| Literature DB >> 30774491 |
Shruti Kate1, Anuradha Chougule2, Amit Joshi1, Vanita Noronha1, Vijay Patil1, Rohit Dusane3, Leena Solanki1, Priyanka Tiwrekar2, Vaishakhi Trivedi1, Kumar Prabhash1.
Abstract
BACKGROUND: The significance of uncommon EGFR mutations in newly diagnosed advanced non-small-cell lung cancer (NSCLC) patients is incompletely known. We aimed to analyze the demographic profile, outcome, and treatment attributes of these patients. PATIENTS AND METHODS: We retrospectively surveyed 5,738 advanced NSCLC patients who underwent EGFR testing in our center from 2013 to 2017 by in-house primer probes on real time PCR platform. Descriptive data were accumulated from electronic medical records. Survival plot was calculated using Kaplan-Meier method and compared between groups using log-rank test.Entities:
Keywords: advanced NSCLC; complex EGFR mutations; dual EGFR mutations; tyrosine kinase inhibitors; uncommon EGFR mutations
Year: 2019 PMID: 30774491 PMCID: PMC6357894 DOI: 10.2147/LCTT.S181406
Source DB: PubMed Journal: Lung Cancer (Auckl) ISSN: 1179-2728
Demographic and clinical profile of the study cohort
| Variables | N=83 (%) | EGFR TKI sensitizing (%) activating mutations |
|---|---|---|
| Median age (in years) | ||
| Median | 55 | 56 |
| Range | 25–82 | 50–63 |
| Sex | ||
| Male | 49 (59) | 141 (62.1) |
| Female | 34 (41) | 86 (37.9) |
| Performance status | ||
| 0, 1 | 53 (63.8) | 110 (48.5) |
| 2 | 21 (25.3) | >1=117 (51.5) |
| 3 | 8 (9.6) | |
| 4 | 1 (1.2) | |
| Smoking habitus | ||
| Current or past smokers | 17 (20.5) | |
| Never-smokers | 54 (65.1) | 168 (74.0) |
| Oral tobacco users | 12 (14.5) | |
| Brain metastases | ||
| Present | 26 (31.3) | 29 (12.8) |
| Absent | 57 (68.6) | 198 (87.2) |
| Histology | ||
| Adenocarcinomas | 80 (96.4) | |
| Squamous | 1 (1.2) | |
| Poorly differentiated | 2 (2.4) | |
| Mixed histology | 0 | |
| Sampling method used for EGFR testing | ||
| Tissue block | 56 (67.4) | |
| Pleura/pericardial fluid block | 12 (14.4) | |
| Blood | 15 (18.0) | |
Note: Copyright ©2017. Dove Medical Press. Adapted from Noronha V, Choughule A, Patil VM, et al. Epidermal growth factor receptor exon 20 mutation in lung cancer: types, incidence, clinical features and impact on treatment. Onco Targets Ther. 2017;10:2903–2908.7
Abbreviation: TKI, tyrosine kinase inhibitor.
Uncommon EGFR mutation frequency and their distribution according to predicted sensitivity to oral TKI
| Uncommon EGFR mutation types | N=83 | % |
|---|---|---|
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| Uncommon EGFR single mutations | ||
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| Exon 18 G719X | 8 | 9.6 |
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| Exon 20 insertion | 15 | 19.3 |
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| Exon T790M | 10 | 12.0 |
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| Exon 20 768I | 3 | 3.6 |
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| Exon 21 L861Q | 3 | 3.6 |
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| Complex dual mutation positivity | 43 | 50.6 |
| Exon 19 deletion + exon 20 T790M | 17 | 20.4 |
| Exon 21 L858 | 15 | 18.0 |
| Exon 18 G719X + exon 20768I | 03 | 3.6 |
| Exon 20 S768I + exon 21 L858R | 02 | 2.4 |
| Exon 18 G719X + exon 20 T790M | 01 | 1.2 |
| Exon 18 G719X + exon 21 L858R | 01 | 1.2 |
| Exon 20 insertion + exon 19 deletion | 01 | 1.2 |
| Exon 21 L858 | 01 | 1.2 |
| Exon 20 T790M + exon 20 S768I | 01 | 1.2 |
| Exon 21 L861I + exon 20 T790M | 01 | 1.2 |
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| Complex triple mutation | 1 | 1.2 |
| Positivity (exon 18 G719X + exon 20 S768I + exon 21 L858R) | ||
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| Uncommon mutation frequency as per predicted TKI sensitivity | ||
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| TKI sensitive single mutations (G719X, S768I, and L861Q) | 14 | 16.8 |
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| TKI insensitive single mutations (exon 20 insertion/T790M) | 25 | 30.1 |
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| TKI sensitive dual mutations | 4 | 4.8 |
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| TKI sensitive/insensitive complex mutations | 40 | 48.2 |
Abbreviation: TKI, tyrosine kinase inhibitor.
