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SETD7 通过 Hippo 信号通路和 HIF-1α 调节软骨细胞分化和糖酵解。

SETD7 regulates chondrocyte differentiation and glycolysis via the Hippo signaling pathway and HIF‑1α.

机构信息

Hospital of Stomatology, Guanghua School of Stomatology, Sun Yat‑sen University, Guangzhou, Guangdong 510055, P.R. China.

Key Laboratory of Oral Medicine, Guangzhou Institute of Oral Disease, Stomatology Hospital of Guangzhou Medical University, Guangzhou, Guangdong 510140, P.R. China.

出版信息

Int J Mol Med. 2021 Dec;48(6). doi: 10.3892/ijmm.2021.5043. Epub 2021 Oct 7.

Abstract

Chondrocytes are well adapted to hypoxia and produce more functional extracellular matrix in low oxygen environments . In our previous study, methyltransferase SET domain containing (SETD)7 regulated chondrocyte activity in hypoxic conditions. However, the precise association between SETD7 and chondrocyte differentiation under low oxygen partial pressure remains unclear. The association between SETD7 and chondrocyte differentiation was studied by silencing SETD7 in chondrocytes . The results showed that the silencing of SETD7 in ATDC5 cells inhibited the Hippo signaling pathway, decreased Yes‑associated protein (YAP) phosphorylation and increased the levels of YAP and hypoxia inducible factor‑1α (HIF‑1α) in the nucleus. YAP combined with HIF‑1α to form a complex that promoted the expression of genes involved in chondrogenic differentiation and the glycolytic pathway. Thus, SETD7 inhibited chondrocyte differentiation and glycolysis via the Hippo signaling pathway. The present study demonstrated that SETD7 was a potential molecular target that maintained the chondrocyte phenotype during cartilage tissue engineering and cartilage‑associated disease.

摘要

软骨细胞能很好地适应低氧环境,并在低氧环境中产生更多功能的细胞外基质。在我们之前的研究中,甲基转移酶 SET 结构域包含(SETD)7 在低氧条件下调节软骨细胞活性。然而,SETD7 与低氧分压下软骨细胞分化之间的确切关联尚不清楚。通过在软骨细胞中沉默 SETD7 来研究 SETD7 与软骨细胞分化之间的关联。结果表明,在 ATDC5 细胞中沉默 SETD7 抑制 Hippo 信号通路,降低 Yes 相关蛋白(YAP)磷酸化水平,增加细胞核中 YAP 和缺氧诱导因子 1α(HIF-1α)的水平。YAP 与 HIF-1α 形成复合物,促进参与软骨分化和糖酵解途径的基因表达。因此,SETD7 通过 Hippo 信号通路抑制软骨细胞分化和糖酵解。本研究表明,SETD7 是维持软骨组织工程和软骨相关疾病中软骨细胞表型的潜在分子靶标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6be6/8510680/d81760698666/IJMM-48-06-05043-g00.jpg

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