The atrial and ventricular myocardial proteome of end-stage lamin heart disease.

Constantin-Cristian Topriceanu, Mashael Alfarih, Alun D Hughes, Hunain Shiwani, Fiona Chan, Saidi A Mohiddin, William Moody, Richard P Steeds, Benjamin O'Brien, Jakob Vowinckel, Petros Syrris, Caroline Coats, Stephen Pettit, Eloisa Arbustini, James C Moon, Gabriella Captur
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Abstract

Lamins A/C (encoded by LMNA gene) can lead to dilated cardiomyopathy (DCM). This pilot study sought to explore the postgenomic phenotype of end-stage lamin heart disease. Consecutive patients with end-stage lamin heart disease (LMNA-group, n = 7) and ischaemic DCM (ICM-group, n = 7) undergoing heart transplantation were prospectively enrolled. Samples were obtained from left atrium (LA), left ventricle (LV), right atrium (RA), right ventricle (RV) and interventricular septum (IVS), avoiding the infarcted myocardial segments in the ICM-group. Samples were analysed using a discovery 'shotgun' proteomics approach. We found that 990 proteins were differentially abundant between LMNA and ICM samples with the LA being most perturbed (16-fold more than the LV). Abundance of lamin A/C protein was reduced, but lamin B increased in LMNA LA/RA tissue compared to ICM, but not in LV/RV. Carbonic anhydrase 3 (CA3) was over-abundant across all LMNA tissue samples (LA, LV, RA, RV, and IVS) when compared to ICM. Transthyretin was more abundant in the LV/RV of LMNA compared to ICM, while sarcomeric proteins such as titin and cardiac alpha-cardiac myosin heavy chain were generally less abundant in RA/LA of LMNA. Protein expression profiling and enrichment analysis pointed towards sarcopenia, extracellular matrix remodeling, deficient myocardial energetics, redox imbalances, and abnormal calcium handling in LMNA samples. Compared to ICM, end-stage lamin heart disease is a biventricular but especially a biatrial disease appearing to have an abundance of lamin B, CA3 and transthyretin, potentially hinting to compensatory responses.

终末期片状心脏病的心房和心室心肌蛋白质组。
Lamins/A/C(由 LMNA 基因编码)可导致扩张型心肌病(DCM)。这项试验性研究旨在探索终末期拉明氏心脏病的基因组后表型。研究人员前瞻性地招募了接受心脏移植的终末期板层心脏病患者(LMNA 组,n = 7)和缺血性扩张型心肌病患者(ICM 组,n = 7)。样本取自左心房(LA)、左心室(LV)、右心房(RA)、右心室(RV)和室间隔(IVS),在 ICM 组中避开梗死的心肌区段。样本采用发现性 "散弹枪 "蛋白质组学方法进行分析。我们发现,在 LMNA 和 ICM 样本中,有 990 种蛋白质的丰度存在差异,其中 LA 受干扰最大(是 LV 的 16 倍)。与 ICM 相比,LMNA LA/RA 组织中层板 A/C 蛋白的丰度降低,但层板 B 蛋白的丰度增加,而 LV/RV 组织中层板 B 蛋白的丰度则没有增加。与 ICM 相比,碳酸酐酶 3(CA3)在所有 LMNA 组织样本(LA、LV、RA、RV 和 IVS)中含量过高。与 ICM 相比,转甲状腺素在 LMNA 的 LV/RV 中含量更高,而在 LMNA 的 RA/LA 中,肉瘤蛋白(如 titin 和心肌α-肌球蛋白重链)的含量普遍较低。蛋白质表达谱分析和富集分析表明,LMNA 样本中存在肌肉疏松症、细胞外基质重塑、心肌能量不足、氧化还原失衡和钙处理异常。与 ICM 相比,终末期板层心肌病是一种双心室疾病,尤其是双心房疾病,似乎有大量的板层 B、CA3 和转甲状腺素,这可能暗示着代偿反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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