KRAS amplification in metastatic colon cancer is associated with a history of inflammatory bowel disease and may confer resistance to anti-EGFR therapy

Favazza, Laura; Parseghian, Christine M.; Kaya, Cihan; Nikiforova, Marina N.; Wald, Abigail I.; Landau, Michael S.; Proksell, Siobhan; Dueker, Jeffrey; Johnston, Elyse; Brand, Randall E.; Bahary, Nathan; Gorantla, Vikram C.; Rhee, John C.; Pingpank, James F.; Choudry, Haroon A.; Lee, Kenneth; Paniccia, Alessandro; Ongchin, Melanie; Zureikat, Amer H.; Bartlett, David L.; Singhi, Aatur D.

doi:10.1038/s41379-020-0560-x

Cited by 23 publications

(13 citation statements)

References 34 publications

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“…Another retrospective study by Favazza et al (11) reported that all eight patients with KRASamplified mCRC showed disease progression at the time of anti-EGFR therapy, and they concluded that KRAS amplification is responsible for the primary resistance to EGFR inhibitors. Meanwhile, RAS amplifications (involving KRAS, NRAS, and HRAS) were correlated with a younger median patient age at initial diagnosis and a history of inflammatory bowel disease (11). In the present case, KRAS amplification was present before chemotherapy, resulting in resistance to cetuximab.…”

Section: Discussionmentioning

confidence: 99%

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An Early-Onset Advanced Rectal Cancer Patient With Increased KRAS Gene Copy Number Showed A Primary Resistance to Cetuximab in Combination With Chemotherapy: A Case Report

et al. 2021

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Mutations in KRAS (codon 12/13), NRAS, BRAFV600E, and amplification of ERBB2 and MET account for 70–80% of anti-epidermal growth factor receptor (EGFR) monoclonal antibody primary resistance. However, the list of anti-EGFR monoclonal antibody primary resistance biomarkers is still incomplete. Herein, we report a case of wild-type RAS/BRAF metastatic colorectal cancer (CRC) with resistance to anti-EGFR monoclonal antibody and chemotherapy. Initially, mutation detection in postoperative tumor tissue by using amplification-refractory mutation system polymerase chain reaction indicated wild-type RAS/BRAF without point mutations, insertion deletions, or fusion mutations. Therefore, we recommended combined therapy of cetuximab and FOLFIRI after failure of platinum-based adjuvant chemotherapy, but the disease continued to progress. Next generation sequencing analysis of the postoperative tumor tissue revealed that KRAS copy number was increased and detected SMAD4, RNF43, and PREX2 mutations. This is the first case of advanced CRC with increased copy numbers of KRAS resistant to cetuximab and chemotherapy, which results in poor patient survival, and other mutated genes may be associated with the outcomes. Our findings indicate KRAS copy number alterations should also be examined, especially with anti-EGFR monoclonal antibody therapy in CRC, since it may be related with the primary resistance to these drugs.

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Section: Discussionmentioning

confidence: 99%

“…KRAS amplification in CRC is a rare event, with an overall prevalence of 0.67–2% ( 11 , 12 ). Previous studies have identified somatic mutations in KRAS as biomarkers for inherent resistance to EGFR-targeted drugs in patients with CRC ( 13 ), with a positive tissue mutation rate of 32–52.1% ( 7 ).…”

Section: Discussionmentioning

confidence: 99%

An Early-Onset Advanced Rectal Cancer Patient With Increased KRAS Gene Copy Number Showed A Primary Resistance to Cetuximab in Combination With Chemotherapy: A Case Report

et al. 2021

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“…KRAS is part of the RAS/MAPK pathway, a signalling pathway that plays a prominent role in cell proliferation and differentiation. This oncogene has long been found to be mutated, and more recently, amplified, in various types of human cancers, such as colorectal and lung cancer [35][36][37][38][39][40]. Even though RAS mutations are rare in human HCC, RAS activation occurs despite the absence of its mutation [41].…”

Section: Constitutive Oncogene Expression Modelmentioning

confidence: 99%

Inducible Liver Cancer Models in Transgenic Zebrafish to Investigate Cancer Biology

