Mutational profile by targeted next generation sequencing of non-small cell lung cancer in the Mexican population

Hernández-Pedro, Norma; Soca-Chafre, Giovanny; Alaez-Versón, Carmen; Carrillo-Sánchez, Karol; Avilés-Salas, Alejandro; Vergara, Edgar; Arrieta, Oscar

doi:10.21149/10113

Abstract:

Objective:

Targeted next-generation sequencing (t-NGS) has revolutionized clinical diagnosis allowing multiplexed detection of genomic alterations. This study evaluated the profile of somatic mutations by t-NGS in Mexican patients with non-small cell lung cancer (NSCLC).

Materials and methods:

Genomic DNA was extracted from 90 lung adenocarcinomas and sequences were generated for a panel of 48 cancer genes. Epidermal Growth Factor Receptor (EGFR) mutations were detected in parallel by quantitative PCR.

Results:

The mutational profile of NSCLC revealed alterations in 27 genes, where TP53 (47.8%) and EGFR (36.7%) exhibited the highest mutation rates. EGFR Q787 mutations were present in 14 cases (15.6%), 10 cases had exon 19 deletions (11.1%), seven cases had L858R (7.8%). The mutational frequency for genes like EGFR, MET, HNF1A, HER2 and GUSB was different compared to caucasian population.

Conclusion:

t-NGS improved NSCLC treatments efficacy due to its sensitivity and specificity. A distinct pattern of somatic mutations was found in Mexican population.

Keywords:
mutational analysis, DNA; adenocarcinoma; lung; DNA sequencing

Resumen:

Objetivo:

La secuenciación dirigida de nueva generación (SNG) permite la detección múltiple de mutaciones. Este estudio evalúa el perfil de mutaciones somáticas por SNG en pacientes mexicanos con cáncer de pulmón de células no pequeñas (CPCNP).

Material y métodos:

Se aisló ADN de 90 muestras de pacientes con CPCNP y se analizarón 48 genes relacionados con cáncer. Las mutaciones del receptor del factor de crecimiento epidérmico (EGFR) se detectaron por PCR cuantitativa. Resultados. Se detectaron alteraciones en 27 genes. Las mutaciones más frecuentes fueron TP53 (47.8%) y EGFR (36.7%). En el gen EGFR, 14 casos fueron mutaciones Q787 (15.6%), 10 presentaron microdeleciones en el exón 19 (11.1%), y siete en L858R (7.8%). La frecuencia de mutación en EGFR, MET, HNF1A, HER2 y GUSB fue diferente en comparación con población caucásica.

Conclusión:

NGS modifica el tratamiento del paciente con CPCNP por su sensibilidad y especificidad para detectar mutaciones. La población mexicana presenta un perfil mutacional particular.

Palabras clave:
análisis mutacional del ADN; adenocarcinoma; pulmón; secuencias de ADN

Introduction

Lung cancer (LC) is the most common cause of global cancer-related mortality, with over a million deaths each year.¹1. Torre LA, Siegel RL, Jemal A. Lung Cancer Statistics. Adv Exp Med Biol. 2016;893:1-19. https://doi.org/10.1007/978-3-319-24223-1_1
https://doi.org/10.1007/978-3-319-24223-... Non-small cell lung cancer (NSCLC) represents 85% of the cases, the most frequent histological subtypes are adenocarcinoma, squamous cell carcinoma, and large cell carcinoma.²2. Arrieta O, Villarreal-Garza C, Zamora J, Blake-Cerda M, de la Mata MD, Zavala DG, et al. Long-term survival in patients with non-small cell lung cancer and synchronous brain metastasis treated with whole-brain radiotherapy and thoracic chemoradiation. Radiat Oncol. 2011;6(1):166. https://doi.org/10.1186/1748-717X-6-166
https://doi.org/10.1186/1748-717X-6-166... ^,³3. Raez LE, Santos ES, Rolfo C, Lopes G, Barrios C, Cardona A, et al. Challenges in facing the lung cancer epidemic and treating advanced disease in Latin America. Clin Lung Cancer. 2016;18(1):e71-9. https://doi.org/10.1016/J.CLLC.2016.05.003
https://doi.org/10.1016/J.CLLC.2016.05.0... NSCLCs are characterized by a unique pattern of genomic aberrations including mutations, amplifications, deletions, and rearrangements/fusions. Genetic profiling has identified driver mutations in over 80% of adenocarcinomas and approximately 47% of squamous cell carcinoma, many of which are relevant for clinical diagnosis and targeted therapy.⁴4. Arrieta O, Cardona AF, Martín C, Más-López L, Corrales-Rodríguez L, Bramuglia G, et al. Updated frequency of EGFR and KRAS mutations in nonsmall-cell lung cancer in Latin America: The Latin-American consortium for the investigation of lung cancer (CLICaP). J Thorac Oncol. 2015;10(5):838-43. https://doi.org/10.1097/JTO.0000000000000481
https://doi.org/10.1097/JTO.000000000000... ^,⁵5. Arrieta O, Cardona AF, Federico-Bramuglia G, Gallo A, Campos-Parra AD, Serrano S, et al. Genotyping non-small cell lung cancer (NSCLC) in Latin America. J Thorac Oncol. 2011;6(11):1955-9. https://doi.org/10.1097/JTO.0B013E31822F655F
https://doi.org/10.1097/JTO.0B013E31822F...

Currently, lung adenocarcinomas are treated on the basis of genomic aberrations to ensure better objective responses. Genomic testing of EGFR and ALK alterations is part of the standard diagnosis in NSCLC.⁶6. Herbst RS, Morgensztern D, Boshoff C. The biology and management of non-small cell lung cancer. Nature. 2018;553(7689):446-54. https://doi.org/10.1038/nature25183
https://doi.org/10.1038/nature25183... Patients harboring EGFR mutations in advanced NSCLC benefit from receiving EGFR tyrosine kinase inhibitors (TKIs), like erlotinib, afatinib, gefitinib and osimertinib.⁷7. Richer AL, Friel JM, Carson VM, Inge LJ, Whitsett TG. Genomic profiling toward precision medicine in non-small cell lung cancer: getting beyond eGFR. Pharmacogenomics Pers Med. 2015;8:63-7. https://doi.org/10.2147/PGPM.S52845
https://doi.org/10.2147/PGPM.S52845... Moreover, crizotinib has shown efficacy for patients with ALK-positive fusions. However, patients harboring sensitizing EGFR mutations develop TKIs resistance within one year.⁸8. Arrieta O, Cardona AF, Corrales L, Campos-Parra AD, Sánchez-Reyes R, Amieva-Rivera E, et al. The impact of common and rare EGFR mutations in response to EGFR tyrosine kinase inhibitors and platinum-based chemotherapy in patients with non-small cell lung cancer. Lung Cancer. 2015;87(2):169-75. https://doi.org/10.1016/j.lungcan.2014.12.009
https://doi.org/10.1016/j.lungcan.2014.1... ^,⁹9. Barrón F, Cardona AF, Corrales L, Ramirez-Tirado LA, Caballe-Perez E, Sanchez G, et al. Characteristics of progression to tyrosine kinase inhibitors predict overall survival in patients with advanced non-small cell lung cancer harboring an EGFR mutation. J Thorac Dis. 2018;10(4):2166-78. https://doi.org/10.21037/jtd.2018.03.106
https://doi.org/10.21037/jtd.2018.03.106...

