Impact of Retroperitoneal Lymphadenopathy (RPLN) on the Outcomes of Locally Advanced Gall Bladder Cancer (GBC) Following Chemotherapy (CT) or Chemotherapy Followed by Consolidation Chemoradiotherapy (CTRT).

IF 1.6 Q4 ONCOLOGY

Journal of Gastrointestinal Cancer Pub Date : 2024-10-19 DOI:10.1007/s12029-024-01124-5

Sushma Agrawal, Nagendra Naik, Parul Priyanka

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引用次数: 0

Abstract

Introduction: Retroperitoneal lymphadenopathy is considered a metastatic disease in GBC; however, some surgical series of radical surgery with enlarged RPLN who underwent RPLN dissection have shown results marginally inferior to those without enlarged RPLN. Radiological RPLN comprises a major proportion of advanced non-metastatic GBC. There is dilemma in the intent of treatment to be offered in such cases. We are reporting our series of outcome of GBC with RPLN treated with first-line CT followed by consolidation CTRT.

Materials and methods: Non-metastatic locally advanced GBC with good performance status (KPS ≥ 80) were initiated on first-line CT (cisplatin-gemcitabine), and thereafter, responders were evaluated by CECT-angiography and PET-CT scan for resectability. If found unresectable, they were offered consolidation CTRT to a dose of 45 Gy by conventional fractionation (3D-CRT technique) along with concurrent capecitabine at 1250 mg/m² to GBC and regional lymphatics including RPLN. Thereafter, boost dose of 9 Gy/5# was given to GBC only. Response assessment was done using CECT abdomen by RECIST criteria v 1.1. Outcomes (overall survival) of the two groups (RPLN vs non-RPLN) were computed with Kaplan-Meier survival curves and chi-square tests using SPSS v 20.

Results: Among 189 patients of advanced non-metastatic GBC recruited from 2011 to 2022, 80 had RPLN. The demographic features of both groups were comparable. Overall, 68% of the patients were women, 30% underwent upfront stenting for obstructive jaundice, and 90% had T3 and T4 disease. Only 10% had undergone upfront laparoscopic staging and had pathologically proven RPLN. Forty percent of the patients received four cycles of CT only and 50% of the patients received six cycles or more and 33% received CTRT. By RECIST criteria, 10% vs 16% achieved complete response (CR), 39% vs 41% achieved partial response (PR), 16% vs 15% achieved stable disease (SD), 2.7% vs 6% had disease progression (PD), and 14.5% vs 3.7% were non-evaluable in non-RPLN group vs RPLN group, respectively. 12% vs 6% could undergo radical surgery in non-RPLN group vs RPLN group (p = 0.03). The median OS was 9 months (95% CI 7.6-10.3 months) vs 10 months (95% CI 8-9.8 months) (p = NS) in non-RPLN group vs RPLN group, respectively. In those who received CT only, the median OS was 7 months vs 8 months, while in those who received CT followed by CTRT, the median OS was 14 months vs 13 months (p = 0.65) in non-RPLN group vs RPLN group, respectively.

Conclusions: Based on this analysis, we conclude that RPLN constitutes a major proportion of advanced non-metastatic GBC and has outcomes similar to those without RPLN if treated with radical intent. RPLN should not be considered a metastatic disease and should be treated with radical intent.

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腹膜后淋巴结病 (RPLN) 对化疗 (CT) 或化疗后巩固放化疗 (CTRT) 的局部晚期胆囊癌 (GBC) 治疗效果的影响。

