Erlotinib as Neoadjuvant Therapy in Stage IIIA (N2) EGFR Mutation-Positive Non-Small Cell Lung Cancer: A Prospective, Single-Arm, Phase II Study.

LESSONS LEARNED: The findings of this prospective, single-arm, phase II study showed that neoadjuvant erlotinib was well tolerated and might improve the radical resection rate in patients with stage IIIA-N2 epidermal growth factor receptor mutation-positive non-small cell lung cancer (NSCLC).Erlotinib shows promise as a neoadjuvant therapy option in this patient population.Next-generation sequencing may be useful for predicting outcomes with preoperative tyrosine kinase inhibitors (TKIs) in patients with NSCLC.Large-scale randomized controlled trials investigating the role of TKIs in perioperative therapy, combining neoadjuvant and adjuvant treatments to enhance personalized therapy for patients in this precision medicine era, are warranted.
BACKGROUND: Information on epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) as neoadjuvant therapy in non-small cell lung cancer (NSCLC) is scarce. We evaluated whether neoadjuvant erlotinib improves operability and survival in patients with stage IIIA-N2 EGFR mutation-positive NSCLC.
METHODS: We conducted a prospective, single-arm, phase II study. Patients received erlotinib 150 mg per day for 56 days in the neoadjuvant period. The primary endpoint was the radical resection rate.
RESULTS: Nineteen patients were included in the final analysis. After erlotinib treatment, 14 patients underwent surgery. The radical resection rate was 68.4% (13/19) with a 21.1% (4/19) rate of pathological downstaging. The objective response rate was 42.1%; 89.5% (17/19) of patients achieved disease control, with a 10.3-month median disease-free survival among patients who underwent surgery. Among all 19 patients who received neoadjuvant therapy, median progression-free survival (PFS) and overall survival were 11.2 and 51.6 months, respectively. Adverse events (AEs) occurred in 36.8% (7/19) of patients, with the most common AE being rash (26.3%); 15.8% experienced grade 3/4 AEs. Quality of life (QoL) improvements were observed after treatment with erlotinib for almost all QoL assessments. Effects of TP53 mutation on prognosis were evaluated in eight patients with adequate tissue samples. Next-generation sequencing revealed that most patients had a TP53 gene mutation (7/8) in addition to an EGFR mutation. No TP53 mutation, or very low abundance, was associated with longer PFS (36 and 38 months, respectively), whereas high abundance was associated with short PFS (8 months).
CONCLUSION: Neoadjuvant erlotinib was well tolerated and may improve the radical resection rate in this patient population. Next-generation sequencing may predict outcomes with preoperative TKIs. © AlphaMed Press; the data published online to support this summary are the property of the authors.

Discussion

Patients with stage IIIA‐N2 NSCLC have a poor prognosis, especially those with EGFR mutations. Sufficient clinical benefit cannot be achieved with chemoradiotherapy without serious safety concerns. EGFR TKI therapy has shown good efficacy and favorable tolerability in patients with EGFR mutation‐positive NSCLC. The TKI erlotinib is approved for first‐line treatment of EGFR mutation‐positive NSCLC; however, its usefulness as neoadjuvant therapy in patients with resectable EGFR mutation‐positive NSCLC remains unclear.

We performed a single‐arm trial to evaluate whether neoadjuvant erlotinib improves operability and survival in patients with stage IIIA‐N2 EGFR mutation‐positive NSCLC. The primary endpoint was the radical resection rate, and the estimated sample size was 30 cases. Of 44 patients diagnosed with stage IIIA‐N2 NSCLC, 25 with EGFR mutation‐positive disease were enrolled. Subsequent retesting with improved sequencing technologies reduced the sample size to 19 patients after an additional 6 patients were excluded (4 were negative for EGFR mutation by amplification‐refractory mutation system polymerase chain reaction sequencing and 2 by next‐generation sequencing [NGS]).

