Concurrent chemoradiotherapy with S‑1 in patients with stage III‑IV oral squamous cell carcinoma: A retrospective analysis of nodal classification based on the neck node level

  • Authors:
    • Ryuji Murakami
    • Akiko Semba
    • Kenta Kawahara
    • Keiya Matsuyama
    • Akimitsu Hiraki
    • Masashi Nagata
    • Ryo Toya
    • Yasuyuki Yamashita
    • Natsuo Oya
    • Hideki Nakayama
  • View Affiliations

  • Published online on: May 29, 2017     https://doi.org/10.3892/mco.2017.1276
  • Pages: 140-144
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Abstract

The aim of the present study was to retrospectively evaluate the treatment outcomes of concurrent chemoradiotherapy (CCRT) with S‑1, an oral fluoropyrimidine anticancer agent, for advanced oral squamous cell carcinoma (SCC). The study population consisted of 47 patients with clinical stage III or IV oral SCC, who underwent CCRT with S‑1. Pretreatment variables, including patient age, clinical stage, T classification, midline involvement of the primary tumor and nodal status, were analyzed as predictors of survival. In addition to the N classification (node‑positive, multiple and contralateral), the prognostic impact of the level of nodal involvement was assessed. Nodal involvement was mainly observed at levels Ib and II; involvement at levels Ia and III‑V was considered to be anterior and inferior extension, respectively, and was recorded as extensive nodal involvement (ENI). The 3‑year overall survival (OS) and progression‑free survival (PFS) rates were 37 and 27%, respectively. A finding of ENI was a significant factor for OS [hazard ratio (HR)=2.16; 95% confidence interval (CI): 1.03‑4.55; P=0.038] and PFS (HR=2.65; 95% CI: 1.32‑5.33; P=0.005); the 3‑year OS and PFS rates in patients with vs. those without ENI were 23 vs. 50% and 9 vs. 43%, respectively. The other variables were not significant. Therefore, CCRT with S‑1 may be an alternative treatment for advanced oral SCC; favorable outcomes are expected in patients without ENI.

Introduction

Advanced oral squamous cell carcinoma (SCC) is commonly treated by combined surgery, radiotherapy and chemotherapy; patients with unresectable disease usually undergo concurrent chemoradiotherapy (CCRT) (17). Although CCRT is considered to be superior to radiotherapy alone in improving survival, it may not be suitable for elderly patients and/or those with poor performance status (7). S-1 is an oral fluoropyrimidine anticancer agent that combines tegafur [a prodrug of 5-fluorouracil (5-FU)], gimeracil (which inhibits the 5-FU degeneration enzyme dihydropyrimidine dehydrogenase) and oteracil (which reduces the gastrointestinal toxicity of 5-FU). Both tegafur and gimeracil in S-1 have been suggested to have radiosensitizing properties (8,9). The pathological effects of preoperative CCRT with S-1 have been demonstrated in operated patients with advanced oral SCC (4,5). Some case reports suggest the possible efficacy of definitive CCRT with S-1 (6). However, further investigations are required to evaluate the treatment outcomes of CCRT with S-1 for inoperable advanced oral SCC.

The tumor-node-metastasis (TNM) staging system is essential for prognosis prediction, treatment tailoring and the comparison of clinical trials. This system has been updated based on technical advances in diagnostic and treatment methods by close cooperation between the Union for International Cancer Control (UICC) and the American Joint Committee on Cancer (AJCC). Although there are distinct criteria for T-staging at different primary sites, N-staging is the same for all head and neck sites, except the nasopharynx and thyroid gland. The International Consensus Guidelines for the neck node level are also used for tailoring neck dissection and radiotherapy in patients with SCC of the head and neck (10,11). In 2013, the guidelines were further updated to reduce treatment variations among different clinicians and to facilitate the conduct of multi-institutional clinical trials (12). N-staging according to the UICC/AJCC criteria takes into consideration single (N1), multiple- (N2b) and contralateral (N2c) nodes, but not the level of nodal involvement. Recent studies have demonstrated that the level of nodal involvement is a prognostic factor in patients with advanced head and neck SCC (13,14).

The aim of the present study was to retrospectively evaluate the treatment outcomes of CCRT with S-1 for advanced oral SCC. Additionally, the prognostic impact of the nodal classification based on the neck node level was assessed.

