Cargando…
The somatic POLE P286R mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy
Early-onset colorectal cancers (EOCRCs) may have biological or genomic features distinct from late-onset CRCs (LOCRCs). Previous studies have mostly focused on the germline predisposition conditions of EOCRCs, but we hypothesized that EOCRCs may have distinct somatic aberrations that accelerate canc...
| Autores principales: | , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Impact Journals LLC
2016
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5356579/ https://www.ncbi.nlm.nih.gov/pubmed/27612425 http://dx.doi.org/10.18632/oncotarget.11862 |
| _version_ | 1782515865625821184 |
|---|---|
| author | Ahn, Sung-Min Ansari, Adnan Ahmad Kim, Jihun Kim, Deokhoon Chun, Sung-Min Kim, Jiyun Kim, Tae Won Park, Inja Yu, Chang-Sik Jang, Se Jin |
| author_facet | Ahn, Sung-Min Ansari, Adnan Ahmad Kim, Jihun Kim, Deokhoon Chun, Sung-Min Kim, Jiyun Kim, Tae Won Park, Inja Yu, Chang-Sik Jang, Se Jin |
| author_sort | Ahn, Sung-Min |
| collection | PubMed |
| description | Early-onset colorectal cancers (EOCRCs) may have biological or genomic features distinct from late-onset CRCs (LOCRCs). Previous studies have mostly focused on the germline predisposition conditions of EOCRCs, but we hypothesized that EOCRCs may have distinct somatic aberrations that accelerate cancer development. To identify the somatic aberrations that accelerate cancer development at an early age, we conducted whole exome sequencing for 28 polyposis-unrelated, microsatellite stable (MSS) EOCRCs with no known germline predisposition conditions. Surprisingly, we found two distinct groups in the context of mutational burden: 6 hypermutated cases with 2325 to 10973 mutations and 22 nonhypermutated cases with 47 to 154 mutations. Further analysis revealed that four of the six hypermutated cases had the same POLE P286R mutation. We validated this finding in 83 MSS EOCRCs and 27 MSS LOCRCs, which revealed that 7.2% of EOCRCs (6/83) had the POLE P286R mutation, which was not found in LOCRCs. Clinicopathologically, EOCRCs with POLE mutations occurred far more frequently in the right colon than in the left colon, affecting men more frequently than women. In summary, we have identified a unique subclass of colon cancer characterized by a hypermutation associated with the POLE mutation. The acquisition of the POLE mutation leading to hypermutation can accelerate cancer development. Clinically, this subset with hypermutation may be susceptible to immune checkpoint blockade. |
| format | Online Article Text |
| id | pubmed-5356579 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2016 |
| publisher | Impact Journals LLC |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-53565792017-03-24 The somatic POLE P286R mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy Ahn, Sung-Min Ansari, Adnan Ahmad Kim, Jihun Kim, Deokhoon Chun, Sung-Min Kim, Jiyun Kim, Tae Won Park, Inja Yu, Chang-Sik Jang, Se Jin Oncotarget Research Paper Early-onset colorectal cancers (EOCRCs) may have biological or genomic features distinct from late-onset CRCs (LOCRCs). Previous studies have mostly focused on the germline predisposition conditions of EOCRCs, but we hypothesized that EOCRCs may have distinct somatic aberrations that accelerate cancer development. To identify the somatic aberrations that accelerate cancer development at an early age, we conducted whole exome sequencing for 28 polyposis-unrelated, microsatellite stable (MSS) EOCRCs with no known germline predisposition conditions. Surprisingly, we found two distinct groups in the context of mutational burden: 6 hypermutated cases with 2325 to 10973 mutations and 22 nonhypermutated cases with 47 to 154 mutations. Further analysis revealed that four of the six hypermutated cases had the same POLE P286R mutation. We validated this finding in 83 MSS EOCRCs and 27 MSS LOCRCs, which revealed that 7.2% of EOCRCs (6/83) had the POLE P286R mutation, which was not found in LOCRCs. Clinicopathologically, EOCRCs with POLE mutations occurred far more frequently in the right colon than in the left colon, affecting men more frequently than women. In summary, we have identified a unique subclass of colon cancer characterized by a hypermutation associated with the POLE mutation. The acquisition of the POLE mutation leading to hypermutation can accelerate cancer development. Clinically, this subset with hypermutation may be susceptible to immune checkpoint blockade. Impact Journals LLC 2016-09-06 /pmc/articles/PMC5356579/ /pubmed/27612425 http://dx.doi.org/10.18632/oncotarget.11862 Text en Copyright: © 2016 Ahn et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. |
| spellingShingle | Research Paper Ahn, Sung-Min Ansari, Adnan Ahmad Kim, Jihun Kim, Deokhoon Chun, Sung-Min Kim, Jiyun Kim, Tae Won Park, Inja Yu, Chang-Sik Jang, Se Jin The somatic POLE P286R mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy |
| title | The somatic POLE P286R mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy |
| title_full | The somatic POLE P286R mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy |
| title_fullStr | The somatic POLE P286R mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy |
| title_full_unstemmed | The somatic POLE P286R mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy |
| title_short | The somatic POLE P286R mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy |
| title_sort | somatic pole p286r mutation defines a unique subclass of colorectal cancer featuring hypermutation, representing a potential genomic biomarker for immunotherapy |
| topic | Research Paper |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5356579/ https://www.ncbi.nlm.nih.gov/pubmed/27612425 http://dx.doi.org/10.18632/oncotarget.11862 |
| work_keys_str_mv | AT ahnsungmin thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT ansariadnanahmad thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT kimjihun thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT kimdeokhoon thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT chunsungmin thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT kimjiyun thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT kimtaewon thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT parkinja thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT yuchangsik thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT jangsejin thesomaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT ahnsungmin somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT ansariadnanahmad somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT kimjihun somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT kimdeokhoon somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT chunsungmin somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT kimjiyun somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT kimtaewon somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT parkinja somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT yuchangsik somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy AT jangsejin somaticpolep286rmutationdefinesauniquesubclassofcolorectalcancerfeaturinghypermutationrepresentingapotentialgenomicbiomarkerforimmunotherapy |