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细胞拼图中的移动板块:来自蝎毒素 Ts14 的神秘肽通过去磷酸化磷蛋白激活 AKT 和 ERK 信号通路并降低心肌细胞收缩性。

Moving Pieces in a Cellular Puzzle: A Cryptic Peptide from the Scorpion Toxin Ts14 Activates AKT and ERK Signaling and Decreases Cardiac Myocyte Contractility via Dephosphorylation of Phospholamban.

机构信息

Departamento de Fisiologia e Biofisica, Universidade Federal de Minas Gerais, Belo Horizonte 31270-901, Brazil.

Department of Biochemistry and Molecular Biology, University of Southern Denmark, Odense 5230, Denmark.

出版信息

J Proteome Res. 2020 Aug 7;19(8):3467-3477. doi: 10.1021/acs.jproteome.0c00290. Epub 2020 Jul 9.

DOI:10.1021/acs.jproteome.0c00290
PMID:32597192
Abstract

Cryptic peptides (cryptides) are biologically active peptides formed after proteolysis of native precursors present in animal venoms, for example. Proteolysis is an overlooked post-translational modification that increases venom complexity. The tripeptide KPP (Lys-Pro-Pro) is a peptide encrypted in the C-terminus of Ts14-a 25-mer peptide from the venom of the scorpion that has a positive impact on the cardiovascular system, inducing vasodilation and reducing arterial blood pressure of hypertensive rats among other beneficial effects. A previous study reported that KPP and its native peptide Ts14 act via activation of the bradykinin receptor B2 (B2R). However, the cellular events underlying the activation of B2R by KPP are unknown. To study the cell signaling triggered by the Ts14 cryptide KPP, we incubated cardiac myocytes isolated from C57BL/6 mice with KPP (10 mol·L) for 0, 5, or 30 min and explored the proteome and phosphoproteome. Our results showed that KPP regulated cardiomyocyte proteins associated with, but not limited to, apoptosis, muscle contraction, protein turnover, and the respiratory chain. We also reported that KPP led to AKT phosphorylation, activating AKT and its downstream target nitric oxide synthase. We also observed that KPP led to dephosphorylation of phospholamban (PLN) at its activation sites (S16 and T17), leading to reduced contractility of treated cardiomyocytes. Some cellular targets reported here for KPP (e.g., AKT, PLN, and ERK) have already been reported to protect the cardiac tissue from hypoxia-induced injury. Hence, this study suggests potential beneficial effects of this scorpion cryptide that needs to be further investigated, for example, as a drug lead for cardiac infarction.

摘要

隐匿肽(cryptides)是在动物毒液中原生前体蛋白水解后形成的生物活性肽,例如。蛋白水解是一种被忽视的翻译后修饰,它增加了毒液的复杂性。三肽 KPP(Lys-Pro-Pro)是一种从蝎子毒液中的 25 肽 Ts14 的 C 末端加密的肽,对心血管系统有积极影响,在其他有益作用中,诱导血管扩张并降低高血压大鼠的动脉血压。先前的一项研究表明,KPP 及其天然肽 Ts14 通过激活缓激肽受体 B2(B2R)发挥作用。然而,KPP 激活 B2R 的细胞事件尚不清楚。为了研究 Ts14 隐匿肽 KPP 触发的细胞信号转导,我们用 KPP(10 mol·L)孵育来自 C57BL/6 小鼠的心肌细胞 0、5 或 30 分钟,并探索了蛋白质组和磷酸蛋白质组。我们的结果表明,KPP 调节与心肌细胞相关的蛋白质,但不仅限于凋亡、肌肉收缩、蛋白质周转和呼吸链。我们还报告说,KPP 导致 AKT 磷酸化,激活 AKT 及其下游靶标一氧化氮合酶。我们还观察到 KPP 导致磷酸化酶磷蛋白(PLN)在其激活部位(S16 和 T17)去磷酸化,导致处理后的心肌细胞收缩力降低。这里报道的 KPP 的一些细胞靶标(例如 AKT、PLN 和 ERK)已经被报道可以保护心脏组织免受缺氧诱导的损伤。因此,这项研究表明这种蝎子隐匿肽可能具有潜在的有益作用,需要进一步研究,例如作为心肌梗死的药物先导。

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