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  4. The association of EGFR amplification with aberrant exon 20 insertion report using the cobas EGFR Mutation Test v2.
 
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The association of EGFR amplification with aberrant exon 20 insertion report using the cobas EGFR Mutation Test v2.

Journal
PloS one
Journal Volume
19
Journal Issue
4
Start Page
e0301120
ISSN
1932-6203
Date Issued
2024
Author(s)
Zhang, Man-San
Yeh, Yi-Chen
HSIEN-NENG HUANG  
Lin, Long-Wei
YEN-LIN HUANG  
Wang, Lei-Chi
Yao, Lai-Jin
Hung, Tze-Chun
Tseng, Yu-Fen
Lee, Yi-Hsuan
WEI-YU LIAO  
JIN-YUAN SHIH  
MIN-SHU HSIEH  
DOI
10.1371/journal.pone.0301120
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/720370
Abstract
Determining the exact type of epidermal growth factor receptor (EGFR) exon 20 insertion (ex20ins) mutation in lung cancer has become important. We found that not all ex20ins mutations reported by cobas EGFR test v2 could be validated by Sanger sequencing even using surgical specimens with high tumor contents. This study aimed to validate the ex20ins results reported by the cobas test and to determine whether there were clinicopathological factors associated with aberrant cobas ex20ins report. In total, 123 cobas-reported cases with ex20ins were retrospectively collected and validated by Sanger sequencing and Idylla assay. Clinicopathological features between ex20ins cobas+/Sanger+ group (n = 71) and cobas+/Sanger- group (n = 52) were compared. The Idylla assay detected ex20ins in 82.6% of cobas+/Sanger+ cases but only in 4.9% of cobas+/Sanger- cases. The cobas+/Sanger- group was significantly associated with higher tumor contents, poorly differentiated patterns, tumor necrosis, and a lower internal control cycle threshold value reported by the Idylla which suggesting the presence of increased EGFR gene copy numbers. EGFR fluorescence in situ hybridization (FISH) revealed the majority of cobas+/Sanger- group had EGFR high copy number gain (16%) or amplification (76%) according to the Colorado criteria. Among cases reported to have concomitant classic EGFR and ex20ins mutations by the cobas, the classic EGFR mutations were all detected by Sanger sequencing and Idylla, while the ex20ins mutations were undetected by Sanger sequencing (0%) or rarely reported by Idylla assay (3%). FISH revealed high EGFR copy number gain (17.9%) and amplification (79.5%) in cases reported having concomitant classic EGFR and ex20ins mutations by the cobas. This study demonstrated an unusually high frequency of EGFR amplification in cases with aberrant cobas ex20ins report which could not be validated by Sanger sequencing or Idylla assay. Ex20ins reported by the cobas test should be validated using other methods especially those reported having concomitant ex20ins and classic EGFR mutations.
SDGs

[SDGs]SDG3

Type
journal article

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