Literature DB >> 29898592

Efficacy and Safety of Afatinib for EGFR-mutant Non-small Cell Lung Cancer, Compared with Gefitinib or Erlotinib.

Youjin Kim¹, Se-Hoon Lee¹, Jin Seok Ahn¹, Myung-Ju Ahn¹, Keunchil Park¹, Jong-Mu Sun¹.

Abstract

PURPOSE: We tried to evaluate whether there are any specific features in treatment outcomes of firstline afatinib in patients with epidermal growth factor receptor (EGFR)-mutant non-small cell lung cancer (NSCLC), compared with gefitinib or erlotinib.
MATERIALS AND METHODS: We analyzed patients treated with first-line afatinib, gefitinib, or erlotinib for advanced EGFR-mutant NSCLC at Samsung Medical Center between 2014 and 2016.
RESULTS: In total, 467 patients received first-line afatinib (n=165), gefitinib (n=230), or erlotinib (n=72). Afatinib was used more often in patients with tumors harboring deletion in exon 19 (Del19), whereas the gefitinib group had more elderly, females, and never smokers. The median progression-free survival (PFS) time for afatinib, gefitinib, and erlotinib was 19.1 months, 13.7 months, and 14.0 months, respectively (p=0.001). The superior PFS of afatinib was more remarkable in subgroups of Del19 or uncommon EGFR mutations. Overall toxicity profiles of the three drugs were comparable, though more grade 3 or 4 toxicities were detected in afatinib (7.3%) compared with gefitinib (2.6%) or erlotinib (1.8%). The common grade 3 or 4 toxicities of afatinib included diarrhea (3.0%), paronychia (2.4%), and skin rash (1.8%). Dose modification was more frequently required in patients treated with afatinib (112/165, 68%), compared with gefitinib (5/230, 2%) and erlotinib (4/72, 6%). Interestingly, however, dose reduction in the afatinib group did not impair its efficacy in terms of PFS (dose reduction vs. no reduction group, 23.5 months vs. 12.4 months).
CONCLUSION: First-line afatinib showed satisfactory efficacy data and manageable toxicity profiles.

Entities: Chemical

Keywords: Afatinib; Epidermal growth factor receptor; First-line therapy; Non-small cell lung carcinoma

Mesh：

Substances：

Year: 2018 PMID： 29898592 PMCID： PMC6473268 DOI： 10.4143/crt.2018.117

Source DB: PubMed Journal: Cancer Res Treat ISSN： 1598-2998 Impact factor: 4.679

Introduction

Non-small cell lung cancer (NSCLC) is one of the leading causes of deaths from cancer worldwide [1]. When used as first-line therapy, first-generation epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) such as gefitinib and erlotinib have improved clinical outcomes in patients with advanced NSCLC harboring EGFR mutations [2,3]. Afatinib, a second-generation EGFR TKI, is an oral, irreversible ErbB family blocker that selectively and potently blocks signaling from all relevant ErbB family receptors (ErbB1, ErbB2, and ErbB4) [4]. In the Phase III LUX-Lung 3 and LUX-Lung 6 trials, first-line afatinib significantly improved progression-free survival (PFS) and objective response rates versus platinum-doublet chemotherapy in patients with EGFR-mutant NSCLC [5,6]. These promising results led to the approval of afatinib in many countries from 2013 onwards. Several large randomized trials have been conducted to compare the clinical efficacies and toxicities of these EGFR TKIs. The WJOG 5108L study was a randomized phase III study comparing gefitinib with erlotinib. It did not demonstrate statistical non inferiority of gefitinib in terms of PFS compared with erlotinib [7]. The LUX-Lung 7 trial compared afatinib with gefitinib as a first-line treatment in patients with advanced NSCLC harboring common EGFR mutations (Del19 and the L858R point mutation) [8]. Although the median PFS times of afatinib and gefitinib were similar (11.0 months vs. 10.9 months), afatinib showed a statistically superior PFS outcome compared to gefitinib (hazard ratio [HR], 0.73; 95% confidence interval [CI], 0.57 to 0.95) [8]. Currently, afatinib, gefitinib, and erlotinib are recommended as first-line therapies for EGFR-mutant NSCLC. However, no rules or guidelines are available to choose one of these drugs for a given patient. Thus, the specific drug is typically chosen according to the physician’s preference or experience. In South Korea, these three TKIs are approved, and one of three TKIs can be chosen by physicians as the first-line therapy for their patients with EGFR-mutant NSCLC. A few years have elapsed since first-line afatinib therapy for EGFR-mutant NSCLC was first reimbursed in Korea (October 2014). Our purpose of this study is to investigate how afatinib is used in real-world practice, and whether it leads to different clinical outcomes compared with gefitinib or erlotinib.