Most patients were female (12/19, 63.2%), the median age was 59 (range, 33–74) years, and all patients had an Eastern Cooperative Oncology Group performance status of 1 and adenocarcinoma histology. After erlotinib treatment, 73.7% of patients (14/19) underwent surgery; the radical resection rate was 68.4% (13/19). Most patients who underwent surgery benefited from neoadjuvant treatment prior to surgical resection and achieved disease control of the target lesion. The objective response rate was 42.1% (8/19) with a 21.1% (4/19) rate of clinical downstaging to T0–3N0M0; 89.5% of patients (17/19) achieved disease control after neoadjuvant therapy (Figure 1). In patients who underwent surgery, postoperative pathology showed that seven patients (50.0%) achieved partial response, seven (50.0%) achieved stable disease, and no patients had progressive disease. Among patients who underwent surgery, median disease‐free survival calculated from the date of surgery and the date of neoadjuvant therapy was 10.3 months and 12.1 months, respectively. Among all patients who received neoadjuvant therapy, the median PFS and overall survival were 11.2 and 51.6 months, respectively.

Figure 1.

Waterfall plot of response to erlotinib neoadjuvant therapy. Bars show data from individual patients. Negative values suggest tumor shrinkage and positive values suggest PD; the dashed lines show the thresholds for a partial response (shrinkage by 30%) or for progressive disease (growth by 20%) according to RECIST criteria.

Abbreviation: PD, progressive disease.

To the best of our knowledge, this is the first study to evaluate the role of neoadjuvant EGFR TKI therapy with erlotinib in patients with stage IIIA‐N2 EGFR mutation‐positive NSCLC. Our findings are encouraging in view of the poor prognosis and limited treatment options available for patients with stage IIIA‐N2 NSCLC.

Trial Information

Lung cancer – NSCLC

Neoadjuvant

None

Phase II

Single arm

Radical resection rate

Pathological complete remission

Objective response rate

Disease‐free survival

Overall survival

Quality of life

Safety

Biomarkers (exploratory)

Drug Information

Erlotinib

Tarceva

Roche Pharmaceuticals

Small molecule

EGFR

150 milligrams (mg) per flat dose

Oral (po)

150 mg per day for two 4‐week cycles

Patient Characteristics

7

12

IIIA

Median (range): 59 (33–74) years

Median (range): 0 (treatement‐naive)

0 —

1 — 19

2 —

3 —

Unknown —

Smoking/nonsmoking: 7/12

Histology (adenocarcinoma), n = 19 (100%)

EGFR mutation (exon 19 deletion), n = 12 (63%)

EGFR mutation (exon 21 L858R mutation), n = 8 (42%)

Primary Assessment Method

155

19

19

19

RECIST version 1.1

n = 0 (0%)

n = 8 (42%)

n = 9 (47%)

n = 2 (11%)

n = 0 (0%)

11 months

52 months

Adverse Events

Serious Adverse Events

Assessment, Analysis, and Discussion

Study completed

Active and should be pursued further

Non‐small cell lung cancer (NSCLC) accounts for approximately 80% of all lung cancer cases and more than 15% of patients with NSCLC present with locally advanced clinical stage IIIA‐N2 disease [1]. Patients with stage IIIA‐N2 NSCLC whose tumors harbor epidermal growth factor receptor (EGFR) mutations are particularly challenging to treat and have a poor prognosis despite preoperative chemoradiotherapy [2]. Several phase III randomized controlled trials evaluated EGFR tyrosine kinase inhibitor (TKI) therapy in patients with EGFR mutation‐positive NSCLC and demonstrated good efficacy and a favorable tolerability profile for EGFR TKI therapy in these patients [3], [4], [5], [6], [7], [8], [9], [10], [11], [12]. Erlotinib was one of the first TKIs approved for the initial treatment of EGFR mutation‐positive NSCLC. In this setting, first‐line erlotinib therapy demonstrated superior efficacy over standard chemotherapy, with a more favorable tolerability profile, without the life‐threatening toxicities associated with chemotherapies [11], [13], [14]. However, there is no consensus on the optimal treatment strategy for patients with stage IIIA‐N2 NSCLC, including those with EGFR mutation‐positive disease. The efficacy and tolerability of preoperative EGFR TKI therapy, although promising, requires further research. Therefore, this clinical trial aimed to evaluate whether erlotinib, as a neoadjuvant therapy, improves operability and overall survival (OS) in patients with stage IIIA‐N2 EGFR mutation‐positive NSCLC.

