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Multi-omic analysis of SDHB-deficient pheochromocytomas and paragangliomas identifies metastasis and treatment-related molecular profiles

Author

Listed:
  • Aidan Flynn

    (University of Melbourne)

  • Andrew D. Pattison

    (University of Melbourne)

  • Shiva Balachander

    (University of Melbourne)

  • Emma Boehm

    (University of Melbourne)

  • Blake Bowen

    (University of Melbourne)

  • Trisha Dwight

    (Royal North Shore Hospital St Leonards NSW)

  • Fernando J. Rossello

    (University of Melbourne
    The Royal Children’s Hospital
    Murdoch Children’s Research Institute
    Monash University)

  • Oliver Hofmann

    (University of Melbourne)

  • Luciano Martelotto

    (University of Melbourne)

  • Maia Zethoven

    (Peter MacCallum Cancer Centre)

  • Lawrence S. Kirschner

    (The Ohio State University)

  • Tobias Else

    (University of Michigan)

  • Lauren Fishbein

    (University of Colorado)

  • Anthony J. Gill

    (University of Sydney
    St Leonards NSW)

  • Arthur S. Tischler

    (Tufts Medical Center)

  • Thomas Giordano

    (University of Michigan)

  • Tamara Prodanov

    (Eunice Kennedy Shriver National Institute of Child Health and Human Development)

  • Jane R. Noble

    (The University of Sydney)

  • Roger R. Reddel

    (The University of Sydney)

  • Alison H. Trainer

    (Peter MacCallum Cancer Centre
    University of Melbourne)

  • Hans Kumar Ghayee

    (University of Florida and Malcom Randall VA Medical Center)

  • Isabelle Bourdeau

    (Center hospitalier de l’Université de Montréal)

  • Marianne Elston

    (University of Auckland)

  • Diana Ishak

    (National Cancer Center Singapore)

  • Joanne Ngeow Yuen Yie

    (National Cancer Center Singapore
    Nanyang Technological University Singapore)

  • Rodney J. Hicks

    (University of Melbourne)

  • Joakim Crona

    (Uppsala University)

  • Tobias Åkerström

    (Uppsala University)

  • Peter Stålberg

    (Uppsala University)

  • Patricia Dahia

    (University of Texas Health Science Center at San Antonio (UTHSCSA))

  • Sean Grimmond

    (University of Melbourne)

  • Roderick Clifton-Bligh

    (Royal North Shore Hospital St Leonards NSW
    University of Sydney)

  • Karel Pacak

    (Eunice Kennedy Shriver National Institute of Child Health and Human Development)

  • Richard W. Tothill

    (University of Melbourne
    University of Melbourne)

Abstract

Hereditary SDHB-mutant pheochromocytomas (PC) and paragangliomas (PG) are rare tumours with a high propensity to metastasize although their clinical behaviour is unpredictable. To characterize the genomic landscape of these tumours and identify metastasis biomarkers, we perform multi-omic analysis on 94 tumours from 79 patients using seven molecular methods. Sympathetic (chromaffin cell) and parasympathetic (non-chromaffin cell) PCPG have distinct molecular profiles reflecting their cell-of-origin and biochemical profile. TERT and ATRX-alterations are associated with metastatic PCPG and these tumours have an increased mutation load, and distinct transcriptional and telomeric features. Most PCPG have quiet genomes with some rare co-operative driver events, including EPAS1/HIF-2α mutations. Two mechanisms of acquired resistance to DNA alkylating chemotherapies are identifiable; MGMT overexpression and mismatch repair-deficiency causing hypermutation. Our comprehensive multi-omic analysis of SDHB-mutant PCPG therefore identifies features of metastatic disease and treatment response, expanding our understanding of these rare neuroendocrine tumours.

Suggested Citation

  • Aidan Flynn & Andrew D. Pattison & Shiva Balachander & Emma Boehm & Blake Bowen & Trisha Dwight & Fernando J. Rossello & Oliver Hofmann & Luciano Martelotto & Maia Zethoven & Lawrence S. Kirschner & T, 2025. "Multi-omic analysis of SDHB-deficient pheochromocytomas and paragangliomas identifies metastasis and treatment-related molecular profiles," Nature Communications, Nature, vol. 16(1), pages 1-20, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-57595-y
    DOI: 10.1038/s41467-025-57595-y
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