Tumour compartment transcriptomics demonstrates the activation of inflammatory and odontogenic programmes in human adamantinomatous craniopharyngioma and identifies the MAPK/ERK pathway as a novel therapeutic target

John Apps; Gabriela Carreno; José Mario González-Meljem; Scott Haston; Romain Guiho; Julie Cooper; Saba Manshaei; Nital Jani; Annett Hölsken; Benedetta Pettorini; Robert J. Beynon; Deborah M. Simpson; Helen C. Fraser; Ying Hong; Shirleen Hallang; T. J. Stone; Alex Virasami; Andrew M. Donson; David Jones; Kristian Aquilina; Helen Spoudeas; Abhijit Joshi; Richard G. Grundy; Lisa Storer; Márta Korbonits; David A. Hilton; Kyoko Tossell; Selvam Thavaraj; Mark A. Ungless; Jesús Gil; Rolf Buslei; Todd C. Hankinson; Darren Hargrave; Colin R. Goding; Cynthia L. Andoniadou; Paul Brogan; Thomas S. Jacques; Hywel Williams; Juan Pedro Martı́nez-Barberá

doi:10.1007/s00401-018-1830-2

Tumour compartment transcriptomics demonstrates the activation of inflammatory and odontogenic programmes in human adamantinomatous craniopharyngioma and identifies the MAPK/ERK pathway as a novel therapeutic target

John Apps(Great Ormond Street Hospital), Gabriela Carreno(University College London), José Mario González-Meljem(Vietnam National Children's Hospital), Scott Haston(University College London), Romain Guiho(University College London), Julie Cooper(University College London), Saba Manshaei(University College London), Nital Jani(University College London), Annett Hölsken(Friedrich-Alexander-Universität Erlangen-Nürnberg), Benedetta Pettorini(University of Liverpool), Robert J. Beynon(University of Liverpool), Deborah M. Simpson(University of Liverpool), Helen C. Fraser(University College London), Ying Hong(University College London), Shirleen Hallang(King's College London), T. J. Stone(Great Ormond Street Hospital), Alex Virasami(Great Ormond Street Hospital), Andrew M. Donson(University of Colorado Anschutz Medical Campus), David Jones(German Cancer Research Center), Kristian Aquilina(Great Ormond Street Hospital), Helen Spoudeas(Great Ormond Street Hospital), Abhijit Joshi(Royal Victoria Infirmary), Richard G. Grundy(University of Nottingham), Lisa Storer(University of Nottingham), Márta Korbonits(William Harvey Research Institute), David A. Hilton(Plymouth Hospital), Kyoko Tossell(MRC London Institute of Medical Sciences), Selvam Thavaraj(King's College London), Mark A. Ungless(MRC London Institute of Medical Sciences), Jesús Gil(MRC London Institute of Medical Sciences), Rolf Buslei(Friedrich-Alexander-Universität Erlangen-Nürnberg), Todd C. Hankinson(University of Colorado Anschutz Medical Campus), Darren Hargrave(Great Ormond Street Hospital), Colin R. Goding(Ludwig Cancer Research), Cynthia L. Andoniadou(Guy's Hospital), Paul Brogan(Great Ormond Street Hospital), Thomas S. Jacques(Great Ormond Street Hospital), Hywel Williams(University College London), Juan Pedro Martı́nez-Barberá(CRUK Lung Cancer Centre of Excellence)

Acta Neuropathologica

March 14, 2018

10.1007/s00401-018-1830-2

Cited by 210Open Access

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Abstract

Adamantinomatous craniopharyngiomas (ACPs) are clinically challenging tumours, the majority of which have activating mutations in CTNNB1. They are histologically complex, showing cystic and solid components, the latter comprised of different morphological cell types (e.g. β-catenin-accumulating cluster cells and palisading epithelium), surrounded by a florid glial reaction with immune cells. Here, we have carried out RNA sequencing on 18 ACP samples and integrated these data with an existing ACP transcriptomic dataset. No studies so far have examined the patterns of gene expression within the different cellular compartments of the tumour. To achieve this goal, we have combined laser capture microdissection with computational analyses to reveal groups of genes that are associated with either epithelial tumour cells (clusters and palisading epithelium), glial tissue or immune infiltrate. We use these human ACP molecular signatures and RNA-Seq data from two ACP mouse models to reveal that cell clusters are molecularly analogous to the enamel knot, a critical signalling centre controlling normal tooth morphogenesis. Supporting this finding, we show that human cluster cells express high levels of several members of the FGF, TGFB and BMP families of secreted factors, which signal to neighbouring cells as evidenced by immunostaining against the phosphorylated proteins pERK1/2, pSMAD3 and pSMAD1/5/9 in both human and mouse ACP. We reveal that inhibiting the MAPK/ERK pathway with trametinib, a clinically approved MEK inhibitor, results in reduced proliferation and increased apoptosis in explant cultures of human and mouse ACP. Finally, we analyse a prominent molecular signature in the glial reactive tissue to characterise the inflammatory microenvironment and uncover the activation of inflammasomes in human ACP. We validate these results by immunostaining against immune cell markers, cytokine ELISA and proteome analysis in both solid tumour and cystic fluid from ACP patients. Our data support a new molecular paradigm for understanding ACP tumorigenesis as an aberrant mimic of natural tooth development and opens new therapeutic opportunities by revealing the activation of the MAPK/ERK and inflammasome pathways in human ACP.

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