Genome-wide methylation profiling differentiates benign from aggressive and metastatic pituitary neuroendocrine tumors

Jelena Jotanovic; Henning Bünsow Boldt; Mark Burton; Marianne Skovsager Andersen; Daniel Bengtsson; Thomas Olsson Bontell; Bertil Ekman; Britt Edén Engström; Ulla Feldt-Rasmussen; Ansgar Heck; Antonia Jakovcevic; Jens Otto L. Jørgensen; Ivana Kraljevic; Jacek Kunicki; John R. Lindsay; Marco Losa; Paul Benjamin Loughrey; Dominique Maiter; Maria Maksymowicz; Emilija Manojlovic-Gacic; Jens Pahnke; Stephan Petersenn; Maria Petersson; Vera Popovic; Oskar Ragnarsson; Åse Krogh Rasmussen; Zita Reisz; Wolfgang Saeger; Camilla Schalin-Jäntti; David Scheie; Maria Rosa Terreni; Olli Tynninen; Ben Whitelaw; Pia Burman; Olivera Casar-Borota

doi:10.1007/s00401-024-02836-5

Genome-wide methylation profiling differentiates benign from aggressive and metastatic pituitary neuroendocrine tumors

Jelena Jotanovic, Henning Bünsow Boldt, Mark Burton, Marianne Skovsager Andersen, Daniel Bengtsson, Thomas Olsson Bontell, Bertil Ekman, Britt Edén Engström, Ulla Feldt-Rasmussen, Ansgar Heck, Antonia Jakovcevic, Jens Otto L. Jørgensen, Ivana Kraljevic, Jacek Kunicki, John R. Lindsay, Marco Losa, Paul Benjamin Loughrey, Dominique Maiter, Maria Maksymowicz, Emilija Manojlovic-GacicJens Pahnke, Stephan Petersenn, Maria Petersson, Vera Popovic, Oskar Ragnarsson, Åse Krogh Rasmussen, Zita Reisz, Wolfgang Saeger, Camilla Schalin-Jäntti, David Scheie, Maria Rosa Terreni, Olli Tynninen, Ben Whitelaw, Pia Burman, Olivera Casar-Borota^*

^*Corresponding author af dette arbejde

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

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Abstract

Aggressive pituitary neuroendocrine tumors (PitNETs)/adenomas are characterized by progressive growth despite surgery and all standard medical therapies and radiotherapy. A subset will metastasize to the brain and/or distant locations and are termed metastatic PitNETs (pituitary carcinomas). Studies of potential prognostic markers have been limited due to the rarity of these tumors. A few recurrent somatic mutations have been identified, and epigenetic alterations and chromosomal rearrangements have not been explored in larger cohorts of aggressive and metastatic PitNETs. In this study, we performed genome-wide methylation analysis, including copy-number variation (CNV) calculations, on tumor tissue specimens from a large international cohort of 64 patients with aggressive (48) and metastatic (16) pituitary tumors. Twelve patients with non-invasive pituitary tumors (Knosp 0–2) exhibiting an indolent course over a 5 year follow-up served as controls. In an unsupervised hierarchical cluster analysis, aggressive/metastatic PitNETs clustered separately from benign pituitary tumors, and, when only specimens from the first surgery were analyzed, three separate clusters were identified: aggressive, metastatic, and benign PitNETs. Numerous CNV events affecting chromosomal arms and whole chromosomes were frequent in aggressive and metastatic, whereas benign tumors had normal chromosomal copy numbers with only few alterations. Genome-wide methylation analysis revealed different CNV profiles and a clear separation between aggressive/metastatic and benign pituitary tumors, potentially providing biomarkers for identification of these tumors with a worse prognosis at the time of first surgery. The data may refine follow-up routines and contribute to the timely introduction of adjuvant therapy in patients harboring, or at risk of developing, aggressive or metastatic pituitary tumors.

