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同源异型蛋白EN2跨质膜的双向转运需要磷脂酰肌醇磷酸(PIP)。

Bidirectional transfer of homeoprotein EN2 across the plasma membrane requires PIP.

作者信息

Amblard Irène, Dupont Edmond, Alves Isabel, Miralvès Julie, Queguiner Isabelle, Joliot Alain

机构信息

Center for Interdisciplinary Research in Biology (CIRB), College de France, CNRS, INSERM, PSL Research University, 75005 Paris, France.

Sorbonne University, Paris, France.

出版信息

J Cell Sci. 2020 Jul 8;133(13):jcs244327. doi: 10.1242/jcs.244327.

Abstract

Homeoproteins are a class of transcription factors sharing the unexpected property of intercellular trafficking that confers to homeoproteins a paracrine mode of action. Homeoprotein paracrine action participates in the control of patterning processes, including axonal guidance, brain plasticity and boundary formation. Internalization and secretion, the two steps of intercellular transfer, rely on unconventional mechanisms, but the cellular mechanisms at stake still need to be fully characterized. Thanks to the design of new quantitative and sensitive assays dedicated to the study of homeoprotein transfer within HeLa cells in culture, we demonstrate a core role of phosphatidylinositol (4,5)-bisphosphate (PIP) together with cholesterol in the translocation of the homeobox protein engrailed-2 (EN2) across the plasma membrane. By using drug and enzyme treatments, we show that both secretion and internalization are regulated according to PIP levels. The requirement for PIP and cholesterol in EN2 trafficking correlates with their selective affinity for this protein in artificial bilayers, which is drastically decreased in a paracrine-deficient mutant of EN2. We propose that the bidirectional plasma membrane translocation events that occur during homeoprotein secretion and internalization are parts of a common process.

摘要

同源结构域蛋白是一类转录因子,具有细胞间运输这一独特特性,赋予了同源结构域蛋白旁分泌作用模式。同源结构域蛋白的旁分泌作用参与调控模式形成过程,包括轴突导向、脑可塑性和边界形成。内化和分泌是细胞间转移的两个步骤,依赖于非常规机制,但其中涉及的细胞机制仍有待充分阐明。通过设计专门用于研究培养的HeLa细胞内同源结构域蛋白转移的新型定量和灵敏检测方法,我们证明了磷脂酰肌醇(4,5)-二磷酸(PIP)与胆固醇在同源盒蛋白engrailed-2(EN2)跨质膜转运过程中发挥核心作用。通过药物和酶处理,我们发现分泌和内化均受PIP水平调控。EN2运输过程中对PIP和胆固醇的需求与其在人工双层膜中对该蛋白的选择性亲和力相关,而在EN2旁分泌缺陷突变体中这种亲和力大幅降低。我们提出,同源结构域蛋白分泌和内化过程中发生的双向质膜转运事件是一个共同过程的组成部分。

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