Oligo-recurrence predicts favorable prognosis of brain-only oligometastases in patients with non-small cell lung cancer treated with stereotactic radiosurgery or stereotactic radiotherapy: a multi-institutional study of 61 subjects

The patients in the current study were treated with SRS or SRT for brain-only NSCLC oligometastases at six university hospitals or major cancer centers (Kitasato University Hospital, Hokkaido University Hospital, Shizuoka Cancer Center, Cancer and Infectious Diseases Tokyo Metropolitan Komagome Hospital, Kyushu University Hospital, and Tohoku University Hospital) between 1996 and 2008. All institutional review boards approved this study (Ethics Committee of Kitasato University School of Medicine (B), Instittutional Review Board of Hokkaido university Hospital for Clinical Research, Ethics Committee of Shizuoka Cancer Center, Ethical Committee of Tokyo Metropolitan Komagome Hospital, Kyushu University Institutional Review Board for Clinical Research, Ethics Committee of Tohoku University Graduate School of Medicine). This study is retrospective. Thus, informed consent of all patients could not be acquired. Then, all institutions engaged in this study announced this study on the web and/or posters at the out-patients clinics at each hospital. If targeted patients would not like to engage in this study, they would convey their refusal to the researchers by face to face, telephone or e-mail. However, no patients proposed not to engage in this study.

Of the following criteria, eligible patients met 1), 2), and 4) or 1), 3), and 4): 1) NSCLC with 1 to 4 brain metastases detected by magnetic resonance imaging (MRI) treated with SRS or SRT; 2) control of the primary lesions (thorax) at the time of SRS or SRT for brain metastases (patients meeting this criterion formed the oligo-recurrence group); 3) with SRS or SRT for brain metastases, concomitant treatment for active primary lesions (thorax) with curative surgery or curative SBRT or curative chemoradiotherapy for primary lesions (sync-oligometastases group, where “sync” indicates “synchronous”) [7, 9]; 4) Karnofsky performance status (KPS) ≥70. The exclusion criteria were: 1) NSCLC with five or more brain metastases detected by MRI; and 2) NSCLC with 1 to 4 brain metastases for which surgery was previously performed.

・We compared the characteristics of oligo-recurrence group and sync-oligometastases.

There were no statistically differences among these two groups as following.

Head rings were attached to the NSCLC patients and fixed to the linear accelerator during SRS. The SRS dose prescription was given at the tumor peripheral margin (GTV + 1 mm = CTV, CTV + 1 mm = PTV) (PTV peripheral dose).

NSCLC patients were treated with SRT while fixed to the linear accelerator by head and face shells. The SRT dose prescription was given at the tumor peripheral margin (GTV + 1 mm = CTV, CTV + 2 mm = PTV) (PTV peripheral dose). SRT was delivered in 4 to 5 fractions.

Because patients in the oligo-recurrence group had controlled primary lesions, no further treatments of thoracic lesions were performed in this group until thoracic relapse. However, the sync-oligometastases group had active thoracic lesions. Therefore, in this group, the thoracic lesions were treated with curative surgery, SBRT (cT1N0M1BRA) and concurrent chemoradiotherapy, or with curative radiation therapy alone. SBRT was mainly performed using 48 Gy/4 fractions (isocenter dose) to the small primary lung cancer. Concurrent chemoradiotherapy and curative radiation therapy alone were mainly performed using 60 Gy/30 fractions (in all cases, the spinal cord dose was under 40 Gy).

In general, the treatment strategy was to attempt to target all gross malignant tumors.

Overall survival (OS), relapse-free survival (RFS), local control of brain metastases (Brain-LC), cranial local control (Cranial–LC), and local control of thoracic lesions (Thoracic-LC) were calculated by the Kaplan-Meier method.

Overall survival was calculated from the date of the start of SRS or SRT for brain metastases, and an event was defined as any death. Relapse-free survival (RFS) was also calculated from the date of the start of SRS or SRT for brain metastases, and the events were defined as any site of relapse and any death. Local control of brain metastases (Brain-LC) was calculated from the date of the start of SRS or SRT for brain metastases, and the event was defined as more than 25 % regrowth (diameter) of brain metastases treated with SRS or SRT. Thus, the emergence of new lesions in the brain was not counted as an event when calculating Brain-LC. Cranial local control (Cranial-LC) was also calculated from the date of the start of SRS or SRT for brain metastases, and the events were any type of cranial relapse, including at the sites of SRS or SRT treatment, as well as the emergence of new lesions in the brain regions not treated with SRS or SRT. Local control for thoracic lesions (Thoracic-LC) was calculated from the date of thoracic lesion control by surgery or SBRT and concurrent chemoradiotherapy. These dates were defined as the surgery date, and the initiation date of SBRT or concurrent chemoradiotherapy. An event was defined as any type of intrathoracic relapse.

For OS, Cranial-LC, Brain-LC, and Thoracic-LC, multivariate analyses were also performed using Cox proportional hazards models. The factors used in these analyses were defined as those that were significant (p < 0.05) or showed a nonsignificant trend toward significance (p < 0.25) on univariate analysis and clinically important factors such as RPA class, which was previously reported to be a prognostic factor for brain metastasis and is widely used for classification.

