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结节病相关肺动脉高压的表型——一个具有挑战性的谜团。

Phenotypes of Sarcoidosis-Associated Pulmonary Hypertension-A Challenging Mystery.

作者信息

Kacprzak Aneta, Tomkowski Witold, Szturmowicz Monika

机构信息

1st Department of Lung Diseases, National Tuberculosis and Lung Diseases Institute, Plocka 26, 01-138 Warsaw, Poland.

出版信息

Diagnostics (Basel). 2023 Oct 5;13(19):3132. doi: 10.3390/diagnostics13193132.

Abstract

Sarcoidosis has been a well-recognised risk factor for pulmonary hypertension (PH) for a long time, but still, the knowledge about this concatenation is incomplete. Sarcoidosis-associated PH (SAPH) is an uncommon but serious complication associated with increased morbidity and mortality among sarcoidosis patients. The real epidemiology of SAPH remains unknown, and its pathomechanisms are not fully explained. Sarcoidosis is a heterogeneous and dynamic condition, and SAPH pathogenesis is believed to be multifactorial. The main roles in SAPH development play: parenchymal lung disease with the destruction of pulmonary vessels, the extrinsic compression of pulmonary vessels by conglomerate masses, lymphadenopathy or fibrosing mediastinitis, pulmonary vasculopathy, LV dysfunction, and portal hypertension. Recently, it has been recommended to individually tailor SAPH management according to the predominant pathomechanism, i.e., SAPH phenotype. Unfortunately, SAPH phenotyping is not a straightforward process. First, there are gaps in our understanding of undergoing processes. Second, the assessment of such a pivotal element as pulmonary vasculature on a microscopic level is non-feasible in SAPH patients antemortem. Finally, SAPH is a dynamic condition, multiple phenotypes usually coexist, and patients can switch between phenotypes during the course of sarcoidosis. In this article, we summarise the basic knowledge of SAPH, describe SAPH phenotypes, and highlight some practical problems related to SAPH phenotyping.

摘要

长期以来,结节病一直是公认的肺动脉高压(PH)危险因素,但即便如此,关于这种关联的认识仍不完整。结节病相关肺动脉高压(SAPH)是一种不常见但严重的并发症,与结节病患者发病率和死亡率增加相关。SAPH的真实流行病学情况仍不明确,其发病机制也未得到充分解释。结节病是一种异质性和动态性疾病,SAPH的发病机制被认为是多因素的。在SAPH发展过程中起主要作用的因素有:伴有肺血管破坏的实质性肺部疾病、结节肿块、淋巴结病或纤维性纵隔炎对肺血管的外在压迫、肺血管病变、左心室功能障碍和门静脉高压。最近,有人建议根据主要发病机制,即SAPH表型,对SAPH进行个体化治疗。不幸的是,SAPH表型分析并非一个简单的过程。首先,我们对相关过程的理解存在空白。其次,在生前对SAPH患者进行微观层面的肺血管这一关键要素评估是不可行的。最后,SAPH是一种动态疾病,多种表型通常并存,并且患者在结节病病程中可能会在不同表型之间转换。在本文中,我们总结了SAPH的基础知识,描述了SAPH表型,并强调了与SAPH表型分析相关的一些实际问题。

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