Background
Small cell lung cancer (SCLC) is characterized by a high propensity for metastases and a poor prognosis, despite it being one of the most chemosensitive solid tumors unlike other types of lung cancer [
1]. 60–70% of patients with SCLC present with metastasis beyond a safe radiotherapy field that is defined as extensive disease (ED), and standard treatment for ED-SCLC patients is systemic chemotherapy with a median survival of about 8–12 months [
2‐
5]. Generally, SCLC patients with interstitial pneumonia (IP) has been excluded in previous clinical studies, and efficacy of cytotoxic chemotherapy for ED-SCLC patients with IP is unclear.
Cigarette smoking and occupational exposures are common contributors not only to lung cancer, especially SCLC, but also to IP [
6‐
9]. The prognosis of patients with IP is poor, and the mean duration from the diagnosis to death is nearly 3–5 years [
10,
11]. In patients with IP, the incidence rate of lung cancer was reported to be approximately 17–48% [
7‐
9]. On the other hand, approximately 15% of patients with lung cancer were diagnosed with IP [
6]. Moreover, in patients with lung cancer with IP, acute exacerbation (AE)-IP was frequently reported after cytotoxic chemotherapy [
12,
13]. and lung cancer with IP was considered as one of poor prognostic factors [
14]. In clinical practice, lung cancer patients with IP are often recommended best supportive care (BSC) alone without systematic chemotherapy, because of high frequency of AE-IP [
15].
Recently, it has been reported that the combination of platinum agents and etoposide for patients with ED-SCLC is feasible as first-line chemotherapy for patients with IP [
16]. However, the safety and efficacy of cytotoxic chemotherapy for ED-SCLC patients with IP remain unclear in clinical settings. This study aims to assess the efficacy of cytotoxic chemotherapy and evaluate clinical factors associated with development of AE-IP with cytotoxic chemotherapy in ED-SCLC patients with IP.
Discussion
This study suggested that systemic chemotherapy was a treatment option in patients with ED-SCLC with IP, although those patients had a high risk of developing AE-IP by cytotoxic drugs. To the best of our knowledge, this is first report demonstrating that high serum concentrations of LDH and CRP before initiating chemotherapy are unfavorable predictive factors for developing AE-IP in patients with ED-SCLC with IP. Togashi et al., reported that patients with SCLC complicated with IP were related with a prognostic factor [
14]. In their cohort, 53 of 122 patients were limited disease SCLC, for whom standard treatment is chemoradiotherapy. Chemoradiotherapy was not recommended for patients with IP to prevent acute exacerbation of IP. It is possible that differences in treatment affected prognosis. In our study, we analyzed 192 ED-SCLC and evaluated the efficacy of chemotherapy. We observed similar survival benefit between ED-SCLC with IP and that without IP. We suggest that systematic chemotherapy is a treatment option even for patients with ED-SCLC combined with IP.
When administering chemotherapy for SCLC patients with IP, clinicians must be wary of developing AE-IP, because patients with AE-IP had demonstrated high mortality in previous studies [
13,
17,
21,
22]. In our study, 7 of 31 patients (23%) with ED-SCLC with IP developed AE-IP. Regarding association between chemotherapy regimen and AE-IP, previous studies have revealed that amrubicin and irinotecan were associated with a high incidence of AE-IP in patients with IP [
23,
24]. In addition, a combination chemotherapy with platinum and etoposide is reported as the preferable first-line chemotherapy regimen for patients with SCLC with IP [
16,
17]. In our study, a majority of patients with IP (
n = 28 of 31) received carboplatin plus etoposide in the all courses of chemotherapy, and 4 (14%) patients developed AE-IP, similar to those previously reported [
13,
17]. Although amrubicin is a potential agent for the treatment of ED-SCLC as a second-line setting, [
25,
26] high incidence of AE-IP induced by amrubicin was reported among SCLC patients with IP, [
23] so AE-IP associated with amrubicin is an issue. In all courses of chemotherapy in our study, 8 patients with IP received amrubicin, and 3 patients (38%) developed AE-IP. On the other hand, 111 patients without IP received amrubicin, and 1 patient (1%) developed AE-IP. This data suggested a high incidence of AE-IP in patients with ED-SCLC with IP treated with amrubicin. For ED-SCLC patients with IP, a combination chemotherapy with platinum and etoposide in the first-line chemotherapy is preferable to prevent developing AE-IP.
