The role of Endoplasmic Reticulum (ER) stress in pulmonary fibrosis

IF 0.7 Cell Pathology Pub Date : 2016-01-01 DOI:10.1515/ersc-2016-0002
M. Korfei, C. Ruppert, Benjamin Loeh, P. Mahavadi, A. Guenther
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引用次数: 5

Abstract

Abstract The activation of Endoplasmic Reticulum (ER) stress and Unfolded Protein Response (UPR) was first observed in patients with familial interstitial pneumonia (FIP) carrying mutations in the C-terminal BRICHOS domain of surfactant protein C (SFTPC). Here, aggresome formation and severe ER stress was demonstrated in type-II alveolar epithelial cells (AECII), which specifically express this very hydrophobic surfactant protein. In subsequent studies, FIP-patients with mutations in the gene encoding surfactant protein A2 (SFTPA2) were discovered, whose overexpression in epithelial cells in vitro also resulted in significant induction of ER stress. Moreover, prominent ER stress in AECII was also observed in FIP-patients not carrying the SFTPC/SFTPA2 mutations, as well as in patients with the more common sporadic forms of IP. Additionally, cases of adult-onset FIP with mutations in Telomerase genes and other telomereassociated components were reported. These mutations were associated with telomere shortening, which is a potential cause for triggering a persistent DNA damage response and replicative senescence in affected cells. Moreover, shortened telomeres were observed directly in the AECII of FIP-patients, and even sporadic IP cases, in the absence of any gene mutations. Here, we try to figure out the possible origins of ER stress in sporadic IP cases and non-SFTPC/SFTPA2-associated FIP.
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内质网应激在肺纤维化中的作用
在携带表面活性蛋白C (SFTPC) C端BRICHOS结构域突变的家族性间质性肺炎(FIP)患者中,首次观察到内质网(ER)应激和未折叠蛋白反应(UPR)的激活。在ii型肺泡上皮细胞(AECII)中,聚集体的形成和严重的内质网应激被证明是特异性表达这种非常疏水的表面活性剂蛋白的。在随后的研究中,发现了编码表面活性剂蛋白A2 (SFTPA2)基因突变的fip患者,其在体外上皮细胞中的过表达也导致了内质网应激的显著诱导。此外,在不携带SFTPC/SFTPA2突变的fip患者以及更常见的散发型IP患者中,也观察到AECII中突出的内质网应激。此外,还报道了端粒酶基因和其他端粒相关成分突变的成人发病FIP病例。这些突变与端粒缩短有关,这是引发持续DNA损伤反应和受影响细胞复制性衰老的潜在原因。此外,在没有任何基因突变的情况下,在fip患者的AECII中直接观察到端粒缩短,甚至在散发性IP病例中也是如此。在这里,我们试图找出零星IP病例和非sftpc / sftpa2相关FIP中内质网应激的可能来源。
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