Figure 1Distribution of uncommon EGFR mutations.
Figure 2Graphs of survival for different types of uncommon mutations.
Notes: (A) OS by type of mutation. (B) OS by type of mutation by predicted TKI sensitivity.
Abbreviations: OS, overall survival; TKI, tyrosine kinase inhibitor.
mPFS and mOS of the cohort by mutation type and predicted TKI sensitivity
| Mutation types | N=83 | mPFS (months) first line therapy | 95% CI | Log rank (Mantel–Cox) | mOS (months) | 95% CI | Log-rank (Mantel–Cox) |
|---|---|---|---|---|---|---|---|
| Specific mutation types | Entire cohort | 6.7 | 4.7–8.6 | 15.8 | 10.1–21.5 | ||
| Exon 18 G719X | 8.4 | 1.8–15.1 | 0.82 | 13.5 | 0–29.9 | ||
| Exon 20 insertion | 6.0 | 2.4–9.6 | 15.8 | 6.2–25.3 | |||
| Exon T790M | 8.2 | 3.4–13.1 | 12.3 | 9.4–15.2 | |||
| Exon 20 768I | 2.0 | NE | 2.0 | 0.9–3.1 | |||
| Exon 21 L861Q | 1.0 | NE | 1.8 | 0–2.6 | |||
| Exon 18 G719X, exon 20 S768I, and exon 21 L858R | 4.8 | NE | 4.8 | NE | |||
| Dual mutations | 6.9 | 3.2–10.7 | 22.6 | 8.2–37.0 | |||
| Mutation types by TKI sensitivity | TKI sensitive single mutation (exon 18/20 768I/21 L861Q) | 6.5 | 0.6–12.4 | 12.7 | 0.0–30.5 | ||
| TKI insensitive single (exon 20 insertion/T790M) | 6.0 | 5.5–6.5 | 12.9 | 11.1–14.7 | |||
| TKI sensitive dual | 4.6 | 0–9.5 | 9.6 | 3.6–15.6 | |||
| TKI sensitive + insensitive complex mutation | 7.8 | 3.1–12.4 | 28.2 | 15.2–41.2 |
Abbreviations: mOS, median overall survival; mPFS, median progression-free survival; NE, not estimable; TKI, tyrosine kinase inhibitor.
Responsiveness to oral TKI
| Mutation types | n | RR (%) | mPFS (months) TKI | 95% CI | ||
|---|---|---|---|---|---|---|
| Specific mutation types | Overall | 9.1 | 6.2–12.0 | |||
| Exon 18 G719X | 5 | 50 | 9.0 | NE | 0.60 | |
| Exon 20 insertion | 7 | 0 | 1.9 | 0.3–3.5 | ||
| Exon 20 T790M | 4 | 24 | 8.2 | 2.9–13.5 | ||
| Exon 20 S768I | 2 | 0 | 1.0 | NE | ||
| Exon 21 L861Q | 2 | 0 | 1.8 | NE | ||
| Complex dual mutations | 36 | 47.2 | 9.4 | 3.3–15.5 | ||
| Complex triple mutation (Exon 18 G719X, exon 20 S768I, and exon 21 L858R) | 1 | 0 | 4.2 | NE | ||
| Mutation type by TKI sensitivity | TKI sensitive single mutations (exon 18/20 768I/21 L861Q) | 9 | 37.5 | 12.8 | 4.7–20.9 | 0.29 |
| TKI insensitive single mutations (exon 20 insertion / T790M) | 12 | 16.6 | 3.7 | 0–11.5 | ||
| TKI sensitive dual mutations | 3 | 66.6 | 9.1 | 1.0–17.1 | ||
| TKI sensitive / insensitive dual mutations | 33 | 45.7 | 9.9 | 0.9–18.9 | ||
Abbreviations: mPFS, median progression-free survival; NE, not estimable; RR, response rates; TKI, tyrosine kinase inhibitor.
