L amino acid transporter structure and molecular bases for the asymmetry of substrate interaction

被引:56
作者
Errasti-Murugarren, Ekaitz [1 ,12 ]
Fort, Joana [1 ,2 ,3 ,12 ]
Bartoccioni, Paola [1 ,2 ,12 ]
Diaz, Lucia [4 ]
Pardon, Els [5 ,6 ]
Carpena, Xavier [7 ]
Espino-Guarch, Meritxell [8 ]
Zorzano, Antonio [1 ,3 ,9 ]
Ziegler, Christine [10 ]
Steyaert, Jan [5 ,6 ]
Fernandez-Recio, Juan [4 ]
Fita, Ignacio [11 ]
Palacin, Manuel [1 ,2 ,3 ]
机构
[1] Barcelona Inst Sci & Technol, Inst Res Biomed IRB Barcelona, Barcelona 08028, Spain
[2] Ctr Invest Biomed Red Enfermedades Raras CIBERER, Barcelona 08028, Spain
[3] Univ Barcelona, Fac Biol, Dept Biochem & Mol Biomed, E-08028 Barcelona, Spain
[4] BSC, Joint BSC CRG IRB Res Program Computat Biol, Dept Life Sci, Barcelona 08034, Spain
[5] VIB VUB Ctr Struct Biol, Pl Laan 2, B-1050 Brussels, Belgium
[6] Vrije Univ Brussel, Struct Biol Brussels, Pl Laan 2, B-1050 Brussels, Belgium
[7] CELLS ALBA Synchrotron Light Source, Barcelona 08290, Spain
[8] Sidra Med, Translat Med, Doha 26999, Qatar
[9] Ctr Invest Biomed Red Diabet & Enfermedades Metab, Barcelona 08028, Spain
[10] Univ Regensburg, Inst Biophys & Biophys Chem, D-95053 Regensburg, Germany
[11] CSIC, IBMB, E-08028 Barcelona, Spain
[12] Unit Excellence Maria de Maeztu, Barcelona 08028, Spain
关键词
LYSINURIC PROTEIN INTOLERANCE; GUI MEMBRANE-BUILDER; MECHANISM; NA+; INHIBITOR; MODEL; SYSTEM; IDENTIFICATION; SIMULATIONS; ACTIVATION;
D O I
10.1038/s41467-019-09837-z
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
L-amino acid transporters (LATs) play key roles in human physiology and are implicated in several human pathologies. LATs are asymmetric amino acid exchangers where the low apparent affinity cytoplasmic side controls the exchange of substrates with high apparent affinity on the extracellular side. Here, we report the crystal structures of an LAT, the bacterial alanine-serine-cysteine exchanger (BasC), in a non-occluded inward-facing conformation in both apo and substrate-bound states. We crystallized BasC in complex with a nanobody, which blocks the transporter from the intracellular side, thus unveiling the sidedness of the substrate interaction of BasC. Two conserved residues in human LATs, Tyr 236 and Lys 154, are located in equivalent positions to the Na1 and Na2 sites of sodium-dependent APC superfamily transporters. Functional studies and molecular dynamics (MD) calculations reveal that these residues are key for the asymmetric substrate interaction of BasC and in the homologous human transporter Asc-1.
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页数:12
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