Brca1 is required for embryonic development of the mouse cerebral cortex to normal size by preventing apoptosis of early neural progenitors

Pulvers, Jeremy N.; Huttner, Wieland B.

doi:10.1242/dev.033498

Cited by 66 publications

(69 citation statements)

References 78 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The BRCA1 gene, for instance, which is associated with an SVA F insertion and is one of the hubs in SVA integrated functional network (Figure 2), was shown to be in a cross talk with the estrogen receptor ESR1 . 23,24 BRCA1 is also known to have a strong role in the control of brain size, 25,26 especially in regions responsible for learning, memory, muscle control and balance. Interestingly, structurally related PGR (progesteronedependent transcription factor) binding sites were shown to be enriched in ancient mammalian TEs linked to evolution of pregnancy, 27 and LTR and Alu elements were also shown to be strongly associated with genes relevant to reproduction.…”

Section: Discussionmentioning

confidence: 99%

Potential impact of primate-specific SVA retrotransposons during the evolution of human cognitive function

et al. 2017

View full text Add to dashboard Cite

The SVA family of hominid-specific non-LTR retrotransposon comprises the youngest group of transposable elements in the human genome. The propagation of the most ancient SVA subfamily took place about 13.5 million years ago, and the youngest SVA subfamily appeared in the human genome after the human/chimpanzee divergence. Functional analysis of genes associated with SVA insertions demonstrated their link to multiple ontological categories, with one of the major categories being attributed to brain function. Further analysis of this subset demonstrated that SVA elements expanded their presence in the human genome at different stages of hominoid evolution and were associated with progressively evolving behavioral features that indicate a potential impact of SVA propagation on the cognitive ability of a modern human. Our analysis suggests a potential role of SVAs in the evolution of human central nervous system and especially in the emergence of functional trends relevant to social and parental behavior. Coevolution of behavioral features and reproductive functions are suggested by our analysis and discussed.

show abstract

Section: Discussionmentioning

confidence: 99%

Potential impact of primate-specific SVA retrotransposons during the evolution of human cognitive function

et al. 2017

View full text Add to dashboard Cite

show abstract

“…In the wild-type mice, BRCA1 is equally expressed in all epidermal compartments, showing that the differential response to Brca1 deletion cannot be explained by the absence of BRCA1 expression from the upper part of the epidermis. The exquisite sensitivity of HF matrix cells upon Brca1 deletion is reminiscent of its role in the early cortical progenitors during brain development (Pulvers and Huttner 2009). Which mechanism could underpin the differential requirement of BRCA1 in different types of SCs?…”

Section: Discussionmentioning

confidence: 99%

BRCA1 deficiency in skin epidermis leads to selective loss of hair follicle stem cells and their progeny

et al. 2012

View full text Add to dashboard Cite

The accurate maintenance of genomic integrity is essential for tissue homeostasis. Deregulation of this process leads to cancer and aging. BRCA1 is a critical mediator of this process. Here, we performed conditional deletion of Brca1 during epidermal development and found that BRCA1 is specifically required for hair follicle (HF) formation and for development of adult HF stem cells (SCs). Mice deficient for Brca1 in the epidermis are hairless and display a reduced number of HFs that degenerate progressively. Surprisingly, the interfollicular epidermis and the sebaceous glands remain unaffected by Brca1 deletion. Interestingly, HF matrix transient amplifying progenitors present increased DNA damage, p53 stabilization, and caspase-dependent apoptosis compared with the interfollicular and sebaceous progenitors, leading to hyperproliferation, apoptosis, and subsequent depletion of the prospective adult HF SCs. Concomitant deletion of p53 and Brca1 rescues the defect of HF morphogenesis and loss of HF SCs. During adult homeostasis, BRCA1 is dispensable for quiescent bulge SCs, but upon their activation during HF regeneration, Brca1 deletion causes apoptosis and depletion of Brca1-deficient bulge SCs. Our data reveal a major difference in the requirement of BRCA1 between different types of epidermal SCs and progenitors and during the different activation stages of adult HF SCs.