Materials and Methods

1. Patients

This retrospective population-based study included patients with NSCLC who received first-line afatinib, gefitinib, or erlotinib at a single institute (Samsung Medical Center) between October 2014 and December 2016. Eligible patients in the clinical database of the hospital were identified and their medical information was extracted from electronic medical records. Patient demographics such as age, sex, smoking history, performance status, and EGFR mutation type were reviewed. Demographic information was obtained for the time at which first-line EGFR TKI treatment was initiated. EGFR mutations were identified using a PNA clamp kit and real-time polymerase chain reaction. Mutations other than Del19 or the L858R point mutation were classified as uncommon EGFR mutations, which also included the de novo T790M mutation. In the efficacy analysis according to EGFR mutation type, the T790M mutation was excluded since tumors harboring T790M are known to be resistant to afatinib, gefitinib, and erlotinib.

2. Evaluation of safety and efficacy

All patients were diagnosed with NSCLC by histologic analysis. Tumor stage was evaluated by chest computed tomography (CT), positron-emission tomography‒CT (PET-CT), and brain magnetic resonance imaging (MRI). If the results of staging work-up procedures performed in hospitals other than Samsung Medical Center were of poor quality, we repeated the procedures at our hospital before the patients started treatment. When starting first-line EGFR TKIs, all patients were informed about the potential adverse events of the TKIs and instructed on how to manage such events if they appear. All patients were recommended to visit the clinic within 2 weeks after starting TKIs so that they could be screened for any adverse events. If any significant adverse event had occurred by the first visit after TKI treatment, dose reduction or a more vigilant follow-up schedule was planned. Otherwise, patients visited every 1 or 2 months for the first 6 months, and every 2 or 3 months thereafter. Tumor responses were checked every 2 or 3 months by chest CT, with or without abdomen/pelvis CT, PET-CT, or brain MRI. Objective response rate was calculated by checking the best response according to the Response Evaluation Criteria in Solid Tumor ver. 1.1 guidelines. PFS was defined as the time from starting first-line TKI to disease progression or death; overall survival was defined as the time from starting first-line TKI to death. Toxicity was graded according to the National Cancer Institute Common Toxicity Criteria, ver. 4.0.

3. Statistical considerations

To compare baseline characteristics among the three groups or treatments, one-way ANOVA or the chi-square test was used. Overall survival was defined as the time from registration to death from any cause or censored at the time of last contact. Progression-free survival (PFS) was defined as the time from registration to documented progression or death without progression. Patients without documented progression or death were censored at the time of the last disease assessment. The survival data were analyzed using the Kaplan-Meier method. Median PFS was calculated using a Cox proportional hazards model. PFS is presented as median values and two-sided 95% CIs. PFS after gefitinib, erlotinib, or afatinib treatment was estimated with a Cox proportional hazards model. For multivariable analysis, a multiple Cox regression model was fitted by adjusting significant prognostic variables (p < 0.05) in the univariable analysis for PFS. All p-values were two-sided and a p < 0.05 was considered statistically significant. Data were analyzed using SPSS ver. 17 (SPSS Inc., Chicago, IL). The data cutoff for the analysis was May 28, 2017.

