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A metabolomics investigation into the effects of HIV protease inhibitors on HPV16 E6 expressing cervical carcinoma cells.

机译:HIV蛋白酶抑制剂对HpV16 E6表达宫颈癌细胞作用的代谢组学研究。

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摘要

Recently, it has been reported that anti-viral drugs, such as indinavir and lopinavir (originally targeted for HIV), also inhibit E6-mediated proteasomal degradation of mutant p53 in E6-transfected C33A cells. In order to understand more about the mode-of-action(s) of these drugs the metabolome of HPV16 E6 expressing cervical carcinoma cell lines was investigated using mass spectrometry (MS)-based metabolic profiling. The metabolite profiling of C33A parent and E6-transfected cells exposed to these two anti-viral drugs was performed by ultra performance liquid chromatography (UPLC)-MS and gas chromatography (GC)-time of flight (TOF)-MS. Using a combination of univariate and multivariate analyses, these metabolic profiles were investigated for analytical and biological reproducibility and to discover key metabolite differences elicited during anti-viral drug challenge. This approach revealed both distinct and common effects of these two drugs on the metabolome of two different cell lines. Finally, intracellular drug levels were quantified, which suggested in the case of lopinavir that increased activity of membrane transporters may contribute to the drug sensitivity of HPV infected cells.
机译:最近,据报道,抗病毒药,例如茚地那韦和洛匹那韦(最初针对HIV),也抑制了E6转染的C33A细胞中E6介导的突变体p53的蛋白酶体降解。为了更多地了解这些药物的作用方式,使用基于质谱(MS)的代谢谱研究了表达HPV16 E6的子宫颈癌细胞系的代谢组。通过超高效液相色谱(UPLC)-MS和气相色谱(GC)-飞行时间(TOF)-MS对暴露于这两种抗病毒药物的C33A亲本和E6转染细胞进行代谢谱分析。结合单变量和多变量分析,研究了这些代谢谱的分析和生物学再现性,并发现了抗病毒药物攻击过程中引起的关键代谢物差异。这种方法揭示了这两种药物对两种不同细胞系代谢组的独特和共同作用。最后,对细胞内药物水平进行了定量,这表明在洛匹那韦的情况下,膜转运蛋白活性的提高可能有助于感染HPV的细胞对药物的敏感性。

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