Background: It is becoming increasingly recognized that weight and nutritional status can impact cancer survival.\nWe have previously shown that obese mice with syngeneic acute lymphoblastic leukemia (ALL) have poorer response\nto chemotherapy treatment than control mice. We therefore investigated whether dietary intervention could improve\noutcome from the most common pediatric cancer, ALL.\nMethods: Diet-induced obese (DIO) mice raised on a 60% calories from fat diet and control mice were implanted with\nsyngeneic ALL cells. Some DIO mice were switched to the low-fat control diet. Survival from ALL was assessed without\nor with chemotherapy treatment starting at the time of the diet switch. Cells from DIO mice before and after diet\nswitch were assessed by FACS for BrdU incorporation and phosphorylation status of AKT, S6K, and EIF2a. Similar\nexperiments were done with human ALL xenografts. Mouse and human ALL cells were cultured in media with 10%\nor 5% fetal bovine serum, and sensitivity to chemotherapies assessed.\nResults: DIO mice had poorer survival (17%) after vincristine monotherapy than control mice on a 10% low fat diet (42%;n = 12/group; p = 0.09, log rank). However, switching obese mice to the low-fat diet prior to initiation of vincristine led to dramatically improved survival (92%, p < 0.01 vs both other groups). In vitro, FBS restriction made murine and human ALL cells more sensitive to vincristine. Interestingly, while serum restriction enhanced ALL sensitivity to dexamethasone and L-asparaginase, dietary switch did not improve survival of DIO mice treated with either drug in monotherapy. Thus, it appears that dietary intervention has a unique effect to improve ALL cell sensitivity to vincristine in vivo.\nConclusions: We report herein that a dietary intervention can improve ALL outcome in a preclinical model. Further work\nis needed to identify the mechanisms of this effect and investigate potential impact on human leukemia in patients.
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