Figure 3Bar graphs show responses observed with TKI in different uncommon mutations.
Notes: (A) Different types of EGFR mutations and response to EGFR TKIs. (B) Different types of EGFR mutations and response to EGFR TKI as per predicted sensitivity.
Abbreviations: PD, progressive disease; PR, partial response; SD, stable disease; TKI, tyrosine kinase inhibitor.
Type of TKI and survival
| Types of TKI | N | RR (%) | mPFS in months (95% CI) | mOS in months (95% CI) | |
|---|---|---|---|---|---|
| First generation TKI | 41 | 48.7 | 9.4 (7.9–10.9) | 18.3 (5.7–30.9) | |
| Second generation TKI | 1 | 100 | 15.28 | NR | |
| Third generation TKI | 15 | 33.3 | 6.0 (5.1–7.0) | 15.9 (6.6–25.2) | |
| Total | 57 | ||||
Abbreviations: mOS, median overall survival; mPFS, median progression-free survival; NR, not reached; RR, response rates; TKI, tyrosine kinase inhibitor.
List of all patients who received TKI therapy, their response, and survival
| Serial number | Mutation type | TKI received | Response | mPFS (months) | mOS (months) |
|---|---|---|---|---|---|
| 1 | Exon 19 deletion + exon 20 T790M | GEF | PR | 25.36 | 85.42 |
| 2 | Exon 21 L858R + exon 20 T790M | GEF | PR | 63.80 | 65.71 |
| 3 | Exon 19 deletion + exon 20 T790M | ERLO | PR | 5.19 | 5.19 |
| 4 | Exon 18 G719X | GEF | PR | 9.03 | 28.98 |
| 5 | Exon 20 insertion | GEF | PD | 2.79 | 22.24 |
| 6 | Exon 19 deletion + exon 20 T790M | GEF | PD | 1.77 | 28.42 |
| 7 | Exon 18 G719X | GEF | PR | 6.77 | 13.50 |
| 8 | Exon 19 deletion + exon 20 T790M | GEF | PR | 29.90 | 32.99 |
| 9 | Exon 19 deletion + exon 20 T790M | ERLO | PR | 19.38 | 33.02 |
| 10 | Exon 20 insertion | ERLO | PD | 1.48 | 1.48 |
| 11 | Exon 20 T790M and exon 21 L858 | GEF | PD | 1.64 | 28.32 |
| 12 | Exon 19 deletion + exon 20 T790M | ERLO | PR | 9.95 | 34.92 |
| 13 | Exon 19 deletion + exon 20 T790M | GEF | PR | 24.57 | 29.83 |
| 14 | Exon 19 deletion + exon 20 T790M | GEF | PR | 27.79 | 27.79 |
| 15 | Exon 19 deletion + exon 20 T790M | ERLO | PR | 15.51 | 22.67 |
| 16 | Exon 20+ VE, exon 21+ VE | ERLO | SD | 5.85 | 5.85 |
| 17 | Exon T790M | GEF | PR | 8.28 | 11.04 |
| 18 | Exon 19 deletion + exon 20 T790M | GEF | PR | 12.09 | 26.22 |
| 19 | Exon 18 G719X + exon 20 T790M | ERLO | SD | 7.49 | 10.25 |
| 20 | Exon 20 T790M mutant | ERLO | PR | 11.01 | 12.35 |
| 21 | Exon 19 deletion + exon 20 T790M | ERLO | SD | 3.09 | 9.26 |
| 22 | Exon 18+ VE + exon 20 768I | ERLO | PR | 9.13 | 9.69 |
| 23 | Exon 18 G719X | ERLO | PR | 16.53 | 16.53 |
| 24 | Exon 18 G719X + exon 21 L858R | GEF | PR | 9.43 | 18.37 |
| 25 | Exon 18 G719X + exon 20 768I | ERLO | PR | 15.28 | 15.28 |
| 26 | Exon 18 G719X, exon 20 S768I, and exon 21 L858R | GEF | PR | 15.34 | 15.34 |
| 27 | Exon 21 L858R, L861Q | GEF | 1.51 | 1.51 | |
