A Phase II Trial of Combined Treatment of Endoscopic Mucosal Resection and Chemoradiotherapy for Clinical Stage I Esophageal Carcinoma: Japan Clinical Oncology Group Study JCOG0508

Yukinori Kurokawa¹^,2, Manabu Muto³, Keiko Minashi⁴, Narikazu Boku⁵, Haruhiko Fukuda¹ for the Gastrointestinal Oncology Study Group of Japan Clinical Oncology Group (JCOG)

¹ Japan Clinical Oncology Group Data Center, Center for Cancer Control and Information Services, National Cancer Center, Tokyo
² Department of Surgery, Osaka National Hospital, Osaka
³ Department of Gastroenterology, Kyoto University, Kyoto
⁴ Division of Digestive Endoscopy and Gastrointestinal Oncology, National Cancer Center Hospital East, Chiba
⁵ Division of Gastrointestinal Oncology, Shizuoka Cancer Center, Shizuoka, Japan

For reprints and all correspondence: Manabu Muto, Department of Gastroenterology, Kyoto University, Kyoto, Japan. E-mail: mmuto{at}kuhp.kyoto-u.ac.jp

Received December 23, 2008; accepted June 7, 2009

Abstract

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INTRODUCTION
JCOG0508 PROTOCOL
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Standard treatment for clinical stage I esophageal cancer withsubmucosal invasion (T1b) has been surgical resection. We conducteda Phase II trial to evaluate the efficacy and the safety ofcombined treatment of endoscopic mucosal resection (EMR) andchemoradiotherapy for clinical stage I (T1b) esophageal cancer.Patients diagnosed as having clinical stage I (T1b) esophagealcancer which is considered to be resectable by EMR are eligible.When pathological examination of the EMR specimen confirms T1btumor with negative or positive resection margin, the patientundergoes chemoradiotherapy. The study continues until 82 patientswith T1b tumor with negative resection margin are enrolled from20 institutions. The primary endpoint is 3-year overall survival(OS) in pT1b cases with negative resection margin. The secondaryendpoints are 3-year OS and progression-free survival in alleligible cases, OS in pT1a-MM cases with margin-negative, complicationsof EMR and adverse events of chemoradiotherapy. The data fromthis trial will be expected to provide a non-surgical treatmentoption to the patients with clinical stage I (T1b) esophagealcancer.

Key Words: superficial esophageal cancer • endoscopic mucosal resection • chemoradiotherapy

INTRODUCTION

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Abstract
INTRODUCTION
JCOG0508 PROTOCOL
Funding
Conflict of interest statement
Appendix
Acknowledgements
References

According to the Japanese Classification of Esophageal Cancerby the Japan Esophageal Society, T1 esophageal tumors definedby the TNM system (6th edition) is further divided into T1a(mucosal) and T1b (submucosal) tumors by the Japanese Classificationof Esophageal Cancer (1). Endoscopic mucosal resection (EMR)is usually indicated for T1a tumor, whereas the standard treatmentfor T1b tumors has been a surgical resection with adequate lymphnode dissection in Japan because of the high incidence of lymphnode metastasis ( $~$ 40%) (2). However, surgical resection oftendeteriorates patient's general condition. Some patients withclinical T1b esophageal cancer are over-treated by surgery witha result of pathological T1a tumor, because the accuracy ofdiagnosis of T1b esophageal cancer is not high.

Recent advance in techniques of EMR including endoscopic submucosaldissection (ESD) enables us to remove the clinical T1b tumorand gives us accurate diagnosis of depth of invasion. However,the patients with T1b are at risk of lymph node metastasis (3)and therefore EMR alone cannot be considered as curative.

