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平衡核苷转运体家族,SLC29。

The equilibrative nucleoside transporter family, SLC29.

作者信息

Baldwin Stephen A, Beal Paul R, Yao Sylvia Y M, King Anne E, Cass Carol E, Young James D

机构信息

School of Biochemistry and Molecular Biology, University of Leeds, LS2 9JT, Leeds, UK.

出版信息

Pflugers Arch. 2004 Feb;447(5):735-43. doi: 10.1007/s00424-003-1103-2. Epub 2003 Jun 28.

Abstract

The human SLC29 family of proteins contains four members, designated equilibrative nucleoside transporters (ENTs) because of the properties of the first-characterised family member, hENT1. They belong to the widely-distributed eukaryotic ENT family of equilibrative and concentrative nucleoside/nucleobase transporters and are distantly related to a lysosomal membrane protein, CLN3, mutations in which cause neuronal ceroid lipofuscinosis. A predicted topology of 11 transmembrane helices with a cytoplasmic N-terminus and an extracellular C-terminus has been experimentally confirmed for hENT1. The best-characterised members of the family, hENT1 and hENT2, possess similar broad substrate specificities for purine and pyrimidine nucleosides, but hENT2 in addition efficiently transports nucleobases. The ENT3 and ENT4 isoforms have more recently also been shown to be genuine nucleoside transporters. All four isoforms are widely distributed in mammalian tissues, although their relative abundance varies: ENT2 is particularly abundant in skeletal muscle. In polarised cells ENT1 and ENT2 are found in the basolateral membrane and, in tandem with concentrative transporters of the SLC28 family, may play a role in transepithelial nucleoside transport. The transporters play key roles in nucleoside and nucleobase uptake for salvage pathways of nucleotide synthesis, and are also responsible for the cellular uptake of nucleoside analogues used in the treatment of cancers and viral diseases. In addition, by regulating the concentration of adenosine available to cell surface receptors, they influence many physiological processes ranging from cardiovascular activity to neurotransmission.

摘要

人类SLC29蛋白家族包含四个成员,因其首个被鉴定的家族成员hENT1的特性而被命名为平衡核苷转运体(ENTs)。它们属于广泛分布的真核生物平衡型和浓缩型核苷/核碱基转运体的ENT家族,与溶酶体膜蛋白CLN3有较远的亲缘关系,CLN3的突变会导致神经元蜡样脂褐质沉积症。hENT1已通过实验证实具有预测的11个跨膜螺旋的拓扑结构,其N端位于细胞质内,C端位于细胞外。该家族中特性研究得最充分的成员hENT1和hENT2,对嘌呤和嘧啶核苷具有相似的广泛底物特异性,但hENT2还能高效转运核碱基。ENT3和ENT4亚型最近也被证明是真正的核苷转运体。所有四种亚型在哺乳动物组织中广泛分布,尽管它们的相对丰度有所不同:ENT2在骨骼肌中尤为丰富。在极化细胞中,ENT1和ENT2存在于基底外侧膜中,并且与SLC28家族的浓缩转运体协同作用,可能在跨上皮核苷转运中发挥作用。这些转运体在核苷酸合成的补救途径的核苷和核碱基摄取中起关键作用,并且还负责细胞摄取用于治疗癌症和病毒疾病的核苷类似物。此外,通过调节细胞表面受体可利用的腺苷浓度,它们影响从心血管活动到神经传递等许多生理过程。

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