Novel in vitro and in vivo data on the cellular localization of Hsp10 in smokers affected by COPD and in lung-derived cell lines exposed to cigarette smoke extract as stressor

S. Corrao, R. Anzalone, M. Iacono, F. Farina, G. Peri, G. Zummo, A. Stefano, P. Brun, B. Balbi, E. Macario, A. Macario, F. Cappello, G. Rocca
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Abstract

Cigarette smoke is a potent stressor for the respiratory system, contributing to pathogenesis, for instance in chronic obstructive pulmonary disease (COPD), but its effects on the expression, function, and cellular localization of mitochondrial chaperonins are still largely unknown. We studied in vivo (airways biopsies) the localization of Hsp10 and Hsp60 in patients (smokers and non-smokers) affected by mild-moderate COPD, and characterized the effects of non-lethal doses of cigarette smoke extract (CSE) on the expression of these molecules in two human cell lines: lung fibroblasts (HFL-1) and bronchial epithelial (16HBE). We applied various in vitro methods: immunohistochemistry (IHC), subcellular fractionation analyses (SFA), Western blotting (WB), immunocytochemistry (ICC), and transmission electron microscopy (TEM) immunogold, and used bioinformatics and databases searches to gather structural in silico data for interpreting and complementing the in vitro results. IHC showed that in smokers and non-smokers COPD patients Hsp10 was localized in both, the cytoplasm and the nucleus of epithelial and lamina propria cells, while Hsp60 was present only in the cytosol. ICC, SFA, and WB on both CSE-exposed cell lines confirmed the presence of nuclear Hsp10, with an increasing trend in parallel to CSE concentration. TEM immunogold further confirmed Hsp10 in the nucleus, in addition to its presence in the cytoplasm and mitochondria, on both cell lines. Bioinformatics and in silico structural analyses indicated that Hsp10 can localize in extramitochondrial sites, such as the nucleus, even if Hsp10 lacks known DNA-binding motifs or nuclear import signals in its primary sequence. Our data suggest a link between exposure to exogenous oxidative stress and cell response, involving Hsp10, which would play roles different from its canonical functions. It is known that Hsp10 can display an array of functions depending on its location: cytoplasm, mitochondria, or extracellular. Here, we show for the first time the presence of Hsp10 in the nucleus of epithelial and stromal human-lung cell lines, paralleling the observations in vivo in COPD patients, and indicating that intranuclear Hsp10 levels are affected by oxidative stress due to an exogenous stressor like cigarette-smoke. The questions now are by what mechanism Hsp10 becomes a resident of the nucleus and what are its functions there.
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关于慢性阻塞性肺病患者和暴露于香烟烟雾提取物作为应激源的肺源细胞系中Hsp10细胞定位的新体外和体内数据
吸烟是呼吸系统的一种强有力的应激源,有助于致病,例如慢性阻塞性肺疾病(COPD),但其对线粒体伴侣蛋白的表达、功能和细胞定位的影响在很大程度上仍然未知。我们在体内(气道活检)研究了患有轻中度COPD的患者(吸烟者和非吸烟者)Hsp10和Hsp60的定位,并表征了非致死剂量的香烟烟雾提取物(CSE)对两种人类细胞系:肺成纤维细胞(HFL-1)和支气管上皮(16HBE)中这些分子表达的影响。我们应用了多种体外方法:免疫组织化学(IHC)、亚细胞分离分析(SFA)、免疫印迹(WB)、免疫细胞化学(ICC)和透射电子显微镜(TEM)免疫金,并使用生物信息学和数据库搜索来收集结构硅数据,以解释和补充体外结果。免疫组化结果显示,在吸烟者和非吸烟者COPD患者中,Hsp10均存在于上皮细胞和固有层细胞的细胞质和细胞核中,而Hsp60仅存在于细胞质中。两种暴露于CSE的细胞株上的ICC、SFA和WB均证实了核Hsp10的存在,且其增加趋势与CSE浓度平行。透射电镜免疫金进一步证实,除了在细胞质和线粒体中存在外,两种细胞系的细胞核中也存在Hsp10。生物信息学和计算机结构分析表明,Hsp10可以定位于线粒体外位点,如细胞核,即使Hsp10的初级序列缺乏已知的dna结合基序或核输入信号。我们的数据表明,暴露于外源性氧化应激和细胞反应之间存在联系,包括Hsp10,它可能发挥与其典型功能不同的作用。已知Hsp10可以根据其位置显示一系列功能:细胞质,线粒体或细胞外。在这里,我们首次发现Hsp10存在于上皮和间质人肺细胞系的细胞核中,与COPD患者体内的观察结果相一致,并表明核内Hsp10水平受到香烟烟雾等外源性应激源引起的氧化应激的影响。现在的问题是Hsp10通过什么机制成为细胞核的居民以及它在那里的功能是什么。
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期刊介绍: The Italian Journal of Anatomy and Embryology, founded in 1901 by Giulio Chiarugi, Anatomist at Florence University, is a peer-reviewed journal sponsored by the Italian Society of Anatomy and Embryology. The journal publishes original papers, invited review articles, historical article, commentaries, obituitary, and book reviews. Its main focus is to understand anatomy through an analysis of structure, function, development and evolution. Priority will be given to studies of that clearly articulate their relevance to the anatomical community. Focal areas include: experimental studies, contributions based on molecular and cell biology and on the application of modern imaging techniques; comparative functional morphology; developmental biology; functional human anatomy; methodological innovations in anatomical research; significant advances in anatomical education. Studies that are essentially descriptive anatomy are appropriate only if they communicate clearly a broader functional or evolutionary significance. All papers should be submitted in English and must be original works that are unpublished and not under consideration by another journal. An international Editorial Board and reviewers from the anatomical disciplines guarantee a rapid review of your paper within two to three weeks after submission.
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