Jatzlau Jerome, Mendez Paul-Lennard, Altay Aybuge, Raaz Lion, Zhang Yufei, Mähr Sophia, Sesver Akin, Reichenbach Maria, Mundlos Stefan, Vingron Martin, Knaus Petra
Institute of Chemistry and Biochemistry - Biochemistry, Freie Universität Berlin, 14195 Berlin, Germany.
Berlin-Brandenburg School for Regenerative Therapies (BSRT), 13353 Berlin, Germany.
iScience. 2023 Jul 17;26(9):107405. doi: 10.1016/j.isci.2023.107405. eCollection 2023 Sep 15.
Bone morphogenetic protein (BMP) signaling and fluid shear stress (FSS) mediate complementary functions in vascular homeostasis and disease development. It remains to be shown whether altered chromatin accessibility downstream of BMP and FSS offers a crosstalk level to explain changes in SMAD-dependent transcription. Here, we employed ATAC-seq to analyze arterial endothelial cells stimulated with BMP9 and/or FSS. We found that BMP9-sensitive regions harbor non-palindromic GC-rich SMAD-binding elements (GGCTCC) and 69.7% of these regions become BMP-insensitive in the presence of FSS. While GATA and KLF transcription factor (TF) motifs are unique to BMP9- and FSS-sensitive regions, respectively, SOX motifs are common to both. Finally, we show that both SOX(13/18) and GATA(2/3/6) family members are directly upregulated by SMAD1/5. These findings highlight the mechano-dependency of SMAD-signaling by a sequential mechanism of first elevated pioneer TF expression, allowing subsequent chromatin opening to eventually providing accessibility to novel SMAD binding sites.
骨形态发生蛋白(BMP)信号传导和流体剪切应力(FSS)在血管稳态和疾病发展中发挥互补作用。BMP和FSS下游染色质可及性的改变是否提供了一种相互作用水平来解释SMAD依赖性转录的变化,仍有待证明。在此,我们采用ATAC-seq分析用BMP9和/或FSS刺激的动脉内皮细胞。我们发现,BMP9敏感区域含有非回文富含GC的SMAD结合元件(GGCTCC),并且在存在FSS的情况下,这些区域中有69.7%对BMP不敏感。虽然GATA和KLF转录因子(TF)基序分别是BMP9和FSS敏感区域所特有的,但SOX基序在两者中都很常见。最后,我们表明SOX(13/18)和GATA(2/3/6)家族成员均被SMAD1/5直接上调。这些发现通过首先升高先驱TF表达、随后允许染色质开放并最终为新的SMAD结合位点提供可及性的顺序机制,突出了SMAD信号传导的机械依赖性。
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