mRECIST与iRECIST标准评价肝细胞癌免疫治疗疗效的对比研究
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1.中国人民解放军陆军军医大学第一附属医院 放射科,重庆 400038;2.中国人民解放军陆军军医大学第一附属医院 核医学科,重庆 400038;3.中国人民解放军陆军军医大学士官学校附属医院 烧伤整形科

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卢红,中国人民解放军陆军军医大学第一附属医院主治医师,主要从事腹部疾病影像诊断方面的研究。

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Comparison of mRECIST and iRECIST criteria in evaluating the efficacy of immunotherapy for hepatocellular carcinoma
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1.Department of Radiology, the First Affiliated Hospital of Army Medical University, Chongqing 400038, China;2.Department of Nuclear Medicine, the First Affiliated Hospital of Army Medical University, Chongqing 400038, China;3.Department of Burn and Plastic Surgery, the Affiliated Hospital of Sergeant School, Army Medical University, Shijiazhuang 050047, China

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    摘要:

    背景与目的 目前免疫治疗逐渐成为肝细胞癌(HCC)患者新的全身治疗方法之一,其治疗效果得到了临床肯定,但是其治疗效果的影像学评估方法仍在不断摸索中,并且影像学评估能有效为临床确定免疫新辅助治疗的主要临床终点提供充足的证据。本研究分析对比实体瘤免疫治疗疗效评价标准(iRECIST)和修订后实体瘤疗效评价标准(mRECIST)对HCC免疫治疗疗效的评价,以期找到更适合HCC免疫治疗疗效的影像学评估方法,便于临床医生制订个体化精准治疗方案。方法 回顾性分析2017—2021年间中国人民解放军陆军军医大学第一附属医院收治行PD-L1单抗免疫治疗HCC患者临床资料,其中男性58例,女性9例。CT或MRI动态增强扫描临床影像学资料包括治疗前1周内及治疗后2、4个月3个时间点。分别采用iRECIST和mRECIST标准进行疗效评估,对比检测两种疗效标准评估结果的差异。结果 PD-L1单抗免疫治疗后2、4个月复查,两种标准疗效评估结果差异有统计学意义(P<0.01);两种评估方法差异主要体现在客观缓解率(ORR),两次复查结果,mRECIST标准ORR所占比例均明显大于iRECIST标准的ORR所占比例,差异有统计学意义(P<0.01);大部分mRECIST标准评估为完全缓解或部分缓解的患者采用iRECIST标准评估为稳定;这两种不同的评估方法均有50%左右患者在初次评定为进展的情况下继续治疗而达到稳定状态或者部分缓解状态。结论 mRECIST标准测量时避开液化坏死区,以“存活肿瘤”对靶病灶进行疗效评价的方式更加客观、科学,避免因肿瘤大小变化不明显但肿瘤负荷明显减少而低估治疗效果。而iRECIST标准提出了未确认的疾病进展和确认的疾病进展的概念,更适用于免疫治疗过程中出现的假性进展等特有反应,故建议在采用mRECIST标准评估“存活肿瘤”的同时应该借鉴iRECIST标准的循环持续评估的模式,对使用mRECIST标准初次评估为进展的患者在进行下一周期治疗后再次评估,尽量避免轻易提前终止治疗,从而可能使更多的患者临床获益,对临床医生制定后续治疗方案也有一定的指导意义。

    Abstract:

    Background and Aims Immunotherapy is emerging as a new systemic treatment method for patients with hepatocellular carcinoma (HCC), with its clinically recognized therapeutic effects. However, imaging evaluation methods for assessing treatment response are still being explored. Imaging assessment is crucial in providing sufficient evidence for determining the primary clinical endpoints of immunotherapy in clinical practice. This study analyzes and compares the efficacy evaluation of immunotherapy in HCC using the Immune-Related Response Evaluation Criteria in Solid Tumors (iRECIST) and the modified Response Evaluation Criteria in Solid Tumors (mRECIST), aims to find a more suitable imaging assessment method for immunotherapy efficacy in HCC and facilitate the development of individualized and precise treatment plans by clinical physicians.Methods A retrospective analysis of clinical data from HCC patients who received PD-L1 monoclonal antibody immunotherapy at the First Affiliated Hospital of the Army Medical University from 2017 to 2021 was conducted. Of the patients, 58 were males, and 9 were females. Clinical imaging data from CT or MRI dynamic contrast-enhanced scans were collected at three time points: one week before treatment and two and four months after treatment initiation. The efficacy evaluations were performed using both iRECIST and mRECIST criteria, and the differences in the evaluation results between the two criteria were compared.Results Evaluation of immunotherapy efficacy using iRECIST and mRECIST criteria two and four months after PD-L1 monoclonal antibody treatment showed statistically significant differences (P<0.01). The main discrepancy between the two evaluation methods was observed in the objective response rate (ORR), with mRECIST showing a significantly higher ORR compared to iRECIST (P<0.01). Many patients who were classified as achieving complete or partial response using mRECIST were categorized as stable diseases according to iRECIST. Both evaluation methods indicated that approximately 50% of patients initially classified as progressive disease continued treatment and achieved stable or partial response status.Conclusion The mRECIST criteria, which measure "viable tumor" while excluding necrotic areas, provide a more objective and scientific approach to evaluate treatment efficacy. This approach prevents underestimation of treatment effects caused by significant tumor burden reduction despite minor changes in tumor size. On the other hand, iRECIST criteria propose concepts of unconfirmed and confirmed disease progression, making them more suitable for unique responses observed during immunotherapy, such as pseudo-progression. Therefore, it is recommended to adopt the mRECIST criteria for assessing "viable tumor" while considering the cyclic reevaluation model of iRECIST criteria to reassess patients initially classified as a progressive disease under mRECIST after the next treatment cycle to avoid premature treatment termination and potentially provide more clinical benefits to patients, as well as to offer guidance for clinicians to make subsequent treatment plans.

