Transcriptome analysis of MENX-associated rat pituitary adenomas identifies novel molecular mechanisms involved in the pathogenesis of human pituitary gonadotroph adenomas

Misu Lee; Ilaria Marinoni; Martin Irmler; Tsambika Psaras; Jürgen B. Honegger; Rudi Beschorner; Natasa Anastasov; Johannes Beckers; Marily Theodoropoulou; Federico Roncaroli; Natalia S. Pellegata

doi:10.1007/s00401-013-1132-7

Transcriptome analysis of MENX-associated rat pituitary adenomas identifies novel molecular mechanisms involved in the pathogenesis of human pituitary gonadotroph adenomas

Misu Lee, Ilaria Marinoni, Martin Irmler, Tsambika Psaras, Jürgen B. Honegger, Rudi Beschorner, Natasa Anastasov, Johannes Beckers, Marily Theodoropoulou, Federico Roncaroli, Natalia S. Pellegata

Life Sciences

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Abstract

Gonadotroph adenomas comprise 15-40 % of all pituitary tumors, are usually non-functioning and are often large and invasive at presentation. Surgery is the first-choice treatment, but complete resection is not always achieved, leading to high recurrence rates. As gonadotroph adenomas poorly respond to conventional pharmacological therapies, novel treatment strategies are needed. Their identification has been hampered by our incomplete understanding of the molecular pathogenesis of these tumors. Recently, we demonstrated that MENX-affected rats develop gonadotroph adenomas closely resembling their human counterparts. To discover new genes/pathways involved in gonadotroph cells tumorigenesis, we performed transcriptome profiling of rat tumors versus normal pituitary. Adenomas showed overrepresentation of genes involved in cell cycle, development, cell differentiation/proliferation, and lipid metabolism. Bioinformatic analysis identified downstream targets of the transcription factor SF-1 as being up-regulated in rat (and human) adenomas. Meta-analyses demonstrated remarkable similarities between gonadotroph adenomas in rats and humans, and highlighted common dysregulated genes, several of which were not previously implicated in pituitary tumorigenesis. Two such genes, CYP11A1 and NUSAP1, were analyzed in 39 human gonadotroph adenomas by qRT-PCR and found to be up-regulated in 77 and 95 % of cases, respectively. Immunohistochemistry detected high P450scc (encoded by CYP11A1) and NuSAP expression in 18 human gonadotroph tumors. In vitro studies demonstrated for the first time that Cyp11a1 is a target of SF-1 in gonadotroph cells and promotes proliferation/survival of rat pituitary adenoma primary cells and cell lines. Our studies reveal clues about the molecular mechanisms driving rat and human gonadotroph adenomas development, and may help identify previously unexplored biomarkers for clinical use.

Original language	English
Pages (from-to)	137-150
Number of pages	14
Journal	Acta Neuropathologica
Volume	126
Issue number	1
DOIs	https://doi.org/10.1007/s00401-013-1132-7
State	Published - Jul 2013

Keywords

CYP11A1
MENX model
NUSAP1
Pituitary gonadotroph adenoma
Transcriptome analysis

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10.1007/s00401-013-1132-7

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Lee, M., Marinoni, I., Irmler, M., Psaras, T., Honegger, J. B., Beschorner, R., Anastasov, N., Beckers, J., Theodoropoulou, M., Roncaroli, F., & Pellegata, N. S. (2013). Transcriptome analysis of MENX-associated rat pituitary adenomas identifies novel molecular mechanisms involved in the pathogenesis of human pituitary gonadotroph adenomas. Acta Neuropathologica, 126(1), 137-150. https://doi.org/10.1007/s00401-013-1132-7

