Tead transcription factors differentially regulate cortical development

Mukhtar, Tanzila; Breda, Jérémie; Grison, Alice; Karimaddini, Zahra; Grobecker, Pascal; Iber, Dagmar; Beisel, Christian; Nimwegen, Erik van; Taylor, Verdon

doi:10.1038/s41598-020-61490-5

Cited by 48 publications

(67 citation statements)

References 49 publications

(63 reference statements)

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“…Similar to sustained Pax6 expression, but in contrast to Insm1 overexpression, the increased level of BPs observed upon conditional expression of a constitutively-active YAP in the BP lineage showed a decreased proportion of Tbr2+ and an increased proportion of Sox2+ BPs. A similar result of increased proliferation in the SVZ was reported in a very recent, independent study in which Yap mRNA (mYAP) instead of constitutively-active YAP was overexpressed in the NPCs of embryonic mouse neocortex [ 110 ]. However, in contrast to Kostic et al [ 109 ], Mukhtar et al [ 110 ] did not report a decrease in Tbr2+ cells in the SVZ when mYAP was overexpressed.…”

Section: Transcriptional Programs That Regulate Neocortical Neurogsupporting

confidence: 77%

“…A similar result of increased proliferation in the SVZ was reported in a very recent, independent study in which Yap mRNA (mYAP) instead of constitutively-active YAP was overexpressed in the NPCs of embryonic mouse neocortex [ 110 ]. However, in contrast to Kostic et al [ 109 ], Mukhtar et al [ 110 ] did not report a decrease in Tbr2+ cells in the SVZ when mYAP was overexpressed.…”

Section: Transcriptional Programs That Regulate Neocortical Neurogsupporting

confidence: 77%

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Transcriptional Regulators and Human-Specific/Primate-Specific Genes in Neocortical Neurogenesis

Vaid

Huttner

2020

IJMS

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During development, starting from a pool of pluripotent stem cells, tissue-specific genetic programs help to shape and develop functional organs. To understand the development of an organ and its disorders, it is important to understand the spatio-temporal dynamics of the gene expression profiles that occur during its development. Modifications in existing genes, the de-novo appearance of new genes, or, occasionally, even the loss of genes, can greatly affect the gene expression profile of any given tissue and contribute to the evolution of organs or of parts of organs. The neocortex is evolutionarily the most recent part of the brain, it is unique to mammals, and is the seat of our higher cognitive abilities. Progenitors that give rise to this tissue undergo sequential waves of differentiation to produce the complete sets of neurons and glial cells that make up a functional neocortex. We will review herein our understanding of the transcriptional regulators that control the neural precursor cells (NPCs) during the generation of the most abundant class of neocortical neurons, the glutametergic neurons. In addition, we will discuss the roles of recently-identified human- and primate-specific genes in promoting neurogenesis, leading to neocortical expansion.

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Section: Transcriptional Programs That Regulate Neocortical Neurogsupporting

confidence: 77%

Section: Transcriptional Programs That Regulate Neocortical Neurogsupporting

confidence: 77%

Transcriptional Regulators and Human-Specific/Primate-Specific Genes in Neocortical Neurogenesis

Vaid

Huttner

2020

IJMS

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“…We receptor binding TF activity that has been implicated in mood disorders (Zhou et al 2009;Shi et al 20011;Shyn et al 2011) (Mukhtar et al 2020). Furthermore, KLF11 (Duncan et al 2012;Duncan et al 2015;Harris et al 2015;Kollert et al 2020), SP1 (Brewer et al 2004;Tamayo et al 2009;Pinacho et al 2011;Fuste et al 2013;Saucedo-Uribe et al 2019;Hung et al 2020), andSP4 (Zou et al 2009;Fuste et al 2013;Young et al 2015) have been found to be involved in the genetic regulation of cell-fate and apoptosis as well as in mood and related psychiatric disorders.…”

Section: Degs and Jaspar Tf Motif Identification Of Group-related Difmentioning

confidence: 99%

Transcription factor motifs associated with anterior insula gene-expression underlying mood disorder phenotypes

