Post-operative chemotherapy improves disease-free survival, but not overall survival in people with oesophageal squamous cell carcinoma

CANCER TREATMENT REVIEWS (2004) 30, 473–477

www.elsevierhealth.com/journals/ctrv

EVIDENCE-BASED ONCOLOGY

Post-operative chemotherapy improves disease-free survival, but not overall survival in people with oesophageal squamous cell carcinoma Abstracted from: Ando N, Iizuka T, Ide H et al. Surgery plus chemotherapy compared with surgery alone for localized squamous cell carcinoma of the thoracic esophagus: a Japan Clinical Oncology Group Study – JCOG9204. Journal of Clinical Oncology 2003;21:4592–6.

Background

Objective

(7%), middle (58%) and lower oesophagus (35%). Lymph node status was N1 for 82% and N0 for 18% of participants. Inclusion criteria: absence of microscopic residual tumour (R0); pathological disease stage of IIA (18%), IIB (29%), III (35%) or IV – positive cervical or celiac nodes (18%); an Eastern Cooperative Oncology Group performance status between 0 and 2; an otherwise normal clinical laboratory profile. Exclusion criteria: additional synchronous or metachronous cancer.

To assess whether post-operative adjuvant chemotherapy is more effective than surgery alone in people with oesophageal squamous cell carcinoma.

Intervention

Evidence to support the administration of postoperative cisplatin plus fluorouracil chemotherapy regimens in people with oesophageal squamous cell carcinoma is lacking.

Setting Seventeen institutions in Japan; recruitment from July 1992 to January 1997.

Method Multicentre randomised controlled trial.

Participants Two hundred and forty two people aged 6 75 years (mean age 59 years, range 40 to 75 years) with histologically proven oesophageal squamous cell carcinoma. Tumours were located in the upper




All participants underwent regional lymphadenectomy, right or left thoracotomy for curative resection by subtotal or total oesophagectomy before randomisation to no further treatment (surgery only group) or two courses of chemotherapy (surgery plus chemotherapy). The chemotherapy regime comprised: cisplatin (80 mg/m2 of body surface area) administered over 2 h on day 1 via slow drip infusion plus fluorouracil (800 mg/m2 of body surface area) administered via continuous infusion from days 1 to 5. A second course of chemotherapy was administered after an interval of 3 weeks. Second course doses were adjusted or suspended altogether depending on the clinical laboratory profile. Median follow-up from time of randomisation was 62.8 months. Of the people randomised to receive post-operative chemotherapy, 21 (17.5%) failed to complete two planned courses, due either to toxicity or participant

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474 refusal, and a further 8 (6.7%) people underwent no chemotherapy.

Main outcomes Disease-free survival (from the date of randomisation to the date of first evidence of relapse or death from any cause); overall survival (from the date of surgery to the date of death or last followup) and adverse events.

Main results Surgery plus chemotherapy improved disease-free survival compared with surgery alone at 5 years (see Evidence Table 1). There was no significant difference in overall survival between groups. One person died as a result of treatment in the surgery plus chemotherapy group (see Evidence Table 2). Information regarding adverse events in the surgery alone group was not reported.

Evidence-based Oncology Allocation Not clear concealment Balanced groups

Analysis

Adequate: groups were balanced at baseline with respect to sex, age, tumour location and pathology Intention to treat; Kaplan–Meier; Cox proportional hazards model

Sources of funding: This study was supported by the Ministry of Health, Labor and Welfare of Japan and the Second Term Comprehensive 10-Year Strategy for Cancer Control. For Correspondence: Nobutoshi Ando, Department of Surgery, Tokyo Dental College, Ichikawa General Hospital, Sugano, Ichikawashi, Chiba, Japan. E-mail: [email protected]. Abstract provided by Bazian Ltd., London.

Commentary Authors’ conclusions Post-operative adjuvant chemotherapy is more effective than surgery alone at improving diseasefree survival in people with oesophageal squamous cell carcinoma.