The pathogenesis of AE-IP by cytotoxic drugs is poorly understood. However, most toxic effects are thought to result from direct cytotoxicity. Active oxygen or either a growth factor, inflammatory cytokine or vascularization factor localized in a part of the lung plays an important role in inducing inflammation, and it is also known that values for these factors increase temporarily after chemotherapy [
27]. Inflammation induced by these factors is considered one of the reasons underlying the development of AE-IP. The increase in the levels of these cytokines may correlate with IP activity and, thus, with active inflammation [
28,
29]. KL-6 and SP-D are known sensitive biomarkers for IP, but there is no consensus of predictive markers for AE-IP although these have been reported previously [
13,
30]. We investigated the significance of KL-6 and SP-D as predictors of AE-IP in ED-SCLC patients treated with chemotherapy and found no statistically significant difference between those who did and did not experience acute exacerbation. Minegishi et al. reported that a high serum concentration of CRP before initiation of chemotherapy was associated with a significant likelihood of a patient developing AE-IP[
13]. By comparing between patients with IP who had AE-IP and patients with IP who did not have AE-IP, we demonstrated that the pretreatment serum levels of LDH and CRP were significantly higher in ED-SCLC patients with IP who developed AE-IP than those who did not develop AE-IP. Among seven patients developed AE-IP, six patients had high LDH (> 275 IU/L; median in ED-SCLC patients with IP) and six patients had high CRP (> 1.51 mg/dl; median in ED-SCLC patients with IP). It was indicated that a high serum concentration of LDH or CRP before initiation of chemotherapy was associated with a significant likelihood of a patient with IP developing AE-IP by cytotoxic drugs (LDH: sensitivity 87%, specificity 63%; CRP: sensitivity 87%, specificity 58%). It is possible that high inflammatory IP is highly activated due to stimulation of cytotoxic drugs and is more likely to cause AE-IP, but the details remain unclear.
In our study, approximately 69 (53.1%) patients without IP and 4 (12.9%) patients with IP received AMR in the initial chemotherapy. Among ED-SCLC without IP, AMR was selected for elderly patients and those with renal dysfunction, SVC syndrome, and poor PS in our clinical practice; thus, ED-SCLC patients without IP might have relatively poor OS compared to patients in previous clinical trials [
30]. Additionally, we compared the OS of ED-SCLC patients with and without IP between the group that received platinum doublet or the group that underwent AMR (Additional file
1: Figure S1). Among ED-SCLC patients who received platinum-based chemotherapy in the initial chemotherapy, the OS of patients with IP (
n = 27) was similar to the OS of those without IP (
n = 60) (11.8 [95% CI: 8.9–14.7] vs. 8.7 [95% CI: 0.4–17.0] months;
P = 0.93; Additional file
1: Figure S1-a). Regardless of the type of initial chemotherapy, the prognosis of ED-SCLC patients with IP may be somewhat poor compared with the prognosis of those without IP. Less choices of therapeutic agents and occurrence of AE-IP can be attributed to this difference. In our study, secondary chemotherapy transfer rates were 59.2 and 35.5% for patients without and with IP, respectively. Among ED-SCLC patients with IP, patients who developed AE-IP showed a poor significantly prognosis compared with those who did not develop AE-IP (4.4 [95% CI: 1.0–7.8] vs. 13.2 [95% CI: 2.1–24.3] months;
P = 0.020; Additional file
2: Figure S2). The OS of ED-SCLC patients with IP who did not develop AE-IP was not different from the prognosis of ED-SCLC patients without IP (10.0 [95% CI: 8.2–11.8] months;
P = 0.173; Additional file
2: Figure S2). Therefore, preventing AE-IP is crucial, and the activity of IP combined with ED-SCLC should be validated using pretreatment markers, such as levels of LDH and CRP, for assessing the risk of developing AE-IP. Early recognition and symptomatic support of acute exacerbation may improve outcomes in these patients.
Finally, this study has certain limitations. First, this was a retrospective study conducted in a single institution; hence, the results cannot be completely regarded as definitive. Second, all our patients were diagnosed with IP using HRCT imaging and laboratory findings, but not based on pathological findings. In the clinical practice, diagnosis of the AE-IP based on clinical and radiological findings is challenging. Thus, we cannot entirely exclude the possibility that our patients had developed lymphangitic carcinomatosis, pneumonitis, various infectious diseases, congestive heart failure, thromboembolism or some other disease, rather than AE-IP.