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A one-gate elevator mechanism for the human neutral amino acid transporter ASCT2

机译:人类中性氨基酸转运蛋白ASCT2的单门升降机机制

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摘要

The human Alanine Serine Cysteine Transporter 2 (ASCT2) is a neutral amino acid exchanger that belongs to the solute carrier family 1 (SLC1A). SLC1A structures have revealed an elevator-type mechanism, in which the substrate is translocated across the cell membrane by a large displacement of the transport domain, whereas a small movement of hairpin 2 (HP2) gates the extracellular access to the substrate-binding site. However, it has remained unclear how substrate binding and release is gated on the cytoplasmic side. Here, we present an inward-open structure of the human ASCT2, revealing a hitherto elusive SLC1A conformation. Strikingly, the same structural element (HP2) serves as a gate in the inward-facing as in the outward-facing state. The structures reveal that SLC1A transporters work as one-gate elevators. Unassigned densities near the gate and surrounding the scaffold domain, may represent potential allosteric binding sites, which could guide the design of lipidic-inhibitors for anticancer therapy.
机译:人丙氨酸丝氨酸半胱氨酸转运蛋白2(ASCT2)是一种中性氨基酸交换剂,属于溶质载体家族1(SLC1A)。 SLC1A结构揭示了一种升降型机制,其中底物通过转运结构域的大位移而跨细胞膜移位,而发夹2(HP2)的小运动则使细胞外通道接近底物结合位点。然而,仍不清楚如何在细胞质侧控制底物结合和释放。在这里,我们介绍了人类ASCT2的内向开放结构,揭示了迄今为止难以捉摸的SLC1A构象。令人惊讶的是,相同的结构元件(HP2)在向内的状态与向外的状态相同。结构表明,SLC1A转运蛋白可作为单门电梯使用。门附近和支架结构域周围的未分配密度可能代表潜在的变构结合位点,这可能指导抗癌治疗脂质抑制剂的设计。

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