Chemoradiotherapy is one of the effective modalities for bothearly and advanced esophageal tumors. Since chemoradiotherapyis less toxic than surgical resection, the usefulness has beentested in several clinical trials (4,5). In Japan, a Phase IItrial (JCOG9708) was conducted to evaluate the efficacy andthe safety of concurrent chemoradiotherapy using 5-fluoraouracil(5-FU) plus cisplatin (CDDP) for T1 tumors (6). However, 22%of patients showed minor relapses that needed to be removedby endoscopic treatment. We have therefore conducted a pilotstudy of EMR followed by chemoradiotherapy and have reportedpromising results (7). Thus, the Japan Clinical Oncology Groupinitiated this multi-institutional Phase II trial (JCOG0508)to evaluate the efficacy and the safety of combined treatmentof EMR and chemoradiotherapy for clinical stage I (cT1bN0) esophagealcancer.

The Protocol Review Committee of JCOG approved the protocolin October 2006 and the study was activated in December 2006.

JCOG0508 PROTOCOL

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Abstract
INTRODUCTION
JCOG0508 PROTOCOL
Funding
Conflict of interest statement
Appendix
Acknowledgements
References

Purpose
The aim of this study is to evaluate the efficacy and the safetyof combined treatment of EMR and chemoradiotherapy for clinicalstage I (T1b) esophageal cancer.

Study Setting
The study is a multi-institutional (20 centers), single-armPhase II trial.

Resources
This study is supported by the Grants-in-Aid for Cancer Research(17S-3, 17S-5, 20S-3, 20S-6) and Health and Labour SciencesResearch Grant for Clinical Cancer Research (17-12) from theMinistry of Health, Labour and Welfare, Japan.

Endpoints
The primary endpoint is 3-year overall survival (OS) in pT1bcases with negative resection margin (comment 4). The secondaryendpoints are 3-year OS and progression-free survival (PFS)in all eligible cases, OS in pT1a-MM (muscularis mucosa) caseswith negative resection margin, complications of EMR and adverseevents of chemoradiotherapy.

In this trial, resection margin is diagnosed from endoscopicfindings immediately after mucosal resection for horizontalmargin and from pathological findings for vertical margin. OSis defined as the time from registration to death from any cause,and it is censored at the last contact day for living patient.PFS is defined as the time from registration to either the firstevent of progression or death from any cause, and it is censoredat the latest day when patient is alive without progression.

Inclusion Criteria
Patients are included in this trial if they meet all of thefollowing criteria: (i) histologically proven squamous cellcarcinoma of the esophagus by endoscopic biopsy, (ii) tumorslocated within the thoracic esophagus, (iii) depth of tumorinvasion is diagnosed as T1b by endoscopy and endoscopic ultrasonography,(iv) the number of multiple intra-esophageal tumors is lessthan three, and the depths of invasion of them are diagnosedas cT1a-EP (carcinoma in situ) or cT1a-LPM (tumor invades laminapropria mucosa), (v) clinically node-negative (cN0) and no metastasisto other organs (cM0), (vi) size of main tumor is $≤$ 5 cm, andcircularity of esophageal lumen is less than three-fourths,(vii) no ulcerative lesion in the tumors, (viii) no intra-esophagealmetastasis, (ix) no prior treatment of chemotherapy or radiationtherapy against any other malignancies, except for previouscurative EMR for pT1 esophageal cancer, (x) aged between 20and 75 years old, (xi) performance status of 0 or 1, (xii) sufficientorgan functions and (xiii) written informed consent.

Exclusion Criteria
Patients are excluded if they meet any of the following criteria:(i) iodine allergy, (ii) enable to discontinue anticoagulantor antiplatelet medications, (iii) synchronous or metachronous(within 5 years) malignancy other than carcinoma in situ, (iv)pregnant or breast-feeding women, (v) severe mental disease,(vi) systemic administration of corticosteroids, (vii) HBs antigenpositive, (viii) active bacterial or fungous infection, (ix)concurrent unstable angina or myocardial infarction within 3months before registration, (x) unstable hypertension, (xi)diabetes mellitus, uncontrolled or controlled with insulin,or (xii) interstitial pneumonia, lung fibrosis or severe emphysema.