| 28 | Exon 21 L861Q | ERLO | PD | 0.92 | 1.05 |
| 29 | Exon 20 insertion | ERLO | SD | 5.75 | 14.09 |
| 30 | Exon 21 L858R + exon 20 T790M | ERLO | 4.83 | 4.83 | |
| 31 | Exon 20 S768IT | ERLO | 4.93 | 9.56 | |
| 32 | Exon 21 L858R + exon 20 T790M | GEF | 4.11 | 5.95 | |
| 33 | Exon 21 L858R + exon 20 T790M | GEF | SD | 12.81 | 20.21 |
| 34 | Exon 18 G719X + exon 20 768I | GEF | 0.26 | 0.26 | |
| 35 | Exon 18 G719X | GEF | 3.15 | 3.15 | |
| 36 | Exon 20 S768I, exon 21 L858R | GEF | 2.04 | 2.04 | |
| 37 | Exon 19 deletion + exon 20 T790M | GEF | PR | 7.98 | 7.98 |
| 38 | Exon 21 L861Q | ERLO | 0.66 | 0.66 | |
| 39 | Exon 21 L858R + exon 20 T790M | GEF | 1.94 | 2.96 | |
| 40 | Exon 20 S768I | ERLO | 4.34 | 6.44 | |
| 41 | Exon 18 G719X | GEF | 3.35 | 3.35 | |
| 42 | Exon 20 insertion | AFA | SD | 5.22 | 5.22 |
| 43 | Exon 21 L858R + exon 20 T790M | OSI | PD | 2.40 | 2.40 |
| 44 | Exon 21 L858R + exon 20 T790M | OSI | PR | 6.08 | 6.54 |
| 45 | Exon 20 insertion | OSI | 1.54 | 1.54 | |
| 46 | Exon 19 deletion + exon 20 T790M | OSI | PD | 2.73 | 25.63 |
| 47 | Exon 21 L858R + exon 20 T790M | OSI | 1.05 | 1.05 | |
| 48 | Exon 20 insertion | OSI | 3.75 | 3.75 | |
| 49 | Exon 21 L858R + exon 20 T790M | OSI | PR | 3.68 | 7.92 |
| 50 | Exon 19 deletion + exon 20 T790M | OSI | PD | 1.35 | 1.35 |
| 51 | Exon 20 insertion | OSI | PD | 0.56 | 0.56 |
| 52 | Exon 21 L861I + exon 20 T790M | OSI | SD | 13.04 | 13.04 |
| 53 | Exon 19 deletion + exon 20 T790M | OSI | PR | 15.57 | 40.51 |
| 54 | Exon 20 T790M and exon 21 L861 | OSI | 3.35 | 3.35 | |
| 55 | Exon 20 insertion | OSI | PR | 15.28 | 15.28 |
| 56 | Exon 21 L858R + exon 20 T790M | OSI | PR | 5.49 | 21.98 |
| 57 | Exon 21 L858R + exon 20 T790M | OSI | PR | 12.71 | 15.93 |
Note:
Response could not be assessed.
Abbreviations: AFA, afatinib; ERLO, erlotinib; GEF, gefitinib; mOS, median overall survival; mPFS, median progression-free survival; OSI, osimertinib; PR, partial response; PD, progressive disease; SD, stable disease; TKI, tyrosine kinase inhibitor.
Comparison of survival times of patients with uncommon EGFR mutations
| Mutation types | mPFS on TKI Yang et al | mPFS on TKI Wu et al | mPFS on TKI Shi et al | mPFS on TKI in this study months (n) |
|---|---|---|---|---|
| Exon 18 G8719X | 10.7 (38) | 3.9 (10) | 8.2 (27) | 9.0 (5) |
| Exon 21 L861Q | 8.7 (7) | 7.6 (17) | 1.8 (2) | |
| Exon 20 S768I | 3.4 (9) | 1.0 (2) | ||
| Dual mutations | 2.9 (14) | 5.3 (20) | 4.2 | 9.4 (36) |
| Exon 20 insertion | 2.7 (23) | 1.4 (25) | 1.9 (7) | |
| Exon 20 T790M | 8.2 (6) |
Notes:
This study by Yang et al, included T790M mutation alone or in combination with other mutations.
Abbreviations: mPFS, median progression-free survival; TKI, tyrosine kinase inhibitor.