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The role of tumor initiating cells in drug resistance of breast cancer: Implications for future therapeutic approaches.

机译:肿瘤起始细胞在乳腺癌耐药中的作用:对未来治疗方法的影响。

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摘要

The ability to prospectively isolate breast cancer cells that initiate tumors when transplanted orthotopically into immunocompromised mice has led to an explosion of work characterizing these cells and establishing ways to target them. Microarray studies screening for novel targets and chemical library screens for effective therapies have implicated signaling pathways, tumor-stromal interactions, miRNAs and possible even piwi-interacting (piRNAs) in the regulation of tumor initiating cell self-renewal. Potential targeting agents including the beta-catenin inhibitor sulforaphane, AKT inhibitor perfosine, hedgehog inhibitor cyclopamine, stromal interaction inhibitor repertaxin, multidrug resistance pump poison dofequifar fumarate, as well as targeted the dual epidermal growth factor family inhibitor lapatinib and many more have all been found to have toxicity against purportedly chemotherapy resistant subpopulations of cancer cells often referred to as tumor initiating cells (TICs). Work using clinical samples is emerging and supports the hypothesis that neoadjuvant chemotherapy can enrich for TICs in residual disease, but strong correlation with long-term outcome is yet to be established. This paper reviews current attempts to targeting TICs and discusses the competing hypotheses to explain breast cancer recurrence and therapy resistance.
机译:当将原位移植到免疫功能低下的小鼠体内时,前瞻性分离引发肿瘤的乳腺癌细胞的能力导致了表征这些细胞并建立靶向它们的方法的工作激增。针对新型靶点的微阵列研究筛选和对有效疗法的化学文库筛选,在调控肿瘤引发细胞自我更新的过程中涉及信号传导途径,肿瘤基质相互作用,miRNA甚至可能是小卵小分子相互作用(piRNA)。潜在的靶向药物包括β-catenin抑制剂萝卜硫烷,AKT抑制剂perfosine,hedgehog抑制剂环巴胺,基质相互作用抑制剂repertaxin,多药耐药泵毒剂dofequifar富马酸酯,以及靶向双重表皮生长因子家族抑制剂lapatinib等等。对据称对化疗具有抵抗力的癌细胞亚群(通常称为肿瘤起始细胞(TIC))具有毒性。使用临床样品的工作正在兴起,并支持了新辅助化疗可以丰富残留疾病中TIC的假说,但与长期结果的密切相关性尚待确立。本文回顾了目前针对TIC的尝试,并讨论了相互竞争的假说来解释乳腺癌的复发和治疗耐药性。

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