4. Ethical statement

This study was reviewed and approved by the institutional review board (IRB No. 2018-02-111) at Samsung Medical Center. The informed consent was waived because this study was done based on the medical record review. The trial was conducted in accordance with the Declaration of Helsinki.

Results

1. Patient characteristics and preference for afatinib, gefitinib, or erlotinib

The patient characteristics are summarized in Table 1. A total of 467 patients with recurrent or metastatic stage IV NSCLC were included in the analysis, each of whom had Del19, L858R point mutation, or an uncommon EGFR mutation. Patients were treated with afatinib (n=165), gefitinib (n=230), or erlotinib (n=72) as the first-line therapy. Patients in the gefitinib group were significantly elderly (median age, 64 years) than those in the afatinib and erlotinib groups (median age, 57 and 59 years, respectively) (p < 0.001). Female patients comprised less than 50% of the afatinib and erlotinib groups, while 74% of the gefitinib group was female (p < 0.001). Performance status was not significantly different among the three groups. The proportion of never smokers was higher in the gefitinib group (78%) than in the afatinib (60%) and erlotinib groups (57%) (p < 0.001). Approximately 70% of patients in the afatinib group had Del19; this percentage was significantly higher than those in the gefitinib (53%) and erlotinib (56%) groups (p=0.002). A total of 31 patients with uncommon EGFR mutation types were included, broken down by treatment group as follows: afatinib (n=14), gefitinib (n=12), and erlotinib (n=5).

Table 1.

Baseline characteristics

Patient characteristic	Afatinib	Gefitinib	Erlotinib	p-value
No. of patients	165	230	72
Age (yr)
Median (range)	57 (30-79)	64 (29-87)	59 (36-77)	< 0.001
< 60	93 (56.4)	79 (34.3)	38 (52.8)	< 0.001
≥ 60	72 (43.6)	151(65.7)	34 (47.2)
Sex
Male	85 (51.5)	60 (26.1)	39 (54.2)	< 0.001
Female	80 (48.5)	170 (73.9)	33 (45.8)
ECOG PS
0	42 (25.5)	56 (24.3)	24 (33.3)	0.658
1	114 (69.0)	160 (69.6)	44 (61.1)
2	9 (5.5)	14 (6.1)	4 (5.6)
Smoking status
Never smoker	99 (60.0)	180 (78.3)	41 (56.9)	< 0.001
Current or ex-smoker	66 (40.0)	50 (21.7)	31 (43.1)
EGFR mutation type
Exon 19 deletion	114 (69.1)	122 (53.0)	40 (55.6)	0.002
Exon 21 L858R	37 (22.4)	96 (41.8)	27 (37.5)
Uncommon EGFR	14 (8.5)	12 (5.2)	5 (6.9)

Values are presented as median (range) or number (%). Uncommon EGFR: the tumor contains a mutation other than del19 or L858R. ECOG, Eastern Cooperative Oncology Group; PS, performance status; EGFR, epidermal growth factor receptor.

2. Survival outcomes according to EGFR TKI therapy

The median follow-up duration for PFS was 17.7 months (95% CI, 16.5 to 18.9). The median PFS times for afatinib, gefitinib, and erlotinib were 19.1 months (95% CI, 12.3 to 25.9), 13.7 months (95% CI, 12.3 to 15.1), and 14.0 months (95% CI, 11.3 to 16.8), respectively (p=0.001) (Fig. 1A). In the univariate analysis for PFS, other clinical characteristics such as common EGFR mutation type (p < 0.001), good performance status (Eastern Cooperative Oncology Group 0 or 1) (p < 0.001), and never smoker status (p=0.014) were associated with longer PFS, while younger age (< 60 years) (p=0.174) and female sex (p=0.523) were not good prognostic factors in terms of predicting PFS. With respect to the other clinical factors considered, afatinib therapy was significantly associated with longer PFS in the multivariate analysis (HR, 0.46; 95% CI, 0.34 to 0.63; p < 0.001).

