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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Glutamine targeting inhibits systemic metastasis in the VM-M3 murine tumor model.
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Glutamine targeting inhibits systemic metastasis in the VM-M3 murine tumor model.

机译:谷氨酰胺靶向抑制VM-M3鼠肿瘤模型中的全身转移。

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Metastatic cancer is a major cause of morbidity and mortality. Current therapeutic options consist of chemotherapy, radiation or targeted therapies. However, these therapies are often toxic, effective over a small range of cancer types or result in drug resistance. Therefore, a more global, less toxic strategy for the management of metastatic cancer is required. Although most cancers display increased glucose metabolism, glutamine is also a major energy substrate for many cancers. We evaluated the antimetastatic potential of 6-diazo-5-oxo-L-norleucine (DON), a glutamine analog, using the new VM mouse model of systemic metastasis. We found that primary tumor growth was approximately 20-fold less in DON-treated mice than in untreated control mice. We also found that DON treatment inhibited metastasis to liver, lung and kidney as detected by bioluminescence imaging and histology. Our findings provide proof of concept that metabolic therapies targeting glutamine metabolism can manage systemic metastatic cancer.
机译:转移性癌症是发病率和死亡率的主要原因。当前的治疗选择包括化学疗法,放射疗法或靶向疗法。然而,这些疗法通常是有毒的,在小范围的癌症类型上有效或导致耐药性。因此,需要用于转移癌的更全面,毒性更小的策略。尽管大多数癌症显示葡萄糖代谢增加,但谷氨酰胺还是许多癌症的主要能量底物。我们使用系统转移的新型VM小鼠模型评估了谷氨酰胺类似物6-重氮基5-氧代-L-正亮氨酸(DON)的抗转移潜力。我们发现在DON处理的小鼠中,原发肿瘤的生长比未处理的对照小鼠低约20倍。我们还发现,通过生物发光成像和组织学检测,DON治疗可抑制肝,肺和肾脏的转移。我们的发现提供了概念证明,即针对谷氨酰胺代谢的代谢疗法可以治疗系统性转移癌。

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