Egr1 调控再生衰老和心脏修复

IF 9.4 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS
Lingling Zhang, Jacob Elkahal, Tianzhen Wang, Racheli Rimmer, Alexander Genzelinakh, Elad Bassat, Jingkui Wang, Dahlia Perez, David Kain, Daria Lendengolts, Roni Winkler, Hanna Bueno-levy, Kfir Baruch Umansky, David Mishaly, Avraham Shakked, Shoval Miyara, Avital Sarusi-Portuguez, Naomi Goldfinger, Amir Prior, David Morgenstern, Yishai Levin, Yoseph Addadi, Baoguo Li, Varda Rotter, Uriel Katz, Elly M. Tanaka, Valery Krizhanovsky, Rachel Sarig, Eldad Tzahor
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引用次数: 0

摘要

衰老在各种生理和病理过程中起着关键作用。我们曾报道过损伤诱导的短暂衰老与心脏再生相关,但再生衰老的多组学特征和分子基础仍然模糊不清。利用蛋白质组学和单细胞 RNA 测序,我们在此报告了成年小鼠心脏的再生衰老多组学特征,并确定了它在新生儿心脏再生和成年小鼠琼脂糖介导的心脏修复中的作用。我们发现早期生长应答蛋白1(Egr1)是这两种模型中再生衰老的调控因子。在新生儿心脏中,Egr1 促进血管生成和心肌细胞增殖。在成人心脏中,胰凝乳蛋白诱导的衰老和修复需要 Egr1,Egr1 由心脏成纤维细胞中的整合素-FAK-ERK-Akt1 轴激活。我们还发现了损伤诱导的衰老相关分泌表型成分-- cathepsins,它能促进细胞外基质降解,并可能有助于减轻纤维化。总之,我们发现了心脏再生过程中再生衰老的分子特征和功能益处,而 Egr1 是这一过程的协调者。Zhang等人的研究表明,Egr1在新生儿心脏再生过程中以及在成年小鼠胰蛋白酶介导的心脏修复过程中调节瞬时衰老,在心脏成纤维细胞的整合素-FAK-ERK-Akt1轴下游发挥作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Egr1 regulates regenerative senescence and cardiac repair

Egr1 regulates regenerative senescence and cardiac repair
Senescence plays a key role in various physiological and pathological processes. We reported that injury-induced transient senescence correlates with heart regeneration, yet the multi-omics profile and molecular underpinnings of regenerative senescence remain obscure. Using proteomics and single-cell RNA sequencing, here we report the regenerative senescence multi-omic signature in the adult mouse heart and establish its role in neonatal heart regeneration and agrin-mediated cardiac repair in adult mice. We identified early growth response protein 1 (Egr1) as a regulator of regenerative senescence in both models. In the neonatal heart, Egr1 facilitates angiogenesis and cardiomyocyte proliferation. In adult hearts, agrin-induced senescence and repair require Egr1, activated by the integrin–FAK–ERK–Akt1 axis in cardiac fibroblasts. We also identified cathepsins as injury-induced senescence-associated secretory phenotype components that promote extracellular matrix degradation and potentially assist in reducing fibrosis. Altogether, we uncovered the molecular signature and functional benefits of regenerative senescence during heart regeneration, with Egr1 orchestrating the process. Zhang et al. show that Egr1 regulates transient senescence during neonatal heart regeneration and upon agrin-mediated cardiac repair in adult mice, acting downstream of the integrin–FAK–ERK–Akt1 axis in cardiac fibroblasts.
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