Originalsprog	Engelsk
Artikelnummer	68
Tidsskrift	Acta Neuropathologica
Vol/bind	148
Udgave nummer	1
Antal sider	17
ISSN	0001-6322
DOI	https://doi.org/10.1007/s00401-024-02836-5
Status	Udgivet - 2024

Bibliografisk note

Funding Information:
The authors thank Svetlana Popova from the research unit (FoU) at Uppsala University Hospital for her assistance in preparing the specimens for DNA extraction. The authors also appreciate the help of Elisabet Englund and Inga Gudinaviciene from the Department of Pathology at Lund University Hospital, as well as Stine Horsk\u00E6r Madsen from the University Hospital in Aarhus, Denmark, for their help in collecting the specimens. Special thanks to the PCR and FISH laboratories in Odense for their excellent technical assistance. The authors are grateful to the biobanks at the participating hospitals for collaboration on the collection of the tissue specimens. Henning Boldt presented the preliminary results of this study at the European Society of Endocrinology Congress held in Stockholm, May 2024. This study has received financial support from Pfizer AB (GRG number 70598835), Recordati AB, the Swedish Medical Society (Svenska L\u00E4kars\u00E4llskapet; grant SLS-961569), Lions Cancerforskningsfond, and U-CAN. The collection of tissue material from patients who underwent surgery at the Uppsala University Hospital was supported by U-CAN, through Uppsala Biobank and the Department of Clinical Pathology, Uppsala University Hospital. OC-B has received Gullstrandstj\u00E4nst 2023-2027 and a grant from the Swedish state under the agreement between the Swedish government and the county councils (ALF). JJ has received a grant from the Swedish state under the same agreement between the Swedish government and the county councils (ALF) and from the Region Uppsala research funds. UF-R\u2019s research salary was sponsored by a grant from Kirsten and Freddy Johansen\u2019s Fund. CS-J received funding from the Helsinki University Hospital Research Funds (TYH2018223) and Finska L\u00E4kares\u00E4llskapet. The funding bodies had no role in the design of the study; collection, analysis, or interpretation of the data; or in the writing of the manuscript.

Publisher Copyright:
© The Author(s) 2024.

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Citationsformater

Jotanovic, J., Boldt, H. B., Burton, M., Andersen, M. S., Bengtsson, D., Bontell, T. O., Ekman, B., Engström, B. E., Feldt-Rasmussen, U., Heck, A., Jakovcevic, A., Jørgensen, J. O. L., Kraljevic, I., Kunicki, J., Lindsay, J. R., Losa, M., Loughrey, P. B., Maiter, D., Maksymowicz, M., ... Casar-Borota, O. (2024). Genome-wide methylation profiling differentiates benign from aggressive and metastatic pituitary neuroendocrine tumors. Acta Neuropathologica, 148(1), Artikel 68. https://doi.org/10.1007/s00401-024-02836-5

Jotanovic, J, Boldt, HB, Burton, M, Andersen, MS, Bengtsson, D, Bontell, TO, Ekman, B, Engström, BE, Feldt-Rasmussen, U, Heck, A, Jakovcevic, A, Jørgensen, JOL, Kraljevic, I, Kunicki, J, Lindsay, JR, Losa, M, Loughrey, PB, Maiter, D, Maksymowicz, M, Manojlovic-Gacic, E, Pahnke, J, Petersenn, S, Petersson, M, Popovic, V, Ragnarsson, O, Rasmussen, ÅK, Reisz, Z, Saeger, W, Schalin-Jäntti, C, Scheie, D, Terreni, MR, Tynninen, O, Whitelaw, B, Burman, P & Casar-Borota, O 2024, 'Genome-wide methylation profiling differentiates benign from aggressive and metastatic pituitary neuroendocrine tumors', Acta Neuropathologica, bind 148, nr. 1, 68. https://doi.org/10.1007/s00401-024-02836-5