Fig. 1.

Progression-free survival (A) and overall survival (B) with afatinib, gefitinib, and erlotinib. TKI, tyrosine kinase inhibitor.

Regarding overall survival, the median follow-up duration was 17.5 months (95% CI, 16.3 to 18.8). There was no statistically significant difference between the EGFR TKI therapy groups (p=0.21) (Fig. 1B).

3. Progression-free survivals of EGFR TKIs according to EGFR mutation types

We next analyzed PFS according to EGFR mutation types. In the subgroup of patients with Del19, the median PFS times for afatinib, gefitinib, and erlotinib were 19.1 months, 15.0 months, and 16.3 months, respectively (p=0.01). In contrast, there was no significant difference in the L858R subgroup (p=0.46) (Fig. 2A and B). For the subgroup of uncommon EGFR mutations, the afatinib group showed much longer PFS (median PFS, not reached) compared with the gefitinib (5.0 months) and erlotinib (6.1 months) groups, though it was not statistically significant due to a small sample size (p=0.06) (Fig. 2C).

Fig. 2.

Progression-free survival of afatinib, gefitinib, and erlotinib according to epidermal growth factor receptor (EGFR) mutation types. (A) Exon 19 deletion. (B) Exon 21 L858R. (C) Uncommon EGFR mutations. TKI, tyrosine kinase inhibitor.

4. Objective response in the uncommon EGFR mutation subgroup

Table 2 shows the uncommon EGFR mutation types and the objective response of patients with each mutation type to each EGFR TKI. A total of 31 patients had uncommon mutations (exon 21 L861 Q, exon 18 G719X, exon 20 insertion, exon 18 G719X+exon 20 S768I, Del19+L747_P753>Q, and exon 21 L858R+H870R) and seven patients (1.4%) had both active and resistant EGFR mutations (T790M). Seven patients had the de novo T790M mutation (afatinib, 4; gefitinib, 3); these patients had no response. Among the patients harboring uncommon mutations other than T790M, objective response was seen in eight out of the 10 patients in the afatinib group, while four out of nine in the gefitinib group showed a response and one out of five in the erlotinib group showed a response.

Table 2.

Objective response rates according to uncommon EGFR mutation

EGFR TKI	Afatinib		Gefitinib		Erlotinib
EGFR TKI	Total	Objective response	Total	Objective response	Total	Objective response
Uncommon EGFR mutation	14	8	12	4	5	1
Uncommon EGFR mutation other than T790M	10	8	9	4	5	1
Uncommon EGFR mutation
Exon 21 L858R+exon 20 T790M	3	0	3	0	0	0
Exon 19 deletion+exon 20 T790M	1	0	0	0	0	0
Exon 21 L861 Q	3	3	4	2	0	0
Exon 18 G719X	3	2	4	2	3	1
Exon 20 insertion	1	0	0	0	2	0
Exon 18 G719X+exon 20 S768I	1	1	1	0	0	0
Exon 19 Deletion+L747_P753>Q	1	1	0	0	0	0
Exon 21 L858R+H870R	1	1	0	0	0	0

EGFR, epidermal growth factor receptor; TKI, tyrosine kinase inhibitor.

5. Toxicity profile

The toxicity profiles were compatible with the expectation (Table 3). The most common adverse events were skin rash, stomatitis, paronychia, and diarrhea. The incidence of grade 1-2 adverse events were comparable among three treatment groups. However, grade 3-4 adverse events were more frequently found in the afatinib group (7.3%), compared with gefitinib (2.6%) and erlotinib groups (1.8%). The common grade 3-4 adverse events of afatinib were diarrhea, paronychia, and skin rash. A total of 10 patients of afatinib permanently discontinued afatinib therapy due to grade 2 paronychia or skin rash (n=3), grade 2 or 3 diarrhea (n=4), grade 2 or 3 stomatitis (n=2), or grade 3 pneumonitis (n=1). One patient with gefitinib hold permanently due to grade 3 interstitial lung disease, and there was no permanent hold in the erlotinib group. No treatment-related deaths occurred for all the three drugs.

