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   decrease of tumor-infiltrating regulatory t cells using pentoxifylline: an ex vivo analysis in triple-negative breast cancer mouse model  
   
نویسنده kazemi mohammad hossein ,shokrollahi barough mahdieh ,ghanavatinejad alireza ,momeni-varposhti zahra ,khorrami samaneh ,sadeghi behnam ,falak reza
منبع iranian journal of allergy, asthma and immunology - 2022 - دوره : 21 - شماره : 2 - صفحه:167 -177
چکیده    Triple-negative breast cancer (tnbc) is the most aggressive type of bc with the highest percentage of tumor-infiltrating lymphocytes (tils). hence, til therapy is considered a promising approach to target tnbc. depletion of regulatory t cells (tregs) in tils can improve the antitumor function of til therapy. pentoxifylline (ptxf) is a xanthine derivative that can modulate the nuclear factor kappa b (nf-κb) signaling and probably affect the treg proportion in tils. we aimed to evaluate the ex vivo effect of ptxf on the proportion of treg cells in the tils derived from a mouse model of tnbc. the 4t1 cells were inoculated subcutaneously to balb/c mice to induce tnbc. tils were isolated from tumor tissue by enzymatic digestion and cultured alone or with 4t1 cells for 24, 48, and 72 h in the presence of interleukin (il)-2 and different concentrations of ptxf. the toxicity of ptxf and its effects on tregs proportion as well as cytokine production was evaluated using mtt assay, flow cytometry, and elisa, respectively. ptxf had no significant impact on the viability of tils. both 500 and 1000 g/ml of ptxf decreased the proportion of tregs in a dose-dependent manner. the level of interferon- and tumor growth factor- in tils supernatant were increased and decreased, respectively.our data suggest that ex vivo treatment of tils with pentoxifylline could decrease the proportion of tregs in the conventional il-2-mediated til expansion and change the cytokine balance of tils in favor of antitumor immune response.
کلیدواژه breast neoplasms; pentoxifylline; regulatory t-lymphocytes; tumor-infiltrating lymphocytes
آدرس iran university of medical sciences, school of medicine, department of immunology, iran. acecr, breast cancer research center, motamed cancer institute, department of atmp, iran, iran university of medical sciences, school of medicine, department of immunology, iran. acecr, breast cancer research center, motamed cancer institute, department of atmp, iran, pasteur institute of iran, department of immunology, iran, shahid beheshti university of medical sciences, hematopoietic stem cell research center, iran, iran university of medical sciences, school of medicine, immunology research center, institute of immunology and infectious disease, department of immunology, iran, acecr, breast cancer research center, motamed cancer institute, department of atmp, iran. karolinska institutet, translational cell therapy research (tcr), intervention and technology (clintec), division of pediatrics, department of clinical science, sweden, iran university of medical sciences, school of medicine, immunology research center, institute of immunology and infectious disease, department of immunology, iran
پست الکترونیکی falak.r@iums.ac.ir
 
     
   
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