Next-generation sequencing (NGS) has improved the diagnosis in NSCLC, and has increased the recognition of mutations like MET, BRAF and HER2 as novel targets for personalized therapies.¹⁰10. Reungwetwattana T, Weroha SJ, Molina JR. Oncogenic pathways, molecularly targeted therapies, and highlighted clinical trials in non-small-cell lung cancer (NSCLC). Clin Lung Cancer 2012;13(4):252l66. https://doi.org/10.1016/j.cllc.2011.09.004
https://doi.org/10.1016/j.cllc.2011.09.0... Furthermore, around 37% of the patients receive targeted therapy based in genomic profile.¹¹11. Tan O, Shrestha R, Cunich M, Schofield DJ. Application of next-generation sequencing to improve cancer management: A review of the clinical effectiveness and cost-effectiveness. Clin Genet. 2018;93(3):533-44. https://doi.org/10.1111/cge.13199
https://doi.org/10.1111/cge.13199... Recently, the evaluation of tumor mutational burden by NGS has been a useful predictor of response to treatment.¹²12. Cheng ML, Oxnard GR. Does TMB impact the effectiveness of TKIs in EGFR-mutant NSCLC? Clin Cancer Res. 2019;25(3):899-900. https://doi.org/10.1158/1078-0432.CCR-18-2368
https://doi.org/10.1158/1078-0432.CCR-18...

The mutation profile of many potentially actionable NSCLC genes in the Mexican population of patients remains largely unexplored. Previous studies by our group have described different NSCLC mutations and their relationship with clinical characteristics, such as never-smokers, female gender, wood smoke exposure and prognosis.¹³13. Soca-Chafre G, Hernández-Pedro N, Aviles-Salas A, Versón CA, Sánchez KC, Cardona AF, et al. Targeted next generation sequencing identified a high frequency genetic mutated profile in wood smoke exposure-related lung adenocarcinoma patients. Oncotarget. 2018;9(55):30499-512. https://doi.org/10.18632/oncotarget.25369
https://doi.org/10.18632/oncotarget.2536... ^,¹⁴14. Arrieta O, Ramírez-Tirado LA, Báez-Saldaña R, Peña-Curiel O, Soca-Chafre G, Macedo-Perez EO. Different mutation profiles and clinical characteristics among Hispanic patients with non-small cell lung cancer could explain the “Hispanic paradox.” Lung Cancer. 2015;90(2):161-6. https://doi.org/10.1016/j.lungcan.2015.08.010
https://doi.org/10.1016/j.lungcan.2015.0... EGFR mutations frequency vary among ethnic groups with 50-60% incidence in Asian patients, 10-15% in Caucasians, and 25-30% in Hispanics, in this population is particularly associated with female gender and never-smoker.⁴4. Arrieta O, Cardona AF, Martín C, Más-López L, Corrales-Rodríguez L, Bramuglia G, et al. Updated frequency of EGFR and KRAS mutations in nonsmall-cell lung cancer in Latin America: The Latin-American consortium for the investigation of lung cancer (CLICaP). J Thorac Oncol. 2015;10(5):838-43. https://doi.org/10.1097/JTO.0000000000000481
https://doi.org/10.1097/JTO.000000000000... ^,¹⁵15. Cardona AF, Zatarain-Barrón ZL, Rojas L, Arrieta O. The reality of complexity: concomitant genomic alterations in patients with EGFR mutations. J Thorac Dis. 2018;10(2):597-9. https://doi.org/10.21037/jtd.2017.12.136
https://doi.org/10.21037/jtd.2017.12.136... This molecular heterogeneity of NSCLC is particularly high in Latin American countries, including Mexico as shown by the Latin-American Consortium for the Investigation of Lung Cancer (CLICaP, by its acronym in Spanish).³3. Raez LE, Santos ES, Rolfo C, Lopes G, Barrios C, Cardona A, et al. Challenges in facing the lung cancer epidemic and treating advanced disease in Latin America. Clin Lung Cancer. 2016;18(1):e71-9. https://doi.org/10.1016/J.CLLC.2016.05.003
https://doi.org/10.1016/J.CLLC.2016.05.0... ^,⁴4. Arrieta O, Cardona AF, Martín C, Más-López L, Corrales-Rodríguez L, Bramuglia G, et al. Updated frequency of EGFR and KRAS mutations in nonsmall-cell lung cancer in Latin America: The Latin-American consortium for the investigation of lung cancer (CLICaP). J Thorac Oncol. 2015;10(5):838-43. https://doi.org/10.1097/JTO.0000000000000481
https://doi.org/10.1097/JTO.000000000000... The aim of this study was to characterize the presence of potentially actionable mutations in NSCLC in Mexican patients by targeted NGS, and compare the mutation frequencies among other populations.

Materials and methods

Study population

A prospective, two-center study was conducted in patients with locally advanced NSCLC (clinical stage IIIA, IIIB) or oligometastatic disease (clinical stage IV) treated at the Thoracic Oncology Clinic of the Instituto Nacional de Cancerología (INCAN) and Instituto Nacional de Enfermedades Respiratorias (INER) from April 2015 to April 2018.

Eligible patients were over 18 years old with histologically confirmed locally advanced NSCLC (clinical stage IIIA and IIIB) or oligometastatic disease (clinical stage IV) according to the eight edition lung cancer stage classification.¹⁶16. Detterbeck FC, Boffa DJ, Kim AW, Tanoue LT. The Eighth Edition Lung Cancer Stage Classification. Chest. 2017;151(1):193-203. https://doi.org/10.1016/j.chest.2016.10.010
https://doi.org/10.1016/j.chest.2016.10.... All recruited patients were required to have a white blood cell count ≥3 000/mm3, platelets ≥100 000/mm3, hemoglobin ≥12 gr/dl, creatinine ≤1.5 mg/dl, total bilirubin levels ≤1.5, transaminase levels (TGO, TGP) ≤2.5 the upper limit of normal (ULN), alkaline phosphatase <5 lower ULN. Patients were excluded if they had a history of prior RT or CT at the primary site, were pregnant or lactating, those using anticoagulants in therapeutic doses, patients with concurrent malignant diseases. All patients signed informed consent. Clinical characteristics such as age, sex, smoking status, tumor stage, histology, metastasis and response to treatment were recorded in a database. The protocol was approved by the scientific committee and ethics committee (15/049/ICI and CEI/1023/15).

Samples

From 2015 to 2018, a total of 90 tumor clinical specimens were analyzed as fresh-frozen and formalin-fixed paraffin-embedded (FFPE) samples. Lung adenocarcinomas were classified by a pathologist according to histology as follows: low (lepidic), intermediate (acinar and papillary) and high grade (solid).

DNA extraction

FFPE samples were deparaffinized previous to DNA extraction. DNA was extracted from both FFPE and fresh frozen biopsies using the Genomic DNA Wizard kit (Promega). DNA quantity was evaluated using a Quantus fluorometer (Promega, Mannheim Germany), the minimum amount of DNA required was 50 ng. DNA quality was evaluated using a Nanodrop 2000 Spectrophotometer (Thermo Fisher Scientific Waltham, MA, USA). DNA extracted from paraffin embedded tissues were analyzed by quantitative PCR (qPCR), with the FFPE QC Kit (Illumina) for detection of inhibitors prior to library preparation.

