Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome Instability

Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome Instability

Sex-related differences have been reported in various cancers, in particular men with lactotroph tumors have a worse prognosis than women. While the underlying mechanism of this sexual dimorphism remains unclear, it has been suggested that a lower estrogen receptor alpha expression may drive the sex...

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Main Authors: Anne Wierinckx, Etienne Delgrange, Philippe Bertolino, Patrick François, Philippe Chanson, Emmanuel Jouanneau, Joël Lachuer, Jacqueline Trouillas, Gérald Raverot
Format: Article
Language:English
Published: Frontiers Media S.A. 2018-11-01
Series:Frontiers in Endocrinology
Subjects:
pituitary tumors
gene expression
estrogen signaling
sexual dimorphism
chromosome
aggressiveness
Online Access:https://www.frontiersin.org/article/10.3389/fendo.2018.00706/full
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language English
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author Anne Wierinckx
Anne Wierinckx
Anne Wierinckx
Etienne Delgrange
Philippe Bertolino
Patrick François
Philippe Chanson
Philippe Chanson
Emmanuel Jouanneau
Emmanuel Jouanneau
Joël Lachuer
Joël Lachuer
Joël Lachuer
Jacqueline Trouillas
Jacqueline Trouillas
Gérald Raverot
Gérald Raverot
Gérald Raverot
spellingShingle Anne Wierinckx
Anne Wierinckx
Anne Wierinckx
Etienne Delgrange
Philippe Bertolino
Patrick François
Philippe Chanson
Philippe Chanson
Emmanuel Jouanneau
Emmanuel Jouanneau
Joël Lachuer
Joël Lachuer
Joël Lachuer
Jacqueline Trouillas
Jacqueline Trouillas
Gérald Raverot
Gérald Raverot
Gérald Raverot
Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome Instability
Frontiers in Endocrinology
pituitary tumors
gene expression
estrogen signaling
sexual dimorphism
chromosome
aggressiveness
author_facet Anne Wierinckx
Anne Wierinckx
Anne Wierinckx
Etienne Delgrange
Philippe Bertolino
Patrick François
Philippe Chanson
Philippe Chanson
Emmanuel Jouanneau
Emmanuel Jouanneau
Joël Lachuer
Joël Lachuer
Joël Lachuer
Jacqueline Trouillas
Jacqueline Trouillas
Gérald Raverot
Gérald Raverot
Gérald Raverot
author_sort Anne Wierinckx
title Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome Instability
title_short Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome Instability
title_full Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome Instability
title_fullStr Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome Instability
title_full_unstemmed Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome Instability
title_sort sex-related differences in lactotroph tumor aggressiveness are associated with a specific gene-expression signature and genome instability
publisher Frontiers Media S.A.
series Frontiers in Endocrinology
issn 1664-2392
publishDate 2018-11-01
description Sex-related differences have been reported in various cancers, in particular men with lactotroph tumors have a worse prognosis than women. While the underlying mechanism of this sexual dimorphism remains unclear, it has been suggested that a lower estrogen receptor alpha expression may drive the sex differences observed in aggressive and malignant lactotroph tumors that are resistant to dopamine agonists. Based on this observation, we aimed to explore the molecular importance of the estrogen pathway through a detailed analysis of the transcriptomic profile of lactotroph tumors from 20 men and 10 women. We undertook gene expression analysis of the selected lactotroph tumors following their pathological grading using the five-tiered classification. Chromosomic alterations were further determined in 13 tumors. Functional analysis showed that there were differences between tumors from men and women in gene signatures associated with cell morphology, cell growth, cell proliferation, development, and cell movement. Hundred-forty genes showed an increased or decreased expression with a minimum 2-fold change. A large subset of those genes belonged to the estrogen receptor signaling pathway, therefore confirming the potent role of this pathway in lactotroph tumor sex-associated aggressiveness. Genes belonging to the X chromosome, such as CTAG2, FGF13, and VEGF-D, were identified as appealing candidates with a sex-linked dysregulation in lactotroph tumors. Through our comparative genomic hybridization analyses (CGH), chromosomic gain, in particular chromosome 19p, was found only in tumors from men, while deletion of chromosome 11 was sex-independent, as it was found in most (5/6) of the aggressive and malignant tumors. Comparison of transcriptomic and CGH analysis revealed four genes (CRB3, FAM138F, MATK, and STAP2) located on gained regions of chromosome 19 and upregulated in lactotroph tumors from men. MATK and STAP2 are both implicated in cell growth and are reported to be associated with the estrogen signaling pathway. Our work confirms the proposed involvement of the estrogen signaling pathway in favoring the increased aggressiveness of lactotroph tumors in men. More importantly, we highlight a number of ER-related candidate genes and further identify a series of target molecules with sex-specific expression that could contribute to the aggressive behavior of lactotroph tumors in men.