In total, 155 patients were screened from July 2011 to June 2014; 44 were diagnosed with stage IIIA‐N2 NSCLC. Of these 44 patients, 25 patients with EGFR mutation‐positive disease were enrolled. Next‐generation sequencing (NGS) was repeated during the 3‐year recruitment period, during which four patients were found to be negative for EGFR mutation (amplification‐refractory mutation system polymerase chain reaction sequencing) and removed from the study. Further NGS analysis reduced our sample to 19 patients with activating EGFR mutations eligible for inclusion in the study (Fig. 1). Most patients (73.7%; 14/19) underwent surgical resection. Baseline demographic and clinical characteristics are shown in Table 1.

Table 1.

Baseline demographic and clinical characteristics

One patient had exon 19 deletion and exon 21 L858R point mutation.

Abbreviations: ECOG, Eastern Cooperative Oncology Group; EGFR, epidermal growth factor receptor; ITT, intention‐to‐treat.

The tumor was resectable in 14 of 19 patients who received neoadjuvant erlotinib, and the radical resection rate in the overall population was 68.4% (13/19; Table 2). Among surgical patients, 35.7% of patients (5/14) had pathological downstaging from N2 to N1/N0, and 50% (7/14) experienced a reduction in tumor size (Table 3). The disease control rate was 89.5% (17/19) after neoadjuvant therapy. A waterfall plot of response to erlotinib neoadjuvant therapy is shown in Figure 2. There was a greater change from baseline in carcinoembryonic antigen level among patients who underwent surgery versus those who did not (Table 4). At the end of follow‐up, most patients received platinum‐based adjuvant chemotherapy (maximum six cycles, mean three cycles); no patients received postoperative radiotherapy. The Kaplan‐Meier curves of disease‐free survival, progression‐free survival (PFS), and OS are shown in Figure 3.

Table 2.

Response and radical resection rates.

The median (range) time from surgery to discharge was 8 (3–15) days.

Abbreviation: ITT, intention‐to‐treat.

Table 3.

TNM stage list for patients who underwent surgical resection.

Abbreviation: TNM, tumor, node, metastasis (cancer staging).

Figure 2.

Patient flowchart.

Abbreviations: EBUS, endobronchial ultrasound; EGFR, epidermal growth factor receptor; NGS, next‐generation sequencing; PD, progressive disease; SAE, serious adverse event.

Table 4.

Trend of serum CEA level before and after neoadjuvant erlotinib treatment.

Estimate of change in CEA level from baseline after 4 weeks. Between‐group difference in change was −53%; p = .031.

Abbreviations: CEA, carcinoembryonic antigen; EGFR TKI, epidermal growth factor receptor tyrosine kinase inhibitor; SD, standard deviation.

Figure 3.

Kaplan‐Meier curves of disease‐free survival (DFS), progression‐free survival (PFS), and overall survival (OS). (A): DFS for 14 patients who underwent surgery (calculated from the date of oral EGFR tyrosine kinase inhibitor to the first date of disease progression). (B): The DFS time of 14 patients who had surgery (calculated from the date of operation to the first date of disease progression). (C): PFS for all 19 patients. (D): OS for all 19 patients. (E): PFS for patients who were smokers. (F): PFS for patients who were nonsmokers.

Abbreviation: CI, confidence interval.

