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SLC25家族线粒体载体的独特性质。

The peculiar properties of mitochondrial carriers of the SLC25 family.

作者信息

Kunji Edmund R S, Mavridou Vasiliki, King Martin S, Cimadamore-Werthein Camila, Jaiquel Baron Stephany, Jones Scott A, King Alannah C, Springett Roger, Chand Deepak, Palmer Shane M, Lacabanne Denis, Tavoulari Sotiria, Ruprecht Jonathan J

机构信息

Cambridge Biomedical Campus, MRC Mitochondrial Biology Unit, University of Cambridge, Keith Peters Building, Cambridge, CB2 0XY, U.K.

Department of Pharmacology, University of Cambridge, Cambridge, United Kingdom.

出版信息

Biochem J. 2025 Jul 23;482(15):BCJ20253171. doi: 10.1042/BCJ20253171.


DOI:10.1042/BCJ20253171
PMID:40706023
Abstract

With 53 members, the SLC25 mitochondrial carriers form the largest solute carrier family in humans. They transport a wide variety of substrates across the mitochondrial inner membrane to generate chemical energy and to supply molecules and ions for growth and maintenance of cells. They are among the smallest transporters in nature, yet they translocate some of the largest molecules without proton leak. With one exception, they are monomeric and have an unusual three-fold pseudo-symmetric structure. These carriers also have a unique transport mechanism, which is facilitated by six structural elements, meaning that all transmembrane helices move separately, but in a co-ordinated way. In addition, there are three functional elements that are an integral part of the alternating access mechanism, which opens and closes the carrier to the mitochondrial matrix or the intermembrane space. The first is a matrix gate, comprising the matrix salt bridge network and glutamine braces on transmembrane helices H1, H3 and H5. The second is a cytoplasmic gate, containing the cytoplasmic salt bridge network and tyrosine braces on transmembrane helices H2, H4 and H6. The third functional element is a single central substrate-binding site, the access to which is controlled by the opening and closing of the two gates in an alternating way. The electrostatic properties of the binding site facilitate the exchange of charged substrates across the inner membrane in the presence of a high membrane potential. Here, we discuss the extraordinary features of mitochondrial carriers, providing new insights into one of the most complex and dynamic transport mechanisms in nature.

摘要

溶质载体家族25(SLC25)线粒体载体由53个成员组成,是人类最大的溶质载体家族。它们将多种底物转运穿过线粒体内膜,以产生化学能量,并为细胞的生长和维持提供分子及离子。它们是自然界中最小的转运蛋白之一,但却能转运一些最大的分子且无质子泄漏。除了一个例外,它们都是单体,具有不寻常的三重假对称结构。这些载体还具有独特的转运机制,由六个结构元件促成,这意味着所有跨膜螺旋都单独移动,但方式协调。此外,还有三个功能元件是交替访问机制不可或缺的一部分,该机制控制载体对线粒体基质或膜间隙的开闭。第一个是基质门,由基质盐桥网络以及跨膜螺旋H1、H3和H5上的谷氨酰胺支撑结构组成。第二个是胞质门,包含胞质盐桥网络以及跨膜螺旋H2、H4和H6上的酪氨酸支撑结构。第三个功能元件是一个单一的中央底物结合位点,其通道由两个门的交替开闭控制。结合位点的静电特性有助于在高膜电位存在的情况下,带电荷的底物跨内膜进行交换。在此,我们讨论线粒体载体的非凡特性,为自然界中最复杂、最具动态性的转运机制之一提供新的见解。

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本文引用的文献

[1]
Molecular basis of pyruvate transport and inhibition of the human mitochondrial pyruvate carrier.

Sci Adv. 2025-4-18

[2]
Proton conductance by human uncoupling protein 1 is inhibited by purine and pyrimidine nucleotides.

EMBO J. 2025-4

[3]
SLC25A38 is required for mitochondrial pyridoxal 5'-phosphate (PLP) accumulation.

Nat Commun. 2025-1-24

[4]
The mitochondrial choline transporter, SLC25A48, regulates urine and blood choline levels in humans.

Kidney Int. 2025-2

[5]
MTCH2 controls energy demand and expenditure to fuel anabolism during adipogenesis.

EMBO J. 2025-2

[6]
Membrane potential stimulates ADP import and ATP export by the mitochondrial ADP/ATP carrier due to its positively charged binding site.

Sci Adv. 2024-11

[7]
Distinct roles for the domains of the mitochondrial aspartate/glutamate carrier citrin in organellar localization and substrate transport.

Mol Metab. 2024-12

[8]
In isolated brown adipose tissue mitochondria, UCP1 is not essential for - nor involved in - the uncoupling effects of the classical uncouplers FCCP and DNP.

Biochim Biophys Acta Bioenerg. 2025-1-1

[9]
Insights into Transient Dimerisation of Carnitine/Acylcarnitine Carrier (SLC25A20) from Sarkosyl/PAGE, Cross-Linking Reagents, and Comparative Modelling Analysis.

Biomolecules. 2024-9-14

[10]
SLC25A48 controls mitochondrial choline import and metabolism.

Cell Metab. 2024-9-3

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