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An integrated functional genomics and metabolomics approach for defining poor prognosis in human neuroendocrine cancers

机译:一种综合的功能基因组学和代谢组学方法用于定义人类神经内分泌癌的不良预后

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摘要

Human neuroendocrine (NE) cancers range from relatively indolent to highly aggressive. In this study, we combine functional genomics with metabolomics to identify features of NE cancers associated with a poor outcome. Analysis of GeneChip datasets of primary prostate tumors, as well as lymph node and liver metastases from transgenic mice with a NE cell cancer, plus derived NE cell lines yielded a signature of 446 genes whose expression is enriched in neoplastic mouse prostatic NE cells. This signature was used for in silico metabolic reconstructions of NE cell metabolism, directed liquid chromatography/tandem MS analysis of metabolites in prostatic NE tumors and cell lines, and analysis of GeneChip datasets of human NE tumors with good or poor prognoses. The results indicate that a distinguishing feature of poor-prognosis NE tumors is a glutamic acid decarboxylase-independent pathway for production of GABA and a pathway for production of imidazole-4-acetate that involves dopa decarboxylase and a membrane-associated amine oxidase, amiloride-binding protein 1. Electrophysiological studies disclosed that imidazole-4-acetate can bind and activate GABAA receptors expressed by transformed NE cells, thus providing a previously uncharacterized paradigm for NE tumor cell signaling. Transcriptional, metabolic, and electrophysiologic features of transformed mouse NE cells are also evident in neural progenitor cells.
机译:人类神经内分泌(NE)癌症的范围从相对惰性到高度侵袭性。在这项研究中,我们将功能基因组学与代谢组学相结合,以鉴定与不良预后相关的NE癌症的特征。对原发性前列腺肿瘤的GeneChip数据集进行分析,以及患有NE细胞癌的转基因小鼠的淋巴结和肝转移,加上衍生的NE细胞系,产生了446个基因的签名,其表达在肿瘤性小鼠前列腺NE细胞中富集。此签名用于NE细胞代谢的计算机代谢重建,前列腺NE肿瘤和细胞系中代谢物的直接液相色谱/串联MS分析以及预后良好或不良的人NE肿瘤的GeneChip数据集。结果表明,预后差的NE肿瘤的一个显着特征是不依赖谷氨酸脱羧酶的GABA生成途径和不依赖谷氨酸脱羧酶和膜相关胺氧化酶阿米洛利-的乙酸4-咪唑生成途径。结合蛋白1.电生理研究表明,咪唑-4-乙酸酯可以结合并激活转化的NE细胞表达的GABAA受体,从而为NE肿瘤细胞信号传导提供了以前未知的范式。转化的小鼠NE细胞的转录,代谢和电生理特征在神经祖细胞中也很明显。

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