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Taurine and Creatine Transporters as Potential Drug Targets in Cancer Therapy

Journal

Publisher

MDPI
DOI: 10.3390/ijms24043788

Keywords

taurine transporter; TauT; creatine transporter; CT-1; cancer; inhibitors

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Cancer cells show uncontrolled growth, proliferation, and impaired apoptosis. The altered expression and function of SLC6 family solute carrier proteins are associated with severe diseases, including cancers. This article discusses the potential role of taurine (SLC6A6) and creatine (SLC6A8) transporters in cancer development and the therapeutic potential of their inhibitors.
Cancer cells are characterized by uncontrolled growth, proliferation, and impaired apoptosis. Tumour progression could be related to poor prognosis and due to this fact, researchers have been working on novel therapeutic strategies and antineoplastic agents. It is known that altered expression and function of solute carrier proteins from the SLC6 family could be associated with severe diseases, including cancers. These proteins were noticed to play important physiological roles through transferring nutrient amino acids, osmolytes, neurotransmitters, and ions, and many of them are necessary for survival of the cells. Herein, we present the potential role of taurine (SLC6A6) and creatine (SLC6A8) transporters in cancer development as well as therapeutic potential of their inhibitors. Experimental data indicate that overexpression of analyzed proteins could be connected with colon or breast cancers, which are the most common types of cancers. The pool of known inhibitors of these transporters is limited; however, one ligand of SLC6A8 protein is currently tested in the first phase of clinical trials. Therefore, we also highlight structural aspects useful for ligand development. In this review, we discuss SLC6A6 and SLC6A8 transporters as potential biological targets for anticancer agents.

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