Targeting the thioredoxin system as a novel strategy against B-cell acute lymphoblastic leukemia

以硫氧还蛋白系统为靶点治疗B细胞急性淋巴细胞白血病的新策略

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作者:Klaudyna Fidyt ,Agata Pastorczak ,Agnieszka Goral ,Kacper Szczygiel ,Wojciech Fendler ,Angelika Muchowicz ,Marcin Adam Bartlomiejczyk ,Joanna Madzio ,Julia Cyran ,Agnieszka Graczyk-Jarzynka ,Eugene Jansen ,Elzbieta Patkowska ,Ewa Lech-Maranda ,Deepali Pal ,Helen Blair ,Anna Burdzinska ,Piotr Pedzisz ,Eliza Glodkowska-Mrowka ,Urszula Demkow ,Karolina Gawle-Krawczyk ,Michal Matysiak ,Magdalena Winiarska ,Przemyslaw Juszczynski ,Wojciech Mlynarski ,Olaf Heidenreich ,Jakub Golab ,Malgorzata Firczuk

Abstract

B-cell precursor acute lymphoblastic leukemia (BCP-ALL) is a genetically heterogeneous blood cancer characterized by abnormal expansion of immature B cells. Although intensive chemotherapy provides high cure rates in a majority of patients, subtypes harboring certain genetic lesions, such as MLL rearrangements or BCR-ABL1 fusion, remain clinically challenging, necessitating a search for other therapeutic approaches. Herein, we aimed to validate antioxidant enzymes of the thioredoxin system as potential therapeutic targets in BCP-ALL. We observed oxidative stress along with aberrant expression of the enzymes associated with the activity of thioredoxin antioxidant system in BCP-ALL cells. Moreover, we found that auranofin and adenanthin, inhibitors of the thioredoxin system antioxidant enzymes, effectively kill BCP-ALL cell lines and pediatric and adult BCP-ALL primary cells, including primary cells cocultured with bone marrow-derived stem cells. Furthermore, auranofin delayed the progression of leukemia in MLL-rearranged patient-derived xenograft model and prolonged the survival of leukemic NSG mice. Our results unveil the thioredoxin system as a novel target for BCP-ALL therapy, and indicate that further studies assessing the anticancer efficacy of combinations of thioredoxin system inhibitors with conventional anti-BCP-ALL drugs should be continued.

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