Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomas

Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomas

Carotid paragangliomas (CPGLs) are rare neuroendocrine tumors that arise from paraganglionic tissue of the carotid body localizing at the bifurcation of carotid artery. These tumors are slowly growing, but occasionally they become aggressive and metastatic. Surgical treatment remains high-risk and e...

Full description

Bibliographic Details
Main Authors: E. N. Lukyanova, A. V. Snezhkina, D. V. Kalinin, A. V. Pokrovsky, A. L. Golovyuk, O. A. Stepanov, E. A. Pudova, G. S. Razmakhaev, M. V. Orlova, A. P. Polyakov, M. V. Kiseleva, A. D. Kaprin, A. V. Kudryavtseva
Format: Article
Language:English
Published: Institute of Cytology and Genetics of Siberian Branch of the Russian Academy of Sciences 2018-09-01
Series:Vavilovskij Žurnal Genetiki i Selekcii
Subjects:
carotid paragangliomas
exome
mutation load
mutations
high-throughput sequencing
Online Access:https://vavilov.elpub.ru/jour/article/view/1659
id doaj-ef0fbefbfd6b43439f7e3c2701551b67
record_format Article
spelling doaj-ef0fbefbfd6b43439f7e3c2701551b672021-09-11T08:41:20ZengInstitute of Cytology and Genetics of Siberian Branch of the Russian Academy of SciencesVavilovskij Žurnal Genetiki i Selekcii2500-04622500-32592018-09-0122672673310.18699/VJ18.416815Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomasE. N. Lukyanova0A. V. Snezhkina1D. V. Kalinin2A. V. Pokrovsky3A. L. Golovyuk4O. A. Stepanov5E. A. Pudova6G. S. Razmakhaev7M. V. Orlova8A. P. Polyakov9M. V. Kiseleva10A. D. Kaprin11A. V. Kudryavtseva12Engelhardt Institute of Molecular Biology, RAS.Engelhardt Institute of Molecular Biology, RAS.Vishnevsky Institute of Surgery, Ministry of Health of the Russian Federation.Vishnevsky Institute of Surgery, Ministry of Health of the Russian Federation.Vishnevsky Institute of Surgery, Ministry of Health of the Russian Federation.Engelhardt Institute of Molecular Biology, RAS.Vishnevsky Institute of Surgery, Ministry of Health of the Russian Federation.National Medical Research Radiological Center, Ministry of Health of the Russian Federation.Peoples’ Friendship University of Russia (RUDN University).National Medical Research Radiological Center, Ministry of Health of the Russian Federation.National Medical Research Radiological Center, Ministry of Health of the Russian Federation.National Medical Research Radiological Center, Ministry of Health of the Russian Federation.Engelhardt Institute of Molecular Biology, RAS; National Medical Research Radiological Center, Ministry of Health of the Russian Federation.Carotid paragangliomas (CPGLs) are rare neuroendocrine tumors that arise from paraganglionic tissue of the carotid body localizing at the bifurcation of carotid artery. These tumors are slowly growing, but occasionally they become aggressive and metastatic. Surgical treatment remains high-risk and extremely challenging; radiation and chemotherapy are poorly effective. The study of molecular pathogenesis of CPGLs will allow developing novel therapeutic approaches and revealing biomarkers. Previously, we performed the exome sequencing of 52 CPGLs and estimated mutational load (ML). Paired histologically normal tissues or blood were unavailable, so potentially germline mutations were excluded from the analysis with strong filtering conditions using 1000 Genomes Project and ExAC databases. In this work, ten genes (ZNF717, CDC27, FRG2C, FAM104B, CTBP2, HLA-DRB1, HYDIN, KMT5A, MUC3A, and PRSS3) characterized by the highest level of mutational load were analyzed. Using several prediction algorithms (SIFT, PolyPhen-2, MutationTaster, and LRT), potentially pathogenic mutations were identified in four genes (CDC27, CTBP2, HYDIN, and KMT5A). Many of these mutations occurred in the majority of cases, and their mutation type was checked using exome sequencing data of blood prepared with the same exome enrichment kit that was used for preparation of exome libraries from CPGLs. The majority of the mutations were germline that can apparently be associated with annotation errors in 1000 Genomes Pro ject and ExAC. However, part of the mutations identified in CDC27, CTBP2, HYDIN, and KMT5A remain potentially pathogenic, and there is a large body of data on the involvement of these genes in the formation and progression of other tumors. This allows considering CDC27, CTBP2, HYDIN, and KMT5A genes as potentially associated with CPGL pathogenesis and requires taking them into account in further investigations. Thus, there is a necessity to improve the methods for identification of cancer-asso ciated genes as well as pathogenic mutations.https://vavilov.elpub.ru/jour/article/view/1659carotid paragangliomasexomemutation loadmutationshigh-throughput sequencing