Patients and methods

Patient characteristics

Between July, 2004 and October, 2011, 49 patients with advanced oral SCC underwent CCRT with a total radiation dose of 60 or 70 Gy. The patients were not initially treated surgically due to technically and/or medically unresectable disease. Of the 49 patients, 47 (24 men and 23 women; median age, 79 years; age range, 45–91 years) fulfilled our inclusion criteria of i) histologically verified SCC of the oral cavity, ii) clinical stage III or IV, iii) no distant metastasis and iv) no previous malignancies. Two patients with a previous head and neck malignancy were excluded. The primary tumors were located in the buccal mucosa (n=4), upper gingiva (n=7), lower gingiva (n=12), hard palate (n=4), tongue (n=16) and floor of the mouth (n=4). The clinical stage according to the UICC/AJCC criteria was identified at a conference of oral surgeons, radiologists and radiation oncologists who interpreted the imaging data. The radiological diagnosis of nodal involvement was based on widely accepted morphological criteria (15,16). Of the 47 tumors, one was T1, 5 were T2, 13 were T3, 15 were T4a and 13 were T4b. Midline involvement of the primary tumor was observed in 24 patients. The clinical node (cN) stage was recorded as cN0 in 13, cN1 in 2, cN2b in 18 and cN2c in 14 patients. The pattern of lymph node involvement according to the clinical findings of the primary tumor, i.e., subsite, T stage and midline involvement, was defined based on the 2013 consensus guidelines (12).

CCRT

A total dose of 60–70 Gy was delivered in 2-Gy fractions using two-three fields. Concurrently, S-1 (Taiho Pharmaceutical, Tokyo, Japan) was administered per os (80 mg/m2/day) for 14 consecutive days followed by a 1-week drug-free period or on the days of irradiation (65 mg/m2/day) (46). The initial radiation fields included the tumor extension and levels I and II, even in cN0 necks; clinically positive as well as equivocal node levels were added in the initial fields. Thereafter, boost irradiation was delivered to the primary tumor and clinically positive nodes. The maximum dose to the spinal cord did not exceed 40 Gy during the two courses of CCRT.

Follow-up evaluation

The patients were followed up to evaluate tumor control. The initial sites of disease progression were classified as local, regional and distant. In patients with failed tumor control salvage surgery, additional radiotherapy and/or additional chemotherapy were considered. Post-treatment survival was measured from the first day of CCRT to the event day or the last day of follow-up. The acute toxicities of CCRT were scored according to the National Cancer Institute Common Terminology Criteria for Adverse Events, version 4.0

Statistical analysis

Pre-treatment variables, including age, clinical stage, T-classification, midline involvement and nodal status, were analyzed as predictors of survival. In addition to the N-classification according to the UICC/AJCC criteria (node-positive, multiple and contralateral), the level of nodal involvement was considered to be a prognostic factor. Overall survival (OS) and progression-free survival (PFS) rates were calculated using the Kaplan-Meier method and compared with the log-rank test. The Cox proportional hazards model was applied to calculate the hazards ratio (HR) and the 95% confidence interval (CI). All statistical computations were performed using commercial software (IBM SPSS Statistics, version 21, IBM Japan, Tokyo). P<0.05 was considered to indicate statistically significant differences.

Results

Pattern of lymph node involvement

According to the clinical findings of the primary tumor, the pattern of nodal involvement is presented in Table I. In each status of the primary tumor, the nodal involvement was mainly observed at levels Ib and II; node-positive disease exhibited nodal involvement at these levels. Involvement at levels Ia and III–V was considered, regardless of the laterality, to be anterior and inferior extension, respectively, and was recorded as extensive nodal involvement (ENI).

Table I.

Clinical nodal level involvement according to the primary tumor characteristics.

Table I.

Clinical nodal level involvement according to the primary tumor characteristics.

