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骨肉瘤治疗的未来方向。

Future directions in the treatment of osteosarcoma.

作者信息

Bishop Michael W, Janeway Katherine A, Gorlick Richard

机构信息

aDepartment of Oncology, St. Jude Children's Research Hospital bDepartment of Pediatrics, University of Tennessee Health Science Center, Memphis, Tennessee cDana-Farber Cancer Institute, Boston, Massachusetts dDivision of Pediatric Hematology/Oncology, The Children's Hospital At Montefiore, Bronx, New York, USA.

出版信息

Curr Opin Pediatr. 2016 Feb;28(1):26-33. doi: 10.1097/MOP.0000000000000298.

Abstract

PURPOSE OF REVIEW

Overall survival rates for osteosarcoma have remained essentially unchanged over the past 3 decades despite attempts to improve outcome via dose intensification and modification based on response. This review describes recent findings from contemporary clinical trials, advances in the comprehension of osteosarcoma biology and genomic complexity, and potential opportunities using targeted and immune-mediated therapies.

RECENT FINDINGS

Recent results from international collaborative trials have failed to demonstrate an ability to improve outcomes using a design in which the randomized question is dictated based on histologic response to preoperative chemotherapy. Novel prognostic markers assessable at diagnosis are vital to identifying subsets of osteosarcoma. Clinical trials focus has now shifted to serial phase II studies of novel agents to evaluate for activity in recurrent and refractory disease. In-depth analyses have revealed profound genomic instability and heterogeneity across patients, with nearly universal TP53 aberration. Although driver mutational events have not clearly been established, frequent derangements in specific pathways may suggest opportunities for therapeutic exploitation. Genomic complexity may lend support to a role for immune-mediated therapies.

SUMMARY

Rigorous preclinical investigations are potentially generating novel strategies for the treatment of osteosarcoma that will inform the next generation of clinical trials, with the opportunity to identify agents that will improve survival outcomes.

摘要

综述目的

尽管过去三十年来一直试图通过强化剂量和根据反应进行调整来改善骨肉瘤的治疗结果,但其总体生存率基本保持不变。本综述描述了当代临床试验的最新发现、对骨肉瘤生物学和基因组复杂性理解的进展以及使用靶向治疗和免疫介导治疗的潜在机会。

最新发现

国际协作试验的近期结果未能证明,采用根据术前化疗的组织学反应来确定随机问题的设计能够改善治疗结果。诊断时可评估的新型预后标志物对于识别骨肉瘤亚组至关重要。目前临床试验的重点已转向对新型药物的系列II期研究,以评估其在复发和难治性疾病中的活性。深入分析揭示了患者之间存在深刻的基因组不稳定性和异质性,几乎普遍存在TP53畸变。虽然尚未明确确定驱动突变事件,但特定途径中的频繁紊乱可能提示有治疗利用的机会。基因组复杂性可能支持免疫介导治疗的作用。

总结

严格的临床前研究可能正在产生治疗骨肉瘤的新策略,这将为下一代临床试验提供信息,并有机会识别出能够改善生存结果的药物。

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