Esophagectomy versus definitive chemoradiotherapy for patients with clinical stage N0 and pathological stage T1b esophageal squamous cell carcinoma after endoscopic submucosal dissection: study protocol for a multicenter randomized controlled trial (Ad-ESD Trial)

Esophageal cancer is the seventh most common malignant tumor and ranks sixth in tumor-related mortality worldwide [1]. In terms of the histological subtypes, adenocarcinoma is frequently observed in Europe and the United States whereas squamous cell carcinoma is the predominant form in China [2].

Tumor invasion of the submucosa (T1b) is a watershed in the treatment of esophageal cancer from endoscopy to esophagectomy. Esophagectomy with extended lymph node dissection is recommend as the primary treatment for pT1b esophageal squamous cell carcinoma (ESCC) because of the high incidence of lymph node metastasis [3, 4]. Previous studies showed that patients with pT1b ESCC after esophagectomy had a favorable 5-year survival rate, which was about 70 ~ 73.6% [5, 6]. Although 30 ~ 50% of these patients have a risk of lymph node metastasis, more than half of them are presented with local superficial lesions [7]. In addition, esophagectomy is associated with a higher morbidity and mortality rate as well as decreased quality of life (QoL) [8]. Therefore, preserving the esophagus has always been the ultimate goal of treatment for low-risk submucosal esophageal cancer.

Previous studies have demonstrated that definitive chemoradiotherapy (dCRT) could achieve a survival rate comparable to that of esophagectomy for submucosal esophageal cancer [9]. However, local failure without distant metastasis after dCRT remains a major challenge to achieve long-term survival [10]. Endoscopic resection (ER) has been demonstrated with satisfied control for submucosal esophageal cancer without lymph node metastasis [11]. Therefore, the combination of ER and dCRT conforms to the aim of non-surgical treatment of submucosal esophageal cancer, which can maximize the removal of primary lesions and additional disposition of residual lesions or potential lymph node metastasis [12‐14]. The Japan Clinical Oncology Group (JCOG) phase II trial (JCOG0508) was the only prospective clinical study conducted to evaluate the efficiency and safety of combined treatment of ER and CRT for clinical stage I ESCC [15]. The results showed that for patients with pT1b with R0 and pT1a with lymphovascular invasion (+) after ER, the 3-year overall survival (OS) was 90.7% (90% confidence interval 84.0%–94.7%) after prophylactic CRT. They concluded that the combination of ER and selective CRT should be considered as a minimally invasive treatment option for clinical stage I ESCC [16].

Considering the encouraging results of JCOG0508 and other previous studies, we hypothesized that, in comparison with esophagectomy, concurrent dCRT may achieve comparable survival results and better QoL for submucosal esophageal cancer. Therefore, we designed this randomized controlled trial (RCT) to compare the two salvage treatments for pT1b ESCC after ER.

The aim of this trial is to compare esophagectomy versus dCRT for patients with clinical stage N0 and pathological stage T1b ESCC after endoscopic submucosal dissection (ESD).

This study is a multicenter, randomized, open-label, phase III trial. All participants will be allocated to the two intervention groups at 1:1 ratio. The flow chart is illustrated in Fig. 1.

Patients with cN0-pT1b ESCC after ESD will receive two concurrent salvage treatments. The intervention randomly assigned with either esophagectomy or dCRT will start at about 3 weeks after ESD, followed by a 60-month follow-up period. To achieve the primary endpoint, 176 patients will be recruited from three high-volume centers (>100 cases of esophagectomies) in China (Shanghai Chest Hospital, Zhongshan Hospital, and Changhai Hospital).

The informed consent document will be obtained from the potential participants or their authorized surrogates after the screening of the inclusion and exclusion criteria. Dr. Su will explain the details of the informed consent document to the participants and their authorized surrogates. The participants will be enrolled in this trial after Dr. Su obtains written permission from participants or their authorized surrogates.

On the consent form, participants will be asked whether they agree to the use of their data; otherwise, they could choose to withdraw from the trial. Participants will also be asked for permission for the research team to share relevant data with people from the institutions which are participating in the research or from regulatory authorities (where relevant). This trial does not involve collecting biological specimens for storage.

The time schedule of enrolment, interventions, assessments, and visits for participants is presented in the following schematic diagram.

According to previous studies, the 5-year OS of patients with pT1b ESCC who underwent esophagectomy was 70 ~ 80% [23] whereas the rate was about 90% in patients who received ER plus chemoradiation [16]. We assumed that the 5-year OS rates were 75% in the esophagectomy group and 90% in the dCRT group. The proportion dropping out of the study is considered to be 5%. Therefore, a sample size of 88 patients in each group is required at a significance level of 5% and a power of 80%.

All patients with cN0-pT1b ESCC diagnosed after ESD treatment are potential candidates in this trial. The endoscopists will register all of these patients and notify the clinical research coordinator (CRC) of this trial, and the CRC will contact and tell potential candidates about this trial. After screening for the eligible criteria, the CRC will set up a meeting with potential candidates or their authorized surrogates and Dr. Su in the outpatient clinic. Dr. Su will explain the details of this trial to them and obtain their signatures.

The three institutions which are participating in this trial are high-volume medical centers with esophagectomy and ESD treatment. According to our estimation of the duration of recruitment, 80 patients will be recruited per year.