肾嗜酸细胞瘤中线粒体DNA突变导致复合体I缺失。

Loss of complex I due to mitochondrial DNA mutations in renal oncocytoma.

作者信息

Mayr Johannes A, Meierhofer David, Zimmermann Franz, Feichtinger Rene, Kögler Christian, Ratschek Manfred, Schmeller Nikolaus, Sperl Wolfgang, Kofler Barbara

机构信息

Department of Pediatrics, University Hospital Salzburg, Paracelsus Medical University, Salzburg, Austria.

出版信息

Clin Cancer Res. 2008 Apr 15;14(8):2270-5. doi: 10.1158/1078-0432.CCR-07-4131.

DOI:10.1158/1078-0432.CCR-07-4131

PMID:18413815

Abstract

PURPOSE

Many solid tumors exhibit abnormal aerobic metabolism characterized by increased glycolytic capacity and decreased cellular respiration. Recently, mutations in the nuclear encoded mitochondrial enzymes fumarate hydratase and succinate dehydrogenase have been identified in certain tumor types, thus demonstrating a direct link between mitochondrial energy metabolism and tumorigenesis. Although mutations in the mitochondrial genome (mitochondrial DNA, mtDNA) also can affect aerobic metabolism and mtDNA alterations are frequently observed in tumor cells, evidence linking respiratory chain deficiency in a specific tumor type to a specific mtDNA mutation has been lacking.

EXPERIMENTAL DESIGN

To identify mitochondrial alterations in oncocytomas, we investigated the activities of respiratory chain enzymes and sequenced mtDNA in 15 renal oncocytoma tissues.

RESULTS

Here, we show that loss of respiratory chain complex I (NADH/ubiquinone oxidoreductase) is associated with renal oncocytoma. Enzymatic activity of complex I was undetectable or greatly reduced in the tumor samples (n = 15). Blue Native gel electrophoresis of the multisubunit enzyme complex revealed a lack of assembled complex I. Mutation analysis of the mtDNA showed frame-shift mutations in the genes of either subunit ND1, ND4, or ND5 of complex I in 9 of the 15 tumors.

CONCLUSION

Our data indicate that isolated loss of complex I is a specific feature of renal oncocytoma and that this deficiency is frequently caused by somatic mtDNA mutations.

摘要

目的

许多实体瘤表现出异常的有氧代谢，其特征为糖酵解能力增强和细胞呼吸减弱。最近，在某些肿瘤类型中已鉴定出核编码的线粒体酶富马酸水合酶和琥珀酸脱氢酶的突变，从而证明了线粒体能量代谢与肿瘤发生之间的直接联系。尽管线粒体基因组（线粒体DNA，mtDNA）中的突变也可影响有氧代谢，且肿瘤细胞中经常观察到mtDNA改变，但缺乏将特定肿瘤类型中的呼吸链缺陷与特定mtDNA突变联系起来的证据。

实验设计

为了鉴定嗜酸细胞瘤中的线粒体改变，我们研究了15例肾嗜酸细胞瘤组织中呼吸链酶的活性并对mtDNA进行了测序。

结果

在此，我们表明呼吸链复合体I（NADH/泛醌氧化还原酶）的缺失与肾嗜酸细胞瘤相关。在肿瘤样本（n = 15）中未检测到或大大降低了复合体I的酶活性。对多亚基酶复合体进行蓝色非变性凝胶电泳显示缺乏组装好的复合体I。mtDNA的突变分析显示，15个肿瘤中有9个在复合体I的亚基ND1、ND4或ND5基因中存在移码突变。

结论

我们的数据表明，孤立的复合体I缺失是肾嗜酸细胞瘤的一个特定特征，并且这种缺陷经常由体细胞mtDNA突变引起。

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肾嗜酸细胞瘤中线粒体DNA突变导致复合体I缺失。

Loss of complex I due to mitochondrial DNA mutations in renal oncocytoma.

作者信息

Mayr Johannes A, Meierhofer David, Zimmermann Franz, Feichtinger Rene, Kögler Christian, Ratschek Manfred, Schmeller Nikolaus, Sperl Wolfgang, Kofler Barbara

机构信息

Department of Pediatrics, University Hospital Salzburg, Paracelsus Medical University, Salzburg, Austria.

出版信息

Clin Cancer Res. 2008 Apr 15;14(8):2270-5. doi: 10.1158/1078-0432.CCR-07-4131.

DOI:10.1158/1078-0432.CCR-07-4131

PMID:18413815

Abstract

PURPOSE

EXPERIMENTAL DESIGN

To identify mitochondrial alterations in oncocytomas, we investigated the activities of respiratory chain enzymes and sequenced mtDNA in 15 renal oncocytoma tissues.

RESULTS

CONCLUSION

Our data indicate that isolated loss of complex I is a specific feature of renal oncocytoma and that this deficiency is frequently caused by somatic mtDNA mutations.

摘要

目的

实验设计

为了鉴定嗜酸细胞瘤中的线粒体改变，我们研究了15例肾嗜酸细胞瘤组织中呼吸链酶的活性并对mtDNA进行了测序。

结果

结论

我们的数据表明，孤立的复合体I缺失是肾嗜酸细胞瘤的一个特定特征，并且这种缺陷经常由体细胞mtDNA突变引起。

肾嗜酸细胞瘤中线粒体DNA突变导致复合体I缺失。

Loss of complex I due to mitochondrial DNA mutations in renal oncocytoma.

作者信息

机构信息

出版信息

PURPOSE

EXPERIMENTAL DESIGN

RESULTS

CONCLUSION

目的

实验设计

结果

结论

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肾嗜酸细胞瘤中线粒体DNA突变导致复合体I缺失。

Loss of complex I due to mitochondrial DNA mutations in renal oncocytoma.

作者信息

机构信息

出版信息

PURPOSE

EXPERIMENTAL DESIGN

RESULTS

CONCLUSION

目的

实验设计

结果

结论

相似文献

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