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Mesenchymal Stem Cells: A New Platform for Targeting Suicide Genes in Cancer Publisher Pubmed



Moradian Tehrani R1 ; Verdi J1, 2 ; Noureddini M1 ; Salehi R3 ; Salarinia R4 ; Mosalaei M3 ; Simonian M3 ; Alani B1 ; Ghiasi MR3 ; Jaafari MR5 ; Mirzaei HR6, 7, 8 ; Mirzaei H9
Authors

Source: Journal of Cellular Physiology Published:2018


Abstract

One of the important strategies for the treatment of cancer is gene therapy which has the potential to exclusively eradicate malignant cells, without any damage to the normal tissues. Gene-directed enzyme prodrug therapy (GDEPT) is a two-step gene therapy approach, where a suicide gene is directed to tumor cells. The gene encodes an enzyme that expressed intracellularly where it is able to convert a prodrug into cytotoxic metabolites. Various delivery systems have been developed to achieve the appropriate levels of tumor restricted expression of chemotherapeutic drugs. Nowadays, mesenchymal stem cells (MSCs) have been drawing great attention as cellular vehicles for gene delivery systems. Inherent characteristics of MSCs make them particularly attractive gene therapy tools in cell therapy. They have been used largely for their remarkable homing property toward tumor sites and availability from many different adult tissues and show anti-inflammatory actions in some cases. They do not stimulate proliferative responses of lymphocytes, suggests that MSCs have low immunogenicity and could avoid immune rejection. This review summarizes the current state of knowledge about genetically modified MSCs that enable to co-transduce a variety of therapeutic agents including suicide genes (i.e., cytosine deaminase, thymidine kinase) in order to exert potent anti-carcinogenesis against various tumors growth. Moreover, we highlighted the role of exosomes released from MSCs as new therapeutic platform for targeting various therapeutic agents. © 2017 Wiley Periodicals, Inc.
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