Department of Biochemistry and Molecular Biology, University of Southern Denmark, Denmark; Lab. of Functional Proteomics, Department of Life Sciences, University of Siena, Siena, Italy.
Lab. of Functional Proteomics, Department of Life Sciences, University of Siena, Siena, Italy.
J Proteomics. 2018 Jan 6;170:28-42. doi: 10.1016/j.jprot.2017.09.013. Epub 2017 Sep 29.
Cystic Fibrosis (CF) is a recessively inherited disease caused by mutations in the Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) gene. CFTR has a pivotal role in the onset of CF, and several proteins are involved in its homeostasis. To study CFTR interactors at protein species level, we used a functional proteomics approach combining 2D-DIGE, mass spectrometry and enrichment analysis. A human bronchial epithelial cell line with cystic fibrosis (CFBE41o-) and the control (16HBE14o-) were used for the comparison. 73 differentially abundant spots were identified and some validated by western-blot. Enrichment analysis highlighted molecular pathways in which ezrin, HSP70, endoplasmin and lamin A/C, in addition to CFTR, were considered central hubs in CFTR homeostasis. These proteins acquire different functions through post-translational modifications, emphasizing the importance of studying the CF proteome at protein species level. Moreover, serpin H1, prelamin A/C, protein-SET and cystatin-B were associated to CF, demonstrating the importance of heat shock response, cross-talk between the cytoskeleton and signal transduction, chronic inflammation and alteration of CFTR gating in the pathophysiology of the disease. These results open new perspectives for the understanding of the proteostasis network, characteristic of CF pathology, and could provide a springboard for new therapeutic strategies.
Homeostasis of CFTR is a dynamic process managed by multiple proteostatic pathways. The used gel-based proteomic approach and enrichment analysis pointed out protein species variations among Human Bronchial (16HBE14o-) and Cystic Fibrosis Bronchial Epithelial cell lines (CFBE41o-) and specific molecular mechanisms involved in CF. In particular, we have highlighted HSP70 (HSP7C), HSP90 (endoplasmin), ERM proteins (ezrin), and lamin-A/C as central hubs of the functional analysis. Moreover, for the first time we consider serpin H1, lamin A/C, protein-SET and cystatin-B important player in CF, affecting acute exacerbation, cytoskeleton reorganization, CFTR gating and chronic inflammation in CF. Due to the presence of different spots corresponding to the same protein, we focalize our attention on the idea that a "protein species discourse" is mandatory to well-define functional roles of proteins. Our approach has permitted to pay attention to the molecular mechanisms which regulate pathways directly or indirectly involved with CFTR defects: heat shock response, cross-talk between cytoskeleton and signal transduction, chronic inflammation and alteration of CFTR gating. Our data could open new perspectives into the understanding of CF, identifying potential targets for drug treatments in order to alleviate Δ508CFTR membrane instability and consequently increase life expectancy for CF patients.
囊性纤维化(CF)是一种由囊性纤维化跨膜电导调节因子(CFTR)基因突变引起的隐性遗传病。CFTR 在 CF 的发病机制中起着关键作用,有几种蛋白参与其动态平衡。为了在蛋白水平上研究 CFTR 的相互作用蛋白,我们采用了一种结合 2D-DIGE、质谱和富集分析的功能蛋白质组学方法。我们使用囊性纤维化(CFBE41o-)和对照(16HBE14o-)的人支气管上皮细胞系进行了比较。鉴定了 73 个差异丰度斑点,并用 Western blot 进行了部分验证。富集分析突出了分子途径,除 CFTR 外,埃兹蛋白、HSP70、内质网蛋白和核纤层 A/C 被认为是 CFTR 动态平衡的中心枢纽。这些蛋白通过翻译后修饰获得不同的功能,强调了在蛋白水平上研究 CF 蛋白质组的重要性。此外,丝氨酸蛋白酶抑制剂 H1、前层粘连蛋白 A/C、蛋白 SET 和胱抑素-B 与 CF 相关,表明热休克反应、细胞骨架与信号转导之间的串扰、慢性炎症和 CFTR 门控改变在疾病的病理生理学中的重要性。这些结果为理解 CF 病理学特征的蛋白质稳态网络提供了新的视角,并为新的治疗策略提供了一个起点。
CFTR 的动态平衡是一个由多个蛋白质稳态途径管理的动态过程。所使用的基于凝胶的蛋白质组学方法和富集分析指出了人支气管(16HBE14o-)和囊性纤维化支气管上皮细胞系(CFBE41o-)之间的蛋白种类变化以及涉及 CF 的特定分子机制。特别是,我们强调了 HSP70(HSP7C)、HSP90(内质网蛋白)、ERM 蛋白(埃兹蛋白)和核纤层 A/C 作为功能分析的中心枢纽。此外,我们首次认为丝氨酸蛋白酶抑制剂 H1、核纤层 A/C、蛋白 SET 和胱抑素-B 是 CF 的重要参与者,影响 CF 的急性加重、细胞骨架重组、CFTR 门控和慢性炎症。由于存在对应于同一蛋白质的不同斑点,我们关注这样一个想法,即“蛋白质种类论述”对于明确蛋白质的功能作用是强制性的。我们的方法使我们注意到调节途径的分子机制,这些途径直接或间接地涉及 CFTR 缺陷:热休克反应、细胞骨架与信号转导之间的串扰、慢性炎症和 CFTR 门控改变。我们的数据可以为理解 CF 提供新的视角,确定药物治疗的潜在靶点,以减轻 Δ508CFTR 膜的不稳定性,从而提高 CF 患者的预期寿命。
