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Idiopathic interstitial pneumonias: clinical findings, pathogenesis, pathology and radiologic findings.

机译:特发性间质性肺炎:临床表现,发病机制,病理学和影像学发现。

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摘要

Idiopathic interstitial pneumonias are currently classified into four categories: usual interstitial pneumonia, nonspecific interstitial pneumonia with fibrosis, acute interstitial pneumonia and desquamative interstitial pneumonia. The fibrotic process in interstitial pneumonias appears to result from a complex interaction between fibroblasts, other lung parenchymal cells and macrophages. The complex relationship between the local release of growth-promoting cytokines by alveolar macrophages and resident fibroblasts represents a necessary step for fibrosis or remodeling after lung injury. Injury to the epithelium and basement membranes is likely necessary for the fibrotic process to occur. Usual interstitial pneumonia, most frequent among interstitial pneumonias and has a poor prognosis, appears on high-resolution CT as patchy subpleural areas of ground-glass attenuation, irregular linear opacity, and honeycombing. Nonspecific interstitial pneumonia with fibrosis, the second most frequent and has a better prognosis than usual interstitial pneumonia, appears as subpleural patchy areas of ground-glass attenuation with associated areas of irregular linear opacity on CT. Acute interstitial pneumonia with high mortality rate presents as extensive bilateral airspace consolidation and patchy or diffuse bilateral areas of ground-glass attenuation. Desquamative interstitial pneumonia with good prognosis presents as patchy subpleural areas of ground-glass attenuation in middle and lower lung zones.
机译:特发性间质性肺炎目前分为四类:普通间质性肺炎,非特异性间质性纤维化肺炎,急性间质性肺炎和脱屑性间质性肺炎。间质性肺炎的纤维化过程似乎是由成纤维细胞,其他肺实质细胞和巨噬细胞之间复杂的相互作用导致的。肺泡巨噬细胞局部释放促进生长的细胞因子与驻留的成纤维细胞之间的复杂关系代表了肺损伤后纤维化或重塑的必要步骤。发生纤维化过程可能需要损伤上皮和基底膜。通常的间质性肺炎在间质性肺炎中最常见且预后较差,在高分辨率CT上表现为斑块状的胸膜下玻璃膜衰减,不规则线性不透明和蜂窝状。非特异性间质性肺炎并发纤维化,是第二常见的,并且比通常的间质性肺炎预后更好,表现为磨玻璃下的胸膜下斑块状区域,以及CT上不规则线性不透明的相关区域。高死亡率的急性间质性肺炎表现为广泛的双边空域合并和双侧或斑块状弥漫性的玻璃液衰减区域。皮下炎斑块状胸膜下区域在肺的中下部肺区衰减较弱,预后良好。

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  • 作者

    Lee, K. S.; Chung, M. P.;

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  • 年度 1999
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