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心脏淀粉样变中的蛋白毒性:淀粉样变轻链影响人心脏细胞内的蛋白质水平。

Proteotoxicity in cardiac amyloidosis: amyloidogenic light chains affect the levels of intracellular proteins in human heart cells.

机构信息

IRCCS SDN, Naples, Italy.

CEINGE-Biotecnologie Avanzate, Naples, Italy.

出版信息

Sci Rep. 2017 Nov 15;7(1):15661. doi: 10.1038/s41598-017-15424-3.

Abstract

AL amyloidosis is characterized by widespread deposition of immunoglobulin light chains (LCs) as amyloid fibrils. Cardiac involvement is frequent and leads to life-threatening cardiomyopathy. Besides the tissue alteration caused by fibrils, clinical and experimental evidence indicates that cardiac damage is also caused by proteotoxicity of prefibrillar amyloidogenic species. As in other amyloidoses, the damage mechanisms at cellular level are complex and largely undefined. We have characterized the molecular changes in primary human cardiac fibroblasts (hCFs) exposed in vitro to soluble amyloidogenic cardiotoxic LCs from AL cardiomyopathy patients. To evaluate proteome alterations caused by a representative cardiotropic LC, we combined gel-based with label-free shotgun analysis and performed bioinformatics and data validation studies. To assess the generalizability of our results we explored the effects of multiple LCs on hCF viability and on levels of a subset of cellular proteins. Our results indicate that exposure of hCFs to cardiotropic LCs translates into proteome remodeling, associated with apoptosis activation and oxidative stress. The proteome alterations affect proteins involved in cytoskeletal organization, protein synthesis and quality control, mitochondrial activity and metabolism, signal transduction and molecular trafficking. These results support and expand the concept that soluble amyloidogenic cardiotropic LCs exert toxic effects on cardiac cells.

摘要

AL 淀粉样变性的特征是免疫球蛋白轻链 (LC) 广泛沉积为淀粉样纤维。心脏受累很常见,可导致危及生命的心肌病。除了纤维引起的组织改变外,临床和实验证据表明,心脏损伤也是由前纤维状淀粉样原纤维物种的蛋白毒性引起的。与其他淀粉样变性一样,细胞水平的损伤机制很复杂,在很大程度上还未定义。我们已经在体外研究了来自 AL 心肌病患者的可溶性致心脏毒性 LC 对原代人心脏成纤维细胞 (hCFs) 的分子变化。为了评估代表性致心脏毒性 LC 引起的蛋白质组改变,我们结合了基于凝胶的无标记鸟枪法分析,并进行了生物信息学和数据验证研究。为了评估我们结果的普遍性,我们研究了多种 LC 对 hCF 活力和细胞内蛋白质亚群水平的影响。我们的结果表明,hCFs 暴露于致心脏毒性 LC 会导致蛋白质组重塑,与细胞凋亡激活和氧化应激有关。蛋白质组改变影响细胞骨架组织、蛋白质合成和质量控制、线粒体活性和代谢、信号转导和分子运输中涉及的蛋白质。这些结果支持并扩展了可溶性致心脏毒性淀粉样变性 LC 对心脏细胞产生毒性作用的概念。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5089/5688098/74380479927f/41598_2017_15424_Fig1_HTML.jpg

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