导言：腹膜后淋巴结病被认为是 GBC 的一种转移性疾病；然而，一些根治性手术系列中，RPLN 淋巴结肿大并接受 RPLN 淋巴结清扫术的患者的治疗效果略逊于 RPLN 淋巴结未肿大的患者。放射性 RPLN 在晚期非转移性 GBC 中占很大比例。对这类病例的治疗意向存在两难。我们报告了我们对伴有RPLN的GBC进行一线CT治疗后再进行CTRT巩固治疗的结果：非转移性局部晚期 GBC 且表现状态良好（KPS ≥ 80）者开始接受一线 CT（顺铂-吉西他滨）治疗，之后通过 CECT 血管造影和 PET-CT 扫描评估有反应者的可切除性。如果发现无法切除，则采用常规分型（3D-CRT 技术）进行 45 Gy 剂量的 CTRT 巩固治疗，同时对 GBC 和区域淋巴（包括 RPLN）使用 1250 mg/m2 的卡培他滨。此后，仅对GBC给予9 Gy/5#的增强剂量。根据RECIST标准1.1版，采用腹部CECT进行反应评估。两组（RPLN 与非 RPLN）的结果（总生存期）通过 Kaplan-Meier 生存曲线计算，并使用 SPSS v 20 进行卡方检验：在2011年至2022年招募的189名晚期非转移性GBC患者中，有80人患有RPLN。两组患者的人口统计学特征相当。总体而言，68%的患者为女性，30%的患者因阻塞性黄疸接受了前期支架植入术，90%的患者患有T3和T4疾病。只有10%的患者接受过腹腔镜前期分期，并经病理证实患有RPLN。40%的患者只接受了4个周期的CT治疗，50%的患者接受了6个周期或更多周期的治疗，33%的患者接受了CTRT治疗。根据RECIST标准，非RPLN组和RPLN组分别有10%和16%的患者获得完全反应（CR），39%和41%的患者获得部分反应（PR），16%和15%的患者获得疾病稳定（SD），2.7%和6%的患者疾病进展（PD），14.5%和3.7%的患者无评估结果。非RPLN组与RPLN组相比，12%对6%可以接受根治性手术（P = 0.03）。非RPLN组与RPLN组的中位OS分别为9个月（95% CI 7.6-10.3个月）与10个月（95% CI 8-9.8个月）（p = NS）。仅接受CT治疗的患者的中位OS为7个月 vs 8个月，而接受CT治疗后再接受CTRT治疗的患者的中位OS为14个月 vs 13个月，非RPLN组 vs RPLN组分别为14个月 vs 13个月（p = 0.65）：根据这一分析，我们得出结论：RPLN 在晚期非转移性 GBC 中占很大比例，如果采用根治性治疗，其结果与无 RPLN 者相似。RPLN不应被视为转移性疾病，应采用根治性治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Gastrointestinal Cancer ONCOLOGY-

CiteScore

3.80

自引率

0.00%

发文量

121

期刊介绍： The Journal of Gastrointestinal Cancer is a multidisciplinary medium for the publication of novel research pertaining to cancers arising from the gastrointestinal tract.The journal is dedicated to the most rapid publication possible.The journal publishes papers in all relevant fields, emphasizing those studies that are helpful in understanding and treating cancers affecting the esophagus, stomach, liver, gallbladder and biliary tree, pancreas, small bowel, large bowel, rectum, and anus. In addition, the Journal of Gastrointestinal Cancer publishes basic and translational scientific information from studies providing insight into the etiology and progression of cancers affecting these organs. New insights are provided from diverse areas of research such as studies exploring pre-neoplastic states, risk factors, epidemiology, genetics, preclinical therapeutics, surgery, radiation therapy, novel medical therapeutics, clinical trials, and outcome studies.In addition to reports of original clinical and experimental studies, the journal also publishes: case reports, state-of-the-art reviews on topics of immediate interest or importance; invited articles analyzing particular areas of pancreatic research and knowledge; perspectives in which critical evaluation and conflicting opinions about current topics may be expressed; meeting highlights that summarize important points presented at recent meetings; abstracts of symposia and conferences; book reviews; hypotheses; Letters to the Editors; and other items of special interest, including:Complex Cases in GI Oncology: This is a new initiative to provide a forum to review and discuss the history and management of complex and involved gastrointestinal oncology cases. The format will be similar to a teaching case conference where a case vignette is presented and is followed by a series of questions and discussion points. A brief reference list supporting the points made in discussion would be expected.