Institute for Diabetes and Obesity (IDO), Helmholtz Diabetes Center (HDC) and German Center for Diabetes Research (DZD) at the Helmholtz Zentrum München, German Research Center for Environmental Health (GmbH), Ingolstädter Landstraße 1, 85764 Neuherberg, Germany.
Biomolecules. 2023 Jun 15;13(6):994. doi: 10.3390/biom13060994.
Glycosylphosphatidylinositol (GPI)-anchored proteins (APs) are anchored at the outer leaflet of the plasma membrane (PM) bilayer by covalent linkage to a typical glycolipid and expressed in all eukaryotic organisms so far studied. Lipolytic release from PMs into extracellular compartments and intercellular transfer are regarded as the main (patho)physiological roles exerted by GPI-APs. The intercellular transfer of GPI-APs relies on the complete GPI anchor and is mediated by extracellular vesicles such as microvesicles and exosomes and lipid-free homo- or heteromeric aggregates, and lipoprotein-like particles such as prostasomes and surfactant-like particles, or lipid-containing micelle-like complexes. In mammalian organisms, non-vesicular transfer is controlled by the distance between donor and acceptor cells/tissues; intrinsic conditions such as age, metabolic state, and stress; extrinsic factors such as GPI-binding proteins; hormones such as insulin; and drugs such as anti-diabetic sulfonylureas. It proceeds either "directly" upon close neighborhood or contact of donor and acceptor cells or "indirectly" as a consequence of the induced lipolytic release of GPI-APs from PMs. Those displace from the serum GPI-binding proteins GPI-APs, which have retained the complete anchor, and become assembled in aggregates or micelle-like complexes. Importantly, intercellular transfer of GPI-APs has been shown to induce specific phenotypes such as stimulation of lipid and glycogen synthesis, in cultured human adipocytes, blood cells, and induced pluripotent stem cells. As a consequence, intercellular transfer of GPI-APs should be regarded as non-genetic inheritance of (acquired) features between somatic cells which is based on the biogenesis and transmission of matter such as GPI-APs and "membrane landscapes", rather than the replication and transmission of information such as DNA. Its operation in mammalian organisms remains to be clarified.
糖基磷脂酰肌醇(GPI)锚定蛋白(APs)通过与典型糖脂的共价连接锚定在质膜(PM)双层的外叶,并在迄今为止研究的所有真核生物中表达。从 PM 到细胞外隔室和细胞间转移的脂解释放被认为是 GPI-APs 发挥的主要(病理)生理作用。GPI-APs 的细胞间转移依赖于完整的 GPI 锚定,并通过细胞外囊泡(如微泡和外泌体)和无脂同型或异型聚合物以及脂蛋白样颗粒(如前列腺素体和表面活性剂样颗粒)或含脂胶束样复合物进行介导。在哺乳动物生物体中,非囊泡转移受供体和受体细胞/组织之间的距离、年龄、代谢状态和应激等内在条件、GPI 结合蛋白等外在因素、胰岛素等激素以及抗糖尿病磺酰脲类药物等药物的控制。它要么通过供体和受体细胞或组织的近距离或接触“直接”进行,要么作为 GPI-APs 从 PM 中诱导性脂解释放的结果“间接”进行。那些从血清中取代 GPI 结合蛋白的 GPI-APs 保留了完整的锚定,并在聚集物或胶束样复合物中组装。重要的是,已经证明 GPI-APs 的细胞间转移会诱导特定表型,例如刺激人脂肪细胞、血细胞和诱导多能干细胞中的脂质和糖原合成。因此,GPI-APs 的细胞间转移应被视为体细胞之间(获得的)特征的非遗传继承,这是基于 GPI-APs 和“膜景观”等物质的生物发生和传递,而不是 DNA 等信息的复制和传递。它在哺乳动物生物体中的运作仍有待阐明。
Zotero 插件