Library construction and Next-Generation Sequencing

The TruSeq Cancer Panel (llumina, CA) for 212 amplicons and 48 cancer-related genes was employed as previously described.¹³13. Soca-Chafre G, Hernández-Pedro N, Aviles-Salas A, Versón CA, Sánchez KC, Cardona AF, et al. Targeted next generation sequencing identified a high frequency genetic mutated profile in wood smoke exposure-related lung adenocarcinoma patients. Oncotarget. 2018;9(55):30499-512. https://doi.org/10.18632/oncotarget.25369
https://doi.org/10.18632/oncotarget.2536... Quality control for concentration and size of genomic libraries was performed with a Quantus fluorometer and a 2100 Bioanalyzer (Agilent Technologies, CA, USA). Targeted sequencing was performed on a MiSeq instrument, with an average sequencing depth per base of 1000X.

Sequence analysis and variant calling

Sequences analysis and variant calling were performed using a bioinformatic pipeline developed for this project. The quality of FASTQ files generated in the sequencer was tested by the FASTQC software. High quality sequences were aligned with BWA against hg19 as human reference genome, and processed with the PICARD tools package, which prepares the alignment to work with the GATK program. The GATK program consists of several modules, the first is responsible for realigning the sites of the genome with high propensity to insertions or deletions. The second module recalibrates the quality of reads and alignments variant calls were made with the muTect software. Statistical filters were applied to the variants to distinguish actual mutations from any possible artifacts. The filtered variants were marked regarding their possible functional consequence by snpEff and Variant Studio. EGFR and KRAS mutations were analyzed in parallel by qPCR using the Rotor-Gene Q and the Scorpions and ARMS technologies.

Statistical tests

Statistical tests were performed using SPSS version 24 (SPSS Inc., Chicago, IL, USA). Continuous variables were summarized as arithmetic mean and standard deviation. Nominal variables were shown as ratios and 95% confidence intervals (CI). The association between categorical variables were assessed using X² or Fisher exact tests, the Bonferroni correction was used for multiple comparisons. The Student t or Mann-Whitney U test were used for comparison of population means depending on data distribution. Progression free survival (PFS) and overall survival (OS) was calculated by Kaplan-Meier method and compared between mutations using the Log Rank or Breslow tests. The multivariate analysis was based on Cox proportion hazard model. A p value <0.05 was considered significant in two- tailed tests.

Results

Demographic characteristics

The clinical-pathological characteristics of the patients are the following: female gender in 76.7% of the cases, median age of 64.5 years with a range of 33-81 years, and 66.7% of 60 years or older (table I). Smokers represented 38.9% of the patients, 43.3% had wood-smoke exposure. The performance status of the patients was predominantly ECOG 0-1 in 84.4%. All cases were adenocarcinomas, 73.3% at advanced stage (IV), predominantly with intermediate histological grade (50%). Metastatic NSCLC was present in 26.7 % of the patients in contralateral lung, followed by bones (24.4%), pulmonary effusion (22.2%) and central nervous system (CNS) (18.9%). The carcinoembryonic antigen was elevated (≥10 ng/ml) in 47.8% of the patients. Chemotherapy was the treatment in 66.2% of the patients, while 33.8% received tyrosine kinase inhibitors (TKIs).

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Table I
Clinical characteristics of lung adenocarcinoma patients (N=90). Mexico, 2018

Somatic mutations

Mutations were found in 27 of 48 cancer-related genes sequenced (table II). TP53 mutations were detected in 43 patients (47.8%). In 36.7% of cases (33/90) mutations in the EGFR gene were found. The most frequent EGFR mutations were Q787 (15.6%), exon 19 deletions (11.1%), L858R mutation in exon 21 (7.8%), and T790M mutation in exon 20 (1.1%). Additional EGFR mutations were A750P and G719A (1.1%). Exon 19 deletions were identified in seven patients by qPCR, while by NGS ten cases were detected. Other mutations were identified, such as in KRAS, MET and PDGFRA (20%), HNF1A (14.4%), APC (12.2%) HER2 (11.1%) and MSH6 (10%). Alterations in lower frequency (<10%) were found in PIK3CA, GUSB, ALK rearrangements, KSR1, KIT, STK11, FLT3, ERBB4, VHL, CTTNB1, NOTCH1, GNAS, FGFR3, CDH1, BRAF, ABL1, FBXW7 and RB1.

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Table II
Molecular profile of somatic mutations in mexican patients with NSCLS (N=90). Mexico, 2018

There were concurrent mutations in TP53 and other genes, including EGFR in 51.2% of the patients (p=0.006), MET in 34.9% (p=0.001), KRAS in 27.9% (p=0.073), and PDGFRA in 39.5% (p<0.001); whereas TP53 mutations were mutually exclusive with HNF1 mutations in 93% of the cases (p=0.054), with APC in 76.7% (p=0.002) and HER2 in 79.1% (p=0.005).

Associations between mutations and clinical characteristics

There was an association between EGFR (p=0.005) and HER2 (p=0.026) mutations with intermediate histological grade. MET (p=0.046), APC (p=0.0051) and PDGFRA (p=0.009) mutations were more frequently in women. MET (p=0.012) and HNF1A (p=0.036) were predominant in patients with pulmonary effusion. TP53 mutations were common in former smokers (p=0.041), while never smokers presented higher incidence of APC mutations (p=0.030) and PDGFRA alterations correlated with ECOG 0-1 (p=0.042).

Survival of NSCLC patients

Table III shows that better PFS was associated with ECOG-PS ≤1, 11.0 vs. 2.4 months, (p=0.025); disease stage IIIB compared to IV, 21.7 vs. 7.7 months, (p=0.024); lymph nodes absent 13.5 vs. 4.8 months (p=0.020); absence of bone metastasis, 15.7 vs. 5.5 months (p=0.009); and no APC mutations, 11.0 vs. 6.4 months (p=0.057). In the multivariate analysis, the only significant factor of poor prognosis for PFS was the presence of APC mutations (HR 3.1 [1.1-8.8], p=0.032).

Factors associated with OS in univariate analysis (table III) were smoking status where current smokers had a median OS of 21.2 months (95%CI 9.8-32.5), former smokers 46.8 months (95%CI not reached) and never smokers 10.2 months (95%CI 5.0-15.4), p=0.027. Another factor was ECOG-PS PS ≤1, 19.5 vs. 1.3 months in, p<0.001. Multivariate analysis of OS showed that ECOG was the only independent factor with HR 2.9 (1.1-7.4), p=0.021.

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Table III
Univariate and multivariate analysis of the factors associated with progression-free survival and overall survival in Mexican patients with NSCLC (N=90). Mexico, 2018

According to data from the cBioportal database,¹⁷17. Cerami E, Gao J, Dogrusoz U, Gross BE, Sumer SO, Aksoy BA, et al. The cBio cancer genomics portal: An pen platform for exploring multidimensional cancer genomics data. Cancer Discov. 2012;2(5):401-4. https://doi.org/10.1158/2159-8290.CD-12-0095
https://doi.org/10.1158/2159-8290.CD-12-... ^,¹⁸18. Gao J, Aksoy BA, Dogrusoz U, Dresdner G, Gross B, Sumer SO, et al. Integrative analysis of complex cancer genomics and clinical profiles using the cBioPortal. Sci Signal. 2013;6(269):1-34. https://doi.org/10.1126/scisignal.2004088
https://doi.org/10.1126/scisignal.200408... we performed a comparison to determine differences in prevalence between the frequencies of somatic mutations in our population with respect to data for Caucasian patients. The Mexican population had a different prevalence of mutations in several genes including EGFR, MET, HNF1A, HER2 and GUSB (table IV). EGFR mutations were present in 36.7 vs. 17% in our population compared to Caucasians, while in MET gene the frequencies were 20 vs. 4%, HNF1A 14.4 vs. 2.7%, GUSB 8.9 vs. 0.5% (p<0.001), respectively, whereas in HER2 the mutation frequencies found were 11.1 vs. 2.2% (p=0.003).