Table 3.

Toxicity profile of afatinib, gefitinib, and erlotinib

Toxicity	Grade 1-2			Grade 3-4
Toxicity	Afatinib	Gefitinib	Erlotinib	Afatinib	Gefitinib	Erlotinib
Total	116 (70.3)	164 (71.3)	53 (73.6)	12 (7.3)	6 (2.6)	3 (1.8)
Rash and acne	76 (46.1)	131 (57.0)	47 (65.3)	3 (1.8)	1 (1.4)	3 (1.8)
Stomatitis	50 (30.3)	31 (13.5)	8 (11.1)	0	0	0
Paronychia	44 (26.7)	21 (9.1)	13 (18.1)	4 (2.4)	0	0
Diarrhea	32 (19.4)	33 (14.3)	13 (18.2)	6 (3.0)	0	0
Dry skin	18 (10.9)	45 (19.6)	12 (16.7)	0	1 (1.4)	0
Pruritus	17 (10.3)	79 (34.3)	21 (29.2)	0	0	0
Anorexia	7 (4.2)	15 (6.5)	7 (9.7)	1 (0.6)	1 (1.4)	0
Nausea/Vomiting	0	4 (1.7)	1 (1.4)	0	0	0
Fatigue	1 (0.6)	3 (1.3)	1 (1.5)	1 (0.6)	0	0
Alopecia	0	15 (6.5)	2 (2.8)	0	1 (1.4)	0
Interstitial lung disease	0	0	0	1 (0.6)	0	0
Increased AST/ALT	0	2 (0.9)	0	0	2 (2.8)	0

Values are presented as number (%). ALT, alanine aminotransferase; AST, aspartate aminotransferase.

6. Dose modification

All patients initiated afatinib, gefitinib, and erlotinib treatment with 40 mg, 250 mg, and 150 mg once daily, respectively. Dose reduction was performed to control adverse events. In the afatinib group, the first dose reduction was from 40 mg to 30 mg per day. If further reduction was needed, the dose was reduced subsequently from 30 mg to 20 mg per day. In accordance with the dose reduction sequence, dose reduction was performed either once or twice in 112 patients (67.8%). The median interval from starting afatinib to the first dose reduction was 4.9 weeks (95% CI, 4.0 to 5.8). Thus, the final afatinib dose was 30 mg per day in 80 patients (48.5%) and 20 mg per day in 32 patients (19.4%). In the gefitinib group, total five patients reduced dose by increasing the administration interval into every other day, due to skin toxicity and hepatotoxicity. Four patients with erlotinib reduced dose to 100 mg per day due to skin toxicity. A total of 10 patients in the afatinib group permanently discontinued afatinib therapy due to grade 2 paronychia or skin rash (n=3), grade 2 or 3 diarrhea (n=4), grade 2 or 3 stomatitis (n=2), or grade 3 pneumonitis (n=1). One patient with gefitinib permanently stopped medication due to skin toxicity and there was no permanent stop case for erlotinib. No treatment-related deaths occurred for all three TKIs. We analyzed whether dose reduction of afatinib affected its efficacy. Interestingly, in the survival analysis according to final afatinib dose, reduction did not impair PFS: the median PFS times for the unreduced group (40 mg) and reduced group (30 mg or 20 mg) were 12.4 months and 23.5 months, respectively (S1 Fig.). When the disease burdens were compared by initial brain metastasis status between two groups, there was no significant difference. There were 19 patients (35%) with brain metastasis in the unreduced group (n=55), while 48 patients (43%) initially presented with metastatic brain tumor in the reduced group (n=112) (p=0.53).

