Ruiz Department of Ophthalmology and Visual Science, The University of Texas Health Science Center at Houston, Houston.
Retina Consultants of Texas, Houston.
JAMA Ophthalmol. 2023 Dec 1;141(12):1133-1138. doi: 10.1001/jamaophthalmol.2023.4825.
Intra-arterial chemotherapy (IAC) has quickly gained popularity as a mainstay of treatment for retinoblastoma. Intra-arterial chemotherapy has been described as having several advantages over systemic chemotherapy, including reducing systemic toxicity and neutropenia; however, studies on the risk of neutropenia after IAC remain limited.
To estimate the incidence of neutropenia after IAC, as well as identify risk factors associated with the development of neutropenia.
DESIGN, SETTING, AND PARTICIPANTS: This case series included pediatric patients with unilateral or bilateral retinoblastoma who were treated with IAC at a single quaternary care center from July 13, 2013, to January 6, 2023.
All patients were treated with IAC and underwent multiple IAC cycles depending on treatment response. The primary chemotherapy agent used was melphalan, but topotecan or carboplatin could be used along with melphalan. Melphalan doses were kept to 0.4 mg/kg or less per cycle. After each IAC cycle, complete blood cell counts were obtained within 10 to 12 days and repeated until the absolute neutrophil count (ANC) was greater than or equal to 1000/μL.
The primary outcome was the minimum ANC after each IAC cycle. The secondary outcome was the development of severe (grade 3 or 4) neutropenia (ANC <1000/μL). Regression analyses were used to identify associations between variables and outcomes. Receiver operating characteristic curves were used to calculate threshold dose for each chemotherapy agent potentially associated with the development of severe neutropenia.
A total of 64 eyes of 49 patients (mean [SD] age, 1.7 [1.2] years; 25 females [51.0%]) with retinoblastoma were treated with 171 cycles of IAC. The mean (SD) nadir ANC was 1325.3 (890.7)/μL and occurred a median (IQR) of 10 (10-14) days (range, 6-28 days) after IAC administration. The frequency distribution of post-IAC neutropenia grades 0, 1, 2, 3, 4, and missing was 31 (18.1% of cycles), 25 (14.6%), 40 (23.4%), 37 (21.6%), 26 (15.2%), and 12 (7.0%), respectively. Factors weakly correlated with a lower ANC were higher melphalan dose (β = -2356 [95% CI, -4120.6 to -611.2]; adjusted R2 = 0.251; P = .01) and higher topotecan dose (β = -4056 [95% CI, -7003.6 to -1344.5]; adjusted R2 = 0.251; P = .006).
In this case series of patients with retinoblastoma, the incidence of severe neutropenia after IAC was nearly 40%, which is higher than previously reported. Extended laboratory monitoring may aid in capturing previously overlooked cases of neutropenia. Topotecan may be associated with the development of neutropenia; limiting topotecan doses, especially in the setting of a high melphalan dose, may be beneficial in reducing the risk of neutropenia.
背景:
局部动脉内化疗(IAC)作为治疗视网膜母细胞瘤的主要方法迅速流行起来。与全身化疗相比,IAC 具有减少全身毒性和中性粒细胞减少的优势;然而,关于 IAC 后中性粒细胞减少风险的研究仍然有限。
目的:
评估 IAC 后中性粒细胞减少的发生率,并确定与中性粒细胞减少发展相关的风险因素。
设计:
这是一项病例系列研究,纳入了在一家四级护理中心接受 IAC 治疗的单侧或双侧视网膜母细胞瘤的儿科患者。
患者:
该研究纳入了从 2013 年 7 月 13 日至 2023 年 1 月 6 日在一家单中心接受 IAC 治疗的患者。
干预措施:
所有患者均接受 IAC 治疗,并根据治疗反应进行多次 IAC 周期。主要化疗药物为美法仑,但也可以与美法仑联合使用拓扑替康或卡铂。每个周期的美法仑剂量保持在 0.4mg/kg 或以下。每次 IAC 后 10 至 12 天内获得全血细胞计数,并重复检查直至绝对中性粒细胞计数(ANC)大于或等于 1000/μL。
主要结局和测量指标:
主要结局是每个 IAC 周期后的最低 ANC。次要结局是严重(3 级或 4 级)中性粒细胞减少症(ANC <1000/μL)的发生。回归分析用于确定变量与结局之间的关联。接收者操作特征曲线用于计算每个可能与严重中性粒细胞减少症发生相关的化疗药物的阈值剂量。
结果:
该研究共纳入了 49 例患者(平均年龄 1.7[1.2]岁;女性 25 例[51.0%])的 64 只眼,接受了 171 个 IAC 周期的治疗。平均(标准差)最低 ANC 为 1325.3(890.7)/μL,中位数(IQR)发生于 IAC 给药后 10(10-14)天(范围 6-28 天)。IAC 后中性粒细胞减少症分级 0、1、2、3、4 和缺失的频率分布分别为 31 次(占周期的 18.1%)、25 次(14.6%)、40 次(23.4%)、37 次(21.6%)、26 次(15.2%)和 12 次(7.0%)。与较低 ANC 相关的因素包括美法仑剂量较高(β=-2356[95%CI,-4120.6 至-611.2];调整后的 R2=0.251;P=0.01)和拓扑替康剂量较高(β=-4056[95%CI,-7003.6 至-1344.5];调整后的 R2=0.251;P=0.006)。
结论:
在这项视网膜母细胞瘤患者的病例系列研究中,IAC 后严重中性粒细胞减少症的发生率接近 40%,高于之前的报告。延长实验室监测可能有助于发现以前被忽视的中性粒细胞减少症病例。拓扑替康可能与中性粒细胞减少症的发生有关;限制拓扑替康剂量,特别是在高美法仑剂量的情况下,可能有助于降低中性粒细胞减少症的风险。
