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Poor Prognosis Colorectal Cancers Display Self-sustained Growth by Niche-mimicry

Description du projet

La reproduction de niche dans le cancer colorectal

De nouvelles données indiquent que les tumeurs développent un microenvironnement complexe et dynamique, un écosystème avoisinant qui nourrit les cellules cancéreuses, influençant leur croissance et leur métastase. Il est essentiel de déterminer l’interaction entre les cellules cancéreuses et leur microenvironnement pour concevoir des thérapies ciblées. Financé par le Conseil européen de la recherche, le projet NIMICRY cible le cancer colorectal: il entend examiner la nouvelle hypothèse selon laquelle les cellules cancéreuses reproduisent la niche tumorale afin de se développer de manière autonome. Les chercheurs étudieront les mécanismes de signalisation des cellules cancéreuses responsables de cette reproduction, en plus de la dynamique clonale. Les résultats apporteront de nouvelles informations sur un concept unique lié à la biologie et la métastase des tumeurs.

Objectif

Colorectal cancer (CRC) is a heterogeneous disease with widely variable clinical outcomes. I previously contributed to a unifying molecular classification of CRC, the consensus molecular subtypes (CMSs). The mesenchymal subtype (CMS4), representing ~25% of all CRC patients, is characterised by early metastatic dissemination and poor response to therapy. This is often attributed to activated and rich stroma and therefore much attention in the field goes to dissecting the interaction of the mesenchyme with the cancer cells in these tumours. However, in this research program I will investigate a radically different hypothesis: Mesenchymal CRCs display self-sustained growth by niche-mimicry (nimicry). I define nimicry as the adoption of niche features by cancer cells, thereby rendering the cancers independent of micro-environmental signals for their expansion. This hypothesis is directly based on preliminary experiments from my laboratory, which demonstrated that mesenchymal CRCs are not dependent on external growth factors for expansion in vitro and display autocrine and paracrine loops that drive self-sustained growth. The abundant stroma in mesenchymal CRCs is secondary to the growth factors and cytokines produced by the tumour cells.

To study this concept, I will employ primary human CRC models in combination with molecular and functional characterisation, to delineate the self-supporting signalling loops in a patient specific fashion. These studies are paralleled by the investigation of clonal dynamics within established human CRCs by means of a novel genetic lineage tracing strategy in combination with quantitative analysis. Dedicated analyses will resolve the impact of nimicry on metastasis formation, therapy resistance and tumour evolution.

These studies into nimicry as a critical concept in tumour biology, will importantly advance our understanding of the signals that drive CRC growth and progression, and will pave the way to new treatment strategies.

Régime de financement

HORIZON-ERC - HORIZON ERC Grants

Institution d’accueil

STICHTING AMSTERDAM UMC
Contribution nette de l'UE
€ 1 949 357,50
Adresse
DE BOELELAAN 1117
1081 HV Amsterdam
Pays-Bas

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Région
West-Nederland Noord-Holland Groot-Amsterdam
Type d’activité
Research Organisations
Liens
Coût total
€ 1 949 357,50

Bénéficiaires (1)