,CFA中存在更严重的通气-灌注不匹配或解剖分流;我们推测,CFA中通气不良的肺实质的灌注是通过在炎症强烈区域形成的新血管进行 的。由于缺氧对并发心脏病的有害影响,这种机制可能导致CFA患者的死亡率高于FASSc患者。

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