Discussion

To our knowledge, this is the first study to comprehensively evaluate the pattern of clinical use of three EGFR TKIs (afatinib, gefitinib, and erlotinib). We found that gefitinib was more commonly used than erlotinib or afatinib in Korea, especially for elderly, which may be due to concerns about treatment related adverse events. A previous retrospective report showed that gefitinib was less associated with significant skin toxicity than the other two TKIs in patients with NSCLC [9]. Compatible with this report, our study also showed that gefitinib was prescribed more often to women, indicating that physicians consider potential cosmetic problems when treating women. Afatinib was more commonly used for patients with tumors harboring Del19. We reason that this observation could be due to a study reporting that the afatinib arm had longer overall survival than the chemotherapy arm in the Del19 subgroup, while this result was not observed in the L858R subgroup [10]. Our results show that afatinib was significantly associated with longer PFS compared with gefitinib and erlotinib, even after adjustment for other potentially confounding prognostic factors. In addition, the significantly longer PFS of afatinib observed even in the Del19 subgroup could preclude the possibility that longer PFS of afatinib for overall population was caused by that more patients with better prognostic factor, Del19, were included in the afatinib group. We confirm the previous data that showed the superior PFS outcome of second-generation EGFR TKIs such as afatinib and dacomitinib to first-generation EGFR TKI such as gefitinib [8,11]. The median PFS times of each TKI in our study (13-19 months) were longer than those (11 months) reported from prospective trials as first-line EGFR TKIs [5,6,8]. Although we do not have a definitive explanation for this result, maintaining TKI treatment for a long-term period with more efficient management of adverse events may in part contribute to the longer PFS. We note that the rate of total grade 3 or 4 adverse events for afatinib, gefitinib, and erlotinib were approximately 7%, 3%, and 2%, respectively, in our study, which is lower than those reported in prospective studies [5-8]. Although gefitinib and erlotinib have both demonstrated efficacy for treating tumors with common EGFR mutations [12-14], their efficacy against tumors with uncommon EGFR mutations is still under investigation. The response rates and median PFS of first-generation EGFR TKIs for uncommon EGFR mutations were reported to be less than 50% and 5 months, respectively [15,16]. Recently, good efficacy of afatinib for treating tumors with uncommon mutations was reported [17,18]. Our study confirms the previous efficacy data of afatinib for NSCLC harboring uncommon EGFR mutations other than T790M. Compared with gefitinib and erlotinib, afatinib treatment yielded a longer PFS for patients with uncommon EGFR mutations, although this difference did not reach statistical significance, possibly due to the small sample size (p=0.06). Based on our results, we recommend afatinib for first-line therapy in patients harboring uncommon EGFR mutations other than the de novo T790M point mutation. The frequency of adverse events was lower than in previous prospective studies and fewer types of adverse events were observed [5,6,8]. This finding could be related to limitations commonly associated with retrospective studies, which are based on medical records. Despite these limitations, we observed a lower rate of significant toxicity (grade 3 or 4). This finding can be explained by the fact that our practice usually includes dose reduction with or without temporary interruption, in addition to appropriate use of oral antibiotics, anti-diarrheal agents, or steroid ointments for the management of adverse events. In our study, more patients underwent dose reduction due to adverse events compared to previous prospective trials [5,6,8]. However, this dose reduction did not impair efficacy outcomes in terms of PFS. Therefore, based on our results, we recommend that physicians reduce the afatinib dose when patients experience unacceptable or prolonged adverse events. However, the relationship between dose reduction and PFS should be interpreted with caution, because there are more opportunities for dose reduction when patients take afatinib for longer periods. However, this bias was unlikely to have significantly affected the results because most dose reduction occurred soon after starting afatinib treatment, with a median time of 4.9 weeks (95% CI, 4.0 to 5.8). In addition, reduced afatinib doses were shown to not impair efficacy in another retrospective study [19]. It showed that there was no difference in time to treatment failure between the group that started afatinib 40 mg and the group that started 30 mg as the first-line therapy for NSCLC [19]. In summary, we evaluated the frequencies of first-line EGFR TKI use in patients with EGFR-mutant NSCLC and found that patient characteristics affected the choice of EGFR TKI. Afatinib showed superior PFS data compared with gefitinib or erlotinib. Afatinib showed more grade 3 or 4 adverse events than gefitinib or erlotinib, though the incidence was much lower than previous data.

