Pretreatment Neutrophil-to-Lymphocyte Ratio and Smoking History as Prognostic Factors in Advanced Non–Small Cell Lung Cancer Patients Treated with Osimertinib
Article information
Abstract
Background
The remarkable efficacy of osimertinib in non‒small cell lung cancer (NSCLC) with acquired T790M mutation has been widely documented in clinical trials and real-world practice. However, some patients show primary resistance to this drug. Even patients who initially show a favorable response have inconsistent clinical outcomes later. Therefore, the aim of this study was to identify additional clinical predictive factors for osimertinib efficacy.
Methods
A prospective cohort of patients with acquired T790M positive stage IV lung adenocarcinoma treated with osimertinib salvage therapy in Hallym University Medical Center were analyzed.
Results
Sixty-one eligible patients were analyzed, including 38 (62%) women and 39 (64%) who never smoked. Their mean age was 63.3 years. The median follow-up after treatment with epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) was 36.0 months (interquartile range, 24.7–50.2 months). The majority (n=45, 74%) of patients were deceased. Based on univariate analysis, low baseline neutrophil-to-lymphocyte ratios (NLR), age ≥50 years, never-smoking history, stage IVA at osimertinib initiation, and prolonged response to previous TKIs (≥10 months) were associated with a significantly longer progression-free survival (PFS). Multivariate analysis showed that never-smoking status (hazard ratio [HR], 0.54; 95% confidence interval [CI], 0.30–0.98; p=0.041) and a baseline NLR less than or equal to 3.5 (HR, 0.23; 95% CI, 0.12–0.45; p<0.001) were independently associated with a prolonged PFS with osimertinib.
Conclusion
Smoking history and high NLR were independent negative predictors of osimertinib PFS in patients with advanced NSCLC developing EGFR T790M resistance after the initial EGFR-TKI treatment.
Introduction
The discovery of epidermal growth factor receptor (EGFR) mutations and EGFR tyrosine kinase inhibitors (TKIs) has changed the paradigm of non‒small cell lung cancer (NSCLC) treatment. The efficacy of TKIs in EGFR mutation‒positive NSCLC has been well established [1,2]. However, although some patients respond well to EGFR-TKIs, some exhibit little or no response, even when they are positive for EGFR-sensitizing mutations. Moreover, some patients show good long-term effects, whereas others develop resistance after a short-term response [3]. The prognosis for patients with EGFR mutations administered with EGFR-TKI therapy could be partially predicted using clinical factors such as female sex, non-smoker status, and Asian race, which are considered as good predictors before the introduction of EGFR mutation testing [1].
NSCLC cells can become resistant to first- and second-generation EGFR-TKIs after approximately one year of treatment [4]. The most common underlying mechanism is the acquired EGFR T790M gatekeeper mutation in exon 20, which accounts for approximately half of cases resistant to EGFR-TKIs [4]. Osimertinib, a third-generation irreversible EGFR-TKI, can selectively inhibit EGFR-TKI‒sensitizing and T790M resistance mutations [5]. The AURA3 study has demonstrated a better efficacy of osimertinib in patients with acquired EGFR T790M mutation NSCLC than platinum plus pemetrexed chemotherapy [5]. Subsequently, this drug was approved in several countries. It is currently used as salvage treatment in patients with the EGFR T790M mutation.
Patients with the acquired EGFR T790M mutation also respond differently to osimertinib treatment. Therefore, there is a need to elucidate the mechanism and analyze prognostic factors for different responses [6,7]. In addition, predictors for response to osimertinib other than the T790M mutation remain unclear. Therefore, the objective of this study was to analyze relationships between clinical factors and osimertinib efficacy in NSCLC patients with the acquired EGFR T790M mutation who were previously treated with EGFR-TKIs.