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Table IV
Comparison between Hispanic and Caucasian population with NSCLC. Mexico, 2018

Discussion

Lung cancer is the human neoplasm with the highest mutation rate after melanoma, with over 10 mutations/Mb for smokers.¹⁹19. Watson IR, Takahashi K, Futreal PA, Chin L. Emerging patterns of somatic mutations in cancer. Nat Rev Genet. 2013;14(10):703-18. https://doi.org/10.1038/nrg3539
https://doi.org/10.1038/nrg3539... The presence of specific driver mutations has led to the development of targeted therapies for specific subsets of patients.²⁰20. Raez LE, Cardona AF, Santos ES, Catoe H, Rolfo C, Lopes G, et al. The burden of lung cancer in Latin-America and challenges in the access to genomic profiling, immunotherapy and targeted treatments. Lung Cancer. 2018;119:7-13. https://doi.org/10.1016/J.LUNGCAN.2018.02.014
https://doi.org/10.1016/J.LUNGCAN.2018.0... ^,²¹21. Tafe LJ, Pierce KJ, Peterson JD, De Abreu F, Memoli VA, Black CC, et al. Clinical genotyping of non-small cell lung cancers using targeted next-generation sequencing: utility of identifying rare and co-mutations in oncogenic driver genes 1. Neoplasia. 2016;18(9):577-83. https://doi.org/10.1016/j.neo.2016.07.010
https://doi.org/10.1016/j.neo.2016.07.01... In this study, we analyzed the mutation profile of NSCLC in the Mexican population, the association with clinical-pathological characteristics, therapeutic response and the contrast with other ethnic groups.

TP53 was the most frequently mutated gene in almost 50% of the patients and it was associated with former tobacco consumption. TP53 mutations had no prognostic value for OS of NSCLC patients. This tumor suppressor gene ranks first among the highly mutated genes in human cancers according to the lung cancer genome database.²²22. Cancer Genome Atlas Research Network. Comprehensive molecular profiling of lung adenocarcinoma. Nature. 2014;511(7511):543-50. https://doi.org/10.1038/nature13385
https://doi.org/10.1038/nature13385... To date, TP53 is not a therapeutic target, nevertheless, it represents a prognostic factor of response. Recently, it has been shown that TP53 mutations correlate with resistance to chemotherapy, worse therapeutic responses and reduced OS of NSCLC patients depending on disease stage and sequencing platforms. Likewise, the biological role of TP53 mutations can be different according to tumor histology and smoking history.²³23. Halvorsen AR, Silwal-Pandit L, Meza-Zepeda LA, Vodak D, Vu P, Sagerup C, et al. TP53 mutation spectrum in smokers and never smoking lung cancer patients. Front Genet. 2016;7:85. https://doi.org/10.3389/fgene.2016.00085
https://doi.org/10.3389/fgene.2016.00085...

TP53 mutations were concurrent with mutations in EGFR, MET, KRAS, and PDGFRA, while they were mutually exclusive with mutations in HNF1, APC and HER2. Concurrent mutations in TP53 and EGFR are frequent in NSCLC and may have impact on response rate, nonetheless, these results are diverse depending on the therapeutic approach. Recently, a comprehensive study by the lung cancer mutation consortium showed the adverse effect of concomitant mutations in TP53-mutated patients with targeted treatments for alterations in EGFR, ALK and ROS1, by developing resistance to chemotherapeutic agents. Moreover, the alterations imposed by TP53/KRAS co-mutations on cell-cycle regulation, control of DNA replication and repair result in higher neoantigen expression of neoantigens including PD-L1 upregulation, thereby increasing tumor immunogenicity.²⁴24. Dearden S, Stevens J, Wu YL, Blowers D. Mutation incidence and coincidence in non small-cell lung cancer: meta-analyses by ethnicity and histology (mutMap). Ann Oncol. 2013 ;24(9):2371-6. https://doi.org/10.1093/annonc/mdt205
https://doi.org/10.1093/annonc/mdt205... ^,²⁵25. Skoulidis F, Byers LA, Diao L, Papadimitrakopoulou VA, Tong P, Izzo J, et al. Co-occurring genomic alterations define major subsets of KRAS-mutant lung adenocarcinoma with distinct biology, immune profiles, and therapeutic vulnerabilities. Cancer Discov . 2015;5(8):861-78. https://doi.org/10.1158/2159-8290.CD-14-1236
https://doi.org/10.1158/2159-8290.CD-14-... Double-mutant tumors with TP53/KRAS co-mutations had significantly shorter OS and developed resistance to chemotherapy compared to wild type tumors. In contrast, TP53/KRAS co-mutation status was predictive of clinical benefit and better PFS in response to PD-1 immunotherapy.²⁶26. Aisner DL, Sholl LM, Berry L, Rossi M, Chen H, Fujimoto J, et al. The impact of smoking and TP53 mutations in lung adenocarcinoma patients with targetable mutations - the Lung Cancer Mutation Consortium (LCMC2). Clin Cancer Res . 2018;24(5):1038-47. https://doi.org/10.1158/1078-0432.CCR-17-2289
https://doi.org/1078-0432.CCR-17-2289... The incidence of other TP53 co-mutations have been recently reported, nevertheless, their prognostic value remains unclear.²³23. Halvorsen AR, Silwal-Pandit L, Meza-Zepeda LA, Vodak D, Vu P, Sagerup C, et al. TP53 mutation spectrum in smokers and never smoking lung cancer patients. Front Genet. 2016;7:85. https://doi.org/10.3389/fgene.2016.00085
https://doi.org/10.3389/fgene.2016.00085...

EGFR mutations are currently the main targetable oncogenic driver in the treatment of NSCLC patients, with improved response rates and less secondary effects than cytotoxic chemotherapy.²⁷27. Arrieta O, Cruz-Rico G, Soto-Perez-de Celis E, Ramírez-Tirado LA, Caballe-Perez E, Martínez-Hernández JN, et al. Reduction in hepatocyte growth factor serum levels is associated with improved prognosis in advanced lung adenocarcinoma patients treated with Afatinib: a Phase II trial. Target Oncol. 2016;11(5):619-29. https://doi.org/10.1007/s11523-016-0425-x
https://doi.org/10.1007/s11523-016-0425-... As previously reported, we found high prevalence of EGFR mutations, mainly exon 19 microdeletions and L858R point mutations in exon 21. In our study there was high concordance between results with qPCR based on Scorpions/ARMS technologies and the NGS platform in the detection of EGFR exon 19 deletions. EGFR mutations were associated with intermediate histological grade in advanced NSCLC. Consistently, a recent study indicated a correlation between moderately differentiated tumor grade and a higher frequency of EGFR mutations in metastatic lung adenocarcinomas. This modifies treatment selection, since patients with high grade or poorly differentiated tumors can be treated with chemotherapy or immunotherapy as first line treatment previous to obtaining the EGFR mutational status.²⁸28. Levy M, Lyon L, Barbero E, Wong J, Suga M, Sam D, et al. Histologic grade is predictive of incidence of epidermal growth factor receptor mutations in metastatic lung adenocarcinoma. Med Sci. 2017;5(4):1-12. https://doi.org/10.3390/medsci5040034
https://doi.org/10.3390/medsci5040034...

