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Network Analysis of Breast Cancer Progression and Reversal Using a Tree-Evolving Network Algorithm

机译:基于进化树网络算法的乳腺癌进展与逆转网络分析

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The HMT3522 progression series of human breast cells have been used to discover how tissue architecture, microenvironment and signaling molecules affect breast cell growth and behaviors. However, much remains to be elucidated about malignant and phenotypic reversion behaviors of the HMT3522-T4-2 cells of this series. We employed a “pan-cell-state” strategy, and analyzed jointly microarray profiles obtained from different state-specific cell populations from this progression and reversion model of the breast cells using a tree-lineage multi-network inference algorithm, Treegl. We found that different breast cell states contain distinct gene networks. The network specific to non-malignant HMT3522-S1 cells is dominated by genes involved in normal processes, whereas the T4-2-specific network is enriched with cancer-related genes. The networks specific to various conditions of the reverted T4-2 cells are enriched with pathways suggestive of compensatory effects, consistent with clinical data showing patient resistance to anticancer drugs. We validated the findings using an external dataset, and showed that aberrant expression values of certain hubs in the identified networks are associated with poor clinical outcomes. Thus, analysis of various reversion conditions (including non-reverted) of HMT3522 cells using Treegl can be a good model system to study drug effects on breast cancer.
机译:人类乳腺细胞HMT3522进程系列已用于发现组织结构,微环境和信号分子如何影响乳腺细胞的生长和行为。然而,关于该系列的HMT3522-T4-2细胞的恶性和表型逆转行为,还有许多事情需要阐明。我们采用了“泛细胞状态”策略,并使用树谱多网络推理算法Treegl共同分析了从不同状态特异性细胞群体从乳腺细胞的这种进展和逆转模型获得的微阵列图谱。我们发现不同的乳腺细胞状态包含不同的基因网络。非恶性HMT3522-S1细胞特有的网络由正常过程中涉及的基因控制,而T4-2-特异的网络则富含与癌症相关的基因。特定于恢复的T4-2细胞各种状况的网络富含提示补偿作用的途径,这与临床数据表明患者对抗癌药物有抗性相一致。我们使用外部数据集验证了发现,并表明所识别网络中某些集线器的异常表达值与不良的临床结果相关。因此,使用Treegl分析HMT3522细胞的各种逆转条件(包括未逆转)可以成为研究药物对乳腺癌的作用的良好模型系统。

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