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Human asparagine synthetase associates with the mitotic spindle

机译:人天冬酰胺合成酶与有丝分裂纺锤体相关

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Cancer cells are characterized by extensive reprogramming of metabolic pathways in order to promote cell division and survival. However, the growth promotion effects of metabolic reprogramming can be due to moonlighting functions of metabolic enzymes as well as the redirection of flux through particular pathways. To identify metabolic enzymes that might have potential moonlighting functions in oncogenesis, we have examined recent screens of the yeast GFP strain collection for metabolic enzymes that have been implicated in cancer metabolism with an unusual subcellular localization. Asparagine synthetase forms filaments in yeast in response to nutrient limitation and is part of a pathway that is a chemotherapy target in acute lymphoblastic leukemia. Interestingly, while yeast asparagine synthetase forms cytoplasmic filaments in response to nutrient stress, human asparagine synthetase is associated with the centrosomes and mitotic spindles. This localization is disrupted by both nocodazole and asparaginase treatments. This failure to localize occurs even though asparagine synthetase is highly upregulated in response to asparaginase treatment. Together, these results argue that human asparagine synthetase undergoes regulated recruitment to the mitotic spindles and that it may have acquired a second role in mitosis similar to other metabolic enzymes that contribute to metabolic reprogramming in cancer cells.
机译:癌细胞的特征在于代谢途径的大量重编程,以促进细胞分裂和存活。但是,代谢重编程对生长的促进作用可能是由于代谢酶的月光作用以及通过特定途径的通量重定向。为了鉴定可能在肿瘤发生中具有潜在月光功能的代谢酶,我们检查了酵母GFP菌株集合的最新筛选,以寻找与癌症代谢有关的异常酶,这些代谢酶具有异常的亚细胞定位。天冬酰胺合成酶响应营养限制而在酵母中形成细丝,并且是急性淋巴细胞白血病化学疗法靶标通路的一部分。有趣的是,虽然酵母天冬酰胺合成酶响应营养胁迫而形成细胞质细丝,但人天冬酰胺合成酶却与中心体和有丝分裂纺锤体相关。诺考达唑和天冬酰胺酶治疗均破坏了该定位。即使天冬酰胺合成酶响应于天冬酰胺酶处理而高度上调,也会发生这种定位失败。总之,这些结果表明,人天冬酰胺合成酶经历了向有丝分裂纺锤体的有规律的募集,并且它可能在有丝分裂中获得了第二种作用,类似于其他有助于癌细胞中代谢重编程的代谢酶。

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