17 in total

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Journal: Lancet Oncol Date: 2015-01-12 Impact factor: 41.316

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Authors: Caicun Zhou; Yi-Long Wu; Gongyan Chen; Jifeng Feng; Xiao-Qing Liu; Changli Wang; Shucai Zhang; Jie Wang; Songwen Zhou; Shengxiang Ren; Shun Lu; Li Zhang; Chengping Hu; Chunhong Hu; Yi Luo; Lei Chen; Ming Ye; Jianan Huang; Xiuyi Zhi; Yiping Zhang; Qingyu Xiu; Jun Ma; Li Zhang; Changxuan You
Journal: Lancet Oncol Date: 2011-07-23 Impact factor: 41.316

4. Afatinib versus cisplatin plus gemcitabine for first-line treatment of Asian patients with advanced non-small-cell lung cancer harbouring EGFR mutations (LUX-Lung 6): an open-label, randomised phase 3 trial.

Authors: Yi-Long Wu; Caicun Zhou; Cheng-Ping Hu; Jifeng Feng; Shun Lu; Yunchao Huang; Wei Li; Mei Hou; Jian Hua Shi; Kye Young Lee; Chong-Rui Xu; Dan Massey; Miyoung Kim; Yang Shi; Sarayut L Geater
Journal: Lancet Oncol Date: 2014-01-15 Impact factor: 41.316

5. Efficacy of EGFR tyrosine kinase inhibitors in patients with EGFR-mutated non-small cell lung cancer except both exon 19 deletion and exon 21 L858R: a retrospective analysis in Korea.

Authors: Jin Ho Baek; Jong-Mu Sun; Young Joo Min; Eun Kyung Cho; Byoung Chul Cho; Joo-Hang Kim; Myung-Ju Ahn; Keunchil Park
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6. EGFR mutations in lung cancer: correlation with clinical response to gefitinib therapy.

Authors: J Guillermo Paez; Pasi A Jänne; Jeffrey C Lee; Sean Tracy; Heidi Greulich; Stacey Gabriel; Paula Herman; Frederic J Kaye; Neal Lindeman; Titus J Boggon; Katsuhiko Naoki; Hidefumi Sasaki; Yoshitaka Fujii; Michael J Eck; William R Sellers; Bruce E Johnson; Matthew Meyerson
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7. Activating mutations in the epidermal growth factor receptor underlying responsiveness of non-small-cell lung cancer to gefitinib.

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Journal: N Engl J Med Date: 2004-04-29 Impact factor: 91.245

8. Gefitinib or carboplatin-paclitaxel in pulmonary adenocarcinoma.

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Journal: N Engl J Med Date: 2009-08-19 Impact factor: 91.245

9. BIBW2992, an irreversible EGFR/HER2 inhibitor highly effective in preclinical lung cancer models.

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Journal: Oncogene Date: 2008-04-14 Impact factor: 9.867

10. Phase III study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with EGFR mutations.

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Authors: Yamin Shu; Qilin Zhang; Xucheng He; Li Chen
Journal: Cancer Manag Res Date: 2021-11-03 Impact factor: 3.989

3. Afatinib 30 mg in the treatment of common and uncommon EGFR-mutated advanced lung adenocarcinomas: a retrospective, single-center, longitudinal study.