Registration
After confirming the inclusion/exclusion criteria by telephoningor faxing the JCOG Data Center, the patients are registeredinto this JCOG0508 trial.

Quality Control of EMR
Twenty institutions among the Gastrointestinal Oncology StudyGroup of the JCOG participate in this trial. All participatingphysicians have agreed to the technical details for EMR. Forquality control of EMR technique and endoscopic diagnosis, weperform central review of the photographs in all patients atthe semi-annual investigators meeting. Regarding an ESD procedure,we permit it only for expert physicians who have significantexperiences in ESD and EMR, and they are registered by the primaryinvestigator (M.M.). The minimum request for ESD permissionis the experience of EMR $≥$ 50 and ESD $≥$ 10 for esophageal carcinoma,ESD $≥$ 50 for gastric cancer and perforation rate $≤$ 2% in total.

Treatment Methods
Endoscopic Mucosal Resection
EMR is performed against esophageal tumors within 30 days fromregistration. The technical methods of EMR approved in thistrial are a two-channel method, a cap method or an esophagealendoscopic mucosal resection-tube method (8). Only the registeredphysicians are allowed to perform ESD in this trial. After EMR,it should be confirmed endoscopically that no iodine-unstainedarea is left. Physicians need to take pictures before and afterEMR and submit them to the primary investigator for qualitycontrol of EMR technique and endoscopic diagnosis.

Chemoradiotherapy
In cases of pT1a tumor with negative resection margin and novascular invasion, no additional treatment after EMR is given.In other cases, chemoradiotherapy was started at 29–70days after EMR. The chemotherapy regimen is continuous 5-FU(700 mg/m²/day, days 1–4 and 29–32) and CDDP (70mg/m²/day, days 1 and 29). The dose of radiotherapy is 41.4Gy/23 Fr/5 weeks (5 days/week) for cases with negative resectionmargin and 50.4 Gy/28 Fr/5 weeks (5 days/week) with boost onthe primary site for the case with positive resection margin,respectively.

Follow-up
Patients are followed with blood tests, upper gastrointestinalendoscopy and computed tomography at least every 4 months for3 years.

Study Design and Statistical Methods
This trial determines the efficacy and the safety of combinedtreatment of EMR and chemoradiotherapy for cT1b esophageal cancerin terms of 3-year OS. Additionally, 3-year OS in all eligiblepatients are evaluated as the most important secondary endpoint.The sample size is 82 for pT1b cases with negative resectionmargin with the power of 90%. In case this hypothesis rejected,the secondary hypothesis for all eligible patients can be testedusing hierarchical method keeping trial-wise ${alpha}$ error nominallevel, one-sided 5%, with the power of 80%. To test the hypothesis,3-year OS estimated by Kaplan–Meier method and its confidenceinterval by Greenwood’s formula is used. The total numberof registered patients is estimated as 137, because the proportionof pT1b cases with margin-negative among all eligible patientsis predicted as $~$ 60%.

This study was registered with UMIN-CTR [www.umin.ac.jp/ctr/],identification number UMIN000000553.

Interim Analysis and Monitoring
Interim analysis is not planned. If the number of cases withtreatment-related death, severe (Grade 4) bleeding or severe(Grade 4) perforation reaches seven, the registration will besuspended unless the JCOG Data and Safety Monitoring Committeeapproves to continue this trial. The JCOG Data Center is responsiblefor data management, central monitoring and statistical analysis.This center also provides semi-annual monitoring reports, eachof which is submitted to and reviewed by the JCOG Data and SafetyMonitoring Committee on demand of the JCOG Data Center. Noneof physicians administering the interventions are involved inthe data analysis. For quality assurance, site-visit audits,not for a specific study basis but for the study group basis,are done by the JCOG Audit Committee.