Method notes

Power calculation

80% power with 290 people to detect an absolute risk increase in 5-year disease-free survival of 13% with surgery plus chemotherapy compared with surgery alone at a 5% level of significance using a 1-sided test. However, only 242 people were enrolled in the study, and smaller differences in response rate cannot be excluded Blinding Nature of intervention precludes blinding of participants Generation of Adequate: randomisation was allocation centrally assigned using a minisequence misation method so that institution and pathologic lymph node status would be balanced

Esophageal cancer remains one of the most challenging malignancies to treat, of all gastrointestinal (GI) tract cancers. In the United States (US), it is estimated that 14,250 new cases and 13,300 deaths due to esophageal cancer will occur in 2004.1 Surgery remains the mainstay of treatment, but as the median survival is only 12 to 16 months, there is increasing interest in the role of adjuvant and neoadjuvant therapy. To date, studies evaluating adjuvant therapy have been inconclusive with regard to benefit. The two largest trials evaluating adjuvant cisplatin and 5-fluorouracil chemotherapy in resectable esophageal cancer have demonstrated conflicting results. The American Intergroup (INT113) trial reported by Kelsen et al. randomized 440 patients to adjuvant chemotherapy plus surgery or surgery alone. The median survival for the two groups was 16.1 months and 14.9 months, respectively ðp ¼ 0:53Þ.2 In contrast, the British Medical Research Council (MRC) trial treated 802 patients in a similar fashion and demonstrated median survivals of 16.8 months and 13.3 months, respectively ðp ¼ 0:004Þ, concluding a positive benefit to post-operative chemotherapy.3 Other trials have been either small or had design flaws complicating their interpretation (Table 1). Even meta-analyses on this subject fail to agree on the relative merits of adjuvant chemotherapy.4;5

Evidence-based Oncology Evidence Table 1

Disease-free and overall survival (intention to treat analysis)

Five-year disease-free survival Five-year overall survival

Evidence Table 2 therapy

475

Surgery alone ðN ¼ 122Þ

Surgery plus chemotherapy ðN ¼ 120Þ

Significance

45% (95% CI 36 to 54%) 52% (95% CI 43 to 61%)

55% (95% CI 46 to 64%) 61% (95% CI 52 to 70%)

p ¼ 0:037 p ¼ 0:13

Mortality and serious (Grade 3 or Grade 4)a adverse events during post-operative chemoSurgery plus post-operative chemotherapy ðN ¼ 120Þ

Absolute risk for mortality Cause of death: lactic acidosis relating to thiamine deficiency Absolute risk of toxicity Granulocytes Nausea/vomiting Leucocytes Platelets Diarrhoea Haemoglobin Arrhythmia Infection Fever a

1 (0.8%)

22 10 5 3 3 2 1 1 1

(18.3%) (8.3%) (4.2%) (2.5%) (2.5%) (1.7%) (0.8%) (0.8%) (0.8%)

Classified according to WHO toxicity criteria.

The trial by Ando et al.6 assesses the role of adjuvant chemotherapy in squamous cell esophageal cancer. In 242 patients from Japan, treatment with either surgery alone or surgery plus two courses of cisplatin and 5-fluorouracil (5FU) resulted in an improved 5-year disease-free survival ðp ¼ 0:037Þ. However, there was no difference in the overall survival between the groups ðp ¼ 0:13Þ. The authors rationalized that the lack of an overall survival benefit may be due to differences in surgical technique between the groups or the more frequent use of off-protocol chemoradiotherapy for recurrence in the surgery alone arm (35%) compared to the chemotherapy arm (25%). Weaknesses of the trial include a small sample size, failure to adhere to the original statistical design, off-protocol chemoradiotherapy, and a significant number of patients lost to follow-up. Ando et al. concluded that adjuvant chemotherapy is beneficial and that it should be used as a control arm for subsequent studies. The conclusions of the trial by Ando et al. are not definitive. The relevance of this trial to the current management of esophageal cancer in the Western world is limited by a number of factors. First, the patient cohort in this trial significantly differs from patients treated in the US or Europe. All patients in the Japanese study had squamous cell carcinoma and had 5-year survivals of 61% and

52% in the two arms. In the US intergroup trial, the 3-year survival was 23% and 26%, and in the MRC trial 2-year survival was 43% and 34%, respectively, for surgery plus chemotherapy versus surgery alone. In addition, adenocarcinoma was the predominant histology in both the US and MRC trials, in contrast to the Japanese study. Second, many patients in the Ando et al. trial had locally advanced disease but, presumably in an attempt to preserve the validity of the trial, off-protocol chemoradiotherapy was restricted to patients with recurrent disease. In the US, preoperative chemoradiotherapy is the standard of care for locally advanced esophageal cancer based on a number of trials demonstrating an improvement in either disease-free or overall survival using this approach.7 Also, patients with adenocarcinoma of the gastroesophageal (GE) junction are treated with post-operative chemoradiotherapy.8 A recent pattern of care study in the US reported combined chemoradiotherapy as being the most commonly employed modality of treatment for esophageal cancer.9 Finally, lack of an overall survival benefit using post-operative cisplatin and 5FU in the Ando et al. trial does not necessarily imply that adjuvant chemotherapy is ineffective. It is possible that had a greater number of cycles of chemotherapy been delivered, more definitive benefit might have been

476

Table 1

Prospective randomized trials of neoadjuvant or adjuvant chemotherapy in esophageal cancer

Author

Year

N

Histology

Treatment

Preop/Postop

Median (months) or 3-year survival

P value

Study limitations

Roth et al.

