RNF43 mutation is associated with aggressive tumor biology along with BRAF V600E mutation in right-sided colorectal cancer

Right-sided colorectal cancer (RCRC) demonstrates worse survival outcome compared with left-sided CRC (LCRC). Recently, the importance of RNF43 mutation and BRAF V600E mutation has been reported in the serrated neoplasia pathway, which is one of the precancerous lesions in RCRC. It was hypothesized...

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Autores principales: Matsumoto, Akio, Shimada, Yoshifumi, Nakano, Mae, Oyanagi, Hidehito, Tajima, Yosuke, Nakano, Masato, Kameyama, Hitoshi, Hirose, Yuki, Ichikawa, Hiroshi, Nagahashi, Masayuki, Nogami, Hitoshi, Maruyama, Satoshi, Takii, Yasumasa, Ling, Yiwei, Okuda, Shujiro, Wakai, Toshifumi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: D.A. Spandidos 2020
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7160543/
https://www.ncbi.nlm.nih.gov/pubmed/32236609
http://dx.doi.org/10.3892/or.2020.7561
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author Matsumoto, Akio
Shimada, Yoshifumi
Nakano, Mae
Oyanagi, Hidehito
Tajima, Yosuke
Nakano, Masato
Kameyama, Hitoshi
Hirose, Yuki
Ichikawa, Hiroshi
Nagahashi, Masayuki
Nogami, Hitoshi
Maruyama, Satoshi
Takii, Yasumasa
Ling, Yiwei
Okuda, Shujiro
Wakai, Toshifumi
author_facet Matsumoto, Akio
Shimada, Yoshifumi
Nakano, Mae
Oyanagi, Hidehito
Tajima, Yosuke
Nakano, Masato
Kameyama, Hitoshi
Hirose, Yuki
Ichikawa, Hiroshi
Nagahashi, Masayuki
Nogami, Hitoshi
Maruyama, Satoshi
Takii, Yasumasa
Ling, Yiwei
Okuda, Shujiro
Wakai, Toshifumi
author_sort Matsumoto, Akio
collection PubMed
description Right-sided colorectal cancer (RCRC) demonstrates worse survival outcome compared with left-sided CRC (LCRC). Recently, the importance of RNF43 mutation and BRAF V600E mutation has been reported in the serrated neoplasia pathway, which is one of the precancerous lesions in RCRC. It was hypothesized that the clinical significance of RNF43 mutation differs according to primary tumor sidedness. To test this hypothesis, the clinicopathological characteristics and survival outcome of patients with RNF43 mutation in RCRC and LCRC were investigated. Stage I–IV CRC patients (n=201) were analyzed. Genetic alterations including RNF43 using a 415-gene panel were investigated. Clinicopathological characteristics between RNF43 wild-type and RNF43 mutant-type were analyzed. Moreover, RNF43 mutant-type was classified according to primary tumor sidedness, i.e., right-sided RNF43 mutant-type or left-sided RNF43 mutant-type, and the clinicopathological characteristics between the two groups were compared. RNF43 mutational prevalence, spectrum and frequency between our cohort and TCGA samples were compared. RNF43 mutation was observed in 27 out of 201 patients (13%). Multivariate analysis revealed that age (≥65), absence of venous invasion, and BRAF V600E mutation were independently associated with RNF43 mutation. Among the 27 patients with RNF43 mutation, 12 patients were right-sided RNF43 mutant-type and 15 left-sided RNF43 mutant-type. Right-sided RNF43 mutant-type was significantly associated with histopathological grade 3, presence of lymphatic invasion, APC wild, BRAF V600E mutation, microsatellite instability-high (MSI-H), and RNF43 nonsense/frameshift mutation compared with left-sided RNF43 mutant-type. Similarly, RNF43 nonsense/frameshift mutations were more frequently observed in RCRC compared with LCRC in the TCGA cohort (P=0.042). Right-sided RNF43 mutant-type exhibited significantly worse overall survival than RNF43 wild-type and left-sided RNF43 mutant-type (P=0.001 and P=0.023, respectively) in stage IV disease. RNF43 mutation may be a distinct molecular subtype which is associated with aggressive tumor biology along with BRAF V600E mutation in RCRC.
