Inhibition of Renin Expression Is Regulated by an Epigenetic Switch From an Active to a Poised State.

IF 6.9 1区 医学 Q1 PERIPHERAL VASCULAR DISEASE Hypertension Pub Date : 2024-09-01 Epub Date: 2024-07-11 DOI:10.1161/HYPERTENSIONAHA.124.22886
Jason P Smith, Robert Paxton, Silvia Medrano, Nathan C Sheffield, Maria Luisa S Sequeira-Lopez, R Ariel Gomez
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Abstract

Background: Renin-expressing cells are myoendocrine cells crucial for the maintenance of homeostasis. Renin is regulated by cAMP, p300 (histone acetyltransferase p300)/CBP (CREB-binding protein), and Brd4 (bromodomain-containing protein 4) proteins and associated pathways. However, the specific regulatory changes that occur following inhibition of these pathways are not clear.

Methods: We treated As4.1 cells (tumoral cells derived from mouse juxtaglomerular cells that constitutively express renin) with 3 inhibitors that target different factors required for renin transcription: H-89-dihydrochloride, PKA (protein kinase A) inhibitor; JQ1, Brd4 bromodomain inhibitor; and A-485, p300/CBP inhibitor. We performed assay for transposase-accessible chromatin with sequencing (ATAC-seq), single-cell RNA sequencing, cleavage under targets and tagmentation (CUT&Tag), and chromatin immunoprecipitation sequencing for H3K27ac (acetylation of lysine 27 of the histone H3 protein) and p300 binding on biological replicates of treated and control As4.1 cells.

Results: In response to each inhibitor, Ren1 expression was significantly reduced and reversible upon washout. Chromatin accessibility at the Ren1 locus did not markedly change but was globally reduced at distal elements. Inhibition of PKA led to significant reductions in H3K27ac and p300 binding specifically within the Ren1 super-enhancer region. Further, we identified enriched TF (transcription factor) motifs shared across each inhibitory treatment. Finally, we identified a set of 9 genes with putative roles across each of the 3 renin regulatory pathways and observed that each displayed differentially accessible chromatin, gene expression, H3K27ac, and p300 binding at their respective loci.

Conclusions: Inhibition of renin expression in cells that constitutively synthesize and release renin is regulated by an epigenetic switch from an active to poised state associated with decreased cell-cell communication and an epithelial-mesenchymal transition. This work highlights and helps define the factors necessary for renin cells to alternate between myoendocrine and contractile phenotypes.

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肾素表达的抑制受表观遗传学从活跃状态到静止状态切换的调控。
背景:表达肾素的细胞是肌内分泌细胞,对维持体内平衡至关重要。肾素受 cAMP、p300(组蛋白乙酰转移酶 p300)/CBP(CREB 结合蛋白)和 Brd4(含溴结构域蛋白 4)蛋白及相关途径的调控。然而,抑制这些通路后发生的具体调控变化尚不清楚:我们用 3 种针对肾素转录所需的不同因子的抑制剂处理 As4.1 细胞(源自小鼠并肾小球细胞的肿瘤细胞,组成型表达肾素):H-89-二盐酸盐,PKA(蛋白激酶 A)抑制剂;JQ1,Brd4 溴域抑制剂;A-485,p300/CBP 抑制剂。我们对处理过的As4.1细胞和对照细胞的生物复制进行了ATAC-seq、单细胞RNA测序、CUT&Tag和染色质免疫沉淀测序,以检测H3K27ac和p300的结合:结果:在每种抑制剂的作用下,Ren1的表达均显著降低,且在洗脱后可逆。Ren1基因座的染色质可及性没有明显变化,但远端元件的染色质可及性全面降低。抑制 PKA 会导致 Ren1 超级增强子区域内的 H3K27ac 和 p300 结合显著减少。此外,我们还发现了在每种抑制处理中共享的富集 TF(转录因子)基团。最后,我们确定了在 3 条肾素调控途径中都有可能发挥作用的 9 个基因,并观察到每个基因在各自的位点上都显示出不同的染色质可及性、基因表达、H3K27ac 和 p300 结合:结论:抑制组成型合成和释放肾素的细胞中肾素的表达是由从活跃状态到静止状态的表观遗传学转换调控的,这种转换与细胞间交流减少和上皮-间质转化有关。这项工作强调并有助于确定肾素细胞在肌内分泌和收缩表型之间交替的必要因素。
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来源期刊
Hypertension
Hypertension 医学-外周血管病
CiteScore
15.90
自引率
4.80%
发文量
1006
审稿时长
1 months
期刊介绍: Hypertension presents top-tier articles on high blood pressure in each monthly release. These articles delve into basic science, clinical treatment, and prevention of hypertension and associated cardiovascular, metabolic, and renal conditions. Renowned for their lasting significance, these papers contribute to advancing our understanding and management of hypertension-related issues.
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