Materials and Methods
1. Study population and design
Data of a cohort of patients with lung adenocarcinoma from the Lung Cancer Registry of Hallym University Medical Center between January 2006 and August 2021 were analyzed. Inclusion criteria were as follows: (1) stage IV lung adenocarcinoma according to the 8th edition of the American Joint Commission on Cancer TNM staging system, (2) previous treatment with first-generation EGFR-TKIs (gefitinib or erlotinib) or second-generation EGFR-TKIs (afatinib) with EGFR-sensitive mutation, (3) acquired EGFR T790M resistance mutation after EGFR-TKI treatment, and (4) osimertinib as a salvage treatment. Host-related factors were age at lung cancer diagnosis, sex, Eastern Cooperative Oncology Group (ECOG) performance status score at osimertinib initiation, and smoking status. Tumor-related factors were primary EGFR mutations, previous EGFR-TKIs, response to previous EGFR-TKIs, and serum neutrophil-to-lymphocyte ratio (NLR) at osimertinib initiation. Blood test results used for the analysis were obtained immediately before osimertinib initiation without showing any symptoms of infection. Patients aged less than 50 years were included in the young-age group. This criterion was based on previous studies on young-age early-onset lung cancer [8,9]. ECOG scores of 0 and 1 were defined as good performance status. Patients who had a previous EGFR-TKI treatment with progression-free survival (PFS) of less than ten months were defined as poor responders [10]. We evaluated the optimal NLR cutoff value for PFS with osimertinib treatment via a receiver operating characteristic curve (area under the curve, 0.741; confidence interval, 0.60–0.88). We selected the NLR cutoff value as 3.5 with the best sensitivity (0.75) and specificity (0.67) based on similar values indicated in previous studies [11,12].
We evaluated tumor response and disease progression every 8 weeks per cohort protocol. If necessary, radiologic evaluations were conducted to assess responses according to the clinician’s judgment, even within this period. Evaluation of responses to EGFR-TKIs was performed by retrospective review of radiologic images of the entire case by two experienced investigators based on the Response Evaluation Criteria in Solid Tumor (RECIST) v1.1 criteria. The attending physician’s evaluation or decision was not included in the efficacy evaluation. We defined PFS as the period from osimertinib initiation to the date of disease progression or death from any cause. Baseline clinical factors were analyzed according to favorable or unfavorable (primary resistant) efficacy group. The favorable efficacy group was defined as those with a PFS of greater than or equal to 6 months with osimertinib treatment. The unfavorable efficacy group was defined as those with a PFS of less than 6 months with osimertinib treatment. The criterion of 6 months was based on the AURA3 study, in which the lower quarter of patients showed a PFS of less than 6 months [5]. Overall survival (OS) was calculated as the time from osimertinib initiation to death from any cause or censorship at the last follow-up. If progression occurred after first-line EGFR-TKI treatment, then biopsy was repeated, if possible. The PNAClamp EGFR mutation detection kit (Panagene, Daejeon, Korea), a peptide nucleic acid-mediated real-time PCR clamping technology, was used to detect acquired EGFR mutations [13]. When tissue-based assays were not feasible, plasma EGFR T790M mutation tests were performed using a Cobas EGFR mutation test v2 (Roche, Pleasanton, CA, USA). If T790M mutation was not detected by one method, another method was employed. However, this was not mandatory. The Institutional Review Board of Hallym University Sacred Heart Hospital approved the study protocol and informed consent was waived owing to the retrospective nature of the study (HALLYM 2020-03-016-001). All methods were carried out in accordance with the approved guidelines and regulations (Declaration of Helsinki).
2. Statistical analysis
Categorical variables were statistically analyzed using Fisher’s exact test. Continuous variables were analyzed using Student’s t-tests or Mann-Whitney U-tests. We used Kaplan-Meier estimates to construct survival curves and calculate median PFS and OS. Cox regression methods (univariate and multivariate) were used to estimate prognostic factors for PFS and OS by adjusting baseline characteristics. All analyses were performed using SPSS Statistics for Windows, version 26.0 (IBM Corp., Armonk, NY, USA).