topic pituitary tumors
gene expression
estrogen signaling
sexual dimorphism
chromosome
aggressiveness
url https://www.frontiersin.org/article/10.3389/fendo.2018.00706/full
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spelling doaj-718ba2bd85d14e10847af69d01b2d8f32020-11-24T22:01:11ZengFrontiers Media S.A.Frontiers in Endocrinology1664-23922018-11-01910.3389/fendo.2018.00706426561Sex-Related Differences in Lactotroph Tumor Aggressiveness Are Associated With a Specific Gene-Expression Signature and Genome InstabilityAnne Wierinckx0Anne Wierinckx1Anne Wierinckx2Etienne Delgrange3Philippe Bertolino4Patrick François5Philippe Chanson6Philippe Chanson7Emmanuel Jouanneau8Emmanuel Jouanneau9Joël Lachuer10Joël Lachuer11Joël Lachuer12Jacqueline Trouillas13Jacqueline Trouillas14Gérald Raverot15Gérald Raverot16Gérald Raverot17Institut Universitaire de Technologie, Université Lyon 1, Université de Lyon, Lyon, FranceCentre de Recherche en Cancérologie de Lyon (CRCL), INSERM U1052, CNRS UMR5286, Université de Lyon, Lyon, FranceProfileXpert, SFR-Est, CNRS UMR-S3453, INSERM US7, Lyon, FranceService d'Endocrinologie, CHU UCL Namur, Université catholique de Louvain, Ottignies-Louvain-la-Neuve, BelgiumCentre de Recherche en Cancérologie de Lyon (CRCL), INSERM U1052, CNRS UMR5286, Université de Lyon, Lyon, FranceService de Neurochirurgie, CHU de Tours, Tours, FranceService d'Endocrinologie et des Maladies de la Reproduction, Assistance Publique-Hôpitaux de Paris, Centre de Référence des Maladies Rares de l'Hypophyse, Hôpital Bicêtre, Le Kremlin-Bicêtre, FranceFaculté de Médecine Paris-Sud, UMR S-1185, Université Paris-Sud, Université Paris-Saclay, Le Kremlin-Bicêtre, FranceService de Neurochirurgie Groupement Hospitalier Est, Hospices Civils de Lyon, Bron, FranceFaculté de Médecine Lyon-Est, Université Lyon 1, Université de Lyon, Lyon, FranceInstitut Universitaire de Technologie, Université Lyon 1, Université de Lyon, Lyon, FranceCentre de Recherche en Cancérologie de Lyon (CRCL), INSERM U1052, CNRS UMR5286, Université de Lyon, Lyon, FranceProfileXpert, SFR-Est, CNRS UMR-S3453, INSERM US7, Lyon, FranceInstitut Universitaire de Technologie, Université Lyon 1, Université de Lyon, Lyon, FranceFaculté de Médecine Lyon-Est, Université Lyon 1, Université de Lyon, Lyon, FranceCentre de Recherche en Cancérologie de Lyon (CRCL), INSERM U1052, CNRS UMR5286, Université de Lyon, Lyon, FranceFaculté de Médecine Lyon-Est, Université Lyon 1, Université de Lyon, Lyon, France0Département d'Endocrinologie, Centre de Référence pour les Maladies Hypophysaires Rares (HYPO), Groupement Hospitalier EST, Hospices Civils de Lyon, Université de Lyon, Lyon, FranceSex-related differences have been reported in various cancers, in particular men with lactotroph tumors have a worse prognosis than women. While the underlying mechanism of this sexual dimorphism remains unclear, it has been suggested that a lower estrogen receptor alpha expression may drive the sex differences observed in aggressive and malignant lactotroph tumors that are resistant to dopamine agonists. Based on this observation, we aimed to explore the molecular importance of the estrogen pathway through a detailed analysis of the transcriptomic profile of lactotroph tumors from 20 men and 10 women. We undertook gene expression analysis of the selected lactotroph tumors following their pathological grading using the five-tiered classification. Chromosomic alterations were further determined in 13 tumors. Functional analysis showed that there were differences between tumors from men and women in gene signatures associated with cell morphology, cell growth, cell proliferation, development, and cell movement. Hundred-forty genes showed an increased or decreased expression with a minimum 2-fold change. A large subset of those genes belonged to the estrogen receptor signaling pathway, therefore confirming the potent role of this pathway in lactotroph tumor sex-associated aggressiveness. Genes belonging to the X chromosome, such as CTAG2, FGF13, and VEGF-D, were identified as appealing candidates with a sex-linked dysregulation in lactotroph tumors. Through our comparative genomic hybridization analyses (CGH), chromosomic gain, in particular chromosome 19p, was found only in tumors from men, while deletion of chromosome 11 was sex-independent, as it was found in most (5/6) of the aggressive and malignant tumors. Comparison of transcriptomic and CGH analysis revealed four genes (CRB3, FAM138F, MATK, and STAP2) located on gained regions of chromosome 19 and upregulated in lactotroph tumors from men. MATK and STAP2 are both implicated in cell growth and are reported to be associated with the estrogen signaling pathway. Our work confirms the proposed involvement of the estrogen signaling pathway in favoring the increased aggressiveness of lactotroph tumors in men. More importantly, we highlight a number of ER-related candidate genes and further identify a series of target molecules with sex-specific expression that could contribute to the aggressive behavior of lactotroph tumors in men.https://www.frontiersin.org/article/10.3389/fendo.2018.00706/fullpituitary tumorsgene expressionestrogen signalingsexual dimorphismchromosomeaggressiveness

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