-
Something wrong with this record ?
RET, NTRK, ALK, BRAF, and MET Fusions in a Large Cohort of Pediatric Papillary Thyroid Carcinomas
B. Pekova, V. Sykorova, S. Dvorakova, E. Vaclavikova, J. Moravcova, R. Katra, J. Astl, P. Vlcek, D. Kodetova, J. Vcelak, B. Bendlova
Language English Country United States
Document type Journal Article, Research Support, Non-U.S. Gov't
PubMed
32495721
DOI
10.1089/thy.2019.0802
Knihovny.cz E-resources
- MeSH
- Point Mutation MeSH
- Child MeSH
- Phenotype MeSH
- Gene Fusion * MeSH
- Genetic Predisposition to Disease MeSH
- Gene Rearrangement MeSH
- Humans MeSH
- Adolescent MeSH
- Young Adult MeSH
- Biomarkers, Tumor genetics MeSH
- Thyroid Neoplasms genetics pathology therapy MeSH
- Thyroid Cancer, Papillary genetics pathology therapy MeSH
- Prognosis MeSH
- Proto-Oncogene Proteins B-raf genetics MeSH
- Proto-Oncogene Proteins c-met genetics MeSH
- Proto-Oncogene Proteins c-ret genetics MeSH
- Receptor, trkA genetics MeSH
- Receptor, trkC genetics MeSH
- Age Factors MeSH
- Check Tag
- Child MeSH
- Humans MeSH
- Adolescent MeSH
- Young Adult MeSH
- Male MeSH
- Female MeSH
- Publication type
- Journal Article MeSH
- Research Support, Non-U.S. Gov't MeSH
Background: Pediatric papillary thyroid carcinoma (PTC) is a rare malignancy, but with increasing incidence. Pediatric PTCs have distinct clinical and pathological features and even the molecular profile differs from adult PTCs. Somatic point mutations in pediatric PTCs have been previously described and studied, but complex information about fusion genes is lacking. The aim of this study was to identify different fusion genes in a large cohort of pediatric PTCs and to correlate them with clinical and pathological data of patients. Methods: The cohort consisted of 93 pediatric PTC patients (6-20 years old). DNA and RNA were extracted from fresh frozen tissue samples, followed by DNA and RNA-targeted next-generation sequencing analyses. Fusion gene-positive samples were verified by real-time polymerase chain reaction. Results: A genetic alteration was found in 72/93 (77.4%) pediatric PTC cases. In 52/93 (55.9%) pediatric PTC patients, a fusion gene was detected. Twenty different types of RET, NTRK3, ALK, NTRK1, BRAF, and MET fusions were found, of which five novel, TPR/RET, IKBKG/RET, BBIP1/RET, OPTN/BRAF, and EML4/MET, rearrangements were identified and a CUL1/BRAF rearrangement that has not been previously described in thyroid cancer. Fusion gene-positive PTCs were significantly associated with the mixture of classical and follicular variants of PTC, extrathyroidal extension, higher T classification, lymph node and distant metastases, chronic lymphocytic thyroiditis, and frequent occurrence of psammoma bodies compared with fusion gene-negative PTCs. Fusion-positive patients also received more doses of radioiodine therapy. The most common fusion genes were the RET fusions, followed by NTRK3 fusions. RET fusions were associated with more frequent lymph node and distant metastases and psammoma bodies, and NTRK3 fusions were associated with the follicular variant of PTC. Conclusions: Fusion genes were the most common genetic alterations in pediatric PTCs. Fusion gene-positive PTCs were associated with more aggressive disease than fusion gene-negative PTCs.
References provided by Crossref.org
- 000
- 00000naa a2200000 a 4500
- 001
- bmc22004804
- 003
- CZ-PrNML
- 005
- 20241111144705.0
- 007
- ta
- 008
- 220113s2020 xxu f 000 0|eng||
- 009
- AR
- 024 7_
- $a 10.1089/thy.2019.0802 $2 doi
- 035 __
- $a (PubMed)32495721
- 040 __
- $a ABA008 $b cze $d ABA008 $e AACR2
- 041 0_
- $a eng
- 044 __
- $a xxu
- 100 1_
- $a Peková Bulanová, Barbora, $u Department of Molecular Endocrinology, Institute of Endocrinology, Prague, Czech Republic $d 1993- $7 xx0256338
- 245 10
- $a RET, NTRK, ALK, BRAF, and MET Fusions in a Large Cohort of Pediatric Papillary Thyroid Carcinomas / $c B. Pekova, V. Sykorova, S. Dvorakova, E. Vaclavikova, J. Moravcova, R. Katra, J. Astl, P. Vlcek, D. Kodetova, J. Vcelak, B. Bendlova
- 520 9_
- $a Background: Pediatric papillary thyroid carcinoma (PTC) is a rare malignancy, but with increasing incidence. Pediatric PTCs have distinct clinical and pathological features and even the molecular profile differs from adult PTCs. Somatic point mutations in pediatric PTCs have been previously described and studied, but complex information about fusion genes is lacking. The aim of this study was to identify different fusion genes in a large cohort of pediatric PTCs and to correlate them with clinical and pathological data of patients. Methods: The cohort consisted of 93 pediatric PTC patients (6-20 years old). DNA and RNA were extracted from fresh frozen tissue samples, followed by DNA and RNA-targeted next-generation sequencing analyses. Fusion gene-positive samples were verified by real-time polymerase chain reaction. Results: A genetic alteration was found in 72/93 (77.4%) pediatric PTC cases. In 52/93 (55.9%) pediatric PTC patients, a fusion gene was detected. Twenty different types of RET, NTRK3, ALK, NTRK1, BRAF, and MET fusions were found, of which five novel, TPR/RET, IKBKG/RET, BBIP1/RET, OPTN/BRAF, and EML4/MET, rearrangements were identified and a CUL1/BRAF rearrangement that has not been previously described in thyroid cancer. Fusion gene-positive PTCs were significantly associated with the mixture of classical and follicular variants of PTC, extrathyroidal extension, higher T classification, lymph node and distant metastases, chronic lymphocytic thyroiditis, and frequent occurrence of psammoma bodies compared with fusion gene-negative PTCs. Fusion-positive patients also received more doses of radioiodine therapy. The most common fusion genes were the RET fusions, followed by NTRK3 fusions. RET fusions were associated with more frequent lymph node and distant metastases and psammoma bodies, and NTRK3 fusions were associated with the follicular variant of PTC. Conclusions: Fusion genes were the most common genetic alterations in pediatric PTCs. Fusion gene-positive PTCs were associated with more aggressive disease than fusion gene-negative PTCs.
