NH2-Terminal Cleavage of Cardiac Troponin I Signals Adaptive Response to Cardiac Stressors

Journal of cellular signaling Pub Date : 2021-09-02 DOI:10.33696/signaling.2.048

C. Warren, M. Halas, H. Feng, B. Wolska, Jian-Ping Jin, R. Solaro

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引用次数: 1

Abstract

Cardiac sarcomeres express a variant of troponin I (cTnI) that contains a unique N-terminal extension of ~30 amino acids with regulatory phosphorylation sites. The extension is important in the control of myofilament response to Ca2+, which contributes to the neuro-humoral regulation of the dynamics of cardiac contraction and relaxation. Hearts of various species including humans express a stress-induced truncated variant of cardiac troponin I (cTnI-ND) missing the first ~30 amino acids and functionally mimicking the phosphorylated state of cTnI. Studies have demonstrated that upregulation of cTnI-ND potentially represents a homeostatic mechanism as well as an adaptive response in pathophysiology including ischemia/reperfusion injury, beta adrenergic maladaptive activation, and aging. We present evidence showing that cTnI-ND can modify the trigger for hypertrophic cardiomyopathy (HCM) by reducing the Ca2+ sensitivity of myofilaments from hearts with an E180G mutation in α-tropomyosin. Induction of this truncation may represent a therapeutic approach to modifying Ca2+-responses in hearts with hypercontractility or heat failure with preserved ejection fraction.

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心肌肌钙蛋白I的nh2末端切割信号对心脏应激源的适应性反应

心肌肌瘤表达一种肌钙蛋白I (cTnI)的变体，它包含一个独特的n端延伸，约30个氨基酸，具有调节磷酸化位点。这种延伸在控制肌丝对Ca2+的反应中是重要的，这有助于心脏收缩和舒张动力学的神经-体液调节。包括人类在内的许多物种的心脏都表达一种应力诱导的心肌肌钙蛋白I (cTnI- nd)的截断变体，缺失了前30个氨基酸，在功能上模仿了cTnI的磷酸化状态。研究表明，cTnI-ND的上调可能代表了一种稳态机制，以及病理生理上的适应性反应，包括缺血/再灌注损伤、β肾上腺素能适应不良激活和衰老。我们提出的证据表明，cTnI-ND可以通过降低α-原肌球蛋白E180G突变的心脏肌丝对Ca2+的敏感性来改变肥厚性心肌病(HCM)的触发因素。诱导这种截断可能代表了一种治疗方法，以改变心肌过度收缩或热衰竭保留射血分数的Ca2+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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Journal of cellular signaling

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