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初级纤毛对于垂体发育中的细胞类型确定和血管生成是必需的。

Primary Cilia are Required for Cell-Type Determination and Angiogenesis in Pituitary Development.

机构信息

Department of Biochemistry, The Jikei University School of Medicine, Tokyo 105-8461, Japan.

Department of Biomolecular Science, Toho University, Chiba 274-8510, Japan.

出版信息

Endocrinology. 2024 Jul 1;165(8). doi: 10.1210/endocr/bqae085.

Abstract

The functional maturation of the pituitary gland requires adequate cell differentiation and vascular network formation. Although spatiotemporal signaling and transcription factors are known to govern pituitary development, the involvement of primary cilia, nonmoving hair-like organelles, remains unclear. In this study, we uncovered the contribution of primary cilia to cell-type determination and vascular network formation during pituitary development. Homozygous knockout mice lacking a ciliary kinase, Dyrk2-/-, exhibit abnormalities in ciliary structure and pituitary hypoplasia, accompanied by varying degrees of failure in differentiation among all types of hormone-producing cells in the anterior lobe. Aberrations in cell differentiation in Dyrk2-/- mice arise from a decrease in the expression of crucial transcription factors, Lhx4, Lhx3, and Prop1, resulting from the inactivity of Hedgehog (Hh) signaling during the early stages of development. Furthermore, the loss of Dyrk2 results in vascular system abnormalities during the middle to late stages of development. Mechanistically, transcriptome analyses revealed the downregulation of vitronectin-integrin αvβ3-VEGFR2 signaling, essential for orchestrating vascular development. Collectively, our findings demonstrate that primary cilia play a pivotal role as critical regulators of cell survival, cell determination, and angiogenesis during pituitary gland development through the activation of Hh signaling. These findings expand our understanding of the potential link between pituitary dysfunction in human disorders and ciliopathies.

摘要

垂体腺的功能成熟需要充分的细胞分化和血管网络形成。尽管时空信号和转录因子被认为可以控制垂体发育,但初级纤毛的参与仍然不清楚。在这项研究中,我们揭示了初级纤毛在垂体发育过程中对细胞类型决定和血管网络形成的贡献。缺乏纤毛激酶 Dyrk2 的纯合敲除小鼠表现出纤毛结构异常和垂体发育不良,同时在前叶中所有产生激素的细胞类型的分化都存在不同程度的失败。Dyrk2-/- 小鼠中细胞分化的异常是由于关键转录因子 Lhx4、Lhx3 和 Prop1 的表达减少所致,这是由于发育早期 Hedgehog (Hh) 信号失活所致。此外,Dyrk2 的缺失导致发育中期到晚期的血管系统异常。从机制上讲,转录组分析显示 vitronectin-整联蛋白 αvβ3-VEGFR2 信号的下调,该信号对于协调血管发育至关重要。总之,我们的研究结果表明,初级纤毛通过激活 Hh 信号,作为垂体发育过程中细胞存活、细胞决定和血管生成的关键调节因子,发挥着关键作用。这些发现扩展了我们对人类疾病中垂体功能障碍与纤毛病之间潜在联系的理解。

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