Results
1. Baseline characteristics
Sixty-one patients with acquired EGFR T790M mutation were enrolled. All patients were followed up until August 20, 2021. They all had histologically confirmed lung adenocarcinoma with EGFR-sensitizing mutations. They were treated with gefitinib, erlotinib, or afatinib until disease progression, at which point they were treated with osimertinib. Clinical characteristics of the study patients are summarized in Table 1. Their mean age was 63.3±11.9 years. There were 38 women (62%) and 39 never-smokers (64%). At osimertinib treatment initiation, 17 (28%) and 44 (72%) patients had disease stages IVA and IVB, respectively. Central nervous system metastasis was present in 24 patients (39%) at osimertinib treatment initiation. Forty patients (66%) initially had EGFR exon 19 deletions and 21 (34%) had an EGFR exon 21 mutation (L858R, 20 patients; L861Q, one patient) before their first EGFR-TKI treatment, whereas none of these patients had a de novo EGFR T790M mutation. The mean baseline NLR at osimertinib treatment was 4.4±3.2. Twenty-six patients (43%) had a high NLR (>3.5).
2. Osimertinib treatment outcomes
The EGFR T790M mutation was identified in 43 patients by tissue re-biopsy (plasma T790M negative, 7/43; plasma test not performed, 36/43) and in 18 patients by plasma sampling (re-biopsy tissue negative, 6/18; re-biopsy not performed, 12/18). Thirty-one (51%) and 30 (49%) patients received osimertinib and cytotoxic chemotherapy as second-line therapy, respectively, followed by osimertinib as third- to eighth-line treatments. With osimertinib treatment, 39 (64%) achieved partial response (PR), 15 (25%) had stable disease (SD), and seven (11%) had progressive disease (PD). At data cutoff, 50 patients (82%) had PD. The overall median PFS following osimertinib treatment was 9.3 months (95% confidence interval [CI], 6.7–11.9 months). Supplementary Table S1 presents a comparison of clinical characteristics of patients with PFS with osimertinib treatment for less than 6 months (unfavorable group) or higher than or equal to six months (favorable group). The baseline NLR at the commencement of osimertinib treatment was higher in the unfavorable group than in the favorable group (5.8±3.9 vs. 3.5±2.3, p=0.016). However, no significant differences in other clinical factors were observed among predefined groups.
3. Clinical factors associated with PFS with osimertinib
Figure 1 shows results of univariate analysis of clinical factors for PFS with osimertinib. The median PFS was significantly longer in patients with a low NLR (≤3.5) at the start of osimertinib treatment than in those with a high NLR (>3.5) (12.3 months vs. 5.7 months, p<0.001). In addition, old age (≥50 years), non-smoking history, stage IVA at osimertinib initiation, and prolonged response to previous TKIs (≥10 months) were associated with a significantly longer PFS (p<0.05). Female sex and good performance (ECOG score, 0–1) were also associated with a prolonged PFS trend, although the result was not significant (p<0.1). Corresponding to the T790M detection method, the median PFS of osimertinib was 3.5 months in the tissue negative/plasma positive group, which was significantly shorter than that in other groups (tissue unknown/plasma positive, 9.4 months, p=0.034; tissue positive/plasma unknown, 9.3 months, p=0.009; and tissue positive/plasma negative, 14.4 months, p=0.010).
Table 2 shows results of analysis using the Cox proportional model of osimertinib PFS. Covariates of multivariate analysis were selected using log-rank tests for the Kaplan-Meier estimation of PFS (p<0.1). The analysis showed that a never-smoking status (hazard ratio [HR], 0.54; 95% CI, 0.30–0.98; p=0.041) and a baseline NLR less than or equal to 3.5 (HR, 0.23; 95% CI, 0.12–0.45; p<0.001) were independent and good predictive factors for PFS after osimertinib treatment (Figure 2). However, there were no differences in clinical characteristics between the PR group and the SD/PD group (Supplementary Table S2).
