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Mesenchymal Stem/Stromal Cell-Based Delivery: A Rapidly Evolving Strategy for Cancer Therapy Publisher



Hassanzadeh A1 ; Altajer AH2 ; Rahman HS3, 4 ; Saleh MM5 ; Bokov DO6 ; Abdelbasset WK7, 8 ; Marofi F9 ; Zamani M10 ; Yaghoubi Y11 ; Yazdanifar M12 ; Pathak Y13, 14 ; Chartrand MS15 ; Jarahian M16
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Source: Frontiers in Cell and Developmental Biology Published:2021


Abstract

Mesenchymal stem/stromal cell (MSC)-based therapy has become an attractive and advanced scientific research area in the context of cancer therapy. This interest is closely linked to the MSC-marked tropism for tumors, suggesting them as a rational and effective vehicle for drug delivery for both hematological and solid malignancies. Nonetheless, the therapeutic application of the MSCs in human tumors is still controversial because of the induction of several signaling pathways largely contributing to tumor progression and metastasis. In spite of some evidence supporting that MSCs may sustain cancer pathogenesis, increasing proofs have indicated the suppressive influences of MSCs on tumor cells. During the last years, a myriad of preclinical and some clinical studies have been carried out or are ongoing to address the safety and efficacy of the MSC-based delivery of therapeutic agents in diverse types of malignancies. A large number of studies have focused on the MSC application as delivery vehicles for tumor necrosis factor-related apoptosis-inducing ligand (TRAIL), chemotherapeutic drug such as gemcitabine (GCB), paclitaxel (PTX), and doxorubicin (DOX), prodrugs such as 5-fluorocytosine (5-FC) and ganciclovir (GCV), and immune cell-activating cytokines along with oncolytic virus. In the current review, we evaluate the latest findings rendering the potential of MSCs to be employed as potent gene/drug delivery vehicle for inducing tumor regression with a special focus on the in vivo reports performed during the last two decades. © Copyright © 2021 Hassanzadeh, Altajer, Rahman, Saleh, Bokov, Abdelbasset, Marofi, Zamani, Yaghoubi, Yazdanifar, Pathak, Chartrand and Jarahian.
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