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title = "Transcriptome analysis of MENX-associated rat pituitary adenomas identifies novel molecular mechanisms involved in the pathogenesis of human pituitary gonadotroph adenomas",

abstract = "Gonadotroph adenomas comprise 15-40 % of all pituitary tumors, are usually non-functioning and are often large and invasive at presentation. Surgery is the first-choice treatment, but complete resection is not always achieved, leading to high recurrence rates. As gonadotroph adenomas poorly respond to conventional pharmacological therapies, novel treatment strategies are needed. Their identification has been hampered by our incomplete understanding of the molecular pathogenesis of these tumors. Recently, we demonstrated that MENX-affected rats develop gonadotroph adenomas closely resembling their human counterparts. To discover new genes/pathways involved in gonadotroph cells tumorigenesis, we performed transcriptome profiling of rat tumors versus normal pituitary. Adenomas showed overrepresentation of genes involved in cell cycle, development, cell differentiation/proliferation, and lipid metabolism. Bioinformatic analysis identified downstream targets of the transcription factor SF-1 as being up-regulated in rat (and human) adenomas. Meta-analyses demonstrated remarkable similarities between gonadotroph adenomas in rats and humans, and highlighted common dysregulated genes, several of which were not previously implicated in pituitary tumorigenesis. Two such genes, CYP11A1 and NUSAP1, were analyzed in 39 human gonadotroph adenomas by qRT-PCR and found to be up-regulated in 77 and 95 % of cases, respectively. Immunohistochemistry detected high P450scc (encoded by CYP11A1) and NuSAP expression in 18 human gonadotroph tumors. In vitro studies demonstrated for the first time that Cyp11a1 is a target of SF-1 in gonadotroph cells and promotes proliferation/survival of rat pituitary adenoma primary cells and cell lines. Our studies reveal clues about the molecular mechanisms driving rat and human gonadotroph adenomas development, and may help identify previously unexplored biomarkers for clinical use.",

keywords = "CYP11A1, MENX model, NUSAP1, Pituitary gonadotroph adenoma, Transcriptome analysis",

author = "Misu Lee and Ilaria Marinoni and Martin Irmler and Tsambika Psaras and Honegger, {J{\"u}rgen B.} and Rudi Beschorner and Natasa Anastasov and Johannes Beckers and Marily Theodoropoulou and Federico Roncaroli and Pellegata, {Natalia S.}",

note = "Funding Information: Acknowledgments We thank E. Samson, D. M{\"o}rzl and E. Pulz for excellent technical assistance, and Dr. P.L. Mellon for providing the LβT2 cell line. This study was supported by grant SFB824 from the Deutsche Forschungsgemeinschaft (DFG) and grant #107973 from the Deutsche Krebshilfe to N.S.P., and also in part by a research grant from Novartis Pharma GmbH, N{\"u}rnberg, Germany.",

year = "2013",

month = jul,

doi = "10.1007/s00401-013-1132-7",

language = "English",

volume = "126",

pages = "137--150",

journal = "Acta Neuropathologica",

issn = "0001-6322",

publisher = "Springer Science and Business Media Deutschland GmbH",

number = "1",

}

Lee, M, Marinoni, I, Irmler, M, Psaras, T, Honegger, JB, Beschorner, R, Anastasov, N, Beckers, J, Theodoropoulou, M, Roncaroli, F & Pellegata, NS 2013, 'Transcriptome analysis of MENX-associated rat pituitary adenomas identifies novel molecular mechanisms involved in the pathogenesis of human pituitary gonadotroph adenomas', Acta Neuropathologica, vol. 126, no. 1, pp. 137-150. https://doi.org/10.1007/s00401-013-1132-7

TY - JOUR

T1 - Transcriptome analysis of MENX-associated rat pituitary adenomas identifies novel molecular mechanisms involved in the pathogenesis of human pituitary gonadotroph adenomas

AU - Lee, Misu

AU - Marinoni, Ilaria

AU - Irmler, Martin

AU - Psaras, Tsambika

AU - Honegger, Jürgen B.

AU - Beschorner, Rudi

AU - Anastasov, Natasa

AU - Beckers, Johannes

AU - Theodoropoulou, Marily

AU - Roncaroli, Federico

AU - Pellegata, Natalia S.

N1 - Funding Information: Acknowledgments We thank E. Samson, D. Mörzl and E. Pulz for excellent technical assistance, and Dr. P.L. Mellon for providing the LβT2 cell line. This study was supported by grant SFB824 from the Deutsche Forschungsgemeinschaft (DFG) and grant #107973 from the Deutsche Krebshilfe to N.S.P., and also in part by a research grant from Novartis Pharma GmbH, Nürnberg, Germany.