Other EGFR alterations found with low frequency were T790M mutation in exon 20 plus the A750P and G719A. Uncommon mutations are present in less than 10% of EGFR-mutant lung cancer and associated with high grade tumors, i.e. poorly differentiated, more aggressive phenotypes and could represent mechanisms of resistance to EGFR-TKI treatments.⁸8. Arrieta O, Cardona AF, Corrales L, Campos-Parra AD, Sánchez-Reyes R, Amieva-Rivera E, et al. The impact of common and rare EGFR mutations in response to EGFR tyrosine kinase inhibitors and platinum-based chemotherapy in patients with non-small cell lung cancer. Lung Cancer. 2015;87(2):169-75. https://doi.org/10.1016/j.lungcan.2014.12.009
https://doi.org/10.1016/j.lungcan.2014.1... There are no targeted therapies for uncommon EGFR mutations, as their responses to TKIs are variable and the role in tumor biology is still unresolved.

In this study, MET exon 14 mutations were present in 20% of the patients, associated with female gender, pulmonary effusion and TP53 mutations. MET gene encodes a tyrosine kinase receptor that binds the hepatocyte growth factor. MET exon 14 codes for a portion of the juxtamembrane domain containing the binding site for ubiquitin ligases that participate in MET protein degradation. Mutations in MET exon 14 mutations cause exon 14 skipping, leading to constitutive signaling and oncogenicity.⁸8. Arrieta O, Cardona AF, Corrales L, Campos-Parra AD, Sánchez-Reyes R, Amieva-Rivera E, et al. The impact of common and rare EGFR mutations in response to EGFR tyrosine kinase inhibitors and platinum-based chemotherapy in patients with non-small cell lung cancer. Lung Cancer. 2015;87(2):169-75. https://doi.org/10.1016/j.lungcan.2014.12.009
https://doi.org/10.1016/j.lungcan.2014.1... A recent study described a relationship between MET mutations, female gender and never smokers. Both MET mutations and amplifications show clinical benefit in NSCLC patients treated with TKIs not specifically designed for MET, having durable partial response with crizotinib and capmatinib and complete metabolic response with cabozantinib independently of histological subtype. Selective MET inhibitors have been developed such as tivantinib, onartuzumab and emibetuzumab with modest clinical benefits.⁸8. Arrieta O, Cardona AF, Corrales L, Campos-Parra AD, Sánchez-Reyes R, Amieva-Rivera E, et al. The impact of common and rare EGFR mutations in response to EGFR tyrosine kinase inhibitors and platinum-based chemotherapy in patients with non-small cell lung cancer. Lung Cancer. 2015;87(2):169-75. https://doi.org/10.1016/j.lungcan.2014.12.009
https://doi.org/10.1016/j.lungcan.2014.1... ^,²⁹29. Gkolfinopoulos S, Mountzios G. Beyond EGFR and ALK: targeting rare mutations in advanced non-small cell lung cancer. Ann Transl Med. 2018;6(8):142. https://doi.org/10.21037/atm.2018.04.28
https://doi.org/10.21037/atm.2018.04.28...

HER2 exon 20 mutations constitute 96% of the mutations in this gene and have been the most studied alterations in NSCLC. Conversely, other HER2 mutations have been described having prognostic value, including S310F/Y, D277G/H/V/Y and I655V.³⁰30. Peters S, Zimmermann S. Targeted therapy in NSCLC driven by HER2 insertions. Transl Lung Cancer Res. 2014;3(2):84-8. https://doi.org/10.3978/j.issn.2218-6751.2014.02.06
https://doi.org/10.3978/j.issn.2218-6751... Among the HER2 mutations in our study, I655V (exon 17) was detected with high frequency. This amino acid change in the transmembrane region increases tyrosine kinase activity leading to oncogenic signaling. I655V is present in different malignancies including breast, gastric and lung cancer. It correlates with aggressive tumor phenotype, poor prognosis and risk of cardiotoxicity during trastuzumab treatment of breast cancer.⁸8. Arrieta O, Cardona AF, Corrales L, Campos-Parra AD, Sánchez-Reyes R, Amieva-Rivera E, et al. The impact of common and rare EGFR mutations in response to EGFR tyrosine kinase inhibitors and platinum-based chemotherapy in patients with non-small cell lung cancer. Lung Cancer. 2015;87(2):169-75. https://doi.org/10.1016/j.lungcan.2014.12.009
https://doi.org/10.1016/j.lungcan.2014.1... ^,³¹31. Garrido-Castro AC, Felip E. HER2 driven non-small cell lung cancer (NSCLC): potential therapeutic approaches. Transl Lung Cancer Res. 2013 ;2(2):122-7. https://doi.org/10.3978/j.issn.2218-6751. 2013 .02.02
https://doi.org/10.3978/j.issn.2218-6751... However, there are few studies in lung cancer and without prognostic value.

In the present study, we found concurrence of HER2 mutations with intermediate histological grade and MET variants, but they were mutually exclusive with TP53 and EGFR mutations. There are no reports describing the association between HER2 mutations and tumor grade, although there is association with female gender, never smokers, adenocarcinomas, it has been reported that it confers a low sensitivity to traditional EGFR-TKIs.⁸8. Arrieta O, Cardona AF, Corrales L, Campos-Parra AD, Sánchez-Reyes R, Amieva-Rivera E, et al. The impact of common and rare EGFR mutations in response to EGFR tyrosine kinase inhibitors and platinum-based chemotherapy in patients with non-small cell lung cancer. Lung Cancer. 2015;87(2):169-75. https://doi.org/10.1016/j.lungcan.2014.12.009
https://doi.org/10.1016/j.lungcan.2014.1... ^,³⁰30. Peters S, Zimmermann S. Targeted therapy in NSCLC driven by HER2 insertions. Transl Lung Cancer Res. 2014;3(2):84-8. https://doi.org/10.3978/j.issn.2218-6751.2014.02.06
https://doi.org/10.3978/j.issn.2218-6751... HER2 mutations in NSCLC have a prevalence of 4% and may have higher clinical impact than gene amplification. Preliminary results from selective inhibitors for HER2 exon 20 mutations such as poziotinib had marked radiologic and clinical response. Additionally, several pan-EGFR irreversible inhibitors such as afatinib, neratinib, and dacomitinib have shown activity in NSCLC patients with HER2 mutations.⁸8. Arrieta O, Cardona AF, Corrales L, Campos-Parra AD, Sánchez-Reyes R, Amieva-Rivera E, et al. The impact of common and rare EGFR mutations in response to EGFR tyrosine kinase inhibitors and platinum-based chemotherapy in patients with non-small cell lung cancer. Lung Cancer. 2015;87(2):169-75. https://doi.org/10.1016/j.lungcan.2014.12.009
https://doi.org/10.1016/j.lungcan.2014.1... ^,³⁰30. Peters S, Zimmermann S. Targeted therapy in NSCLC driven by HER2 insertions. Transl Lung Cancer Res. 2014;3(2):84-8. https://doi.org/10.3978/j.issn.2218-6751.2014.02.06
https://doi.org/10.3978/j.issn.2218-6751... ^,³²32. Sullivan I, Planchard D. Next-Generation EGFR tyrosine kinase inhibitors for treating EGFR-mutant lung cancer beyond first line. Front Med. 2017;3:76. https://doi.org/10.3389/fmed.2016.00076
https://doi.org/10.3389/fmed.2016.00076...

