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γH2AX在接受顺铂和分次照射的肿瘤中的表达。

gammaH2AX expression in tumors exposed to cisplatin and fractionated irradiation.

作者信息

Bañuelos C Adriana, Banáth Judit P, Kim Joo-Young, Aquino-Parsons Christina, Olive Peggy L

机构信息

Medical Biophysics Department, British Columbia Cancer Research Centre, Vancouver, British Columbia, Canada.

出版信息

Clin Cancer Res. 2009 May 15;15(10):3344-53. doi: 10.1158/1078-0432.CCR-08-3114. Epub 2009 Apr 28.

Abstract

PURPOSE

Is retention of gammaH2AX foci useful as a biomarker for predicting the response of xenograft tumors to cisplatin with X-ray? Is a similar approach feasible using biopsies from patients with cervical cancer?

EXPERIMENTAL DESIGN

Mice bearing SiHa, WiDr, or HCT116 xenograft tumors were exposed to cisplatin and/or three daily doses of 2 Gy. Tumors were excised 24 h after treatment and single cells were analyzed for clonogenic fraction and retention of gammaH2AX foci. Tumor biopsies were examined using 47 paraffin-embedded sections from untreated tumors and 24 sections from 8 patients undergoing radiochemotherapy for advanced cancer of the cervix.

RESULTS

Residual gammaH2AX measured 24 h after cisplatin injection accurately predicted surviving fraction in SiHa and WiDr xenografts. When a clinically equivalent protocol using cisplatin and fractionated irradiation was employed, the fraction of xenograft cells lacking gammaH2AX ranked survival accurately but underestimated tumor cell kill. Residual gammaH2AX foci were detected in clinical samples; on average, only 25% of tumor nuclei exhibited one or more gammaH2AX foci before treatment and 74% after the start of treatment.

CONCLUSION

gammaH2AX can provide useful information on the response of human tumors to the combination of cisplatin and radiation, but prediction becomes less accurate as more time elapses between treatment and tumor biopsy. Use of residual gammaH2AX as a biomarker for response is feasible when cell survival exceeds approximately 20%, but heterogeneity in endogenous and treatment-induced gammaH2AX must be considered.

摘要

目的

γH2AX 灶的保留能否作为预测异种移植肿瘤对顺铂联合 X 射线反应的生物标志物?对于宫颈癌患者的活检样本,采用类似方法是否可行?

实验设计

将携带 SiHa、WiDr 或 HCT116 异种移植肿瘤的小鼠暴露于顺铂和/或每日 3 次、每次 2 Gy 的辐射下。治疗后 24 小时切除肿瘤,对单细胞进行克隆形成率和 γH2AX 灶保留情况分析。使用来自未经治疗肿瘤的 47 个石蜡包埋切片以及来自 8 例晚期宫颈癌接受放化疗患者的 24 个切片对肿瘤活检样本进行检查。

结果

顺铂注射后 24 小时测得的残余 γH2AX 准确预测了 SiHa 和 WiDr 异种移植瘤的存活分数。当采用临床等效的顺铂联合分次照射方案时,缺乏 γH2AX 的异种移植细胞分数能准确排列存活情况,但低估了肿瘤细胞杀伤效果。在临床样本中检测到残余 γH2AX 灶;平均而言,治疗前仅 25%的肿瘤细胞核显示一个或多个 γH2AX 灶,治疗开始后为 74%。

结论

γH2AX 可提供有关人类肿瘤对顺铂与放疗联合反应的有用信息,但随着治疗与肿瘤活检之间时间间隔的延长,预测准确性会降低。当细胞存活率超过约 20%时,将残余 γH2AX 用作反应生物标志物是可行的,但必须考虑内源性和治疗诱导的 γH2AX 的异质性。

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