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GCSH antisense regulation determines breast cancer cells’ viability

机译:GCSH反义调控决定乳腺癌细胞的生存能力

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Since it is known that cancer cells exhibit a preference for increased glycine consumption, the respective glycine metabolizing enzymes are in focus of many research projects. However, no cancer associated studies are available for the Glycine Cleavage System Protein H (GCSH) to date. Our initial analysis revealed a GCSH-overexpression of the protein-coding transcript variant 1 (Tv1) in breast cancer cells and tissue. Furthermore, a shorter (391?bp) transcript variant (Tv*) was amplified with an increased expression in healthy breast cells and a decreased expression in breast cancer samples. The Tv1/Tv* transcript ratio is 1.0 in healthy cells on average, and between 5–10 in breast cancer cells. Thus, a GCSH-equilibrium at the transcript level is likely conceivable for optimal glycine degradation. A possible regulative role of Tv* was proven by Tv1-Tv*-RNA-binding and overexpression studies which consequently led to serious physiological alterations: decreased metabolic activity, release of the lactate dehydrogenase, increased extracellular acidification, and finally necrosis as a result of impaired plasma membranes. In contrast, Tv1-overexpression led to an additional increase in cellular vitality of the tumor cells, primarily due to the acceleration of the mitochondrial glycine decarboxylation activity. Ultimately, we provide the first evidence of a sensitive GCSH-antisense regulation which determines cancerous cell viability.
机译:由于已知癌细胞表现出对增加的甘氨酸消耗的偏好,因此各个甘氨酸代谢酶是许多研究项目的重点。但是,迄今为止,尚无针对甘氨酸裂解系统蛋白H(GCSH)的癌症相关研究。我们的初步分析显示了在乳腺癌细胞和组织中GCSH过表达蛋白质编码转录变体1(Tv1)。此外,扩增了较短的(391bp)转录物变体(Tv *),在健康的乳腺癌细胞中表达增加,而在乳腺癌样品中表达降低。 Tv1 / Tv *转录本比率在健康细胞中平均为1.0,在乳腺癌细胞中平均为5-10。因此,在转录水平上的GCSH平衡对于最佳的甘氨酸降解是可能的。 Tv1-Tv * -RNA结合和过表达研究证明了Tv *的可能调节作用,从而导致严重的生理变化:代谢活性降低,乳酸脱氢酶释放,细胞外酸化增加以及由于坏死导致的坏死质膜受损。相反,Tv1过表达导致肿瘤细胞的细胞活力进一步增加,这主要是由于线粒体甘氨酸脱羧活性的提高。最终,我们提供了敏感的GCSH反义调控的初步证据,该调控决定了癌细胞的生存能力。

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