Adenomatous polyposis coli (APC) is a tumor suppressor gene mutated in 80% of colon carcinomas and less frequently in other malignancies including liver, breast and lung cancer.³²32. Sullivan I, Planchard D. Next-Generation EGFR tyrosine kinase inhibitors for treating EGFR-mutant lung cancer beyond first line. Front Med. 2017;3:76. https://doi.org/10.3389/fmed.2016.00076
https://doi.org/10.3389/fmed.2016.00076... In our study, we found APC mutations in NSCLC that correlated with never smokers, were mutually exclusive with TP53 mutations and predicted poor prognosis. APC is part of the B-catenin degradation complex in the Wnt pathway. APC mutations induce nuclear B-catenin accumulation leading oncogene activation. APC mutations have been associated with nonsmokers in colorectal cancer.³³33. De Nicola F, Goeman F, Pallocca M, Sperati F, Pizzuti L, Melucci E, et al. Deep sequencing and pathway-focused analysis revealed multigene oncodriver signatures predicting survival outcomes in advanced colorectal cancer. Oncogenesis. 2018;7(7):1-10. https://doi.org/10.1038/s41389-018-0066-2
https://doi.org/10.1038/s41389-018-0066-... These mutations are generally insertions/deletions that modify frameshifts, introduce premature stop codons and loss of function via truncation of APC protein. Current therapies for APC loss in cancer inhibit signaling through the canonical Wnt/B-catenin pathway downstream of APC or aim to restore normal APC expression. APC and TP53 mutations occur early in the initiation of carcinogenesis, but they are not documented as mutually exclusive alterations.³⁴34. Rieth J, Subramanian S. Mechanisms of intrinsic tumor resistance to immunotherapy. Int J Mol Sci. 2018;19(5):1-13. https://doi.org/10.3390/ijms19051340
https://doi.org/10.3390/ijms19051340... Although these alterations alone may not be sufficient to have a significant impacto on OS concomitant TP53 and APC mutations have been described as a more aggressive molecular phenotype with implications for worse prognosis in PFS/OS.⁴4. Arrieta O, Cardona AF, Martín C, Más-López L, Corrales-Rodríguez L, Bramuglia G, et al. Updated frequency of EGFR and KRAS mutations in nonsmall-cell lung cancer in Latin America: The Latin-American consortium for the investigation of lung cancer (CLICaP). J Thorac Oncol. 2015;10(5):838-43. https://doi.org/10.1097/JTO.0000000000000481
https://doi.org/10.1097/JTO.000000000000...

There are differences in lung cancer incidence among different ethnic groups. While EGFR mutations appear in around 15% of North American and European patients, 40% of Asian patients, and between 2 to 14% of Afro-American patients, the frequency of EGFR mutations in Mexico is 27%.⁴4. Arrieta O, Cardona AF, Martín C, Más-López L, Corrales-Rodríguez L, Bramuglia G, et al. Updated frequency of EGFR and KRAS mutations in nonsmall-cell lung cancer in Latin America: The Latin-American consortium for the investigation of lung cancer (CLICaP). J Thorac Oncol. 2015;10(5):838-43. https://doi.org/10.1097/JTO.0000000000000481
https://doi.org/10.1097/JTO.000000000000... ^,³⁵35. Barrón F, Zatarain-Barrón ZL, Cardona AF, Arrieta O. Extending the curve: survival of EGFR-mutated lung cancer patients in the 21st century. J Thorac Dis. 2018;10(3):1265-8. https://doi.org/10.21037/jtd.2018.03.28
https://doi.org/10.21037/jtd.2018.03.28... In our study, the prevalence of EGFR mutations was 36.7% compared to 17% in Caucasians. Other important differences in mutation frequency between the two populations were present in known oncogenic drivers of NSCLC such as MET and HER2, while the frequency of KRAS mutation was higher in Caucasians as expected although not statistically significant. The incidence of KRAS mutations in NSCLC in Latin America is approximately 14-17% as reported by the CLICaP.⁴4. Arrieta O, Cardona AF, Martín C, Más-López L, Corrales-Rodríguez L, Bramuglia G, et al. Updated frequency of EGFR and KRAS mutations in nonsmall-cell lung cancer in Latin America: The Latin-American consortium for the investigation of lung cancer (CLICaP). J Thorac Oncol. 2015;10(5):838-43. https://doi.org/10.1097/JTO.0000000000000481
https://doi.org/10.1097/JTO.000000000000... MET mutation profile also differs in type and frequency according to ethnicity. In our study, HER2 mutations were present in 11.1% of the Mexican patients in contrast to 2.2% in Caucasians and 3.9% in Asians. Similarly to EGFR mutations, HER2 mutations are associated with adenocarcinoma histology, female gender and never smokers and have favorable response to TKI and antibody treatments.²³23. Halvorsen AR, Silwal-Pandit L, Meza-Zepeda LA, Vodak D, Vu P, Sagerup C, et al. TP53 mutation spectrum in smokers and never smoking lung cancer patients. Front Genet. 2016;7:85. https://doi.org/10.3389/fgene.2016.00085
https://doi.org/10.3389/fgene.2016.00085... A higher incidence of HER2 mutations in our population opens the opportunity to improve response rates and overall survival with novel targeted therapies.

Conclusions

This study provides a profile of somatic mutations for NSCLC in the Mexican population. The main genomic alterations were present in TP53, EGFR, KRAS, MET, PDGFRA, HNF1A, APC, HER2 and MSH6. This mutation profile shows differences with other ethnic groups. Further studies are warranted to evaluate the germline molecular features underlying the relationship between ethnicity, somatic mutation rates, clinical responses and survival of NSCLC patients.

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Publication Dates

Publication in this collection
20 Mar 2020
Date of issue
May-Jun 2019

History

Received
23 Oct 2018
Accepted
05 Apr 2019

This is an open-access article distributed under the terms of the Creative Commons Attribution License

[1] ¹
Torre LA, Siegel RL, Jemal A. Lung Cancer Statistics. Adv Exp Med Biol. 2016;893:1-19. https://doi.org/10.1007/978-3-319-24223-1_1
» https://doi.org/10.1007/978-3-319-24223-1_1

[2] ²
Arrieta O, Villarreal-Garza C, Zamora J, Blake-Cerda M, de la Mata MD, Zavala DG, et al Long-term survival in patients with non-small cell lung cancer and synchronous brain metastasis treated with whole-brain radiotherapy and thoracic chemoradiation. Radiat Oncol. 2011;6(1):166. https://doi.org/10.1186/1748-717X-6-166
» https://doi.org/10.1186/1748-717X-6-166

[3] ³
Raez LE, Santos ES, Rolfo C, Lopes G, Barrios C, Cardona A, et al Challenges in facing the lung cancer epidemic and treating advanced disease in Latin America. Clin Lung Cancer. 2016;18(1):e71-9. https://doi.org/10.1016/J.CLLC.2016.05.003
» https://doi.org/10.1016/J.CLLC.2016.05.003

[4] ⁴
Arrieta O, Cardona AF, Martín C, Más-López L, Corrales-Rodríguez L, Bramuglia G, et al Updated frequency of EGFR and KRAS mutations in nonsmall-cell lung cancer in Latin America: The Latin-American consortium for the investigation of lung cancer (CLICaP). J Thorac Oncol. 2015;10(5):838-43. https://doi.org/10.1097/JTO.0000000000000481
» https://doi.org/10.1097/JTO.0000000000000481

