评估癌症合并胶原血管疾病患者接受分次放射治疗的毒性效应。
Assessment of Toxic Effects Associated With Dose-Fractionated Radiotherapy Among Patients With Cancer and Comorbid Collagen Vascular Disease.
机构信息
Department of Radiation Oncology, University of California, Los Angeles, Los Angeles.
Department of Radiation Oncology, MD Anderson Cancer Center, University of Texas, Houston.
出版信息
JAMA Netw Open. 2021 Feb 1;4(2):e2034074. doi: 10.1001/jamanetworkopen.2020.34074.
IMPORTANCE
The adoption of alternative fractionated radiotherapy regimens for the treatment of patients with cancer and comorbid collagen vascular disease (CVD) is controversial among oncologists because of concerns about potentially severe toxic effects; however, the association between fractionated radiotherapy and toxic effects in the modern era has not been well studied.
OBJECTIVE
To compare acute and late toxic effects among patients with cancer and comorbid CVD who received dose-fractionated radiotherapy.
DESIGN, SETTING, AND PARTICIPANTS: This retrospective cohort study examined 197 adult patients with cancer and CVD who received radiotherapy at a single-institution tertiary academic center over a 12-year period (February 1, 2007, to April 30, 2019), with a median follow-up of 23 months (range, 0-108 months). Data were analyzed from February 1 to August 31, 2020.
EXPOSURES
Three dose-fractionated radiotherapy regimens: conventional fractionation (CF; ≤2 Gy per fraction), moderate hypofractionation (MH; >2 Gy to <5 Gy per fraction), and ultrahypofractionation (UH; ≥5 Gy per fraction).
MAIN OUTCOMES AND MEASURES
The main outcomes were the incidence and severity of acute and late radiotherapy-associated toxic effects, which were assessed separately by dose-fractionation regimen. Toxic effects occurring within 90 days after radiotherapy completion were considered acute, and toxic effects occurring after that 90-day period were considered late. Secondary goals were to identify covariates associated with toxic effects and to characterize the incidence of CVD symptom flares (defined as worsening clinical symptoms and/or worsening results [transient or permanent] on associated blood tests compared with baseline, as documented by managing physicians) after radiotherapy.
RESULTS
Of 197 patients with cancer and comorbid CVD (mean [SD] age, 69 [12] years; 134 women [68.0%]; and 149 White participants [75.6%]), 80 patients (40.6%) received CF radiotherapy, 55 patients (27.9%) received MH radiotherapy, and 62 patients (31.5%) received UH radiotherapy. The most common CVD diagnoses were rheumatoid arthritis (74 patients [37.6%]), psoriasis (54 patients [27.4%]), systemic lupus erythematosus (34 patients [17.3%]), and scleroderma (8 patients [4.1%]). The most common radiotherapy sites were the breast (48 patients [24.4%]), thorax (25 patients [12.7%]), central nervous system (24 patients [12.2%]), and prostate (23 patients [11.7%]). Data on acute toxic effects were available for 188 patients (95.4%) and missing for 9 patients (4.6%). Data on late toxic effects were available for 142 patients (72.1%) and missing for 55 patients (27.9%). Over 12 years, the unadjusted incidences of severe acute toxic effects associated with CF, MH, and UH radiotherapy were 5.4% (95% CI, 0.3%-10.5%), 7.4% (95% CI, 0.4%-14.4%), and 1.7% (95% CI, 0%-5.0%), respectively. The incidences of severe late toxic effects associated with CF, MH, and UH radiotherapy were 8.3% (95% CI, 1.3%-15.3%), 0%, and 2.2% (95% CI, 0%-6.4%), respectively. No significant associations were found between severe acute or late toxic effects by dose fractionation regimen. In the multivariable analysis, MH radiotherapy was associated with a lower likelihood of developing late toxic effects (odds ratio [OR], 0.21; 95% CI, 0.05-0.83; P = .03) compared with CF radiotherapy. Those who received UH radiotherapy had a lower likelihood of experiencing late toxic effects (OR, 0.22; 95% CI, 0.04-1.21; P = .08). A total of 19 of 80 patients (23.8%), 15 of 55 patients (27.3%), and 10 of 62 patients (16.1%) experienced CVD symptom flares after receiving CF, MH, and UH radiotherapy, respectively (P = .33).