The median overall survival of all 61 patients reached 26 months (95 % CI: 17.5–34.5 months). The 2-year and 5-year OS rates were 60.7 and 15.2 %, respectively (Fig. 1).

The results of univariate analysis of prognostic factors for OS are shown in Table 3. Oligostatus (p = 0.001) and the number of metastatic or recurrent lesions (p = 0.031) were both significant prognostic factors. Oligostatus was a powerful factor (Fig. 2); the sync-oligometastases group achieved a median OS of 18 months (95 % CI: 14.8–21.2 months) and a 5-year OS of 0 %. On the other hand, the oligo-recurrence group achieved a median OS of 41 months (95 % CI: 27.8–54.2 months) and a 5-year OS of 18.6 %.

However, RPA, the most frequently used standard for the prediction of prognosis of patients with brain metastases, achieved no significance for OS of NSCLC oligometastases. RPA class I achieved a median OS of 30 months (95 % CI: 8.6–51.4 months), and RPA class II achieved a median OS of 25 months (95 % CI: 10.6–39.4 months) (p = 0.319). These results were almost identical (Fig. 3). Furthermore, newly proposed prognostic classification, GPA also achieved no significance for OS of NSCLC oligometastases. Intermediate Prognosis Group of GPA scoring 1.5–3.0 achieved a median OS of 26 months (95 % CI: 16.9–35.1 months), and Favorable Prognostic Group of GPA scoring 3.5–4.0 achieved a median OS 25 months (95 % CI: 0.0–51.8 months) (p = 0.577) These results were almost identical (Table 3). This was a very important finding of the current analysis. In addition, a multivariate analysis was performed using the factors that were found to be significant on univariate analysis (oligostatus, the number of metastatic or recurrent lesions), those that showed a nonsignificant trend toward significance (p < 0.25), and clinically important factors (RPA, histopathology, KPS score, interval to brain recurrence (DFI), thoracic stage). The results of multivariate analysis are shown in Table 4. Oligo-recurrence was extracted as the only independent prognostic factor (hazard ratio: 0.253; 95 % CI: 0.082–0.043) (p = 0.025).

The median relapse-free survival reached 10 months (95 % CI: 7.32–12.7 months), and the 2-year and the 5-year RFS rates were 30.3 and 6.6 %, respectively.

Cranial-LC for all patients achieved a median of 30 months (95%CI: 18.1–41.8 months), and 2-year Cranial-LC and 5-year Cranial-LC rates were 68.1 and 10.7 %, respectively. Univariate analysis of Cranial-LC was performed. There were no significant factors for prognosis in Cranial-LC. A Cox proportional hazards model multivariate analysis of Cranial-LC was performed using factors with a nonsignificant trend toward significance and clinically important factors (oligostatus, the number of brain metastases or recurrences, and whole brain irradiation). Multivariate analysis also found no significant factors.

Brain-LC of all patients achieved a median LC rate of not reached, and 2-year Brain-LC and 5-year Brain-LC rates were 80.3 and 66.3 %, respectively (Fig. 4). The results of univariate analysis of Brain-LC are described in Table 5. Histopathology (p = 0.017) and the maximum tumor diameter (≥3 cm) (p = 0.002) were significant prognostic factors. However, the relationship between histopathology and the maximum tumor diameter (<3 cm) was evaluated, and there was a correlation between histopathology and the maximum tumor diameter. Nine of 11 tumors with squamous cell carcinoma had a maximum tumor diameter <3 cm (81.8 %). On the other hand, 68 of 69 adenocarcinomas had a maximum tumor diameter <3 cm (98.6 %), and 6 of 9 NSCLCs with other histology had a maximum tumor diameter < 3 cm (66.7 %). Thus, adenocarcinoma tumors had a tendency to be smaller than squamous cell carcinoma or other NSCLC tumors. Histopathology was therefore excluded from the multivariate analysis, and maximum tumor diameter was included. The results of the Cox proportional hazards model multivariate analysis are shown in Table 6. The maximum tumor diameter showed a nonsignificant trend toward significance (the maximum tumor diameter was ≥3 cm; hazard ratio 3.81; 95 % CI: 0.95–15.3) (p = 0.059).

Thoracic-LC of all patients achieved a median LC rate of not reached, and 2-year Thoracic-LC and 5-year Thoracic-LC rates were 80.5 and 64.3 %, respectively. Univariate analysis of Thoracic-LC was performed. Only oligostatus (p = 0.035) and use of systemic chemotherapy (p = 0.022) were significant prognostic factors. However, the relationship between oligostatus and systemic chemotherapy was investigated, and a significant correlation between these two factors was found. In the oligo-recurrence group, 12 of 50 patients (24 %) underwent systemic chemotherapy. On the other hand, in the sync-oligometastases group, 7 of 11 patients (63.6 %) underwent systemic chemotherapy. Thus, systemic chemotherapy was excluded from the multivariate analysis. The multivariate analysis thus included only oligostatus and one clinically important factor (thoracic stage). Oligostatus was not an independent prognostic factor (hazard ratio for oligo-recurrence: 0.405; 95 % CI: 0.121–1.353) (p = 0.142).