1988

20 19

SCC

Preop + postop

9 9

NS

Small

Schlag et al.

1991

24

SCC

Surgery Cisplatin/Vindesine/ Bleomycin Surgery

Preop

10

NS

NS

Randomized + nonrandomized in the paper 2 x 2 factorial design

22 Nygaard et al.

1992

50

Cisplatin/5FU SCC

56

Surgery

10 Preop

Cisplatin/bleomycin

Maipang et al.

1994

22 24

SCC

Pouliquen et al.

1996

68

SCC

Surgery Cisplatin/Vinblastine/ Bleomycin Surgery

Ando et al.

1997

52 100

SCC

Law et al.

1997

105 73

Kok et al.

1997

74 74

Kelsen et al.

1998

Ancona et al.

2001

13% 6% 17 17

NS

Small

Postop

14

NS

Cisplatin/Vindesine Surgery

Postop

13 45%

Some patients had R2 resections

NS

Small

SCC

Cisplatin/5FU Surgery

Preop

48% 13

NS

Small

SCC

Cisplatin/5FU Surgery

Preop

17 11

0.002

Only in abstract form

74 234

Adeno/SCC

Cisplatin/Etoposide Surgery

Preop + postop

18.5 16

NS

233 47

SCC

Cisplatin/5FU Surgery

Preop

15 24

Decreased surgery in chemotherapy arm

NS

R0 resection not performed in all patients Small

47

Cisplatin/5FU

25

Wang et al.

2001

50

Adeno/SCC

Surgery

Preop

32%

<0.05

MRC

2002

50 402

Adeno/SCC

Cisplatin-based Surgery

Preop

46% 13

0.004

Ando et al.

2003

SCC

Cisplatin/5FU Surgery

Preop

17 122

Off protocol radiotherapy

NS

Off protocol chemoradiotherapy

400

Cisplatin/5FU *

120

5-year survival; SCC, squamous cell carcinoma; Adeno, adenocarcinoma; Preop, pre-operative chemotherapy; Postop, post-operative chemotherapy; NS, non-significant.

Evidence-based Oncology

Preop

Evidence-based Oncology observed. A similar trial performed today in the US or Europe in adenocarcinoma patients, as accrual for a trial of this size in squamous cell patients is likely to be difficult, would be expected to incorporate newer chemotherapy regimens, which are potentially more efficacious and usually given preoperatively to facilitate better tolerance, increase resectability rates, and treat micrometastatic disease. The use of epirubicin, cisplatin and 5FU (ECF), and docetaxel, cisplatin and 5FU (DCF) has significantly improved survival in patients with metastatic cancer of the upper GI tract, when compared to other combination chemotherapy including cisplatin/5FU. Adjuvant ECF has improved disease-free survival in patients with resected gastric and GE cancers although follow-up was too premature to detect an overall survival difference.10 Other regimens such as irinotecan and cisplatin have also shown promising response rates (57%) and await investigation in phase III trials.11 We await the outcomes of trials using these regimens in the perioperative management of esophageal cancer. Despite the limitations of the trial by Ando et al., with respect to current practice in the Western world, a clearly positive or negative result would have provided further insight on the role of adjuvant chemotherapy in esophageal cancer. Unfortunately, this trial, like its predecessors, engenders more questions than firm conclusions. Although, while probably best interpreted as a negative trial due to the lack of an overall survival benefit, supporters of adjuvant chemotherapy will be encouraged by the marginal statistically significant improvement in diseasefree survival which was the primary endpoint of the study. Current practice will not change based on the results of the study by Ando et al. but these results provide continued support for the role of chemotherapy in the multidisciplinary management of potentially resectable esophageal cancer. Future trials in esophageal cancer must focus on newer more active chemotherapy and targeted therapies with or without radiotherapy. As chemoresponsive patients have consistently been shown to have an improved survival compared to non-responders, perhaps more important is the identification of chemoresponsive patients for the selected use of adjuvant therapy. Hopefully, with better patient selection and staging we can positively impact on the challenging prognosis of this disease.

477 Quality Assessment (scale 1 ¼ fair; 4 ¼ excellent) Relevance Validity Applicability Feasibility Impact Knowledge context

4 3 3 3 3 4

Gregory D. Leonard Eileen M. O Reilly Memorial Sloan Kettering Cancer Center New York, NY, USA

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