CONCLUSIONS AND RELEVANCE
In this study, the incidences of unadjusted severe toxic effects over 12 years were less than 10% and were not significantly associated with dose fractionation. When clinically indicated, patients with cancer and comorbid CVD may not require immediate exclusion from the receipt of currently used hypofractionated radiotherapy regimens.
重要性
由于担心潜在的严重毒性作用,肿瘤科医生对接受癌症合并胶原血管疾病 (CVD) 患者的替代分割放疗方案的采用存在争议;然而,在现代,关于分割放疗与毒性作用之间的关联尚未得到很好的研究。
目的
比较患有 CVD 的癌症患者接受剂量分割放疗后的急性和迟发性毒性作用。
设计、设置和参与者:这项回顾性队列研究调查了在一家单机构三级学术中心接受放疗的 197 名成年癌症合并 CVD 患者,研究时间为 12 年(2007 年 2 月 1 日至 2019 年 4 月 30 日),中位随访时间为 23 个月(范围,0-108 个月)。数据于 2020 年 2 月 1 日至 8 月 31 日进行分析。
暴露情况
三种剂量分割放疗方案:常规分割(CF;每分次≤2 Gy)、中度超分割(MH;每分次>2 Gy 至<5 Gy)和超超分割(UH;每分次≥5 Gy)。
主要结局和测量
主要结局是急性和迟发性放疗相关毒性作用的发生率和严重程度,分别根据剂量分割方案进行评估。放疗完成后 90 天内发生的毒性作用被认为是急性的,而在此 90 天之后发生的毒性作用被认为是迟发性的。次要目标是确定与毒性作用相关的协变量,并描述放疗后 CVD 症状恶化(定义为与基线相比,临床症状恶化和/或相关血液检查结果恶化[暂时或永久性],由主治医生记录)的发生率。
结果
在 197 名患有癌症合并 CVD 的患者中(平均[SD]年龄,69[12]岁;134 名女性[68.0%];149 名白人患者[75.6%]),80 名患者(40.6%)接受 CF 放疗,55 名患者(27.9%)接受 MH 放疗,62 名患者(31.5%)接受 UH 放疗。最常见的 CVD 诊断是类风湿关节炎(74 名患者[37.6%])、银屑病(54 名患者[27.4%])、系统性红斑狼疮(34 名患者[17.3%])和硬皮病(8 名患者[4.1%])。最常见的放疗部位是乳房(48 名患者[24.4%])、胸部(25 名患者[12.7%])、中枢神经系统(24 名患者[12.2%])和前列腺(23 名患者[11.7%])。188 名患者(95.4%)有急性毒性作用数据,9 名患者(4.6%)缺失。142 名患者(72.1%)有迟发性毒性作用数据,55 名患者(27.9%)缺失。在 12 年期间,CF、MH 和 UH 放疗相关严重急性毒性作用的未调整发生率分别为 5.4%(95%CI,0.3%-10.5%)、7.4%(95%CI,0.4%-14.4%)和 1.7%(95%CI,0%-5.0%)。CF、MH 和 UH 放疗相关严重迟发性毒性作用的发生率分别为 8.3%(95%CI,1.3%-15.3%)、0%和 2.2%(95%CI,0%-6.4%)。剂量分割方案与严重急性或迟发性毒性作用之间无显著关联。在多变量分析中,MH 放疗与 CF 放疗相比,发生迟发性毒性作用的可能性较低(比值比[OR],0.21;95%CI,0.05-0.83;P=0.03)。接受 UH 放疗的患者发生迟发性毒性作用的可能性较低(OR,0.22;95%CI,0.04-1.21;P=0.08)。80 名患者中有 19 名(23.8%)、55 名患者中有 15 名(27.3%)、62 名患者中有 10 名(16.1%)在接受 CF、MH 和 UH 放疗后出现 CVD 症状恶化(P=0.33)。
结论和相关性
在这项研究中,12 年内未调整的严重毒性作用发生率低于 10%,且与剂量分割无关。在临床上有指征时,患有癌症合并 CVD 的患者可能不需要立即排除在目前使用的低分割放疗方案之外。
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