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Adamantinomatous craniopharyngioma as a model to understand paracrine and senescence-induced tumourigenesis

José Mario González-Meljem, Juan Pedro Martı́nez-Barberá

2021Cellular and Molecular Life Sciences57 citationsDOIOpen Access PDF

Abstract

Cellular senescence is a process that can prevent tumour development in a cell autonomous manner by imposing a stable cell cycle arrest after oncogene activation. Paradoxically, senescence can also promote tumour growth cell non-autonomously by creating a permissive tumour microenvironment that fuels tumour initiation, progression to malignancy and metastasis. In a pituitary tumour known as adamantinomatous craniopharyngioma (ACP), cells that carry oncogenic β-catenin mutations and overactivate the WNT signalling pathway form cell clusters that become senescent and activate a senescence-associated secretory phenotype (SASP). Research in mouse models of ACP has provided insights into the function of the senescent cell clusters and revealed a critical role for SASP-mediated activities in paracrine tumour initiation. In this review, we first discuss this research on ACP and subsequently explore the theme of paracrine tumourigenesis in other tumour models available in the literature. Evidence is accumulating supporting the notion that paracrine signalling brought about by senescent cells may underlie tumourigenesis across different tumours and cancer models.

Topics & Concepts

Paracrine signallingSenescenceBiologyCancer researchCell biologyWnt signaling pathwayCellCell cycleAutocrine signallingPhenotypeCraniopharyngiomaSignal transductionCell cultureGeneticsReceptorEndocrinologyGenePituitary Gland Disorders and TreatmentsRetinoids in leukemia and cellular processesGlioma Diagnosis and Treatment
Adamantinomatous craniopharyngioma as a model to understand paracrine and senescence-induced tumourigenesis | Litcius