show abstract

“…5A). BRCA1 possesses E3 ubiquitin ligase activity (15), accumulates at leading edges in migrating cells (23), and is expressed during brain development (24), particularly in proliferative zones (Fig. 5B).…”

Section: Brca1 Is Expressed In Cholinergic Neurons: Implications For Mglmentioning

confidence: 99%

Nerve growth factor scales endocannabinoid signaling by regulating monoacylglycerol lipase turnover in developing cholinergic neurons

Keimpema

Tortoriello

Alpár

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Endocannabinoid, particularly 2-arachidonoyl glycerol (2-AG), signaling has recently emerged as a molecular determinant of neuronal migration and synapse formation during cortical development. However, the cell type specificity and molecular regulation of spatially and temporally confined morphogenic 2-AG signals remain unexplored. Here, we demonstrate that genetic and pharmacological manipulation of CB 1 cannabinoid receptors permanently alters cholinergic projection neuron identity and hippocampal innervation. We show that nerve growth factor (NGF), implicated in the morphogenesis and survival of cholinergic projection neurons, dose-dependently and coordinately regulates the molecular machinery for 2-AG signaling via tropomyosine kinase A receptors in vitro. In doing so, NGF limits the sorting of monoacylglycerol lipase (MGL), rate limiting 2-AG bioavailability, to proximal neurites, allowing cell-autonomous 2-AG signaling at CB 1 cannabinoid receptors to persist at atypical locations to induce superfluous neurite extension. We find that NGF controls MGL degradation in vitro and in vivo and identify the E3 ubiquitin ligase activity of breast cancer type 1 susceptibility protein (BRCA1) as a candidate facilitating MGL's elimination from motile neurite segments, including growth cones. BRCA1 inactivation by cisplatin or genetically can rescue and reposition MGL, arresting NGF-induced growth responses. These data indicate that NGF can orchestrate endocannabinoid signaling to promote cholinergic differentiation and implicate BRCA1 in determining neuronal morphology.axon guidance | basal forebrain | neurotrophin | protein stability | choline acetyltransferase C B 1 cannabinoid receptors (CB 1 Rs) are the targets of marijuana (Cannabis spp.)-derived phytocannabinoids and endocannabinoids, including 2-arachidonoyl glycerol (2-AG) (1). 2-AG liberated from postsynaptic neurons serves as a retrograde messenger to limit neurotransmitter release from many mature presynapses (1). However, 2-AG signaling also emerges as a molecular determinant of cortical development (2-4). Despite recent advances, the contribution of endocannabinoids (specifically 2-AG) to neuronal diversification and the development of synaptic connectivity in subcortical territories remains unknown. Cholinergic projection neurons within a continuum of magnocellular nuclei in the basal forebrain (5) are appealing candidates for developmental 2-AG actions considering their CB 1 R expression (1) and the endocannabinoid sensitivity of acetylcholine release in adulthood (6).Cholinergic afferents innervating the cerebral cortex are essential for learning and memory (5, 7). A favored approach to rescue cholinergic neurotransmission under disease conditions relies on neurotrophins to maintain the molecular identity, synaptic signaling, and survival of cholinergic neurons (8, 9). Nerve growth factor (NGF) appears particularly efficacious to promote the phenotypic differentiation and synaptic connectivity of postnatal cholinergic projection neurons (9, 10), as ill...

show abstract

Brca1 is required for embryonic development of the mouse cerebral cortex to normal size by preventing apoptosis of early neural progenitors

Cited by 66 publications

References 78 publications

Potential impact of primate-specific SVA retrotransposons during the evolution of human cognitive function

Potential impact of primate-specific SVA retrotransposons during the evolution of human cognitive function

BRCA1 deficiency in skin epidermis leads to selective loss of hair follicle stem cells and their progeny

Nerve growth factor scales endocannabinoid signaling by regulating monoacylglycerol lipase turnover in developing cholinergic neurons

Contact Info

Product

Resources

About