[5] ⁵
Arrieta O, Cardona AF, Federico-Bramuglia G, Gallo A, Campos-Parra AD, Serrano S, et al Genotyping non-small cell lung cancer (NSCLC) in Latin America. J Thorac Oncol. 2011;6(11):1955-9. https://doi.org/10.1097/JTO.0B013E31822F655F
» https://doi.org/10.1097/JTO.0B013E31822F655F

[6] ⁶
Herbst RS, Morgensztern D, Boshoff C. The biology and management of non-small cell lung cancer. Nature. 2018;553(7689):446-54. https://doi.org/10.1038/nature25183
» https://doi.org/10.1038/nature25183

[7] ⁷
Richer AL, Friel JM, Carson VM, Inge LJ, Whitsett TG. Genomic profiling toward precision medicine in non-small cell lung cancer: getting beyond eGFR. Pharmacogenomics Pers Med. 2015;8:63-7. https://doi.org/10.2147/PGPM.S52845
» https://doi.org/10.2147/PGPM.S52845

[8] ⁸
Arrieta O, Cardona AF, Corrales L, Campos-Parra AD, Sánchez-Reyes R, Amieva-Rivera E, et al The impact of common and rare EGFR mutations in response to EGFR tyrosine kinase inhibitors and platinum-based chemotherapy in patients with non-small cell lung cancer. Lung Cancer. 2015;87(2):169-75. https://doi.org/10.1016/j.lungcan.2014.12.009
» https://doi.org/10.1016/j.lungcan.2014.12.009

[9] ⁹
Barrón F, Cardona AF, Corrales L, Ramirez-Tirado LA, Caballe-Perez E, Sanchez G, et al Characteristics of progression to tyrosine kinase inhibitors predict overall survival in patients with advanced non-small cell lung cancer harboring an EGFR mutation. J Thorac Dis. 2018;10(4):2166-78. https://doi.org/10.21037/jtd.2018.03.106
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Study Population	Characteristics	All (N=90) % (n/N)
Gender	Female	76.7 (69/90)
Gender	Male	23.3 (21/90)
Age	Median (Range)	64.5 (33-81)
	<60 years	33.3 (30/90)
	≥60 years	66.7 (60/90)
Tobacco-smoking exposure and smoking index	Median (Range)	12.25 (0-120)
	Never-smokers	61.1 (55/90)
	Former-smokers	25.6 (23/90)
	Current-smokers	13.3 (12/90)
Wood-smoke exposure	Absent	56.7 (51/90)
Wood-smoke exposure	Present	43.3 (39/90)
ECOG PS	0-1	84.4 (76/90)
ECOG PS	2+	15.6 (14/90)
Disease stage	IIIB	26.7 (24/90)
Disease stage	IV	73.3 (66/90)
Histological grade	High	13.3 (12/90)
	Intermediate	50.0 (45/90)
	Low	36.7 (33/90)

Metastasis
Lung	Absent	72.2 (65/89)
Lung	Present	26.7 (24/89)
Bone	Absent	74.4 (67/89)
Bone	Present	24.4 (22/89)
Pulmonary effusion	Absent	76.7 (69/89)
Pulmonary effusion	Present	22.2 (20/89)
CNS	Absent	80.0 (72/89)
CNS	Present	18.9 (17/89)
Lymph nodes	Absent	90.0 (81/89)
Lymph nodes	Present	8.9 (8/89)
Liver	Absent	90.0 (81/89)
Liver	Present	8.9 (8/89)
Liver	Absent	90.0 (81/89)
Liver	Present	8.9 (8/89)
Adrenal	Absent	93.3 (84/89)
Adrenal	Present	5.6 (5/89)
Other	Absent	88.9 (80/89)
Other	Present	10.0 (9/89)
CEA	<10 ng/ml	43.3 (39/82)
	≥10 ng/ml	47.8 (43/82)

Gene		All (N=90) % (n/N)

TP53	Negative	52.2 (47/90)
TP53	Positive	47.8 (43/90)
EGFR	Negative	63.3 (57/90)
EGFR	Positive	36.7 (33/90)
EGFR exons	Exon 19 (Deletion)	11.1 (10/90)
	Exon 21 (L858R)	7.8 (7/90)
	Exon 20 (T790M)	1.1 (1/90)
	Exon 20 (Q787)	15.6 (14/90)
	Other	2.2 (4/90)
KRAS	Negative	80.0 (72/90)
KRAS	Positive	20.0 (18/90)
MET	Negative	80.0 (72/90)
MET	Positive	20.0 (18/90)
PDGFRA	Negative	80.0 (72/90)
PDGFRA	Positive	20.0 (18/90)
HNF1A	Negative	85.6 (77/90)
HNF1A	Positive	14.4 (13/90)
APC	Negative	87.8 (79/90)
APC	Positive	12.2 (11/90)
HER2	Negative	88.9 (80/90)
HER2	Positive	11.1 (10/90)
MSH6	Negative	90.0 (84/90)
MSH6	Positive	10.0 (9/90)
PIK3CA	Negative	91.1 (82/90)
PIK3CA	Positive	8.9 (8/90)
GUSB	Negative	91.1 (82/90)
GUSB	Positive	8.9 (8/90)
ALK fusions	Negative	87.8 (79/85)
ALK fusions	Positive	6.7 (6/85)
KSR1	Negative	94.4 (85/90)
KSR1	Positive	5.6 (5/90)
KIT	Negative	96.7 (87/90)
KIT	Positive	3.3 (3/90)
STK11	Negative	96.7 (87/90)
STK11	Positive	3.3 (3/90)
FLT3	Negative	98.7 (88/90)
FLT3	Positive	2.2 (2/90)
ERBB4	Negative	97.8 (88/90)
ERBB4	Positive	2.2 (2/90)
VHL	Negative	97.8 (88/90)
VHL	Positive	2.2 (2/90)
CTNNB1	Negative	97.8 (88/90)
CTNNB1	Positive	2.2 (2/90)
NOTCH1	Negative	97.8 (88/90)
NOTCH1	Positive	2.2 (2/90)
GNAS	Negative	98.9 (89/90)
GNAS	Positive	1.1 (1/90)
FGFR3	Negative	98.1 (89/90)
FGFR3	Positive	1.1 (1/90)
CDH1	Negative	98.9 (89/90)
CDH1	Positive	1.1 (1/90)
BRAF	Negative	98.9 (89/90)
	Positive	1.1 (1/90)
ABL1	Negative	98.9 (89/90)
	Positive	1.1 (1/90)
FBXW7	Negative	98.9 (89/90)
	Positive	1.1 (1/90)
RB1	Negative	98.9 (89/90)
	Positive	1.1 (1/90)

		Progression-free survival				Overall survival
		Univariate analysis		Multivariate analysis		Univariate analysis		Multivariate analysis
		Mean, 95%CI	p-Value	HR (95%CI)	p-Value	Mean, 95%CI	p-Value	HR (95%CI)	p-Value

