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L-type amino acid transport and cancer: targeting the mTORC1 pathway to inhibit neoplasia

机译:L型氨基酸转运与癌症:靶向mTORC1途径抑制肿瘤形成

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The L-type amino acid transporter (LAT) family are Nasup+/sup-independent transporters, which deliver neutral amino acids into cells. The four LATs, LAT1 (SLC7A5), LAT2 (SLC7A8), LAT3 (SLC43A1) and LAT4 (SLC43A2), are responsible for the majority of cellular leucine uptake. They show increased expression in many cancers, and are critical for control of protein translation and cell growth through the mTORC1 pathway. The increased transporter expression observed in cancers is regulated by transcriptional pathways such as hormone receptors, c-myc and nutrient starvation responses. We review the expression and function of the LAT family in cancer, as well as the recent development of specific inhibitors targeting LAT1 or LAT3. These LAT family inhibitors may be useful adjuvant therapeutics in multiple cancers.
机译:L型氨基酸转运蛋白(LAT)家族是Na + 无关的转运蛋白,可将中性氨基酸输送到细胞中。 LAT1(SLC7A5),LAT2(SLC7A8),LAT3(SLC43A1)和LAT4(SLC43A2)这四个LAT负责大部分细胞亮氨酸的摄取。它们在许多癌症中显示出增加的表达,并且对于通过mTORC1途径控制蛋白质翻译和细胞生长至关重要。在癌症中观察到的转运蛋白表达增加受转录途径如激素受体,c-myc和营养饥饿反应的调节。我们审查了LAT家族在癌症中的表达和功能,以及针对LAT1或LAT3的特异性抑制剂的最新发展。这些LAT家族抑制剂在多种癌症中可能是有用的辅助治疗剂。

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