Funding

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Abstract
INTRODUCTION
JCOG0508 PROTOCOL
Funding
Conflict of interest statement
Appendix
Acknowledgements
References

This study was supported by a grant from the Ministry of Healthand Welfare of Japan (H20-Ganrinsho-Ippan-015).

Conflict of interest statement

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INTRODUCTION
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Conflict of interest statement
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None declared.

Appendix

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The initially participating hospitals are as follows: IwatePrefectural Central Hospital, Ibaragi Prefectural Central Hospital,Tochigi Cancer Center Hospital, National Cancer Center HospitalEast, National Cancer Center Hospital, Tokyo Metropolitan Cancerand Infectious diseases Center Komagome Hospital, Showa UniversityHospital, Cancer Institute Ariake Hospital, Kitasato UniversityEast Hospital, Kanagawa Cancer Center Hospital, Ishikawa PrefecturalCentral Hospital, Saku Central Hospital, Shizuoka Cancer CenterHospital, Aichi Cancer Center Central Hospital, Kyoto UniversityHospital, Osaka Medical Center for Cancer and CardiovascularDisease, Osaka City Medical Center, and Osaka Medical CollegeHospital.

Acknowledgements

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INTRODUCTION
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Funding
Conflict of interest statement
Appendix
Acknowledgements
References

The authors thank Dr Seiichiro Yamamoto and Mr Taro Shibatafor statistical study design, and Dr Kenichi Nakamura for valuablecomments to the manuscript.

References

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Abstract
INTRODUCTION
JCOG0508 PROTOCOL
Funding
Conflict of interest statement
Appendix
Acknowledgements
References

1 Japanese Classification of Esophageal Cancer. (2008) 10th edition. Tokyo: Japan Esophageal Society, Kanehara, Co. Ltd.

2 Kato H, Tachimori Y, Mizobuchi S, Igaki H, Ochiai A. Cervical, mediastinal, and abdominal lymph node dissection (three-field dissection) for superficial esophageal carcinoma of the thoracic esophagus. Cancer (1993) 72:2879–82.[CrossRef][Web of Science][Medline]

3 Kodama M, Kakegawa T. Treatment of superficial cancer of the esophagus: a summary of responses to a questionnaire on superficial cancer of the esophagus in Japan. Surgery (1998) 123:432–9.[Web of Science][Medline]

4 Herskovic A, Martz K, al-Sarraf M, Leichman L, Brindle J, Vaitkevicius V, et al. Combined chemotherapy and radiotherapy compared with radiotherapy alone in patients with cancer of the esophagus. N Engl J Med (1992) 326:1593–8.[Abstract]

5 Ohtsu A, Boku N, Muro K, Chin K, Muto M, Yoshida S, et al. Definitive chemoradiotherapy for T4 and/or M1 lymph node squamous cell carcinoma of the esophagus. J Clin Oncol (1999) 17:2915–21.[Abstract/Free Full Text]

6 Kato H, Udagawa H, Togo A, Ando N, Tanaka O, Shinoda M, et al. A phase II trial of chemo-radiotherapy in patients with stage I esophageal squamous cell carcinoma: Japan Clinical Oncology Group study (JCOG9708). Proc Am Soc Clin Oncol (2003) 22. abstr 1147.

7 Minashi K, Ohtsu A, Mera K, Muto M, Yano T, Tahara M, et al. Combination of endoscopic mucosal resection and chemoradiotherapy as a nonsurgical treatments for patients with clinical stage I esophageal squamous cell carcinoma. J Clin Oncol (2007) 25(Suppl 18):4529.

8 Makuuchi H. Esophageal endoscopic mucosal resection (EEMR) tube. Surg Laparosc Endosc (1996) 6:160–1.[Web of Science][Medline]

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Japanese Journal of Clinical Oncology

A Phase II Trial of Combined Treatment of Endoscopic Mucosal Resection and Chemoradiotherapy for Clinical Stage I Esophageal Carcinoma: Japan Clinical Oncology Group Study JCOG0508