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Clinically relevant biomarkers in targeted radiotherapy

机译:靶向放射治疗中的临床相关生物标志物

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Three classic parameters have been recognized as predictors or biomarkers of radiation response: intrinsic radiosensitivity, degree of hypoxia and repopulation capacity of clonogenic cells during a course of fractionated radiation therapy. Although good functional assays exist to measure these tumor parameters, and their use has led to the understanding of factors affecting outcome after radiotherapy, their application in clinical practice is hampered by technical difficulties, the length of time needed to obtain results and the lack of prospective randomized clinical trials. Recently, with the progress in molecular biology, genome-wide screening methods have been used to look for genetic signatures that can distinguish between good and bad outcome after radiotherapy. One of the most promising candidates is the epidermal growth factor receptor which is overexpressed or mutated in a variety of malignancies, such lung and head and neck cancer. Inhibition of this receptor has led to radio-sensitization with the prolongation of median survival in several cancers. Since there is significant variability in the response of patients with the same disease to radiotherapy, it would be very valuable to be able to predict which patients would benefit from a molecularly targeted therapy administered with concomitant radiation in order to increase the response rate (and cure rate) of those patients with radioresistant tumors. Optimally, this assay should be able to provide results in an efficient and reproducible manner and detect tumor genetic mutations that would provide specificity to the intervention. One approach currently in clinical practice to overcome intrinsic radioresistance and repopulation is stereotactic body radiotherapy coupled with image-guided radiation, a highly precise and powerful form of radiation, allowing radiation oncologist to treat tumors with more aggressive biological doses of radiation without causing serious normal tissues injury.
机译:三个经典参数已被公认是放射反应的预测指标或生物标记:固有放射敏感性,缺氧程度和分次放疗过程中克隆细胞的再填充能力。尽管存在良好的功能测定方法来测量这些肿瘤参数,并且它们的使用引起了对放疗后影响预后的因素的了解,但它们在临床实践中的应用受到技术难题,获得结果所需时间的长短以及缺乏前瞻性的阻碍随机临床试验。最近,随着分子生物学的进步,全基因组筛选方法已用于寻找可以区分放疗后好与坏结果的遗传特征。最有前途的候选者之一是表皮生长因子受体,它在多种恶性肿瘤(例如肺癌和头颈癌)中过表达或突变。抑制该受体已导致放射致敏作用,延长了几种癌症的中位生存期。由于相同疾病的患者对放疗的反应存在显着差异,因此能够预测哪些患者将从伴随放疗的分子靶向治疗中受益,从而提高缓解率(并治愈),将非常有价值。率的那些患者。最佳地,该测定法应该能够以有效且可再现的方式提供结果,并检测将为干预提供特异性的肿瘤遗传突变。目前,临床实践中克服固有放射线抵抗力和人口繁殖的一种方法是立体定向身体放射疗法与图像引导的放射线结合,影像引导放射线是一种高度精确且强大的放射线形式,允许放射线肿瘤学家以更具侵略性的生物剂量放射线治疗肿瘤,而不会引起严重的正常组织受伤。

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