接受胰腺癌放化疗患者血液学毒性和化疗剂量强度的预测因素
Predictors of Hematologic Toxicity and Chemotherapy Dose Intensity in Patients Undergoing Chemoradiation for Pancreatic Cancer.
作者信息
Shaikh Talha, Wang Lora S, Egleston Brian, Burki Meher, Hoffman John P, Cohen Steven J, Meyer Joshua E
机构信息
Departments of Radiation Oncology.
Biostatistics.
出版信息
Am J Clin Oncol. 2018 Jan;41(1):59-64. doi: 10.1097/COC.0000000000000227.
OBJECTIVES
Intensity-modulated radiation therapy (IMRT) has been shown to decrease abdominal toxicity in patients undergoing chemoradiation (CRT) for pancreatic cancer. We evaluated whether IMRT impacts the rates of hematologic toxicity and chemotherapy dose intensity in patients undergoing CRT.
METHODS
We retrospectively reviewed patients with borderline resectable or locally advanced pancreatic cancer undergoing CRT between 2006 and 2012. Exclusion criteria included receipt of non-gemcitabine therapy, chemotherapy before CRT, or abnormal baseline hematologic indices. Endpoints included total gemcitabine dose received, dose intensity, unplanned dose reductions, and hematologic toxicity (WBC, ANC, platelet, and hemoglobin). Patient/treatment factors were evaluated for their relationship to the above endpoints during CRT and within the first 3 months post-CRT. Statistical analysis was performed using the Fisher exact test and regression models. Because of the multiple comparisons in the presented analysis, a false discovery rate adjustment was performed at the 5% false discovery rate level.
RESULTS
Eighty-five patients met the inclusion criteria. Fifty-eight (68.2%) patients received treatment with IMRT, and 27 (31.8%) patients were treated with 3D-conformal radiation. During CRT, there was no relationship between radiation technique and gemcitabine dose received, dose intensity, or hematologic grade 3+ toxicity. Post-CRT, there was no relationship between radiation technique and total gemcitabine dose received, dose intensity, or dose reduction. Patients receiving IMRT were more likely to have ANC grade 3+ toxicity (P=0.007) post-CRT, although this was no longer statistically significant after correction. There were no other relationships between treatment technique and hematologic toxicity.
CONCLUSIONS
IMRT technique may be associated with higher hematologic toxicity in patients undergoing CRT for pancreatic cancer. Given the expanding use of CRT, additional study is needed to identify the impact of IMRT on myelosuppression in these patients.
目的
调强放射治疗(IMRT)已被证明可降低接受胰腺癌放化疗(CRT)患者的腹部毒性。我们评估了IMRT对接受CRT患者血液学毒性发生率和化疗剂量强度的影响。
方法
我们回顾性分析了2006年至2012年间接受CRT的可切除边缘或局部晚期胰腺癌患者。排除标准包括接受非吉西他滨治疗、CRT前化疗或基线血液学指标异常。终点指标包括接受的吉西他滨总剂量、剂量强度、计划外剂量减少以及血液学毒性(白细胞、中性粒细胞绝对值、血小板和血红蛋白)。评估患者/治疗因素与CRT期间及CRT后前3个月内上述终点指标的关系。采用Fisher精确检验和回归模型进行统计分析。由于本分析中的多重比较,在5%的错误发现率水平上进行了错误发现率调整。
结果
85例患者符合纳入标准。58例(68.2%)患者接受IMRT治疗,27例(31.8%)患者接受三维适形放疗。在CRT期间,放疗技术与接受的吉西他滨剂量、剂量强度或血液学3级及以上毒性之间无相关性。CRT后,放疗技术与接受的吉西他滨总剂量、剂量强度或剂量减少之间无相关性。接受IMRT的患者在CRT后更有可能出现中性粒细胞绝对值3级及以上毒性(P = 0.007),尽管校正后这不再具有统计学意义。治疗技术与血液学毒性之间无其他相关性。
结论
IMRT技术可能与接受CRT的胰腺癌患者较高的血液学毒性相关。鉴于CRT的使用不断增加,需要进一步研究以确定IMRT对这些患者骨髓抑制的影响。
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