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分割随访化疗可延迟骨转移性前列腺癌耐药性的出现。

Fractionated follow-up chemotherapy delays the onset of resistance in bone metastatic prostate cancer.

作者信息

Warman Pranav I, Kaznatcheev Artem, Araujo Arturo, Lynch Conor C, Basanta David

机构信息

Duke University, Durham, NC, USA.

Integrated Mathematical Oncology, H. Lee Moffitt Cancer Center and Research Institute, Tampa, FL, USA.

出版信息

Games (Basel). 2018 Jun;9(2). doi: 10.3390/g9020019. Epub 2018 Apr 23.

Abstract

Prostate cancer to bone metastases are almost always lethal. This results from the ability of metastatic prostate cancer cells to co-opt bone remodeling leading to what is known as the . Understanding how tumor cells can disrupt bone homeostasis through their interactions with the stroma and how metastatic tumors respond to treatment is key to the development of new treatments for what remains an incurable disease. Here we describe an evolutionary game theoretical model of both the homeostatic bone remodeling and its co-option by prostate cancer metastases. This model extends past the evolutionary aspects typically considered in game theoretical models by also including ecological factors such as the physical microenvironment of the bone. Our model recapitulates the current paradigm of the "vicious cycle" driving tumor growth and sheds light on the interactions of heterogeneous tumor cells with the bone microenvironment and treatment response. Our results show that resistant populations naturally become dominant in the metastases under conventional cytotoxic treatment and that novel schedules could be used to better control the tumor and the associated bone disease compared to the current standard of care. Specifically, we introduce fractionated follow up therapy - chemotherapy where dosage is administered initially in one solid block followed by alternating smaller doeses and holidays - and argue that it is better than either a continuous application or a periodic one. Furthermore, we also show that different regimens of chemotherapy can lead to different amounts of pathological bone that are known to correlate with poor quality of life for bone metastatic prostate cancer patients.

摘要

前列腺癌发生骨转移几乎总是致命的。这是由于转移性前列腺癌细胞能够操控骨重塑,从而导致所谓的……了解肿瘤细胞如何通过与基质的相互作用破坏骨稳态,以及转移性肿瘤如何对治疗作出反应,是开发针对这种仍无法治愈疾病的新疗法的关键。在此,我们描述了一个关于骨稳态重塑及其被前列腺癌转移灶利用的进化博弈理论模型。该模型超越了博弈理论模型中通常考虑的进化方面,还纳入了诸如骨的物理微环境等生态因素。我们的模型概括了驱动肿瘤生长的“恶性循环”的当前范式,并揭示了异质性肿瘤细胞与骨微环境及治疗反应之间的相互作用。我们的结果表明,在传统细胞毒性治疗下,耐药群体在转移灶中自然占据主导地位,与当前的标准治疗相比,新的治疗方案可用于更好地控制肿瘤及相关骨疾病。具体而言,我们引入了分次后续治疗——化疗,即剂量先一次性给予一大块,然后交替给予较小剂量并设置间隔期——并认为这比持续应用或定期应用更好。此外,我们还表明,不同的化疗方案会导致不同量的病理性骨,而这已知与骨转移性前列腺癌患者的生活质量差相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f343/7864372/a6c7215feb82/nihms-1665907-f0001.jpg

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