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首页> 外文期刊>Cancer Management and Research >Pathogenic Heteroplasmic Somatic Mitochondrial DNA Mutation Confers Platinum-Resistance and Recurrence of High-Grade Serous Ovarian Cancer
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Pathogenic Heteroplasmic Somatic Mitochondrial DNA Mutation Confers Platinum-Resistance and Recurrence of High-Grade Serous Ovarian Cancer

机译:致病性异质体细胞线粒体DNA突变赋予铂抗性和高等血液癌癌的复发性

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Purpose:Platinum resistance is a primary barrier to improving the survival rate of ovarian cancer. The relationship between mtDNA somatic mutations and response to platinum-based chemotherapy in ovarian cancer has not been well clarified.Patients and Methods:Here, we employed the next-generation sequencing (NGS) platform to identify mtDNA mutations of the unrelated high-grade serous ovarian cancer (HGSOC) patients.Results:We identified 569 germline variants and 28 mtDNA somatic mutations, and found the platinum-sensitive relapsed HGSOC patients had more synonymous mutations while the platinum-resistant relapsed HGSOC patients had more missense mutations in the mtDNA somatic mutations. Meanwhile, we found that the HGSOC patients who harbored heteroplasmic pathogenic mtDNA somatic mutations had significantly higher prevalence of both platinum-resistance and relapse than those without (80.0% versus 16.7%, p=0.035). Additionally, we observed that the tumor tissues had significantly higher lactate-to-pyruvate (L/P) ratio than the paired nontumor tissues (p0.001), and L/P ratio of tumors with any heteroplasmic pathogenic mtDNA mutations was significantly higher than that of the tumors free of pathogenic mtDNA mutations (p=0.025).Conclusion:Our findings indicate that these heteroplasmic pathogenic mtDNA somatic mutations may cause decreased respiratory chain activity and lead to the metabolism remodeling that seem to be beneficial for progression of both platinum-based chemotherapy resistance and relapse.? 2020 Ni et al.
机译:目的:铂抗性是提高卵巢癌的存活率的主要障碍。 MTDNA体细胞突变与对卵巢癌中铂化疗的反应的关系尚未得到很好的澄清。患者和方法:这里,我们使用下一代测序(NGS)平台来鉴定无关的高级浆液的MTDNA突变卵巢癌(HGSOC)患者。结果:我们确定了569种种系变体和28个MTDNA体细胞突变,发现铂敏感复发的HGSOC患者具有更多同义突变,而铂抗性复发的HGSOC患者在MTDNA躯体突变中具有更多的畸形突变。同时,我们发现,患有异质致病性MTDNA体细胞突变的HGSOC患者显着高于铂抗性和复发的普遍性(80.0%对16.7%,P = 0.035)。另外,我们观察到,肿瘤组织具有明显高于乳酸 - 丙酮酸(L / P)比比配对的不言组织(P <0.001),肿瘤的L / P比与任何异质致病性MTDNA突变显着高于肿瘤的肿瘤(p = 0.025)。结论:我们的研究结果表明,这些异质致病性MTDNA体细胞突变可能导致呼吸链活性降低并导致代谢重塑,似乎有利于铂 - 铂的进展基于化疗抵抗和复发。 2020 Ni等人。

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