collection DOAJ
language English
format Article
sources DOAJ
author E. N. Lukyanova
A. V. Snezhkina
D. V. Kalinin
A. V. Pokrovsky
A. L. Golovyuk
O. A. Stepanov
E. A. Pudova
G. S. Razmakhaev
M. V. Orlova
A. P. Polyakov
M. V. Kiseleva
A. D. Kaprin
A. V. Kudryavtseva
spellingShingle E. N. Lukyanova
A. V. Snezhkina
D. V. Kalinin
A. V. Pokrovsky
A. L. Golovyuk
O. A. Stepanov
E. A. Pudova
G. S. Razmakhaev
M. V. Orlova
A. P. Polyakov
M. V. Kiseleva
A. D. Kaprin
A. V. Kudryavtseva
Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomas
Vavilovskij Žurnal Genetiki i Selekcii
carotid paragangliomas
exome
mutation load
mutations
high-throughput sequencing
author_facet E. N. Lukyanova
A. V. Snezhkina
D. V. Kalinin
A. V. Pokrovsky
A. L. Golovyuk
O. A. Stepanov
E. A. Pudova
G. S. Razmakhaev
M. V. Orlova
A. P. Polyakov
M. V. Kiseleva
A. D. Kaprin
A. V. Kudryavtseva
author_sort E. N. Lukyanova
title Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomas
title_short Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomas
title_full Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomas
title_fullStr Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomas
title_full_unstemmed Analysis of mutations in CDC27, CTBP2, HYDIN and KMT5A genes in carotid paragangliomas
title_sort analysis of mutations in cdc27, ctbp2, hydin and kmt5a genes in carotid paragangliomas
publisher Institute of Cytology and Genetics of Siberian Branch of the Russian Academy of Sciences
series Vavilovskij Žurnal Genetiki i Selekcii
issn 2500-0462
2500-3259
publishDate 2018-09-01
description Carotid paragangliomas (CPGLs) are rare neuroendocrine tumors that arise from paraganglionic tissue of the carotid body localizing at the bifurcation of carotid artery. These tumors are slowly growing, but occasionally they become aggressive and metastatic. Surgical treatment remains high-risk and extremely challenging; radiation and chemotherapy are poorly effective. The study of molecular pathogenesis of CPGLs will allow developing novel therapeutic approaches and revealing biomarkers. Previously, we performed the exome sequencing of 52 CPGLs and estimated mutational load (ML). Paired histologically normal tissues or blood were unavailable, so potentially germline mutations were excluded from the analysis with strong filtering conditions using 1000 Genomes Project and ExAC databases. In this work, ten genes (ZNF717, CDC27, FRG2C, FAM104B, CTBP2, HLA-DRB1, HYDIN, KMT5A, MUC3A, and PRSS3) characterized by the highest level of mutational load were analyzed. Using several prediction algorithms (SIFT, PolyPhen-2, MutationTaster, and LRT), potentially pathogenic mutations were identified in four genes (CDC27, CTBP2, HYDIN, and KMT5A). Many of these mutations occurred in the majority of cases, and their mutation type was checked using exome sequencing data of blood prepared with the same exome enrichment kit that was used for preparation of exome libraries from CPGLs. The majority of the mutations were germline that can apparently be associated with annotation errors in 1000 Genomes Pro ject and ExAC. However, part of the mutations identified in CDC27, CTBP2, HYDIN, and KMT5A remain potentially pathogenic, and there is a large body of data on the involvement of these genes in the formation and progression of other tumors. This allows considering CDC27, CTBP2, HYDIN, and KMT5A genes as potentially associated with CPGL pathogenesis and requires taking them into account in further investigations. Thus, there is a necessity to improve the methods for identification of cancer-asso ciated genes as well as pathogenic mutations.
topic carotid paragangliomas
exome
mutation load
mutations
high-throughput sequencing
url https://vavilov.elpub.ru/jour/article/view/1659
work_keys_str_mv AT enlukyanova analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT avsnezhkina analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT dvkalinin analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT avpokrovsky analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT algolovyuk analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT oastepanov analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT eapudova analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT gsrazmakhaev analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT mvorlova analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT appolyakov analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT mvkiseleva analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT adkaprin analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
AT avkudryavtseva analysisofmutationsincdc27ctbp2hydinandkmt5agenesincarotidparagangliomas
_version_ 1717756558867169280

Similar Items