The use of whole exome sequencing and murine patient derived xenografts as a method of chemosensitivity testing in sarcoma.

Clinical Sarcoma Research Pub Date : 2018-03-08 eCollection Date: 2018-01-01 DOI:10.1186/s13569-018-0090-1
Nicholas Calvert, Jiansha Wu, Sophie Sneddon, Jennifer Woodhouse, Richard Carey-Smith, David Wood, Evan Ingley
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引用次数: 4

Abstract

Background: Soft tissue and bone sarcoma represent a broad spectrum of different pathology and genetic variance. Current chemotherapy regimens are derived from randomised trials and represent empirical treatment. Chemosensitivity testing and whole exome sequencing (WES) may offer personalized chemotherapy treatment based on genetic mutations.

Methods: A pilot, prospective, non-randomised control experimental study was conducted. Twelve patients with metastatic bone or soft tissue sarcoma that had failed first line chemotherapy treatment were enrolled for this study. Human tissue taken at surgical biopsy under general anaesthetic was divided between two arms of the trial. Subsections of the tumour were used for WES and the remainder was implanted subcutaneously in immunodeficient mice (PDX). Results of WES were analysed using a bioinformatics pipeline to identify mutations conferring susceptibility to kinase inhibitors and common chemotherapeutic agents. PDX models exhibiting successful growth underwent WES of the tumour and subsequent chemosensitivity testing.

Results: WES was successful in all 12 patients, with successful establishment PDX tumours models in seven patients. WES identified potential actionable therapeutics in all patients. Significant variation in predicted therapeutics was demonstrated between three PDX samples and their matched tumour samples.

Conclusion: Analysis of WES of fresh tumour specimens via a bioinformatics pipeline may identify potential actionable chemotherapy agents. Further research into this field may lead to the development of personalized cancer therapy for sarcoma.

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使用全外显子组测序和小鼠患者来源的异种移植物作为肉瘤化疗敏感性测试的方法。
背景:软组织和骨肉瘤表现出广泛的不同病理和遗传变异。目前的化疗方案来自随机试验,代表经验性治疗。化疗敏感性测试和全外显子组测序(WES)可以提供基于基因突变的个性化化疗治疗。方法:采用前瞻性、非随机对照试验研究。12例在一线化疗失败的转移性骨或软组织肉瘤患者参加了这项研究。在全身麻醉下,在手术活检中采集的人体组织被分为两组。肿瘤切片用于WES,其余部分皮下植入免疫缺陷小鼠(PDX)。使用生物信息学管道对WES结果进行分析,以确定对激酶抑制剂和常见化疗药物易感性的突变。显示成功生长的PDX模型进行肿瘤WES和随后的化学敏感性测试。结果:12例患者WES均成功,7例患者成功建立PDX肿瘤模型。WES在所有患者中确定了潜在的可行治疗方法。在三个PDX样本及其匹配的肿瘤样本之间证明了预测治疗方法的显着差异。结论:通过生物信息学管道对新鲜肿瘤标本的WES进行分析,可以确定潜在可行的化疗药物。对这一领域的进一步研究可能会导致针对肉瘤的个性化癌症治疗的发展。
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期刊介绍: Clinical Sarcoma Research considers for publication articles related to research on sarcomas, including both soft tissue and bone. The journal publishes original articles and review articles on the diagnosis and treatment of sarcomas along with new insights in sarcoma research, which may be of immediate or future interest for diagnosis and treatment. The journal also considers negative results, especially those from studies on new agents, as it is vital for the medical community to learn whether new agents have been proven effective or ineffective within subtypes of sarcomas. The journal also aims to offer a forum for active discussion on topics of major interest for the sarcoma community, which may be related to both research results and methodological topics.
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