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靶向侵袭性癌症,特别关注脑肿瘤的草氨酸盐。

Oxamate targeting aggressive cancers with special emphasis to brain tumors.

机构信息

Department of Biochemistry, Acibadem M.A.A. University, Istanbul, Turkey.

Department of Biochemistry, Acibadem M.A.A. University, Istanbul, Turkey.

出版信息

Biomed Pharmacother. 2022 Mar;147:112686. doi: 10.1016/j.biopha.2022.112686. Epub 2022 Feb 4.

DOI:10.1016/j.biopha.2022.112686
PMID:35124385
Abstract

Cancer is one of the main causes of human mortality and brain tumors, including invasive pituitary adenomas, medulloblastomas and glioblastomas are common brain malignancies with poor prognosis. Therefore, the development of innovative management strategies for refractory cancers and brain tumors is important. In states of mitochondrial dysfunction - commonly encountered in malignant cells - cells mostly shift to anaerobic glycolysis by increasing the expression of LDHA (Lactate Dehydrogenase-A) gene. Oxamate, an isosteric form of pyruvate, blocks LDHA activity by competing with pyruvate. By blocking LDHA, it inhibits protumorigenic cascades and also induces ROS (reactive oxygen species)-induced mitochondrial apoptosis of cancer cells. In preclinical studies, oxamate blocked the growth of invasive pituitary adenomas, medulloblastomas and glioblastomas. Oxamate also increases temozolomide and radiotherapy sensitivity of glioblastomas. Oxamate is highly polar, which may preclude its clinical utilization due to low penetrance through cell membranes. However, this obstacle could be overcome with nanoliposomes. Moreover, different oxamate analogs were developed which inhibit LDHC4, an enzyme also involved in cancer progression and germ cell physiology. Lastly, phenformin, an antidiabetic agent, exerts anticancer effects via complex I inhibition in the mitochondria and leading the overproduction of ROS. Oxamate combination with phenformin reduces the lactic acidosis-causing side effect of phenformin while inducing synergistic anticancer efficacy. In sum, oxamate as a single agent and more efficiently with phenformin has high potential to slow the progression of aggressive cancers with special emphasis to brain tumors.

摘要

癌症是人类死亡的主要原因之一,脑肿瘤包括侵袭性垂体腺瘤、髓母细胞瘤和胶质母细胞瘤是常见的恶性脑肿瘤,预后不良。因此,开发针对难治性癌症和脑肿瘤的创新管理策略非常重要。在线粒体功能障碍的状态下 - 在恶性细胞中常见 - 细胞通过增加 LDHA(乳酸脱氢酶 A)基因的表达,主要转向无氧糖酵解。氨甲酰基,一种与丙酮酸等电子的形式,通过与丙酮酸竞争来阻断 LDHA 活性。通过阻断 LDHA,它抑制了促肿瘤级联反应,并诱导了癌细胞的 ROS(活性氧)诱导的线粒体凋亡。在临床前研究中,氨甲酰基抑制了侵袭性垂体腺瘤、髓母细胞瘤和胶质母细胞瘤的生长。氨甲酰基还增加了替莫唑胺和顺铂治疗胶质母细胞瘤的敏感性。氨甲酰基高度极性,由于低透过细胞膜,可能会限制其临床应用。然而,这一障碍可以通过纳米脂质体来克服。此外,还开发了不同的氨甲酰基类似物,抑制了 LDHC4,一种也参与癌症进展和生殖细胞生理学的酶。最后,二甲双胍是一种抗糖尿病药物,通过在线粒体中抑制复合物 I 并导致 ROS 过度产生发挥抗癌作用。氨甲酰基与二甲双胍联合使用可减少二甲双胍引起的乳酸酸中毒的副作用,同时诱导协同抗癌疗效。总之,氨甲酰基作为单一药物,与二甲双胍联合使用,具有减缓侵袭性癌症进展的巨大潜力,特别是对脑肿瘤。

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