Prospero-related homeobox 1 gene (Prox1) is regulated by canonical Wnt signaling and has a stage-specific role in adult hippocampal neurogenesis

Karalay, Özlem; Doberauer, Kathrin; Vadodaria, Krishna C.; Knobloch, Marlen; Berti, Lucia; Miquelajáuregui, Amaya; Schwark, Manuela; Jagasia, Ravi; Taketo, Makoto Mark; Tarabykin, Victor; Lie, Dieter Chichung; Jessberger, Sebastian

doi:10.1073/pnas.1013456108

Cited by 175 publications

(178 citation statements)

References 42 publications

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“…Our study found that the neuronal identity of DG cells was bi-potent during the late stages of these extended periods. By contrast, mature granule cells in the adult DG do not alter their identity upon Prox1 depletion, as previously suggested (Karalay et al, 2011). However, our results demonstrate that the loss of Prox1 in mature DG cells results in a mixed pattern of both DG granule cell and CA3 pyramidal cell gene expression.…”

Section: Neuronal Phenotype Plasticity In Postmitotic Dg Cellscontrasting

confidence: 52%

“…Wnt signaling from the cortical hem, a known morphogen of hippocampal development (Lee et al, 2000;Mangale et al, 2008), is likely to play a crucial role in this process. Wnt signaling postmitotically regulates the expression of Prox1 and NeuroD during adult neurogenesis (Kuwabara et al, 2009;Karalay et al, 2011). Likewise, we observed that Prox1 expression depends on Wnt signaling in immature cells migrating towards the DG primordium (T.I., A.M., H.K., H.E.…”

Section: Specification Of Hippocampal Neuronal Identitymentioning

confidence: 68%

“…Prox1 plays a crucial role in cell fate determination and in cell cycle regulation during the development of the lymphatic vascular system, lens and retina Dyer et al, 2003;Harvey et al, 2005). Recently, knockout (and knockdown) studies of the Prox1 gene have been reported, in which Prox1 was conditionally depleted by using Nestin-Cre; this resulted in the loss of Prox1 from progenitor cells and also throughout their postmitotic progeny, and revealed that Prox1 is essential for the survival of intermediate progenitors and for their descendent neurons in the DG (Lavado et al, 2010;Karalay et al, 2011). However, the roles that Prox1 plays in postmitotic neuronal cells of the DG during development and adulthood remain to be investigated.…”

Section: Introductionmentioning

confidence: 99%

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Prox1 postmitotically defines dentate gyrus cells by specifying granule cell identity over CA3 pyramidal cell fate in the hippocampus

Iwano¹,

Masuda²,

et al. 2012

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The brain is composed of diverse types of neurons that fulfill distinct roles in neuronal circuits, as manifested by the hippocampus, where pyramidal neurons and granule cells constitute functionally distinct domains: cornu ammonis (CA) and dentate gyrus (DG), respectively. Little is known about how these two types of neuron differentiate during hippocampal development, although a set of transcription factors that is expressed in progenitor cells is known to be required for the survival of granule cells. Here, we demonstrate in mice that Prox1, a transcription factor constitutively expressed in the granule cell lineage, postmitotically functions to specify DG granule cell identity. Postmitotic elimination of Prox1 caused immature DG neurons to lose the granule cell identity and in turn terminally differentiate into the pyramidal cell type manifesting CA3 neuronal identity. By contrast, Prox1 overexpression caused opposing effects on presumptive hippocampal pyramidal cells. These results indicate that the immature DG cell has the potential to become a granule cell or a pyramidal cell, and Prox1 defines the granule cell identity. This bi-potency is lost in mature DG cells, although Prox1 is still required for correct gene expression in DG granule cells. Thus, our data indicate that Prox1 acts as a postmitotic cell fate determinant for DG granule cells over the CA3 pyramidal cell fate and is crucial for maintenance of the granule cell identity throughout the life.

