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Overcoming Drug Resistance and Treating Advanced Prostate Cancer.

机译:克服耐药性和治疗晚期前列腺癌。

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摘要

Most of the prostate cancers (PCa) in advanced stage will progress to castration-resistant prostate cancer (CRPC). Within CRPC group, 50-70% of the patients will develop bone metastasis in axial and other regions of the skeleton. Once PCa cells spread to the bone, currently, no treatment regimens are available to eradicate the metastasis, and cancer- related death becomes inevitable. In 2012, it is estimated that there will be 28,170 PCa deaths in the United States. Thus, PCa bone metastasis-associated clinical complications and treatment resistance pose major clinical challenges. In this review, we will present recent findings on the molecular and cellular pathways that are responsible for bone metastasis of PCa. We will address several novel mechanisms with a focus on the role of bone and bone marrow microenvironment in promoting PCa metastasis, and will further discuss why prostate cancer cells preferentially metastasize to the bone. Additionally, we will discuss novel roles of several key pathways, including angiogenesis and extracellular matrix remodeling in bone marrow and stem cell niches with their relationship to PCa bone metastasis and poor treatment response. We will evaluate how various chemotherapeutic drugs and radiation therapies may allow aggressive PCa cells to gain advantageous mutations leading to increased survival and rendering the cancer cells to become resistant to treatment. The novel concept relating several key survival and invasion signaling pathways to stem cell niches and treatment resistance will be reviewed. Lastly, we will provide an update of several recently developed novel drug candidates that target metastatic cancer microenvironments or niches, and discuss the advantages and significance provided by such therapeutic approaches in pursuit of overcoming drug resistance and treating advanced PCa.
机译:大多数晚期前列腺癌(PCa)都会发展为去势抵抗性前列腺癌(CRPC)。在CRPC组中,50-70%的患者会在骨骼的轴向和其他区域发展出骨转移。目前,一旦PCa细胞扩散到骨骼,就没有可用的治疗方法来根除转移,因此与癌症相关的死亡将不可避免。据估计,2012年美国将有28,170名PCa死亡。因此,PCa骨转移相关的临床并发症和治疗耐药性构成了主要的临床挑战。在这篇综述中,我们将介绍导致PCa骨转移的分子和细胞途径的最新发现。我们将着重介绍几种新颖的机制,重点是骨骼和骨髓微环境在促进PCa转移中的作用,并将进一步讨论为什么前列腺癌细胞优先转移到骨骼。此外,我们将讨论几种关键途径的新作用,包括骨髓和干细胞壁ches中的血管生成和细胞外基质重塑及其与PCa骨转移和不良治疗反应的关系。我们将评估各种化疗药物和放射疗法如何使侵略性PCa细胞获得有利的突变,从而导致存活率提高并使癌细胞对治疗产生抵抗力。将审查有关干细胞生态位和治疗抗性的几个关键的生存和入侵信号转导途径的新概念。最后,我们将提供针对转移癌微环境或生态位的几种新近开发的新型药物候选物的更新,并讨论这种治疗方法在克服耐药性和治疗晚期PCa方面的优势和意义。

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