Ipsilateral (contralateral) neck node level

Primary tumor characteristicsnIaIbIIIIIIVV
Subsite
  Buccal mucosa433 (1)31
  Upper gingiva75 (2)6 (3)11
  Lower gingiva1246 (2)3 (1)
  Hard palate4231
  Tongue16310 (3)11 (2)7 (1)3
  Floor of the mouth42 (1)3 (2)4 (2)3 (1)2
T classification
  1–3193812 (1)5 (1)3
  4a153 (1)9 (6)7 (4)5 (1)1
  4b13312 (3)11 (4)53
Midline involvement
  No23113 (3)14 (3)23
  Yes248 (1)16 (6)16 (6)13 (2)4
  Total479 (1)29 (9)30 (9)15 (2)70
Accomplishment of CCRT with S-1

All 47 patients underwent radiotherapy as planned; however, the oral administration of S-1 was discontinued in 7 patients who manifested acute toxicity. All 47 patients experienced transient acute mucositis ranging from grade 1 to 3. The toxicities of grade 3 were mucositis (n=16) and dermatitis (n=4). No grade ≥4 adverse events were encountered.

Outcome and survival analysis

Adjuvant chemotherapy with S-1 was continued for 1–27 months (median, 5 months) in 24 patients without drug-related adverse events. During a median follow-up of 22 months (range, 4–89 months), 19, 8 and 2 patients suffered local, regional and distant progression, respectively. All locoregional progressions (n=27) were observed within the full-dose irradiated regions; 7 patients underwent salvage resection for locoregional progression. The 2 distant progressions were lung metastases. Of the 47 patients in this series, 30 succumbed to primary (n=23) or intercurrent disease (n=7); the 3-year OS and PFS rates were 37 and 27%, respectively.

Anterior extension to level Ia was a statistically significant prognostic factor for OS (P=0.008) and PFS (P=0.001); however, inferior extension to level III–V was not statistically significant for OS (P=0.099) and PFS (P=0.052). Of 22 patients with ENI, including anterior and inferior extension, 10, 8 and 2 suffered local, regional and distant progression, respectively. Consequently, ENI based on the neck node level was a significant prognostic factor for OS (P=0.038) and PFS (P=0.005); the 3-year OS and PFS rates in patients with vs. those without ENI were 23 vs. 50% and 9 vs. 43%, respectively (Figs. 1 and 2). Other variables, including the N classification according to the UICC/AJCC criteria, were not significant (Table II).

Table II.

Prognostic factors for overall and progression-free survival.

Table II.

Prognostic factors for overall and progression-free survival.

Overall survivalProgression-free survival


Prognostic factorsnMedian (months)HR (95% CI)P-valueMedian (months)HR (95% CI)P-value
Total4722.5 11.3
Age, years 0.586 0.615
  <792322.51 11.31
  ≥792417.51.22 (0.59–2.53) 9.51.19 (0.61–2.31)
Clinical stage 0.270 0.292
  III859.71 17.91
  IV3917.51.80 (0.63–5.16) 9.51.66 (0.64–4.31)
T classification 0.684 0.897
  1–31917.91 11.31
  42822.50.86 (0.42–1.78) 10.41.05 (0.53–2.07)
Midline involvement 0.433 0.083
  No2328.31 17.91
  Yes2416.21.33 (0.65–2.73) 6.91.80 (0.92–3.53)
Node positivity 0.990 0.650
  No1327.91 17.91
  Yes3419.81.00 (0.45–2.18) 8.91.19 (0.57–2.48)
Multiple nodes 0.538 0.538
  No1528.31 17.91
  Yes3217.51.28 (0.58–2.80) 8.91.25 (0.61–2.57)
Contralateral node 0.330 0.306
  No3327.91 11.31
  Yes1417.51.46 (0.68–3.12) 7.71.44 (0.71–2.90)
Level Ia involvement 0.008 0.001
  No3828.31 12.31
  Yes916.52.83 (1.27–6.33) 4.83.56 (1.60–7.94)
Level III–V involvement 0.099 0.052
  No3028.31 15.01
  Yes1714.31.85 (0.88–3.88) 8.91.95 (0.98–3.87)
ENIa 0.038 0.005
  No2559.71 21.61
  Yes2216.22.16 (1.03–4.55) 7.72.65 (1.32–5.33)

a Nodal involvement at uncommon levels, i.e., anterior extension to level Ia and/or inferior extension to levels III–V. CI, confidence interval; ENI, extensive nodal involvement; HR, hazards ratio.