To date, the selection of an optimal treatment regimen for patients with stage IIIA‐N2 NSCLC remains controversial, and there is no standard of care for these patients. Our results suggest that neoadjuvant erlotinib improved the likelihood of surgery and was associated with a good resection rate as shown by the high rate of prospective downstaging in patients with stage IIIA‐N2 NSCLC. In a study by Noh et al., 52.3% of patients with stage IIIA‐N2 NSCLC experienced progressive disease with concurrent chemoradiotherapy, and 7 of 65 patients died from pulmonary radiation therapy‐related adverse events (AEs). In this study, the authors reported a resection rate of 86.4% (456/528) among patients judged as medically operable [15]. Dy et al. found that chemotherapy achieved a relatively positive induction response and a radical resection rate of 94% among patients with early‐stage IB to IIIA NSCLC who underwent surgery [16]. A small study of patients with resectable IIIA‐N2 NSCLC that compared erlotinib versus gemcitabine/carboplatin as neoadjuvant therapy reported response rates of 58.3% versus 25.0% (p = .18), and 54.2% (13/24) patients underwent surgical resection [17]. Compared with these studies, our study demonstrated a strong disease control rate (89.5%) and downstage tumor rate (21.1%). Of note, among the 14 patients who underwent surgery, all but one (93%, 13/14) underwent radical resection. Importantly, patients achieved a median PFS of 11.2 months and median OS of 51.6 months. Taken together, these findings support the use of erlotinib prior to surgery to improve the radical resection rate and long‐term survival of patients with IIIA‐N2 NSCLC.

Erlotinib as neoadjuvant therapy was well tolerated. AEs occurred in 36.8% (7/19) of patients (Table 5). No patients died from treatment‐related AEs, and only one patient had a grade 4 AE; these findings are comparable with those of a previous study [13]. A comparison of Functional Assessment of Cancer Therapy‐Lung and Lung Cancer Symptom Scale scores before and after erlotinib treatment demonstrated improved quality of life after treatment with neoadjuvant erlotinib (Table 6).

Table 5.

Adverse events during erlotinib therapya

Adverse events occurred in 36.8% (7/19) of patients.

Patient had hepatitis.

Adverse event was not related to erlotinib induction.

Abbreviations: —, not occurred; CTCAE, Common Terminology Criteria for Adverse Events.

Table 6.

Quality of life in all patients and in patients who underwent surgery

FACT‐L data were missing for two patients prior to surgery.

LCSS data were missing for one patient prior to surgery.

Abbreviations: CI, confidence interval; FACT‐L, Functional Assessment of Cancer Therapy‐Lung; LCSS, Lung Cancer Symptom Scale; TOI, Trial Outcome Index.

Adequate tissue samples from before neoadjuvant therapy and after surgery were available for eight patients only. Tumor samples for these patients were analyzed for 68 genes by NGS (Tables 7 and 8 and Fig. 4). Patients who benefited most from neoadjuvant erlotinib therapy (cases 6 and 7), with PFS lasting over 36 months, had no TP53 mutation or very low TP53 abundance. Conversely, the patient with the greatest TP53 abundance (case 8) had limited benefits in PFS (8 months) and OS (16 months). These findings indicate that additional biomarkers may play an important role in predicting response to TKI therapy in the neoadjuvant setting. These results are consistent with, and supportive of, previous findings [18], suggesting that TP53 gene mutation is independently associated with shorter OS in NSCLC.

Table 7.

List of 68 genes in next‐generation sequencing analysis

Table 8.

Clinical information of next‐generation sequencing analysis

Abbreviations: F, female; M, male; OS, overall survival; p, pathological; PFS, progression‐free survival; PR, partial response; SD, stable disease; LN: lymph node.

Figure 4.

Next‐generation sequencing analysis of mutation abundance and CEA level for eight cases (A)–(D).

Abbreviations: CEA, carcinoembryonic antigen; EGFR, epidermal growth factor receptor.

We acknowledge that the small sample size of our study represents a major limitation. We recruited a specific subset of patients with NSCLC who, in addition to having stage IIIA‐N2 disease, were positive for activating EGFR mutations. Our center is one of the largest for clinical lung cancer research in China, yet we encountered challenges with recruiting patients. Nevertheless, we believe that the findings from this study raise important clinical questions and will be helpful for informing larger controlled trials in the future.

In our study, neoadjuvant erlotinib was well tolerated and improved the rate of radical resection in patients with stage IIIA‐N2 EGFR mutation‐positive NSCLC. NGS analysis allowed us to identify markers that may help predict the clinical course of IIIA‐N2 NSCLC. If of predictive value, markers of TP53 abundance could be used to guide preoperative application of TKIs. Given our findings and those of other small studies, we look forward to large‐scale randomized controlled trials investigating the role of TKIs in perioperative therapy, combining neoadjuvant and adjuvant treatments to enhance personalized therapy for patients in this precision medicine era.