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相互矛盾的信息:衰竭及恢复过程中的人类心肌转录模式

Mixed messages: transcription patterns in failing and recovering human myocardium.

作者信息

Margulies Kenneth B, Matiwala Sunil, Cornejo Carla, Olsen Henrik, Craven William A, Bednarik Daniel

机构信息

Cardiovascular Research Center, Cardiovascular Research Institute, University of Pennsylvania School of Medicine, Temple University School of Medicine, Philadelphia, Pa 19104-6160, USA.

出版信息

Circ Res. 2005 Mar 18;96(5):592-9. doi: 10.1161/01.RES.0000159390.03503.c3. Epub 2005 Feb 17.

Abstract

In previous studies, mechanical support of medically refractory hearts with a left ventricular assist device (LVAD) has induced regression of many morphological and functional abnormalities characteristic of failing human hearts. To identify transcriptional adaptations in failing and LVAD-supported hearts, we performed a comprehensive transcription analysis using the Affymetrix microarray platform and 199 human myocardial samples from nonfailing, failing, and LVAD-supported human hearts. We also used a novel analytical strategy that defines patterns of interest based on multiple intergroup comparisons. Although over 3088 transcripts exhibited significantly altered abundance in heart failure, most of these did not exhibit a consistent response to LVAD support based on our analysis. Of those 238 with a consistent response to LVAD support, more than 75% exhibited persistence or exacerbation of HF-associated transcriptional abnormalities whereas only 11%, 5%, and 2% exhibited partial recovery, normalization, and overcorrection responses, respectively. Even among genes implicated by previous reports of LVAD-associated myocardial improvements, partial or complete normalization of transcription did not predominate. The magnitude of differences in transcript abundance between nonfailing and failing hearts, and between failing an LVAD-supported hearts, tended to be low with changes greater than or equal to 2-fold infrequently observed. Our results indicate that morphological or functional myocardial improvements may occur without widespread normalization of pathological transcriptional patterns. These observations also suggest that many failure-associated transcriptional changes have only a limited role in regulating cardiac structure and function and may represent epiphenomena and/or nonspecific myocardial plasticity responses. Differences in mRNA localization, translation efficiency, and posttranslational protein modifications or interactions may be more pivotal in regulating myocardial structure and function.

摘要

在先前的研究中,使用左心室辅助装置(LVAD)对药物难治性心脏进行机械支持已使许多人类衰竭心脏特有的形态和功能异常出现消退。为了确定衰竭心脏和LVAD支持的心脏中的转录适应性变化,我们使用Affymetrix微阵列平台以及来自非衰竭、衰竭和LVAD支持的人类心脏的199份人类心肌样本进行了全面的转录分析。我们还采用了一种新颖的分析策略,该策略基于多个组间比较来定义感兴趣的模式。尽管超过3088个转录本在心力衰竭中表现出丰度的显著改变,但根据我们的分析,其中大多数对LVAD支持并未表现出一致的反应。在对LVAD支持有一致反应的238个转录本中,超过75%表现出与心力衰竭相关的转录异常持续存在或加重,而分别只有11%、5%和2%表现出部分恢复、正常化和过度校正反应。即使在先前报道与LVAD相关的心肌改善有关的基因中,转录的部分或完全正常化也并不占主导。非衰竭心脏与衰竭心脏之间,以及衰竭心脏与LVAD支持的心脏之间,转录本丰度的差异幅度往往较低,很少观察到变化大于或等于2倍的情况。我们的结果表明,心肌形态或功能的改善可能在病理转录模式未广泛正常化的情况下发生。这些观察结果还表明,许多与衰竭相关的转录变化在调节心脏结构和功能方面仅起有限作用,可能代表附带现象和/或非特异性心肌可塑性反应。mRNA定位、翻译效率以及翻译后蛋白质修饰或相互作用的差异可能在调节心肌结构和功能方面更为关键。

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