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title = "Genome-wide methylation profiling differentiates benign from aggressive and metastatic pituitary neuroendocrine tumors",

abstract = "Aggressive pituitary neuroendocrine tumors (PitNETs)/adenomas are characterized by progressive growth despite surgery and all standard medical therapies and radiotherapy. A subset will metastasize to the brain and/or distant locations and are termed metastatic PitNETs (pituitary carcinomas). Studies of potential prognostic markers have been limited due to the rarity of these tumors. A few recurrent somatic mutations have been identified, and epigenetic alterations and chromosomal rearrangements have not been explored in larger cohorts of aggressive and metastatic PitNETs. In this study, we performed genome-wide methylation analysis, including copy-number variation (CNV) calculations, on tumor tissue specimens from a large international cohort of 64 patients with aggressive (48) and metastatic (16) pituitary tumors. Twelve patients with non-invasive pituitary tumors (Knosp 0–2) exhibiting an indolent course over a 5 year follow-up served as controls. In an unsupervised hierarchical cluster analysis, aggressive/metastatic PitNETs clustered separately from benign pituitary tumors, and, when only specimens from the first surgery were analyzed, three separate clusters were identified: aggressive, metastatic, and benign PitNETs. Numerous CNV events affecting chromosomal arms and whole chromosomes were frequent in aggressive and metastatic, whereas benign tumors had normal chromosomal copy numbers with only few alterations. Genome-wide methylation analysis revealed different CNV profiles and a clear separation between aggressive/metastatic and benign pituitary tumors, potentially providing biomarkers for identification of these tumors with a worse prognosis at the time of first surgery. The data may refine follow-up routines and contribute to the timely introduction of adjuvant therapy in patients harboring, or at risk of developing, aggressive or metastatic pituitary tumors.",

keywords = "Aggressive pituitary tumor, Methylation analysis, Pituitary adenoma, Pituitary carcinoma, Pituitary neuroendocrine tumor",

author = "Jelena Jotanovic and Boldt, {Henning B{\"u}nsow} and Mark Burton and Andersen, {Marianne Skovsager} and Daniel Bengtsson and Bontell, {Thomas Olsson} and Bertil Ekman and Engstr{\"o}m, {Britt Ed{\'e}n} and Ulla Feldt-Rasmussen and Ansgar Heck and Antonia Jakovcevic and J{\o}rgensen, {Jens Otto L.} and Ivana Kraljevic and Jacek Kunicki and Lindsay, {John R.} and Marco Losa and Loughrey, {Paul Benjamin} and Dominique Maiter and Maria Maksymowicz and Emilija Manojlovic-Gacic and Jens Pahnke and Stephan Petersenn and Maria Petersson and Vera Popovic and Oskar Ragnarsson and Rasmussen, {{\AA}se Krogh} and Zita Reisz and Wolfgang Saeger and Camilla Schalin-J{\"a}ntti and David Scheie and Terreni, {Maria Rosa} and Olli Tynninen and Ben Whitelaw and Pia Burman and Olivera Casar-Borota",

note = "Correction: https://doi.org/10.1007/s00401-024-02836-5 Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2024",

doi = "10.1007/s00401-024-02836-5",

language = "English",

volume = "148",

journal = "Acta Neuropathologica",

issn = "0001-6322",

publisher = "Springer",

number = "1",

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TY - JOUR

T1 - Genome-wide methylation profiling differentiates benign from aggressive and metastatic pituitary neuroendocrine tumors

AU - Jotanovic, Jelena

AU - Boldt, Henning Bünsow

AU - Burton, Mark

AU - Andersen, Marianne Skovsager

AU - Bengtsson, Daniel

AU - Bontell, Thomas Olsson

AU - Ekman, Bertil

AU - Engström, Britt Edén

AU - Feldt-Rasmussen, Ulla

AU - Heck, Ansgar

AU - Jakovcevic, Antonia

AU - Jørgensen, Jens Otto L.

AU - Kraljevic, Ivana

AU - Kunicki, Jacek

AU - Lindsay, John R.