    表 1 治疗后2、4个月患者iRECIST标准与mRECIST标准评价结果[n(%)]Table 1 Evaluation of iRECIST and mRECIST criteria at 2 and 4 months after treatment [n (%)]
    图1 mRECIST标准CR与iRECIST标准iUPD病例 A:治疗前病灶长径约为9 mm,动脉期强化病灶长径9 mm;B:治疗后,病灶长径20 mm,但动脉期无异常强化,mRECIST标准评价为CR,iRECIST标准评价为iUPDFig.1 Case of CR determined by mRECIST criteria and iUPD determined by iRECIST criteria A: Before treatment, the lesions longest diameter was approximately 9 mm, and arterial phase enhancement showed a lesion with a longest diameter of 9 mm; B: After treatment, the lesions longest diameter increased to 20 mm, but there was no abnormal enhancement in the arterial phase, and the evaluation is classified as CR according to mRECIST criteria, whereas according to iRECIST criteria, the evaluation is classified as iUPD
    图2 mRECIST标准CR与iRECIST标准iSD病例 A:治疗前病灶长径约为13 mm,动脉期强化病灶长径8 mm;B:治疗后,病灶长径14 mm,但动脉期无异常强化,mRECIST标准评价为CR,iRECIST标准评价为iSDFig.2 Case of CR determined by mRECIST criteria and iSD determined by iRECIST criteria A: Before treatment, the lesions longest diameter was approximately 13 mm, and arterial phase enhancement showed a lesion with a longest diameter of 8 mm; B: After treatment, the lesions longest diameter increased to 14 mm, but there was no abnormal enhancement in the arterial phase, and the evaluation is classified as CR according to mRECIST criteria, whereas according to iRECIST criteria, the evaluation is classified as iSD
    图3 mRECIST标准PR与iRECIST标准iSD病例 A:治疗前病灶长径约为113 mm,动脉期强化病灶长径113 mm;B:治疗后,病灶长径114 mm,动脉期强化病灶长径约42 mm,mRECIST标准评价为PR,iRECIST标准评价为iSDFig.3 Case of PR determined by mRECIST criteria and iSD determined by iRECIST criteria A: Before treatment, the lesions longest diameter was approximately 113 mm, and arterial phase enhancement showed a lesion with a longest diameter of 113 mm; B: After treatment, the lesions longest diameter increased to 114 mm, but in the arterial phase, enhancement showed a lesion with a longest diameter of approximately 42 mm, and the evaluation is classified as PR according to mRECIST criteria, whereas according to iRECIST criteria, the evaluation is classified as iSD
    图4 mRECIST标准PD与iRECIST标准iUPD病例 A:治疗前病灶长径约为8 mm,动脉期强化病灶长径8 mm;B:治疗后,病灶长径17 mm,动脉期强化病灶长径约17 mm,mRECIST标准评价为PD,iRECIST标准评价为iUPDFig.4 Case of PD determined by mRECIST criteria and iUPD determined by iRECIST criteria A: Before treatment, the lesions longest diameter was approximately 8 mm, and arterial phase enhancement showed a lesion with a longest diameter of 8 mm; B: After treatment, the lesions longest diameter increased to 17 mm, and in the arterial phase, enhancement showed a lesion with a longest diameter of approximately 17 mm, and the evaluation is classified as PD according to mRECIST criteria, whereas according to iRECIST criteria, the evaluation is classified as iUPD
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卢红,陈伟,王健,吴宗乾,刘赫,胡晓飞,王田. mRECIST与iRECIST标准评价肝细胞癌免疫治疗疗效的对比研究[J].中国普通外科杂志,2023,32(7):1023-1031.
DOI:10.7659/j. issn.1005-6947.2023.07.007

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  • 收稿日期:2023-03-06
  • 最后修改日期:2023-05-16
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  • 在线发布日期: 2023-11-03