Exploiting Cysteine Residues of SLC Membrane Transporters as Targets for Drugs
Author(s) -
Scalise Mariafrancesca,
Console Lara,
Galluccio Michele,
Pochini Lorena,
Tonazzi Annamaria,
Giangregorio Nicola,
Indiveri Cesare
Publication year - 2019
Publication title -
slas discovery
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.002
H-Index - 17
eISSN - 2472-5560
pISSN - 2472-5552
DOI - 10.1177/2472555219856601
Subject(s) - transporter , cysteine , biochemistry , computational biology , function (biology) , membrane protein , chemistry , organelle , membrane transport protein , amino acid , drug discovery , biology , membrane , microbiology and biotechnology , gene , enzyme
The observation that cysteine is the top gainer amino acid during evolution attracted the attention of scientists dealing with protein chemistry. The thiol group of cysteine, indeed, is a potential site for several types of reactions with variable specificity and strength. This feature proved to be promising also in the field of membrane transporters that represent boundary proteins fundamental for cell homeostasis. These proteins are classified, according to the driving force for transport, in primary or secondary active transporters. Another frequently used classification is nowadays based on phylogenesis. Two major groups are identified that take into account both criteria: the ABC and the SLC transporters, the second being much more numerous. The cellular localization of the transporters makes them very attractive for drug design. Moreover, the presence of at least one cysteine residue in all the annotated SLC transporters, so far, highlights the possibility of using the thiol (SH) residue for covalent drug targeting. Even if a delay exists in this research field due to the scarce knowledge of structure/function relationships, the setup of novel experimental tools for studying SLC proteins of plasma and organelle membranes opens an important perspective in pharmacology.
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