- 650 _2
- $a mladiství $7 D000293
- 650 _2
- $a věkové faktory $7 D000367
- 650 _2
- $a nádorové biomarkery $x genetika $7 D014408
- 650 _2
- $a dítě $7 D002648
- 650 _2
- $a ženské pohlaví $7 D005260
- 650 12
- $a fúze genů $7 D050939
- 650 _2
- $a genová přestavba $7 D015321
- 650 _2
- $a genetická predispozice k nemoci $7 D020022
- 650 _2
- $a lidé $7 D006801
- 650 _2
- $a mužské pohlaví $7 D008297
- 650 _2
- $a fenotyp $7 D010641
- 650 _2
- $a bodová mutace $7 D017354
- 650 _2
- $a prognóza $7 D011379
- 650 _2
- $a protoonkogenní proteiny B-raf $x genetika $7 D048493
- 650 _2
- $a protoonkogenní proteiny c-met $x genetika $7 D019859
- 650 _2
- $a protoonkogenní proteiny c-ret $x genetika $7 D051096
- 650 _2
- $a receptor trkA $x genetika $7 D020917
- 650 _2
- $a receptor trkC $x genetika $7 D020812
- 650 _2
- $a papilární karcinom štítné žlázy $x genetika $x patologie $x terapie $7 D000077273
- 650 _2
- $a nádory štítné žlázy $x genetika $x patologie $x terapie $7 D013964
- 650 _2
- $a mladý dospělý $7 D055815
- 655 _2
- $a časopisecké články $7 D016428
- 655 _2
- $a práce podpořená grantem $7 D013485
- 700 1_
- $a Sykorova, Vlasta $u Department of Molecular Endocrinology, Institute of Endocrinology, Prague, Czech Republic
- 700 1_
- $a Dvorakova, Sarka $u Department of Molecular Endocrinology, Institute of Endocrinology, Prague, Czech Republic
- 700 1_
- $a Vaclavikova, Eliska $u Department of Molecular Endocrinology, Institute of Endocrinology, Prague, Czech Republic
- 700 1_
- $a Moravcova, Jitka $u Department of Molecular Endocrinology, Institute of Endocrinology, Prague, Czech Republic
- 700 1_
- $a Katra, Rami $u Department of Ear, Nose and Throat, 2nd Faculty of Medicine, Charles University in Prague and Motol University Hospital, Prague, Czech Republic
- 700 1_
- $a Astl, Jaromir $u Department of Otorhinolaryngology and Maxillofacial Surgery, 3rd Faculty of Medicine, Military University Hospital, Prague, Czech Republic
- 700 1_
- $a Vlcek, Petr $u Department of Nuclear Medicine and Endocrinology, and 2nd Faculty of Medicine, Charles University in Prague and Motol University Hospital, Prague, Czech Republic
- 700 1_
- $a Nováková Kodetová, Daniela, $u Department of Pathology and Molecular Medicine, 2nd Faculty of Medicine, Charles University in Prague and Motol University Hospital, Prague, Czech Republic $d 1953- $7 jo2002104665
- 700 1_
- $a Vcelak, Josef $u Department of Molecular Endocrinology, Institute of Endocrinology, Prague, Czech Republic
- 700 1_
- $a Bendlova, Bela $u Department of Molecular Endocrinology, Institute of Endocrinology, Prague, Czech Republic
- 773 0_
- $w MED00004519 $t Thyroid $x 1557-9077 $g Roč. 30, č. 12 (2020), s. 1771-1780
- 856 41
- $u https://pubmed.ncbi.nlm.nih.gov/32495721 $y Pubmed
- 910 __
- $a ABA008 $b sig $c sign $y p $z 0
- 990 __
- $a 20220113 $b ABA008
- 991 __
- $a 20241111144703 $b ABA008
- 999 __
- $a ok $b bmc $g 1752102 $s 1155953
- BAS __
- $a 3
- BAS __
- $a PreBMC
- BMC __
- $a 2020 $b 30 $c 12 $d 1771-1780 $e 20200701 $i 1557-9077 $m Thyroid $n Thyroid $x MED00004519
- LZP __
- $a Pubmed-20220113