PY - 2013/7

Y1 - 2013/7

N2 - Gonadotroph adenomas comprise 15-40 % of all pituitary tumors, are usually non-functioning and are often large and invasive at presentation. Surgery is the first-choice treatment, but complete resection is not always achieved, leading to high recurrence rates. As gonadotroph adenomas poorly respond to conventional pharmacological therapies, novel treatment strategies are needed. Their identification has been hampered by our incomplete understanding of the molecular pathogenesis of these tumors. Recently, we demonstrated that MENX-affected rats develop gonadotroph adenomas closely resembling their human counterparts. To discover new genes/pathways involved in gonadotroph cells tumorigenesis, we performed transcriptome profiling of rat tumors versus normal pituitary. Adenomas showed overrepresentation of genes involved in cell cycle, development, cell differentiation/proliferation, and lipid metabolism. Bioinformatic analysis identified downstream targets of the transcription factor SF-1 as being up-regulated in rat (and human) adenomas. Meta-analyses demonstrated remarkable similarities between gonadotroph adenomas in rats and humans, and highlighted common dysregulated genes, several of which were not previously implicated in pituitary tumorigenesis. Two such genes, CYP11A1 and NUSAP1, were analyzed in 39 human gonadotroph adenomas by qRT-PCR and found to be up-regulated in 77 and 95 % of cases, respectively. Immunohistochemistry detected high P450scc (encoded by CYP11A1) and NuSAP expression in 18 human gonadotroph tumors. In vitro studies demonstrated for the first time that Cyp11a1 is a target of SF-1 in gonadotroph cells and promotes proliferation/survival of rat pituitary adenoma primary cells and cell lines. Our studies reveal clues about the molecular mechanisms driving rat and human gonadotroph adenomas development, and may help identify previously unexplored biomarkers for clinical use.

AB - Gonadotroph adenomas comprise 15-40 % of all pituitary tumors, are usually non-functioning and are often large and invasive at presentation. Surgery is the first-choice treatment, but complete resection is not always achieved, leading to high recurrence rates. As gonadotroph adenomas poorly respond to conventional pharmacological therapies, novel treatment strategies are needed. Their identification has been hampered by our incomplete understanding of the molecular pathogenesis of these tumors. Recently, we demonstrated that MENX-affected rats develop gonadotroph adenomas closely resembling their human counterparts. To discover new genes/pathways involved in gonadotroph cells tumorigenesis, we performed transcriptome profiling of rat tumors versus normal pituitary. Adenomas showed overrepresentation of genes involved in cell cycle, development, cell differentiation/proliferation, and lipid metabolism. Bioinformatic analysis identified downstream targets of the transcription factor SF-1 as being up-regulated in rat (and human) adenomas. Meta-analyses demonstrated remarkable similarities between gonadotroph adenomas in rats and humans, and highlighted common dysregulated genes, several of which were not previously implicated in pituitary tumorigenesis. Two such genes, CYP11A1 and NUSAP1, were analyzed in 39 human gonadotroph adenomas by qRT-PCR and found to be up-regulated in 77 and 95 % of cases, respectively. Immunohistochemistry detected high P450scc (encoded by CYP11A1) and NuSAP expression in 18 human gonadotroph tumors. In vitro studies demonstrated for the first time that Cyp11a1 is a target of SF-1 in gonadotroph cells and promotes proliferation/survival of rat pituitary adenoma primary cells and cell lines. Our studies reveal clues about the molecular mechanisms driving rat and human gonadotroph adenomas development, and may help identify previously unexplored biomarkers for clinical use.

KW - CYP11A1

KW - MENX model

KW - NUSAP1

KW - Pituitary gonadotroph adenoma

KW - Transcriptome analysis

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U2 - 10.1007/s00401-013-1132-7

DO - 10.1007/s00401-013-1132-7

M3 - Article

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AN - SCOPUS:84879601809

SN - 0001-6322

VL - 126

SP - 137

EP - 150

JO - Acta Neuropathologica

JF - Acta Neuropathologica

IS - 1

ER -

Transcriptome analysis of MENX-associated rat pituitary adenomas identifies novel molecular mechanisms involved in the pathogenesis of human pituitary gonadotroph adenomas

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Keywords

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