AU - Losa, Marco

AU - Loughrey, Paul Benjamin

AU - Maiter, Dominique

AU - Maksymowicz, Maria

AU - Manojlovic-Gacic, Emilija

AU - Pahnke, Jens

AU - Petersenn, Stephan

AU - Petersson, Maria

AU - Popovic, Vera

AU - Ragnarsson, Oskar

AU - Rasmussen, Åse Krogh

AU - Reisz, Zita

AU - Saeger, Wolfgang

AU - Schalin-Jäntti, Camilla

AU - Scheie, David

AU - Terreni, Maria Rosa

AU - Tynninen, Olli

AU - Whitelaw, Ben

AU - Burman, Pia

AU - Casar-Borota, Olivera

PY - 2024

Y1 - 2024

N2 - Aggressive pituitary neuroendocrine tumors (PitNETs)/adenomas are characterized by progressive growth despite surgery and all standard medical therapies and radiotherapy. A subset will metastasize to the brain and/or distant locations and are termed metastatic PitNETs (pituitary carcinomas). Studies of potential prognostic markers have been limited due to the rarity of these tumors. A few recurrent somatic mutations have been identified, and epigenetic alterations and chromosomal rearrangements have not been explored in larger cohorts of aggressive and metastatic PitNETs. In this study, we performed genome-wide methylation analysis, including copy-number variation (CNV) calculations, on tumor tissue specimens from a large international cohort of 64 patients with aggressive (48) and metastatic (16) pituitary tumors. Twelve patients with non-invasive pituitary tumors (Knosp 0–2) exhibiting an indolent course over a 5 year follow-up served as controls. In an unsupervised hierarchical cluster analysis, aggressive/metastatic PitNETs clustered separately from benign pituitary tumors, and, when only specimens from the first surgery were analyzed, three separate clusters were identified: aggressive, metastatic, and benign PitNETs. Numerous CNV events affecting chromosomal arms and whole chromosomes were frequent in aggressive and metastatic, whereas benign tumors had normal chromosomal copy numbers with only few alterations. Genome-wide methylation analysis revealed different CNV profiles and a clear separation between aggressive/metastatic and benign pituitary tumors, potentially providing biomarkers for identification of these tumors with a worse prognosis at the time of first surgery. The data may refine follow-up routines and contribute to the timely introduction of adjuvant therapy in patients harboring, or at risk of developing, aggressive or metastatic pituitary tumors.

AB - Aggressive pituitary neuroendocrine tumors (PitNETs)/adenomas are characterized by progressive growth despite surgery and all standard medical therapies and radiotherapy. A subset will metastasize to the brain and/or distant locations and are termed metastatic PitNETs (pituitary carcinomas). Studies of potential prognostic markers have been limited due to the rarity of these tumors. A few recurrent somatic mutations have been identified, and epigenetic alterations and chromosomal rearrangements have not been explored in larger cohorts of aggressive and metastatic PitNETs. In this study, we performed genome-wide methylation analysis, including copy-number variation (CNV) calculations, on tumor tissue specimens from a large international cohort of 64 patients with aggressive (48) and metastatic (16) pituitary tumors. Twelve patients with non-invasive pituitary tumors (Knosp 0–2) exhibiting an indolent course over a 5 year follow-up served as controls. In an unsupervised hierarchical cluster analysis, aggressive/metastatic PitNETs clustered separately from benign pituitary tumors, and, when only specimens from the first surgery were analyzed, three separate clusters were identified: aggressive, metastatic, and benign PitNETs. Numerous CNV events affecting chromosomal arms and whole chromosomes were frequent in aggressive and metastatic, whereas benign tumors had normal chromosomal copy numbers with only few alterations. Genome-wide methylation analysis revealed different CNV profiles and a clear separation between aggressive/metastatic and benign pituitary tumors, potentially providing biomarkers for identification of these tumors with a worse prognosis at the time of first surgery. The data may refine follow-up routines and contribute to the timely introduction of adjuvant therapy in patients harboring, or at risk of developing, aggressive or metastatic pituitary tumors.

KW - Aggressive pituitary tumor

KW - Methylation analysis

KW - Pituitary adenoma

KW - Pituitary carcinoma

KW - Pituitary neuroendocrine tumor

U2 - 10.1007/s00401-024-02836-5

DO - 10.1007/s00401-024-02836-5

M3 - Journal article

C2 - 39580368

AN - SCOPUS:85209875877

SN - 0001-6322

VL - 148

JO - Acta Neuropathologica

JF - Acta Neuropathologica

IS - 1

M1 - 68

ER -