OVERALL		10.1 (4.0-16.2)				15.2 (9.3-21.1)
Gender	Female	9.4 (5.3-13.5)	0.21			15.2 (5.9-24.5)	0.737
Gender	Male	21.7 (0.0-48.3)	0.21			15.7 (9.3-22.1)	0.737
Age	<60 years	9.2 (4.6-13.9)	0.982			12.9 (2.5-23.3)	0.939
Age	≥60 years	10.7 (2.2-19.2)	0.982			16.6 (8.5-24.7)	0.939
Tobacco exposure	Never smoker	8.1 (3.4-12.8)	0.051	0.834 (0.50-1.3)	0.479	10.2 (5.0-15.4)	0.027	0.68 (0.43-1.0)	0.098
	Former smoker	21.7 (1.8-41.6)				46.8 (NR)
	Current smoker	NR (NR)				21.2 (9.8-32.5)
Wood-smoke expossure	Absent	11.0 (2.4-19.6)	0.131			21.1 (11.7-30.6)	0.103
Wood-smoke expossure	Present	7.7 (2.4-12.9)	0.131			10.2 (1.2-19.2)	0.103
ECOG PS	0-1	11.0 (4.4-17.5)	0.025	1.5 (0.59-4.25)		19.5 (13.5-25.5)	<0.001	2.9 (1.1-7.4)	0.021
ECOG PS	2+	2.4 (1.3-3.6)	0.025	1.5 (0.59-4.25)	0.36	1.3 (1.2-6.5)	<0.001	2.9 (1.1-7.4)	0.021
Disease stage	IIIB	21.7 (13.3-30.1)	0.024	2.3 (0.91-5.8)		21.2 (13.2-29.1)	0.322
Disease stage	IV	7.7 (3.2-12.2)	0.024	2.3 (0.91-5.8)	0.07	12.8 (6.4-19.2)	0.322
Histological grade	High	16.0 (0.0-34.2)	0.556			12.1 (0.0-31.8)	0.512
	Intermediate	6.4 (0.65-12.2)				15.5 (3.4-27.5)
	Low	11.0 (4.9-17.0)				15.2 (3.8-26.6)

Metastasis

CNS	Absent	11.0 (3.4-18.5)	0.181			15.2 (7.0-23.4)	0.762
CNS	Present	5.2 (0.9-10.4)	0.181			13.6 (4.3-22.9)	0.762
Lung	Absent	10.7 (4.9-16.5)	0.517			12.8 (5.0-20.5)	0.843
Lung	Present	4.8 (3.7-5.9)	0.517			16.6 (9.7-23.5)	0.843
Pulmonary effusion	Absent	10.7 (2.9-18.4)	0.816			15.5 (9.6-21.3)	0.963
Pulmonary effusion	Present	9.4 (3.1-15.7)	0.816			10.2 (0.0-26.2)	0.963
Lymph nodes	Absent	13.5 (6.5-20.4)	0.02	1.8 (0.62-5.1)		13.6 (6.4-20.7)	0.993
Lymph nodes	Present	4.8 (0.0-10.4)	0.02	1.8 (0.62-5.1)	0.24	15.2 (0.0-32.3)	0.993
Liver	Absent	11.0 (4.1-17.9)	0.756			15.5 (9.2-21.7)	0.988
Liver	Present	5.7 (3.7-7.7)	0.756			9.7 (0.0-25.1)	0.988
Bone	Absent	15.7 (8.3-23.1)	0.009	1.4 (0.69-2.9)		18.3 (9.2-27.5)	0.16
Bone	Present	5.5 (4.3-6.7)	0.009	1.4 (0.69-2.9)	0.329	8.6 (2.4-14.8)	0.16
CEA	<10 ng/ml	18.3 (9.2-27.3)	0.167			15.7 (9.5-21.9)	0.37
CEA	≥10 ng/ml	10.7 (4.2-17.2)	0.167			21.2 (11.0-31.4)	0.37
Chemotherapy	No	14.6(6.3-22.9)	0.503			20.8 (11.7-30.0)	0.152
Chemotherapy	Yes	87.1 (2.1-14.1)	0.503			12.9 (3.1-22.7)	0.152
EGFR	Negative	13.5 (2.9-24.1)	0.492			12.8 (3.4-22.2)	0.43
EGFR	Positive	9.2 (2.7-15.7)	0.492			17.7 (10.0-25.3)	0.43
KRAS	Negative	10.7 (5.3-16.1)	0.946			15.7 (9.9-21.5)	0.934
KRAS	Positive	5.2 (0.0-26.1)	0.946			7.5 (0.0-19.1)	0.934
MSH6	Negative	11.0 (5.1-16.8)	0.063			15.2 (9.6-20.8)	0.792
MSH6	Positive	6.4 (2.3-6.0)	0.063			22.1 (0.0-64.8)	0.792
TP53	Negative	11.0 (2.7-19.22)	0.514			15.2 (5.4-25.0)	0.469
TP53	Positive	8.1 (1.7-14.5)	0.514			15.5 (7.0-23.9)	0.469
HER 2	Negative	10.7 (5.0-16.4)	0.628			15.2 (9.6-20.8)	0.438
HER 2	Positive	5.7 (3.5-7.9)	0.628			9.7 (0.0-24.9	0.438
HNF1A	Negative	9.2 (4.8-13.6)	0.765			13.6 (6.0-21.1)	0.621
HNF1A	Positive	18.3 (8.1-28.5)	0.765			18.5 (8.9-28.2)	0.621
PIK3CA	Negative	10.7 (4.7-16.9)	0.184			13.6 (7.3-19.8)	0.677
PIK3CA	Positive	4.8 (2.1-7.5)	0.184			19.5 (0.0-44.9)	0.677
MET	Negative	13.5 (6.8 (20.2)	0.183			15.5 (9.7-21.2)	0.668
MET	Positive	4.8 (3.3-6.3)	0.183			7.5 (2.6-12.4)	0.668
APC	Negative	11.0 (4.2-17.8)	0.057	3.1 (1.1-8.8)	0.032	15.5 (9.6-21.3)	0.742
APC	Positive	6.4 (3.4-9.4)	0.057	3.1 (1.1-8.8)	0.032	7.5 (0.0-28.6)	0.742
ALK FISH	Negative	10.7 (4.8-16.6)	0.993			15.7 (10.2-21.2)	0.515
ALK FISH	Positive	2.9 (0.0-20.4)	0.993			4.0 (1.7-6.36)	0.515
PDGFRA	Negative	13.5 (5.6-21.4)	0.071			12.9 (7.3-18.6)	0.273
PDGFRA	Positive	4.8 (2.6-7.0)	0.071			22.1 (6.3-38.0)	0.273
GUSB	Negative	10.7 (5.2-16.2)	0.893			15.2 (9.5-20.9)	0.374
GUSB	Positive	5.7 (3.1-8.3)	0.893			9.7 (NR)	0.374

Saúde Pública

Saúde Pública

Mutational profile by targeted next generation sequencing of non-small cell lung cancer in the Mexican population

Perfil mutacional por secuenciación de nueva generación en cáncer de pulmón de células no pequeñas en población mexicana.

Abstract:

Objective:

Materials and methods:

Results:

Conclusion:

Resumen:

Objetivo:

Material y métodos:

Conclusión:

Introduction

Materials and methods

Study population

Samples

DNA extraction

Library construction and Next-Generation Sequencing

Sequence analysis and variant calling

Statistical tests

Results

Demographic characteristics

Somatic mutations

Associations between mutations and clinical characteristics

Survival of NSCLC patients

Discussion

Conclusions

References

Publication Dates

History

Hispanics N= 90			Caucasians N=183
Genes	n	%	n	%	P Value*

TP53	43	47.8	93	51	0,636
EGFR	33	36.7	31	17	<0.001*
KRAS	18	20	49	27	0,221
MET	18	20	7	4	<0.001*
PDGFRA	18	20	15	8	0,005
HNF1A	13	14.4	5	2.7	<0.001*
APC	11	12.2	9	5	0,029
HER2	10	11.1	4	2.2	0.003*
MSH6	9	10	4	2.2	0,012
PIK3CA	8	8.9	7	4	0,084
GUSB	8	8.9	1	0.5	<0.001*