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新辅助治疗治疗鳞状食管癌的反应-代谢反应与组织病理学的相关性。

Treatment Response to Neoadjuvant Therapy in Squamous Esophageal Cancer-Correlation Between Metabolic Response and Histopathology.

机构信息

Department of Surgical Oncology, Tata Memorial Hospital, Mumbai, India.

Thoracic Surgery, Department of Surgical Oncology, Tata Memorial Centre, Homi Bhabha National Institute, Mumbai, India.

出版信息

J Gastrointest Cancer. 2024 Jun;55(2):820-828. doi: 10.1007/s12029-024-01013-x. Epub 2024 Feb 3.

Abstract

PURPOSE

Esophageal cancer is among the leading causes of cancer-related mortality worldwide. Patients presenting with localized and loco-regionally advanced cancer without distant metastases have reasonable survival with multimodality management. Adequate and comprehensive staging is the backbone for proper selection of patients fit for curative treatment. Positron emission tomography (PET) in combination with contrast-enhanced computed tomography (CECT) is utilized as the standard staging modality. Multimodality treatment has been able to achieve evaluable tumor responses including pathological complete response (pCR). It is, therefore, necessary to understand whether the impact of neoadjuvant therapy can be evaluated on imaging, i.e., standardized uptake value (SUV) on PET scan done for response assessment and if this can be correlated with histopathological response and later, with survival. Squamous cell carcinoma (SCC) is more common globally and in the Indian subcontinent; hence, we chose this subgroup to evaluate our hypothesis.

METHODS

This is a single institution, retrospective study. Out of the 1967 patients who were treated between 2009 and 2019, 1369 (78.54%) patients had SCC. Out of these, 44 received NACTRT, whereas 1325 received NACT followed by curative surgery. The standardized uptake value (SUV) of 18-fluorodeoxyglucose was recorded during pre- and post-neoadjuvant treatment (NAT) using positron emission tomography (PET). The histopathology of the final resection specimen was evaluated using the Mandard tumor regression grade (TRG) criteria with response being graded from 0 to 5 as no residual tumor (NRT), scanty residual tumor (SRT), and residual tumor We attempted to find a cut-off value of the post neoadjuvant SUV of the primary tumor site which correlated with achievement of better histopathological response.

RESULTS

Out of 1325 patients of SCC esophagus who underwent surgery, 943 patients had available data of TRG, and it was categorized into the 0-2 category which had 325 patients (34.5%) and 3-5 category, 618 patients (65.5%). The SUV was taken only from the PET scans done at our institution, so as to achieve a more homogenous cohort, and this was available for 186 patients, 151 from the NACT group and 35 from the NACTRT group. The ROC method was used to find the cut-off for SUV (5.05) in the NACT cohort, which depicted significant difference in the outcome. Out of these, 93 patients who underwent NACT had SUV > 5.05 and 58 had SUV < 5.05. It was found that the subjective and objective histopathological scores correlated at a p value of < 0.0001. Specifically, the majority of cases with SRT tended to be in the 3-5 category of TRG, whereas cases with NRT are predominantly in the 0-2 category. In the ≥ 5.05 category of SUV, there were 76 cases with SRT. In the NACT cohort, the < 5.05 category of SUV, there are 26 cases with SRT and 32 cases with NRT. Among cases with SRT, 74.5% had SUV ≥ 5.05, while 25.5% had SUV < 5.05. Among cases with NRT, 34.7% had SUV ≥ 5.05, while 65.3% had SUV < 5.05 (p value 0.007). No significant association was found in the radio-pathological correlation in the NACTRT group.

CONCLUSION

Our study confirms the correlation of post neoadjuvant chemotherapy PET SUV with histopathological response, the cut-off of SUV being 5.05 in our cohort. This confirms the predictive value of FDG PET as demonstrated in other studies. Furthermore, its prognostic value with respect to survival has been verified in multiple other studies. With larger scale randomized studies, we may be able to identify the group of patients who have borderline operability anatomically as well as physiologically, where alternative treatment regimens may be indicated to improve outcomes.

摘要

目的

食管癌是全球癌症相关死亡的主要原因之一。对于没有远处转移的局部和局部晚期癌症患者,如果采用多模式管理,其生存时间较长。充分和全面的分期是选择适合治愈性治疗的患者的基础。正电子发射断层扫描(PET)联合对比增强计算机断层扫描(CECT)被用作标准分期方式。多模式治疗已能够实现可评估的肿瘤反应,包括病理完全缓解(pCR)。因此,有必要了解新辅助治疗的影响是否可以在影像学上进行评估,即用于反应评估的 PET 扫描的标准化摄取值(SUV),以及这种评估是否可以与组织病理学反应相关,进而与生存相关。鳞状细胞癌(SCC)在全球和印度次大陆更为常见;因此,我们选择了这个亚组来验证我们的假设。

方法

这是一项单机构回顾性研究。在 2009 年至 2019 年间接受治疗的 1967 名患者中,有 1369 名(78.54%)患者患有 SCC。其中,44 名患者接受了新辅助放化疗(NACTRT),1325 名患者接受了新辅助化疗(NACT),然后进行了根治性手术。使用正电子发射断层扫描(PET)在新辅助治疗(NAT)前后记录 18-氟脱氧葡萄糖的标准化摄取值(SUV)。使用 Mandard 肿瘤回归分级(TRG)标准评估最终切除标本的组织病理学,并将反应分为 0 至 5 级,即无残留肿瘤(NRT)、残留肿瘤较少(SRT)和残留肿瘤。我们试图找到原发性肿瘤部位新辅助后 SUV 的截止值,该值与实现更好的组织病理学反应相关。

结果

在接受手术的 1325 名 SCC 食管患者中,有 943 名患者的 TRG 数据可用,分为 0-2 级,有 325 名患者(34.5%),3-5 级,618 名患者(65.5%)。SUV 仅取自我们机构进行的 PET 扫描,以获得更同质的队列,有 186 名患者可获得 SUV 数据,其中 151 名来自 NACT 组,35 名来自 NACTRT 组。使用 ROC 方法找到 NACT 队列中 SUV 的截止值(5.05),这表明结果存在显著差异。在这些患者中,93 名接受 NACT 的患者 SUV > 5.05,58 名患者 SUV < 5.05。发现主观和客观组织病理学评分在 p 值 < 0.0001 时有相关性。具体而言,SRT 倾向于处于 TRG 的 3-5 级的大多数情况下,而 NRT 则主要处于 0-2 级。在 SUV 的 ≥ 5.05 类别中,有 76 例 SRT。在 NACT 队列中,SUV < 5.05 类别中,有 26 例 SRT 和 32 例 NRT。在 SRT 病例中,74.5%的 SUV ≥ 5.05,而 25.5%的 SUV < 5.05。在 NRT 病例中,34.7%的 SUV ≥ 5.05,而 65.3%的 SUV < 5.05(p 值 0.007)。在 NACTRT 组中,未发现放射病理学相关性。

结论

我们的研究证实了新辅助化疗后 PET SUV 与组织病理学反应的相关性,我们队列中的 SUV 截止值为 5.05。这证实了 FDG PET 的预测价值,如其他研究所示。此外,它在多个其他研究中已被证明具有生存预后价值。通过更大规模的随机研究,我们可能能够确定在解剖学和生理学上具有边缘可操作性的患者群体,在这些患者群体中,替代治疗方案可能有助于改善结果。

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