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Section: Neuronal Phenotype Plasticity In Postmitotic Dg Cellscontrasting

confidence: 52%

Section: Specification Of Hippocampal Neuronal Identitymentioning

confidence: 68%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Prox1 postmitotically defines dentate gyrus cells by specifying granule cell identity over CA3 pyramidal cell fate in the hippocampus

Iwano¹,

Masuda²,

et al. 2012

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“…Similarly, Prox1 induces the exit of retinal progenitor cells from the cell cycle and promotes horizontal cell differentiation (Dyer et al 2003). Prox1 overexpression resulted in enhanced neuronal differentiation, whereas knockdown of Prox1 impaired the generation of neurons (Karalay et al 2011). Notably, Prospero has been shown to regulate cell cycle progression because loss of Prospero induced aberrant expression of cell cycle genes such as cyclin A (cycA), cyclin E (cycE), and string (srg) and resulted in increased mitotic activity (Li and Vaessin 2000).…”

Section: Prox1: the Master Regulator For Lymphatic Developmentmentioning

confidence: 99%

“…Moreover, regulators of Prox1 have been reported in other types of cells. In colon cancer cells ) and hippocampus cells (Karalay et al 2011), Prox1 is regulated by the Wnt signal through two binding sites of b-catenin/TCF found in the Prox1 enhancer region at 249 kb and 243 kb upstream of the Prox1 start codon, which induce colon cancer progression and neuronal cell differentiation, respectively. Mash1 (Torii et al 1999) and Foxe3 (Medina-Martinez et al 2005) were found to regulate Prox1 expression in the nervous system and lens, respectively.…”

Section: Prox1: the Master Regulator For Lymphatic Developmentmentioning

confidence: 99%

The New Era of the Lymphatic System: No Longer Secondary to the Blood Vascular System

Choi

Lee²,

Hong

2012

Cold Spring Harbor Perspectives in Medicine

116

104

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The blood and lymphatic systems are the two major circulatory systems in our body. Although the blood system has been studied extensively, the lymphatic system has received much less scientific and medical attention because of its elusive morphology and mysterious pathophysiology. However, a series of landmark discoveries made in the past decade has begun to change the previous misconception of the lymphatic system to be secondary to the more essential blood vascular system. In this article, we review the current understanding of the development and pathology of the lymphatic system. We hope to convince readers that the lymphatic system is no less essential than the blood circulatory system for human health and well-being.

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Wnt/β‐catenin signaling in brain development and mental disorders: keeping TCF7L2 in mind

et al. 2019

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Canonical Wnt signaling, which is transduced by β‐catenin and lymphoid enhancer factor 1/T cell‐specific transcription factors (LEF1/TCFs), regulates many aspects of metazoan development and tissue renewal. Although much evidence has associated canonical Wnt/β‐catenin signaling with mood disorders, the mechanistic links are still unknown. Many components of the canonical Wnt pathway are involved in cellular processes that are unrelated to classical canonical Wnt signaling, thus further blurring the picture. The present review critically evaluates the involvement of classical Wnt/β‐catenin signaling in developmental processes that putatively underlie the pathology of mental illnesses. Particular attention is given to the roles of LEF1/TCFs, which have been discussed surprisingly rarely in this context. Highlighting recent discoveries, we propose that alterations in the activity of LEF1/TCFs, and particularly of transcription factor 7‐like 2 (TCF7L2), result in defects previously associated with neuropsychiatric disorders, including imbalances in neurogenesis and oligodendrogenesis, the functional disruption of thalamocortical circuitry and dysfunction of the habenula.

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Prospero-related homeobox 1 gene (Prox1) is regulated by canonical Wnt signaling and has a stage-specific role in adult hippocampal neurogenesis

Cited by 175 publications

References 42 publications

Prox1 postmitotically defines dentate gyrus cells by specifying granule cell identity over CA3 pyramidal cell fate in the hippocampus

Prox1 postmitotically defines dentate gyrus cells by specifying granule cell identity over CA3 pyramidal cell fate in the hippocampus

The New Era of the Lymphatic System: No Longer Secondary to the Blood Vascular System

Wnt/β‐catenin signaling in brain development and mental disorders: keeping TCF7L2 in mind

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