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正常组织反应的预测标志物:幻想还是现实?

Predictive markers for normal tissue reactions: fantasy or reality?

作者信息

Fernet M, Hall J

机构信息

Institut Curie-recherche, centre universitaire, bâtiments 110-112, 91405 Orsay, France.

出版信息

Cancer Radiother. 2008 Nov;12(6-7):614-8. doi: 10.1016/j.canrad.2008.07.013. Epub 2008 Aug 26.

Abstract

Interpatient heterogeneity in normal tissue reactions varies considerably, yet the genetic determinants and the molecular mechanisms of therapeutic radiation sensitivity remain poorly understood. Predictive assays and markers for normal tissue reactions are still in their infancy, although some progress has been made, particularly, for predicting late toxicity. For instance the T-lymphocyte radiation-induced apoptosis assay was shown to significantly predict differences in late toxicity between individuals and an 18 gene classifier based on radiation-induced expression in subcutaneous fibroblasts has also been identified that differentiated between patients with a high and low risk of radiation-induced fibrosis. However, the technical set-up for gene expression measurements means that this latter assay is unlikely to be introduced soon into a routine clinical setting but has importantly allowed the identification of genes that are involved in the fibrotic process. Serum markers have also been identified that show potential for the prediction of patients who will develop acute and late pulmonary toxicity. Few genetic predictive markers for normal tissue reaction have been identified and validated. Many of the single nucleotide polymorphism association studies have been limited by size and the inclusion of subjects with different kinds of radiation morbidity. International collaboration to assemble well-defined cohorts and technological progress should mean that the identification and validation of such markers using candidate gene approaches and whole genome association studies, which have been successful in other research areas, will make rapid progress.

摘要

正常组织反应的患者间异质性差异很大,但治疗性放射敏感性的遗传决定因素和分子机制仍知之甚少。尽管已经取得了一些进展,特别是在预测晚期毒性方面,但正常组织反应的预测分析和标志物仍处于起步阶段。例如,T淋巴细胞辐射诱导凋亡试验被证明能显著预测个体间晚期毒性的差异,并且还确定了一种基于皮下成纤维细胞辐射诱导表达的18基因分类器,该分类器能够区分辐射诱导纤维化风险高和低的患者。然而,基因表达测量的技术设置意味着后一种试验不太可能很快应用于常规临床环境,但它重要地使得能够识别参与纤维化过程的基因。还确定了血清标志物,这些标志物显示出预测将发生急性和晚期肺毒性患者的潜力。很少有正常组织反应的遗传预测标志物被识别和验证。许多单核苷酸多态性关联研究受到样本量的限制,并且纳入了患有不同类型辐射发病率的受试者。通过国际合作来组建明确的队列以及技术进步,应该意味着使用候选基因方法和全基因组关联研究来识别和验证此类标志物将取得快速进展,而这些方法在其他研究领域已经取得了成功。

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