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An inhibitor of human asparagine synthetase suppresses proliferation of an L-asparaginase-resistant leukemia cell line

机译:人天冬酰胺合成酶抑制剂抑制抗L-天冬酰胺酶的白血病细胞系的增殖

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摘要

Drug resistance in lymphoblastic and myeloblastic leukemia cells is poorly understood, with several lines of evidence suggesting that resistance can be correlated with upregulation of human asparagine synthetase (hASNS) expression, although this hypothesis is controversial. New tools are needed to investigate this clinically important question, including potent hASNS inhibitors. In vitro experiments show an adenylated sulfoximine to be a slow-onset, tight-binding inhibitor of hASNS with nanomolar affinity. This binding affinity represents a 10-fold improvement over that reported for the only other well-characterized hASNS inhibitor. The adenylated sulfoximine has a cytostatic effect on L-asparaginase-resistant MOLT-4 cells cultured in the presence of L-asparaginase, an enzyme that depletes L-asparagine in the growth medium. These observations represent direct evidence that potent hASNS inhibitors may prove to be effective agents for the clinical treatment of acute lymphoblastic leukemia.
机译:人们对淋巴细胞和粒细胞白血病细胞的耐药性了解甚少,尽管有这样的论点尚存争议,但有几条证据表明耐药性可能与人天冬酰胺合成酶(hASNS)表达的上调相关。需要新的工具来研究这个临床上重要的问题,包括有效的hASNS抑制剂。体外实验表明,腺苷酸化的亚砜亚胺是一种缓慢的,紧密结合的hASNS抑制剂,具有纳摩尔摩尔亲和力。该结合亲和力代表比报道的唯一其他特征明​​确的hASNS抑制剂提高了10倍。腺苷酸化的亚砜亚胺对在L-天冬酰胺酶(一种在生长培养基中消耗L-天冬酰胺的酶)存在下培养的L-天冬酰胺酶耐药的MOLT-4细胞具有细胞抑制作用。这些观察结果直接表明有效的hASNS抑制剂可能被证明是用于临床治疗急性淋巴细胞白血病的有效药物。

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