4. OS after osimertinib treatment
Forty-five patients (74%) were deceased by the end of the study. The median OS of all patients was 17.5 months (95% CI, 13.4–21.5 months) after osimertinib treatment. The univariate analysis showed that patients with a good performance status (ECOG 0–1), low baseline NLR (≤3.5), and stage IVA at osimertinib initiation had significantly longer OS (Figure 1). Corresponding to T790M detection methods, the median OS was 4.8 months in the tissue negative/plasma positive group, which was significantly shorter than that in other groups (tissue positive/plasma unknown, 17.5 months, p=0.005; tissue positive/plasma negative, the median OS was not reached). Multivariate Cox regression analysis revealed that performance status and NLR were independent prognostic factors for OS (ECOG 0–1: HR, 0.35; 95% CI, 0.18–0.67; p=0.002; low NLR: HR, 0.17; 95% CI, 0.09–0.34; p<0.001) (Table 3).
Discussion
This real-world study showed that osimertinib PFS in patients with acquired T790M mutation after primary EGFR-TKI treatment was shortened by a smoking history and a high baseline NLR. In addition, NLR was an independent prognostic factor for OS after osimertinib treatment together with ECOG performance status.
EGFR mutations in advanced stage NSCLC are powerful markers for screening patients with the corresponding driving mutation and predicting the efficacy of EGFR-TKI [14]. On the other hand, among patients with EGFR mutations, 20%–30% develop primary resistance to EGFR-TKI therapy [14,15]. Therefore, additional factors that may determine the prognosis of EGFR-TKIs are continuously being studied. Recently, as the accessibility of genetic profiling has increased, some studies have suggested that co-mutations in genes other than EGFR are essential for determining the therapeutic response [14,15]. Furthermore, the authors have reported that the EGFR-TKIs efficacy decreases when there is a concomitant mutation, particularly with more mutations or a specific type of mutation (e.g., an oncogene mutation) related to a poor outcome [14,15]. Therefore, determining which clinical characteristics in these groups might provide clues to elucidate the complicated carcinogenesis of EGFR lung cancer and select these patients for more individualized treatment is essential.
Results of studies on clinical factors related to first- and second-generation EGFR-TKIs efficacy are as follows. A subgroup analysis of randomized clinical trials (RCTs) comparing EGFR-TKIs to cytotoxic chemotherapy indirectly has revealed prognostic factors of the efficacy of EGFR-TKI treatment in EGFR mutation‒positive NSCLC. In the IPASS study (gefitinib vs. carboplatin-paclitaxel), gefitinib prolonged the PFS in the older subgroup (≥65 years) more significantly than in the younger subgroup [1]. In the LUX-lung 3 trial (afatinib vs. pemetrexed plus cisplatin), significantly longer PFS and OS with afatinib were observed in patients with the EGFR 19del mutation than in those with the L858R mutation [2,16]. A meta-analysis of seven RCTs, including this trial, confirmed the benefit of EGFR-TKI regardless of past smoking history, but showed a more significant prolongation of PFS in never-smokers by meta-regression analysis [17]. However, because these were results from a subgroup analysis of TKIs efficacy compared to cytotoxic agents, the prognostic evaluation based on specific clinical factors had limitations. On the other hand, previous real-world studies analyzing patients receiving EGFR-TKIs only did not show consistent prognostic factors. Although there was a problem with the small number of subjects, other reasons were the inclusion of cases with unconfirmed EGFR mutations, the omission of important prognostic factors, and inconsistent EGFR test methods or treatment processes within one study [18,19]. However, well-designed recent studies have reported that smoking history can affect the efficacy of first-and 2nd-generation TKIs through multivariate analysis [20-22].
