FOXG1 sequentially orchestrates subtype specification of postmitotic cortical projection neurons

Yang, Mengjie; Su, Mingzhao; Liu, Bin; Zhou, Kaixing; Sun, Congli; Ba, Ru; Yu, Baocong; Zhang, Baoshen; Zhang, Zhe; Fan, Wenxin; Wang, Kun; Zhong, Min; Han, Junhai; Zhao, Chunjie

doi:10.1126/sciadv.abh3568

Cited by 14 publications

(29 citation statements)

References 73 publications

(145 reference statements)

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“…Here, we showed a loss of RSC-PyNs (UL) and marked down-regulation of SATB2 in Foxg1 cKO mice. When viewed alongside our earlier findings that FOXG1 specifies neocortical callosal projection neurons through direct activation of Satb2 ( 10 ), our data support the notion that FOXG1 may also specify RSC-PyNs (UL) by acting as a transcriptional activator of Satb2 .…”

Section: Discussionsupporting

confidence: 84%

“…To explore whether FOXG1 directly represses Tbr1 during the specification of CA1-PyNs, we first performed ChIP-qPCR and detected a strong FOXG1 occupancy at a putative binding site 700 bp upstream of the Tbr1 transcription start site, as previously reported ( 10 ) ( Fig. 6B ).…”

Section: Resultsmentioning

confidence: 63%

“…Pou3f1 was reported to regulate transcription in differentiated neocortical neurons ( 41 ). Bcl11b and Fezf2 are known to be the key determinants for cortical subcerebral projection neurons ( 10 ).…”

Section: Resultsmentioning

confidence: 99%

“…RNA isolation, reverse transcription, and qPCR analysis RNA isolation, reverse transcription, and qPCR were performed as previously described (10). Neuro2a cells were harvested 72 hours after Zbtb20-shRNA or Tbr1-shRNA transfection.…”

Section: Luciferase Assaymentioning

confidence: 99%

“…The Forkhead-box TF FOXG1 has been demonstrated to control a variety of developmental processes ranging from dorsal-ventral pattern formation of the telencephalon and cell fate determination to cortical circuit specialization by exerting both repressive and activating functions ( 9 , 10 ). However, no study has examined the contribution of FOXG1 to postmitotic cell type specificity in the MP or the downstream targets of FOXG1 at single-cell resolution.…”

Section: Introductionmentioning

confidence: 99%

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FOXG1 drives transcriptomic networks to specify principal neuron subtypes during the development of the medial pallium

Yang

Zhang

et al. 2023

Sci. Adv.

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The medial pallium (MP) is the major forebrain region underlying learning and memory, spatial navigation, and emotion; however, the mechanisms underlying the specification of its principal neuron subtypes remain largely unexplored. Here, by postmitotic deletion of FOXG1 (a transcription factor linked to autism spectrum disorders and FOXG1 syndrome) and single-cell RNA sequencing of E17.5 MP in mice, we found that FOXG1 controls the specification of upper-layer retrosplenial cortical pyramidal neurons [RSC-PyNs (UL)], subiculum PyNs (SubC-PyNs), CA1-PyNs, CA3-PyNs, and dentate gyrus granule cells (DG-GCs) in the MP. We uncovered subtype-specific and subtype-shared FOXG1-regulated transcriptomic networks orchestrating MP neuron specification. We further demonstrated that FOXG1 transcriptionally represses Zbtb20 , Prox1 , and Epha4 to prevent CA3-PyN and DG-GC identities during the specification of RSC-PyNs (UL) and SubC-PyNs; FOXG1 directly activates Nr4a2 to promote SubC-PyN identity. We showed that TBR1, controlled by FOXG1 during CA1-PyN specification, was down-regulated. Thus, our study illuminates MP principal neuron subtype specification and related neuropathogenesis.

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Section: Discussionsupporting

confidence: 84%

Section: Resultsmentioning

confidence: 63%

Section: Resultsmentioning

confidence: 99%

Section: Luciferase Assaymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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FOXG1 drives transcriptomic networks to specify principal neuron subtypes during the development of the medial pallium

Yang

Zhang

et al. 2023

Sci. Adv.

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Menin Deficiency Induces Autism‐Like Behaviors by Regulating Foxg1 Transcription and Participates in Foxg1‐Related Encephalopathy

Zhuang,

Leng,

et al. 2024

Advanced Science

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FOXG1 syndrome is a developmental encephalopathy caused by FOXG1 (Forkhead box G1) mutations, resulting in high phenotypic variability. However, the upstream transcriptional regulation of Foxg1 expression remains unclear. This report demonstrates that both deficiency and overexpression of Men1 (protein: menin, a pathogenic gene of MEN1 syndrome known as multiple endocrine neoplasia type 1) lead to autism‐like behaviors, such as social defects, increased repetitive behaviors, and cognitive impairments. Multifaceted transcriptome analyses revealed that Foxg1 signaling is predominantly altered in Men1 deficiency mice, through its regulation of the Alpha Thalassemia/Mental Retardation Syndrome X‐Linked (Atrx) factor. Atrx recruits menin to bind to the transcriptional start region of Foxg1 and mediates the regulation of Foxg1 expression by H3K4me3 (Trimethylation of histone H3 lysine 4) modification. The deficits observed in menin deficient mice are rescued by the over‐expression of Foxg1, leading to normalized spine growth and restoration of hippocampal synaptic plasticity. These findings suggest that menin may have a putative role in the maintenance of Foxg1 expression, highlighting menin signaling as a potential therapeutic target for Foxg1‐related encephalopathy.

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Rare predicted deleterious FEZF2 variants are associated with a neurodevelopmental phenotype

Garber,

Weingarten,

Abreu

et al. 2024

American J of Med Genetics Pt A

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FEZF2 encodes a transcription factor critical to neurodevelopment that regulates other neurodevelopment genes. Rare variants in FEZF2 have previously been suggested to play a role in autism, and cases of 3p14 microdeletions that include FEZF2 share a neurodevelopmental phenotype including mild dysmorphic features and intellectual disability. We identified seven heterozygous predicted deleterious variants in FEZF2 (three frameshifts, one recurrent missense in two independent cases, one nonsense, and one complete gene deletion) in unrelated individuals with neurodevelopmental disorders including developmental delay/intellectual disability, autism, and/or attention‐deficit/hyperactivity. Variants were confirmed to be de novo in five of seven cases and paternally inherited from an affected father in one. Predicted deleterious variants in FEZF2 may affect the expression of genes that are involved in fate choice pathways in developing neurons, and thus contribute to the neurodevelopmental phenotype. Future studies are needed to clarify the mechanism by which FEZF2 leads to this neurodevelopmental disorder.

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FOXG1 sequentially orchestrates subtype specification of postmitotic cortical projection neurons

Cited by 14 publications

References 73 publications

FOXG1 drives transcriptomic networks to specify principal neuron subtypes during the development of the medial pallium

FOXG1 drives transcriptomic networks to specify principal neuron subtypes during the development of the medial pallium

Menin Deficiency Induces Autism‐Like Behaviors by Regulating Foxg1 Transcription and Participates in Foxg1‐Related Encephalopathy

Rare predicted deleterious FEZF2 variants are associated with a neurodevelopmental phenotype

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