Whole-exome identifies RXRG and TH germline variants in familial isolated prolactinoma

Flavia M. Melo; Patrícia P. Couto; Allen E. Bale; Luciana Bastos-Rodrigues; Flavia M. Passos; Raony G.C. Lisboa; Jessica M.Y. Ng; Tom Curran; Eduardo P. Dias; Eitan Friedman; Luiz De Marco

doi:10.1016/j.cancergen.2016.05.065

Whole-exome identifies RXRG and TH germline variants in familial isolated prolactinoma

Flavia M. Melo, Patrícia P. Couto, Allen E. Bale, Luciana Bastos-Rodrigues, Flavia M. Passos, Raony G.C. Lisboa, Jessica M.Y. Ng, Tom Curran, Eduardo P. Dias, Eitan Friedman, Luiz De Marco^*

^*Corresponding author for this work

Clinical Departments

Research output: Contribution to journal › Article › peer-review

6 Scopus citations

Abstract

Familial isolated pituitary adenoma (FIPA) is a rare genetic disorder. In a subset of FIPA families AIP germline mutations have been reported, but in most FIPA cases the exact genetic defect remains unknown. The present study aimed to determine the genetic basis of FIPA in a Brazilian family. Three siblings presented with isolated prolactin genes. Further mutation screening was performed using whole-exome sequencing and all likely causative mutations were validated by Sanger sequencing. In silico analysis and secreting pituitary adenoma diagnosed through clinical, biochemical and imaging testing. Sanger sequencing was used to genotype candidate prolactinoma-mutated additional predictive algorithms were applied to prioritize likely pathogenic variants. No mutations in the coding and flanking intronic regions in the MEN1, AIP and PRLR genes were detected. Whole-exome sequencing of three affected siblings revealed novel, predicted damaging, heterozygous variants in three different genes: RXRG, REXO4 and TH. In conclusion, the RXRG and TH possibly pathogenic variants may be associated with isolated prolactinoma in the studied family. The possible contribution of these genes to additional FIPA families should be explored.

Original language	English
Pages (from-to)	251-257
Number of pages	7
Journal	Cancer genetics
Volume	209
Issue number	6
DOIs	https://doi.org/10.1016/j.cancergen.2016.05.065
State	Published - 1 Jun 2016

Funding

Funders	Funder number
INCT em Medicina Molecular	573646/2008-2, CBB-APQ-00075-09
Conselho Nacional de Desenvolvimento Científico e Tecnológico	405053/2013-4
Fundação de Amparo à Pesquisa do Estado de Minas Gerais	APQ-00220-14

Keywords

FIPA
Familial isolated prolactinoma
PRL
whole exome

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10.1016/j.cancergen.2016.05.065

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title = "Whole-exome identifies RXRG and TH germline variants in familial isolated prolactinoma",

abstract = "Familial isolated pituitary adenoma (FIPA) is a rare genetic disorder. In a subset of FIPA families AIP germline mutations have been reported, but in most FIPA cases the exact genetic defect remains unknown. The present study aimed to determine the genetic basis of FIPA in a Brazilian family. Three siblings presented with isolated prolactin genes. Further mutation screening was performed using whole-exome sequencing and all likely causative mutations were validated by Sanger sequencing. In silico analysis and secreting pituitary adenoma diagnosed through clinical, biochemical and imaging testing. Sanger sequencing was used to genotype candidate prolactinoma-mutated additional predictive algorithms were applied to prioritize likely pathogenic variants. No mutations in the coding and flanking intronic regions in the MEN1, AIP and PRLR genes were detected. Whole-exome sequencing of three affected siblings revealed novel, predicted damaging, heterozygous variants in three different genes: RXRG, REXO4 and TH. In conclusion, the RXRG and TH possibly pathogenic variants may be associated with isolated prolactinoma in the studied family. The possible contribution of these genes to additional FIPA families should be explored.",

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author = "Melo, \{Flavia M.\} and Couto, \{Patr{\'i}cia P.\} and Bale, \{Allen E.\} and Luciana Bastos-Rodrigues and Passos, \{Flavia M.\} and Lisboa, \{Raony G.C.\} and Ng, \{Jessica M.Y.\} and Tom Curran and Dias, \{Eduardo P.\} and Eitan Friedman and \{De Marco\}, Luiz",

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doi = "10.1016/j.cancergen.2016.05.065",

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AU - Couto, Patrícia P.

AU - Bale, Allen E.

AU - Bastos-Rodrigues, Luciana

AU - Passos, Flavia M.

AU - Lisboa, Raony G.C.

AU - Ng, Jessica M.Y.

AU - Curran, Tom

AU - Dias, Eduardo P.

AU - Friedman, Eitan

AU - De Marco, Luiz

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AB - Familial isolated pituitary adenoma (FIPA) is a rare genetic disorder. In a subset of FIPA families AIP germline mutations have been reported, but in most FIPA cases the exact genetic defect remains unknown. The present study aimed to determine the genetic basis of FIPA in a Brazilian family. Three siblings presented with isolated prolactin genes. Further mutation screening was performed using whole-exome sequencing and all likely causative mutations were validated by Sanger sequencing. In silico analysis and secreting pituitary adenoma diagnosed through clinical, biochemical and imaging testing. Sanger sequencing was used to genotype candidate prolactinoma-mutated additional predictive algorithms were applied to prioritize likely pathogenic variants. No mutations in the coding and flanking intronic regions in the MEN1, AIP and PRLR genes were detected. Whole-exome sequencing of three affected siblings revealed novel, predicted damaging, heterozygous variants in three different genes: RXRG, REXO4 and TH. In conclusion, the RXRG and TH possibly pathogenic variants may be associated with isolated prolactinoma in the studied family. The possible contribution of these genes to additional FIPA families should be explored.

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Whole-exome identifies RXRG and TH germline variants in familial isolated prolactinoma

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