Elsevier

Developmental Biology

Volume 442, Issue 2, 15 October 2018, Pages 236-248
Developmental Biology

Canonical Wnt signaling regulates patterning, differentiation and nucleogenesis in mouse hypothalamus and prethalamus

https://doi.org/10.1016/j.ydbio.2018.07.021Get rights and content
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Highlights

  • Canonical Wnt signaling regulates anteroposterior patterning in the hypothalamus.

  • Canonical Wnt signaling regulates differentiation of GABAergic neurons in both prethalamus and hypothalamus.

  • Canonical Wnt signaling regulates differentiation and nucleogenesis of multiple hypothalamic neuronal subtypes.

  • Canonical Wnt signaling in hypothalamic neuroepithelium regulates pituitary morphogenesis and differentiation.

Abstract

The hypothalamus is a small, but anatomically and functionally complex region of the brain whose development is poorly understood. In this study, we have explored its development by studying the canonical Wnt signaling pathway, generating gain and loss of function mutations of beta-catenin (Ctnnb1) in both hypothalamic and prethalamic neuroepithelium. Deletion of Ctnnb1 resulted in an anteriorized and hypoplastic hypothalamus. Posterior structures were lost or reduced, and anterior structures were expanded. In contrast, overexpression of a constitutively active mutant form of Ctnnb1 resulted in severe hyperplasia of prethalamus and hypothalamus, and expanded expression of a subset of posterior and premamillary hypothalamic markers. Moderate defects in differentiation of Arx-positive GABAergic neural precursors were observed in both prethalamus and hypothalamus of Ctnnb1 loss of function mutants, while in gain of function mutants, their differentiation was completely suppressed, although markers of prethalamic progenitors were preserved. Multiple other region-specific markers, including several specific posterior hypothalamic structures, were also suppressed in Ctnnb1 gain of function mutations. Severe, region-specific defects in hypothalamic nucleogenesis were also observed in both gain and loss of function mutations of Ctnnb1. Finally, both gain and loss of function of Ctnnb1 also produced severe, non-cell autonomous disruptions of pituitary development. These findings demonstrate a central and multifaceted role for canonical Wnt signaling in regulating growth, patterning, differentiation and nucleogenesis in multiple diencephalic regions.

Abbreviations

ArcN
arcuate nucleus
EmThal
thalamic eminence
ID
intrahypothalamic diagonal
MM
mamillary hypothalamus
PMN
premamillary hypothalamus
PrThal
prethalamus
PvN
paraventricular nucleus
SMN
supramammilary hypothalamus
SCN
suprachiasmatic nucleus
VMH
ventromedial hypothalamus

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