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发现 N-羟基吲哚类人乳酸脱氢酶同工酶 A(LDH-A)抑制剂作为针对癌细胞的饥饿剂。

Discovery of N-hydroxyindole-based inhibitors of human lactate dehydrogenase isoform A (LDH-A) as starvation agents against cancer cells.

机构信息

Dipartimento di Scienze Farmaceutiche, Università di Pisa, Via Bonanno 6, 56126 Pisa, Italy.

出版信息

J Med Chem. 2011 Mar 24;54(6):1599-612. doi: 10.1021/jm101007q. Epub 2011 Feb 18.

Abstract

Highly invasive tumor cells are characterized by a metabolic switch, known as the Warburg effect, from "normal" oxidative phosphorylation to increased glycolysis even under sufficiently oxygenated conditions. This dependence on glycolysis also confers a growth advantage to cells present in hypoxic regions of the tumor. One of the key enzymes involved in glycolysis, the muscle isoform of lactate dehydrogenase (LDH-A), is overexpressed by metastatic cancer cells and is linked to the vitality of tumors in hypoxia. This enzyme may be considered as a potential target for new anticancer agents, since its inhibition cuts cancer energetic and anabolic supply, thus reducing the metastatic and invasive potential of cancer cells. We have discovered new and efficient N-hydroxyindole-based inhibitors of LDH-A, which are isoform-selective (over LDH-B) and competitive with both the substrate (pyruvate) and the cofactor (NADH). The antiproliferative activity of these compounds was confirmed on a series of cancer cell lines, and they proved to be particularly effective under hypoxic conditions. Moreover, NMR experiments showed that these compounds are able to reduce the glucose-to-lactate conversion inside the cell.

摘要

高侵袭性肿瘤细胞的特征是代谢开关的改变,即“正常”氧化磷酸化向增加的糖酵解转变,即使在氧合条件充分的情况下也是如此。这种对糖酵解的依赖性也赋予了肿瘤缺氧区域存在的细胞生长优势。糖酵解中涉及的关键酶之一是肌肉同工型乳酸脱氢酶(LDH-A),转移性癌细胞过度表达该酶,并与肿瘤在缺氧环境下的活力有关。该酶可以被视为新型抗癌药物的潜在靶点,因为其抑制作用会切断癌细胞的能量和合成代谢供应,从而降低癌细胞的转移和侵袭潜力。我们已经发现了新型有效的基于 N-羟基吲哚的 LDH-A 抑制剂,它们具有同工酶选择性(优于 LDH-B),并且与底物(丙酮酸)和辅因子(NADH)竞争。这些化合物的抗增殖活性已在一系列癌细胞系上得到证实,并且在缺氧条件下它们被证明特别有效。此外,NMR 实验表明,这些化合物能够降低细胞内的葡萄糖向乳酸的转化。

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