Discussion

Multimodal therapeutic strategies are crucial for the treatment of advanced oral SCC; the 5-year OS rates for operated cases were reported to be approximately 50% (1719). Patients with unresectable disease usually undergo CCRT; the 3-year OS rates of CCRT with cisplatin-based chemotherapy were reported to be 20–30% (13). Although CCRT is superior to radiotherapy alone in improving survival, increasing toxicity must be considered (20,21). To improve treatment outcomes, CCRT with S-1 was administered to patients with advanced oral SCC. In this series, the 3-year OS rate was 37%. Particularly in the 25 patients without ENI, the 3-year OS and PFS rates were 50 and 43%, respectively. These outcomes were similar to or better than the results achieved with standard CCRT using continuous drug infusion, suggesting that CCRT with S-1 may be a feasible alternative treatment.

When nodal involvement at uncommon levels is classified as ENI, the nodal classification based on the neck node level may be a better predictor compared with the UICC/AJCC criteria; the finding of ENI should be taken into account for comparing clinical trials. As the neck node level descends from the submandibular to the supraclavicular region, nodal involvement was considered primarily at levels Ib and II and involvement at levels III–V was defined as inferior extension. The incidence of nodal involvement at level Ia had not been elucidated, as the majority of previous studies on the distribution of nodal involvement did not subdivide level I into Ia and Ib. Otherwise, level I was considered to be only submandibular nodes (level Ib) (22). Woolgar reviewed 439 patients who underwent neck dissection for oral or oropharyngeal cancer and reported no cases with isolated involvement at level Ia (23). Lymphatic drainage from organs follows several pathways that include main collection and alternative routes (11). These findings support the findings of the present study and level Ia is considered to be an uncommon site representing an alternative route due to the involvement at more common levels.

This retrospective study had certain limitations. Pathological confirmation of the nodal status could not be obtained, as our patients underwent CCRT after clinical staging based on radiological examinations. However, up-to-date radiological examinations may yield a correct determination of nodal involvement (15,16). This study included several elderly patients (median age, 79 years). Intercurrent diseases affect the treatment outcomes and our retrospective study may have included patients treated with palliative intent. Despite these limitations, CCRT with S-1 is feasible and effective in patients with advanced oral SCC. Our study population consisted of inoperable patients with stage III or IV oral SCC. Therefore, node-negative patients had unresectable T3 or T4 tumors, whereas T1 and T2 tumors had nodal involvement. The selection bias may provide no correlation between the UICC/AJCC criteria and survival. Although our data demonstrated that a finding of ENI, i.e., nodal involvement at uncommon levels, is of prognostic relevance, the criteria of ENI should be assessed for each primary site of head and neck SCCs with different lymphatic pathways. Prospective studies are required to validate the treatment outcomes of CCRT with S-1 and the prognostic impact of the nodal classification based on the neck node level.

Acknowledgements

The present study was supported by the Japan Society for the Promotion of Science KAKENHI (grant no. 25461918).

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Murakami R, Semba A, Kawahara K, Matsuyama K, Hiraki A, Nagata M, Toya R, Yamashita Y, Oya N, Nakayama H, Nakayama H, et al: Concurrent chemoradiotherapy with S‑1 in patients with stage III‑IV oral squamous cell carcinoma: A retrospective analysis of nodal classification based on the neck node level. Mol Clin Oncol 7: 140-144, 2017
APA
Murakami, R., Semba, A., Kawahara, K., Matsuyama, K., Hiraki, A., Nagata, M. ... Nakayama, H. (2017). Concurrent chemoradiotherapy with S‑1 in patients with stage III‑IV oral squamous cell carcinoma: A retrospective analysis of nodal classification based on the neck node level. Molecular and Clinical Oncology, 7, 140-144. https://doi.org/10.3892/mco.2017.1276
MLA
Murakami, R., Semba, A., Kawahara, K., Matsuyama, K., Hiraki, A., Nagata, M., Toya, R., Yamashita, Y., Oya, N., Nakayama, H."Concurrent chemoradiotherapy with S‑1 in patients with stage III‑IV oral squamous cell carcinoma: A retrospective analysis of nodal classification based on the neck node level". Molecular and Clinical Oncology 7.1 (2017): 140-144.
Chicago
Murakami, R., Semba, A., Kawahara, K., Matsuyama, K., Hiraki, A., Nagata, M., Toya, R., Yamashita, Y., Oya, N., Nakayama, H."Concurrent chemoradiotherapy with S‑1 in patients with stage III‑IV oral squamous cell carcinoma: A retrospective analysis of nodal classification based on the neck node level". Molecular and Clinical Oncology 7, no. 1 (2017): 140-144. https://doi.org/10.3892/mco.2017.1276