Lee¹,

Li²,

Gong³

2021

Cancers

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Primary liver cancer is one of the most prevalent and deadly cancers, which incidence continues to increase while treatment response remains poor; thus, in-depth understanding of tumour events is necessary to develop more effective therapies. Animal models for liver cancer are powerful tools to reach this goal. Over the past decade, our laboratory has established multiple oncogene transgenic zebrafish lines that can be robustly induced to develop liver cancer. Histological, transcriptomic and molecular analyses validate the use of these transgenic zebrafish as experimental models for liver cancer. In this review, we provide a comprehensive summary of our findings with these inducible zebrafish liver cancer models in tumour initiation, oncogene addiction, tumour microenvironment, gender disparity, cancer cachexia, drug screening and others. Induced oncogene expression causes a rapid change of the tumour microenvironment such as inflammatory responses, increased vascularisation and rapid hepatic growth. In several models, histologically-proven carcinoma can be induced within one week of chemical inducer administration. Interestingly, the induced liver tumours show the ability to regress when the transgenic oncogene is suppressed by the withdrawal of the chemical inducer. Like human liver cancer, there is a strong bias of liver cancer severity in male zebrafish. After long-term tumour progression, liver cancer-bearing zebrafish also show symptoms of cancer cachexia such as muscle-wasting. In addition, the zebrafish models have been used to screen for anti-metastasis drugs as well as to evaluate environmental toxicants in carcinogenesis. These findings demonstrated that these inducible zebrafish liver cancer models provide rapid and convenient experimental tools for further investigation of fundamental cancer biology, with the potential for the discovery of new therapeutic approaches.

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“…The mutual exclusivity of EGFR amplification and KRAS mutations has been described in lung adenocarcinoma and colorectal carcinoma (CRC) and co-expression caused cytotoxic effect on cells 39 , 40 . Even though the incidence of KRAS amplification compared to its mutation is low, such as less than10% of patients with gastric cancer or CRC and 17% in EAC, clinical features of patients with KRAS amplification are distinct, and the amplification is usually associated with poor prognosis in these patients 41 – 44 . The oncogenic effect of wild type KRAS amplification is mediated through the increased receptor tyrosine kinase-dependent activation of the Ras pathway in CRC 45 .…”

Section: Discussionmentioning

confidence: 99%

“…Like in gastric cancer, EAC, and CRC patients, KRAS amplification is associated with worse survival in ESCC patients 38 . Similar to mutant KRAS , wild type KRAS amplification confers EGFR inhibitor resistance 41 . Therefore, ESCC patients may benefit from detailed EGFR profiling and determination of tumor KRAS amplification status before targeted therapies.…”

Section: Discussionmentioning

confidence: 99%

Exome sequencing identifies novel somatic variants in African American esophageal squamous cell carcinoma

Erkizan¹,

Sukhadia

Natarajan³

et al. 2021

Sci Rep

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Esophageal cancer has a strikingly low survival rate mainly due to the lack of diagnostic markers for early detection and effective therapies. In the U.S., 75% of individuals diagnosed with esophageal squamous cell carcinoma (ESCC) are of African descent. African American ESCC (AA ESCC) is particularly aggressive, and its biological underpinnings remain poorly understood. We sought to identify the genomic abnormalities by conducting whole exome sequencing of 10 pairs of matched AA esophageal squamous cell tumor and control tissues. Genomic analysis revealed diverse somatic mutations, copy number alterations (SCNAs), and potential cancer driver genes. Exome variants created two subgroups carrying either a high or low tumor mutation burden. Somatic mutational analysis based on the Catalog of Somatic Mutations in Cancer (COSMIC) detected SBS16 as the prominent signature in the high mutation rate group suggesting increased DNA damage. SBS26 was also detected, suggesting possible defects in mismatch repair and microsatellite instability. We found SCNAs in multiple chromosome segments, encoding MYC on 8q24.21, PIK3CA and SOX2 on 3q26, CCND1, SHANK2, CTTN on 11q13.3, and KRAS on 12p12. Amplifications of EGFRvIII and EGFRvIVa mutants were observed in two patients, representing a novel finding in ESCC that has potential clinical relevance. This present exome sequencing, which to our knowledge, represents the first comprehensive exome analysis exclusively in AA ESCC, and highlights novel mutated loci that might explain the aggressive nature of AA ESCC and lead to the development of diagnostic and prognostic markers as well as therapeutic targets.

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KRAS amplification in metastatic colon cancer is associated with a history of inflammatory bowel disease and may confer resistance to anti-EGFR therapy

Cited by 23 publications

References 34 publications

An Early-Onset Advanced Rectal Cancer Patient With Increased KRAS Gene Copy Number Showed A Primary Resistance to Cetuximab in Combination With Chemotherapy: A Case Report

An Early-Onset Advanced Rectal Cancer Patient With Increased KRAS Gene Copy Number Showed A Primary Resistance to Cetuximab in Combination With Chemotherapy: A Case Report

Inducible Liver Cancer Models in Transgenic Zebrafish to Investigate Cancer Biology

Exome sequencing identifies novel somatic variants in African American esophageal squamous cell carcinoma

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