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spelling pubmed-71605432020-04-17 RNF43 mutation is associated with aggressive tumor biology along with BRAF V600E mutation in right-sided colorectal cancer Matsumoto, Akio Shimada, Yoshifumi Nakano, Mae Oyanagi, Hidehito Tajima, Yosuke Nakano, Masato Kameyama, Hitoshi Hirose, Yuki Ichikawa, Hiroshi Nagahashi, Masayuki Nogami, Hitoshi Maruyama, Satoshi Takii, Yasumasa Ling, Yiwei Okuda, Shujiro Wakai, Toshifumi Oncol Rep Articles Right-sided colorectal cancer (RCRC) demonstrates worse survival outcome compared with left-sided CRC (LCRC). Recently, the importance of RNF43 mutation and BRAF V600E mutation has been reported in the serrated neoplasia pathway, which is one of the precancerous lesions in RCRC. It was hypothesized that the clinical significance of RNF43 mutation differs according to primary tumor sidedness. To test this hypothesis, the clinicopathological characteristics and survival outcome of patients with RNF43 mutation in RCRC and LCRC were investigated. Stage I–IV CRC patients (n=201) were analyzed. Genetic alterations including RNF43 using a 415-gene panel were investigated. Clinicopathological characteristics between RNF43 wild-type and RNF43 mutant-type were analyzed. Moreover, RNF43 mutant-type was classified according to primary tumor sidedness, i.e., right-sided RNF43 mutant-type or left-sided RNF43 mutant-type, and the clinicopathological characteristics between the two groups were compared. RNF43 mutational prevalence, spectrum and frequency between our cohort and TCGA samples were compared. RNF43 mutation was observed in 27 out of 201 patients (13%). Multivariate analysis revealed that age (≥65), absence of venous invasion, and BRAF V600E mutation were independently associated with RNF43 mutation. Among the 27 patients with RNF43 mutation, 12 patients were right-sided RNF43 mutant-type and 15 left-sided RNF43 mutant-type. Right-sided RNF43 mutant-type was significantly associated with histopathological grade 3, presence of lymphatic invasion, APC wild, BRAF V600E mutation, microsatellite instability-high (MSI-H), and RNF43 nonsense/frameshift mutation compared with left-sided RNF43 mutant-type. Similarly, RNF43 nonsense/frameshift mutations were more frequently observed in RCRC compared with LCRC in the TCGA cohort (P=0.042). Right-sided RNF43 mutant-type exhibited significantly worse overall survival than RNF43 wild-type and left-sided RNF43 mutant-type (P=0.001 and P=0.023, respectively) in stage IV disease. RNF43 mutation may be a distinct molecular subtype which is associated with aggressive tumor biology along with BRAF V600E mutation in RCRC. D.A. Spandidos 2020-06 2020-03-23 /pmc/articles/PMC7160543/ /pubmed/32236609 http://dx.doi.org/10.3892/or.2020.7561 Text en Copyright: © Matsumoto et al. This is an open access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which permits use and distribution in any medium, provided the original work is properly cited, the use is non-commercial and no modifications or adaptations are made.
spellingShingle Articles
Matsumoto, Akio
Shimada, Yoshifumi
Nakano, Mae
Oyanagi, Hidehito
Tajima, Yosuke
Nakano, Masato
Kameyama, Hitoshi
Hirose, Yuki
Ichikawa, Hiroshi
Nagahashi, Masayuki
Nogami, Hitoshi
Maruyama, Satoshi
Takii, Yasumasa
Ling, Yiwei
Okuda, Shujiro
Wakai, Toshifumi
RNF43 mutation is associated with aggressive tumor biology along with BRAF V600E mutation in right-sided colorectal cancer
title RNF43 mutation is associated with aggressive tumor biology along with BRAF V600E mutation in right-sided colorectal cancer
title_full RNF43 mutation is associated with aggressive tumor biology along with BRAF V600E mutation in right-sided colorectal cancer
title_fullStr RNF43 mutation is associated with aggressive tumor biology along with BRAF V600E mutation in right-sided colorectal cancer
title_full_unstemmed RNF43 mutation is associated with aggressive tumor biology along with BRAF V600E mutation in right-sided colorectal cancer
title_short RNF43 mutation is associated with aggressive tumor biology along with BRAF V600E mutation in right-sided colorectal cancer
title_sort rnf43 mutation is associated with aggressive tumor biology along with braf v600e mutation in right-sided colorectal cancer
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7160543/
https://www.ncbi.nlm.nih.gov/pubmed/32236609
http://dx.doi.org/10.3892/or.2020.7561
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