The T790M mutation was confirmed in about half of cases where resistance developed after EGFR-TKI treatment. Based on results of the AURA3 trial, 6.5% of patients with the acquired EGFR T790M mutation showed rapid progression after osimertinib treatment [5]. In a subgroup analysis, no specific clinical factors were associated with osimertinib efficacy. However, the AURA3 trial did not represent all real-world patients (only patients with an ECOG score of 0–1 were enrolled; 96% of patients were treated with osimertinib as second-line after first-line TKIs). A retrospective real-world study by Kato et al. [6] have reported that an older age and an ECOG score of 0–1 are good predictors for PFS after osimertinib treatment in 30 patients with the acquired EGFR T790M mutation. Yoshimura et al. have reported that a prolonged PFS history with previous EGFR-TKIs is a predictive factor for subsequent osimertinib treatment among 27 patients [7]. Similar to previous generation TKI studies, each study showed different results. Therefore, similar to previous studies, the leading cause of the heterogeneity was the small case number. However, factors that were non-significant in our multivariate analysis tended to be prognostic factors in univariate analysis, consistent with those previous reports. Interestingly, Chang et al. [23] have recently reported that osimertinib efficacy is diminished in a group of patients who have a complex mutation apart from the T790M mutation.
EGFR mutations are more frequently identified in NSCLC in non-smokers. However, approximately 30% of mutation-positive patients are reported to have a smoking history [20]. In our study, the low efficacy of osimertinib in patients with a history of smoking might indicate that inhibition of EGFR activation alone does not entirely block the carcinogenesis pathway. Smoking can induce various genetic alterations in lung cancer. The most frequently observed co-occurring alteration with EGFR mutations is TP53 mutation, which is highly related to smoking. The effect of TP53 mutation on the EGFR-TKI therapy has been demonstrated in several clinical studies and preclinical studies [24]. Recently, Kim et al. [15] have reported a significantly reduced PFS and a worse OS of osimertinib treatment in patients with acquired T790M mutation with a TP53 accompanying mutation. A preclinical study has reported that cigarette smoke extract (CSE) and tobacco smoke-derived carcinogen can upregulate the c-MET pathway, which induces resistance to EGFR-TKI in 19del mutation cell lines [25]. Ahn et al. [26] have shown that c-MET amplification in re-biopsy histology is associated with previous smoking history in the case of progression after EGFR-TKI treatment. Li et al. [27] have reported that CSE can inhibit the effect of EGFR-TKIs through Src activation and epithelial to mesenchymal transition. The above results are also consistent with next-generation sequencing data showing that a higher tumor mutation burden can lead to lower EGFR-TKI responses [28].
Additional studies have identified relationships between systemic inflammation and tumorigenesis factors such as tumor angiogenesis, invasion, and metastasis [29,30]. Tumor-related inflammation is correlated with neutrophilia, lymphopenia, or both in peripheral blood. It is also associated with a poor prognosis in patients with various carcinomas [31]. In addition, neutrophils play a role as a metastasis promoter by trapping and migrating tumor cells using extracellular traps [32]. Moreover, tumor-associated neutrophils may support tumor angiogenesis and invasion by producing matrix metalloproteinase-9 and vascular endothelial growth factors [32]. Previous reports have suggested that an elevated NLR is a useful prognostic biomarker in early [33], locally advanced [34], and advanced stages of lung cancer [35], as well as various treatment modalities in lung cancer patients [36,37]. In a small number of studies, a high NLR is also an independent poor prognostic marker for PFS or OS after first- or second-generation EGFR-TKI treatment [12,38]. To the best of our knowledge, our study is the first to report that NLR elevation is correlated with poor osimertinib efficacy in patients with acquired T790M mutation.
