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首页> 外文期刊>Differentiation: The Journal of the International Society of Differentiation >Prostate tumor-stroma interaction: molecular mechanisms and opportunities for therapeutic targeting.
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Prostate tumor-stroma interaction: molecular mechanisms and opportunities for therapeutic targeting.

机译:前列腺肿瘤-基质相互作用:治疗靶点的分子机制和机会。

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摘要

Maintenance of cell and tissue homeostasis is dependent upon the dynamic balance of cell proliferation, differentiation, and apoptosis through interactions between cells and their microenvironment. The unique prostatic cellular phenotypes are induced and maintained by interaction between epithelium and adjacent stroma through intimate intercellular signaling pathways. In this article, we summarize current advances in the tumor-stroma interaction and its biologic and therapeutic implications. We specifically emphasize current studies of the possible factors driving the vicious cycle cells that may be responsible for carcinogenesis and metastasis to bone. Stroma responds both genotypically and phenotypically to tumor epithelium upon co-culture under 3-D conditions. Likewise, the emerging carcinoma responds to stromal signals that drive progression to malignancy. A vicious cycle mediated by soluble and insoluble molecules secreted by tumor cells and stroma appear be the critical factors supporting and sustaining tumor colonization in bone. Co-targeting tumor and stroma with therapeutic agents has yielded promising results both in pre-clinical models of prostate cancer and bony metastasis and in clinical trials of patients treated with a dual tumor and stroma targeting strategies. In conclusion, understanding and targeting the interaction of the tumor and its stromal microenvironmant may improve the prognosis, reduce the suffering and increase the survival of patients with advanced cancer metastasis.
机译:细胞和组织动态平衡的维持取决于细胞与其微环境之间相互作用的细胞增殖,分化和凋亡的动态平衡。独特的前列腺细胞表型是通过上皮细胞与邻近基质之间通过紧密的细胞间信号传导途径相互作用而诱导和维持的。在本文中,我们总结了肿瘤-基质相互作用及其生物学和治疗意义的最新进展。我们特别强调对驱动恶性循环细胞的可能因素的最新研究,这些恶性循环细胞可能与骨骼的癌变和转移有关。在3D条件下共培养时,基质在基因型和表型上均对肿瘤上皮有反应。同样,正在出现的癌对基质信号产生反应,该信号可驱动肿瘤进展。由肿瘤细胞和间质分泌的可溶性和不溶性分子介导的恶性循环似乎是支持和维持肿瘤在骨骼中定植的关键因素。在治疗前列腺癌和骨转移的临床前模型以及采用双重肿瘤和基质靶向治疗策略的患者的临床试验中,将肿瘤与基质与治疗剂共同靶向已经取得了可喜的结果。总之,了解和靶向肿瘤及其基质微环境的相互作用可以改善晚期癌症转移患者的预后,减少其痛苦并提高其生存率。

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