Authors: Jie Qian; Xuanting Ye; Aimi Huang; Ruoyan Qin; Yuqing Cai; Yiqian Xue; Shi Zhang; Weimin Wang; Liwen Xiong; Aiqin Gu
Journal: J Thorac Dis Date: 2022-06 Impact factor: 3.005

4. Clinical Benefit of Tyrosine Kinase Inhibitors in Advanced Lung Cancer with EGFR-G719A and Other Uncommon EGFR Mutations.

Authors: Kartik Sehgal; Deepa Rangachari; Paul A VanderLaan; Susumu S Kobayashi; Daniel B Costa
Journal: Oncologist Date: 2020-10-06

5. Non-small Cell Lung Cancer as a Chronic Disease - A Prospective Study from the Czech TULUNG Registry.

Authors: Monika Bratova; Bara Karlinova; Jana Skrickova; Milos Pesek; Vitezslav Kolek; Leona Koubkova; Michal Hrnciarik; Jana Krejci; Magda Barinova; Libor Havel; Ivona Grygarkova; Kristian Brat
Journal: In Vivo Date: 2020 Jan-Feb Impact factor: 2.155

6. The impact of different first-line EGFR-TKIs on the clinical outcome of sequential osimertinib treatment in advanced NSCLC with secondary T790M.

Authors: Yen-Hsiang Huang; Jeng-Sen Tseng; Kuo-Hsuan Hsu; Kun-Chieh Chen; Kang-Yi Su; Sung-Liang Yu; Jeremy J W Chen; Tsung-Ying Yang; Gee-Chen Chang
Journal: Sci Rep Date: 2021-06-08 Impact factor: 4.379

7. Real-World Treatment Patterns, Epidermal Growth Factor Receptor (EGFR) Testing and Outcomes in EGFR-Mutated Advanced Non-small Cell Lung Cancer Patients in Belgium: Results from the REVEAL Study.

Authors: Kristof Cuppens; Liesbet Lodewyckx; Ingel Demedts; Lore Decoster; Benoît Colinet; Koen Deschepper; Annelies Janssens; Daniella Galdermans; Thierry Pieters
Journal: Drugs Real World Outcomes Date: 2021-03-12

Review 8. Afatinib as First-Line Treatment in Asian Patients with EGFR Mutation-Positive NSCLC: A Narrative Review of Real-World Evidence.

Authors: Shun Lu; Jin-Yuan Shih; Tae-Won Jang; Chong-Kin Liam; Yongfeng Yu
Journal: Adv Ther Date: 2021-03-17 Impact factor: 3.845

9. Afatinib in EGFR TKI-Naïve Patients with Locally Advanced or Metastatic EGFR Mutation-Positive Non-Small Cell Lung Cancer: A Pooled Analysis of Three Phase IIIb Studies.

Authors: Antonio Passaro; Filippo de Marinis; Hai-Yan Tu; Konstantin K Laktionov; Jifeng Feng; Artem Poltoratskiy; Jun Zhao; Eng Huat Tan; Maya Gottfried; Victor Lee; Dariusz Kowalski; Cheng Ta Yang; B J Srinivasa; Laura Clementi; Tejaswini Jalikop; Dennis Chin Lun Huang; Agnieszka Cseh; Keunchil Park; Yi-Long Wu
Journal: Front Oncol Date: 2021-07-09 Impact factor: 6.244

10. Survival analysis of afatinib versus erlotinib for individuals with advanced del19 lung adenocarcinoma with asymptomatic brain metastasis after pemetrexed-cisplatin chemotherapy: a retrospective study.

Authors: Ye Jiang; Wenli Chen; Weiguang Yu; Ning Shi; Guowei Han; Shuai Mao; Xinlei Zhang; Meiji Chen
Journal: J Int Med Res Date: 2020-08 Impact factor: 1.671