We found osimertinib to have inconsistent efficacy in the univariate analysis, varying according to different T790M detection methods. Previously, in the post-hoc analysis of plasma samples from the phase I AURA trial, the PFS of osimertinib in the tissue T790M negative/plasma T790M positive group was shorter than that in the tissue positive/plasma positive group (4.2 months vs. 9.3 months, p=0.002) [39]. In another retrospective study, the tissue negative/plasma positive group showed a poor objective response rate of only 7.6% [40]. Tumor heterogeneity might explain this discrepancy. It could be assumed that different resistance mechanisms for previous EGFR-TKIs occurred in multiple metastatic tumors in the same patient [41]. On the other hand, the tissue positive/plasma negative group showed the most prolonged PFS in our study, although such result did not reach statistical significance. In the AURA3 trial (all subjects must have confirmation of re-biopsy tissue T790M mutation), the PFS in tissueand plasma circulating tumor DNA (ctDNA)- T790M positive subgroup was approximately two months shorter than that of patients in the intention-to-treat population (8.2 months vs. 10.1 months) [5]. Hong et al. [40] have also reported a better efficacy in the tissue positive/plasma negative group. The absence of plasma ctDNA of T790M mutation in systemic circulation may mean that metastasis is indolent [40]. Interestingly, in our study, the high NLR was found in one of seven patients (14.3%) in the tissue positive/plasma negative group and four of six patients (66.7%) in the tissue negative/plasma positive group. Further studies are needed to determine the relationship of ctDNA with peripheral blood NLR in lung cancer.
Regarding the effect of age on PFS with subsequent osimertinib treatment, Kato et al. [6] have found that an older age is a good independent prognostic factor. In our study, the age factor showed a difference in univariate analysis. No known biological or other mechanism explained the difference in the effect of EGFR-TKIs depending on age groups. In a previous report, uncommon EGFR mutations, which have lower EGFRTKI response rates, are more prevalent in a young-age group [42]. However, this hypothesis could not be applied to the study by Kato et al. [6], in which there were two uncommon mutations at old age.
Limitations of our study include its retrospective nature and the relatively limited number of patients. However, we could reduce some bias and minimize missing data because the same protocol was used for diagnostic testing and treatment within a prospective lung cancer cohort. Moreover, the observation period was sufficiently long. We were able to analyze survival data, which were highly maturated. During the response evaluation of EGFR-TKIs, the investigators were not blinded to other clinical features or laboratory results. To overcome this limitation, independent investigators, other than an individual patient’s treating physician, reviewed the radiologic images of all cases and re-evaluated the response strictly according to the RECIST criteria. Lastly, there are limitations in interpreting results of prognosis according to T790M detection methods because several confounding factors acted in selecting T790M test methods. In addition, both tissue biopsy and plasma tests were not routinely performed for all patients.
Smoking history and a low NLR were found to be associated with good outcomes with osimertinib treatment in patients with NSCLC developing EGFR T790M resistance after the initial EGFR-TKI treatment. Furthermore, a poor performance status and high NLR were poor prognostic factors for OS in these patients. Additional large-scale studies are needed to validate these results.
Notes
Authors’ Contributions
Conceptualization: Park JY, Jang SH. Formal analysis: Lee CY, Kim T, Chung SJ, Lee YJ. Data curation: Park JY, Jang SH, Lee CY, Kim T, Chung SJ, Lee YJ, Kim HI, Kim JH, Park S, Hwang YI, Jung KS. Validation: Kim HI, Kim JH, Park S. Investigation: Lee CY, Kim T, Chung SJ, Lee YJ. Supervision: Jang SH, Hwang YI, Jung KS. Writing - original draft: Park JY, Jang SH. Writing - review and editing: Park JY, Jang SH, Lee CY, Kim T, Chung SJ, Lee YJ, Kim HI, Kim JH, Park S, Hwang YI, Jung KS. Approval of final manuscript: all authors.
Conflicts of Interest
Ki-Suck Jung serves as editor-in-chief of the Tuberculosis of Respiratory Diseases, but has no role in the decision to publish this article. All remaining authors have declared no conflicts of interest.
Funding
No funding to declare.
Supplementary Material
Supplementary material can be found in the journal homepage (http://www.e-trd.org).