Jabbi

Arasappan

Eickhoff³

et al. 2019

Preprint

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Background: Mood disorders represent a major cause of morbidity and mortality worldwide but their pathophysiology remains obscure. Gene expression profiles, especially with regards to the interactive influence of genes within the expression profiles underlying pathological brain phenotypes associated with mood disorders remains largely undefined. Methods:Because the anterior insula is reduced in volume in patients with mood disorders, RNA was extracted from postmortem mood disorder samples and compared with unaffected control samples for RNA-sequencing identification of differentially expressed genes (DEGs) in a) bipolar disorder (BD; n=37), and b) major depressive disorder (MDD n=30) vs controls (n=33), and c) low vs high Axis-I comorbidity (a measure of psychiatric morbidity burden). Given the regulatory role of transcription factors (TFs) in gene expression via specific-DNA-binding domains (motifs), we used JASPAR TF binding database to identify TF-motifs. Results:We found that DEGs in BD-vs-controls, MDD-vs-controls, and high-vs-low Axis-I comorbidity burden were enriched for TF-motifs known to regulate expression of toll-like receptor signaling genes, cellular homeostatic-control genes, and genes involved in embryonic, cellular, organ and brain developmental processes.Discussion: Robust image-guided transcriptomics was applied by targeting the gray matter volume reduction in the anterior insula in mood disorders, to guide independent postmortem identification of TF motifs regulating DEG. TF motifs were identified for immune, cellular, embryonic and neurodevelopmental processes. Conclusion:Our results provided novel information about the hierarchical relationship between gene regulatory networks, the TFs that control them, and proximate underlying neuroanatomical phenotypes in mood disorders.

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“…Prenatal HFD exposure can impact DNA methylation of several genes related to dietary fat intake (62,63) as well as the levels and activity of several transcription factors that have been associated with brain development (64), such as transcriptional enhancer factor-1 (TEF-1), yes-associated protein-1 (YAP-1), and the family of peroxisome proliferatoractivated receptors (PPARs), that in turn effect the expression of some of the orexigenic neuropeptides (65)(66)(67)(68). The transcription factors TEF-1 and YAP-1 has been linked to prenatal HFD effects and plays a large role in organ formation and brain development during embryogenesis (69)(70)(71)(72), and activation of these transcription factors have been found to control neuronal proliferation and differentiation (73)(74)(75). Both TEF-1 and YAP-1 were inactivated or decreased during in utero HFD exposure and may promote increased neurogenesis events (65).…”

Section: Dietary Fat On Stimulating Neurochemical Systems In the Hypomentioning

confidence: 99%

Behavioral Feeding Circuit: Dietary Fat-Induced Effects of Inflammatory Mediators in the Hypothalamus

Poon

2020

Front. Endocrinol.

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Excessive dietary fat intake has extensive impacts on several physiological systems and can lead to metabolic and nonmetabolic disease. In animal models of ingestion, exposure to a high fat diet during pregnancy predisposes offspring to increase intake of dietary fat and causes increase in weight gain that can lead to obesity, and without intervention, these physiological and behavioral consequences can persist for several generations. The hypothalamus is a region of the brain that responds to physiological hunger and fullness and contains orexigenic neuropeptide systems that have long been associated with dietary fat intake. The past fifteen years of research show that prenatal exposure to a high fat diet increases neurogenesis of these neuropeptide systems in offspring brain and are correlated to behavioral changes that induce a pro-consummatory and obesogenic phenotype. Current research has uncovered several potential molecular mechanisms by which excessive dietary fat alters the hypothalamus and involve dietary fatty acids, the immune system, gut microbiota, and transcriptional and epigenetic changes. This review will examine the current knowledge of dietary fat-associated changes in the hypothalamus and the potential pathways involved in modifying the development of orexigenic peptide neurons that lead to changes in ingestive behavior, with a special emphasis on inflammation by chemokines.

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Tead transcription factors differentially regulate cortical development

Cited by 48 publications

References 49 publications

Transcriptional Regulators and Human-Specific/Primate-Specific Genes in Neocortical Neurogenesis

Transcriptional Regulators and Human-Specific/Primate-Specific Genes in Neocortical Neurogenesis

Transcription factor motifs associated with anterior insula gene-expression underlying mood disorder phenotypes

Behavioral Feeding Circuit: Dietary Fat-Induced Effects of Inflammatory Mediators in the Hypothalamus

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