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Constitutive activation of canonical Wnt signaling disrupts choroid plexus epithelial fate

Arpan Parichha, Varun Suresh, Mallika Chatterjee, Aditya Kshirsagar, Lihi Ben‐Reuven, Tsviya Olender, Makoto M. Taketo, Velena Radošević, Mihaela Bobić‐Rasonja, Sara Trnski, Michael J. Holtzman, Nataša Jovanov Milošević, Orly Reiner, Shubha Tole

2022Nature Communications69 citationsDOIOpen Access PDF

Abstract

The choroid plexus secretes cerebrospinal fluid and is critical for the development and function of the brain. In the telencephalon, the choroid plexus epithelium arises from the Wnt- expressing cortical hem. Canonical Wnt signaling pathway molecules such as nuclear β-CATENIN are expressed in the mouse and human embryonic choroid plexus epithelium indicating that this pathway is active. Point mutations in human β-CATENIN are known to result in the constitutive activation of canonical Wnt signaling. In a mouse model that recapitulates this perturbation, we report a loss of choroid plexus epithelial identity and an apparent transformation of this tissue to a neuronal identity. Aspects of this phenomenon are recapitulated in human embryonic stem cell derived organoids. The choroid plexus is also disrupted when β-Catenin is conditionally inactivated. Together, our results indicate that canonical Wnt signaling is required in a precise and regulated manner for normal choroid plexus development in the mammalian brain.

Topics & Concepts

Choroid plexusWnt signaling pathwayCell biologyBiologyBeta-cateninEmbryonic stem cellCerebrospinal fluidLRP5CateninEpitheliumLRP6AnatomySignal transductionNeuroscienceCentral nervous systemGeneticsGeneWnt/β-catenin signaling in development and cancerEpigenetics and DNA MethylationPluripotent Stem Cells Research