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The potential role of sigma-1 receptors in lipid transport and lipid raft reconstitution in the brain: Implication for drug abuse

机译:sigma-1受体在脑脂质转运和脂质筏重构中的潜在作用:对药物滥用的影响

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The brain is highly enriched in lipids. However, the molecular biological roles of lipids in the brain have been largely unexplored. Although, in 1990s, several studies have demonstrated the roles of lipids in a variety of neuronal functions and certain neurological diseases, the involvement of lipids in drug dependence, if any, is almost totally unknown. Sigma-1 receptors are brain-enriched proteins that interact with psychostimulants such as cocaine and methamphetamine. Sigma-1 receptors possess a putative sterol-binding pocket and are predominantly expressed on the endoplasmic reticulum (ER) where most lipids and their precursors are synthesized. Sigma-1 receptors are involved in drug-seeking behaviors and in psychostimulant-induced behavioral sensitization. Recent studies demonstrated that sigma-1 receptors target the lipid-storing subcompartments of the ER and are colocalized with cholesterol and neutral lipids. Sigma-1 receptors form detergent-insoluble lipid microdomains (lipid rafts) on the ER subcompartments and can translocate on the ER when stimulated. Upregulation of sigma-1 receptors affect the levels of plasma membrane lipid rafts by changing the lipid components therein. The membrane reconstitution thus induced by sigma-1 receptors in turn affects functions of proteins residing in plasma membrane lipid rafts including tropic factor receptors and tyrosine kinases. Specifically, we recently found that sigma-1 receptors modulate MAP kinase activation induced by tropic factors, neuritegenesis and oligodendrocyte differentiation-all related to lipid raft reconstitution. Sigma-1 receptors may thus play a role in psychostimulant-induced long-lasting morphological changes in the brain via the capacity of sigma-1 receptors in regulating ER lipid transport and the resultant plasma membrane lipid raft reconstitution. Published by Elsevier Inc.
机译:大脑富含脂质。然而,脂质在脑中的分子生物学作用尚未得到充分探索。尽管在1990年代,几项研究证明了脂质在多种神经元功能和某些神经系统疾病中的作用,但几乎完全不知道脂质是否与药物依赖性有关。 Sigma-1受体是一种富含大脑的蛋白质,可与精神刺激药如可卡因和甲基苯丙胺相互作用。 Sigma-1受体具有公认的固醇结合口袋,并主要在内质网(ER)上表达,在该内质网中,大多数脂质及其前体均被合成。 Sigma-1受体参与药物寻找行为和精神刺激剂诱发的行为敏化。最近的研究表明,sigma-1受体靶向内质网的储脂小室,并与胆固醇和中性脂质共定位。 Sigma-1受体在ER子隔间形成去污剂不溶性脂质微区(脂质筏),并在刺激时可在ER上移位。 sigma-1受体的上调通过改变其中的脂质成分而影响质膜脂质筏的水平。因此,由sigma-1受体诱导的膜重构反过来会影响存在于质膜脂质筏中的蛋白质的功能,这些蛋白筏包括回归因子受体和酪氨酸激酶。具体而言,我们最近发现sigma-1受体可调节由热带因子,神经突发生和少突胶质细胞分化诱导的MAP激酶活化-所有这些都与脂质筏重构有关。因此,Sigma-1受体可能通过sigma-1受体调节ER脂质转运和最终质膜脂质筏重建的能力,在精神刺激剂诱导的大脑长期形态变化中起作用。由Elsevier Inc.发布

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