Insights into the Etiology of Mammalian Neural Tube Closure Defects from Developmental, Genetic and Evolutionary Studies

Juriloff, D. M.; Harris, Muriel J.

doi:10.3390/jdb6030022

Cited by 53 publications

(51 citation statements)

References 223 publications

(405 reference statements)

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“…A critical step in the closure of the mouse midbrain is the transformation of the neural plate from convex to concave ( Figure 1A–C ; Nikolopoulou et al, 2017 ; Vijayraghavan and Davidson, 2017 ; Juriloff and Harris, 2018 ). Prior to closure, the cranial neural plate has an open, rams-horn shape ( Figure 1C ).…”

Section: Resultsmentioning

confidence: 99%

“…During development, neuroepithelial cells undergo extensive remodeling to transform a flat sheet into a fully closed tube that gives rise to the brain and spinal cord of the animal. Distinct genetic circuits are required for neural tube closure in different regions along the head-to-tail axis, translating positional information into location-appropriate cell behaviors (Wilde et al, 2014;Aw and Devenport, 2017;Nikolopoulou et al, 2017;Juriloff and Harris, 2018). Although many studies have focused on mechanisms of neural tube closure in the spinal cord, one-third of human neural tube defects arise from a failure of closure in the cranial region, resulting in exencephaly-an inoperable and terminally lethal birth defect (Zaganjor et al, 2016).…”

Section: Introductionmentioning

confidence: 99%

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Sonic hedgehog signaling directs patterned cell remodeling during cranial neural tube closure

Brooks

Islam

Anderson

et al. 2020

eLife

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Neural tube closure defects are a major cause of infant mortality, with exencephaly accounting for nearly one-third of cases. However, the mechanisms of cranial neural tube closure are not well understood. Here we show that this process involves a tissue-wide pattern of apical constriction controlled by Sonic hedgehog (Shh) signaling. Midline cells in the mouse midbrain neuroepithelium are short with large apical surfaces, whereas lateral cells are taller and undergo synchronous apical constriction, driving neural fold elevation. Embryos lacking the Shh effector Gli2 fail to produce appropriate midline cell architecture, whereas embryos with expanded Shh signaling, including the IFT-A complex mutants Ift122 and Ttc21b and embryos expressing activated Smoothened, display apical constriction defects in lateral cells. Disruption of lateral, but not midline, cell remodeling results in exencephaly. These results reveal a morphogenetic program of patterned apical constriction governed by Shh signaling that generates structural changes in the developing mammalian brain.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Sonic hedgehog signaling directs patterned cell remodeling during cranial neural tube closure

Brooks

Islam

Anderson

et al. 2020

eLife

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“…Two potential hypotheses for this reduced proliferation are (a) an overall reduction in cellular metabolism due to C2 treatment impacting mitochondrial function, and (b) ciliary disruption due to C2 treatment disrupts cellular functionality and division. Ceramides are implicated in reducing the mitochondrial respiration of skeletal muscle cells, and several lines of study have indicated a potential role of primary cilium in the development of NTDs . Ceramides are reported to regulate the generation and elongation of primary cilium .…”

Section: Discussionmentioning

confidence: 99%

“…Ceramides are implicated in reducing the mitochondrial respiration of skeletal muscle cells, 71,72 and several lines of study have indicated a potential role of primary cilium in the development of NTDs. [73][74][75][76] Ceramides are reported to regulate the generation and elongation of primary cilium. 77,78 Future studies will examine cellular metabolism in the early embryo and explore the role of ceramides in regulating primary cilia during neural tube closure under high C2 conditions.…”

Section: Embryonic Defect Datamentioning

confidence: 99%

Ceramide: a novel inducer for neural tube defects

Ross

Piorczynski

Harvey

et al. 2019

Developmental Dynamics

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Background Circulating plasma ceramides, a class of bioactive sphingolipids, are elevated in metabolic disorders, including obesity. Infants of women with these disorders are at 2‐ to 3‐fold greater risk for developing a neural tube defect (NTD). This study aimed to test the effects of embryonic exposure to C2‐ceramides (C2) during neural tube closure. Preliminary data shows an increase in NTDs in chick embryos after C2 exposure, and addresses potential mechanisms. Results Cell and embryo models were used to examine redox shifts after ceramide exposure. While undifferentiated P19 cells were resistant to ceramide exposure, neuronally differentiated P19 cells exhibited an oxidizing shift. Consistent with these observations, GSH E h curves revealed a shift to a more oxidized state in C2 treated embryos without increasing apoptosis or changing Pax3 expression, however cell proliferation was lower. Neural tube defects were observed in 45% of chick embryos exposed to C2, compared to 12% in control embryos. Conclusions C2 exposure during critical developmental stages increased the frequency of NTDs in the avian model. Increased ROS generation in cell culture, along with the more oxidative GSH E h profiles of C2 exposed cells and embryos, support a model wherein ceramide affects neural tube closure via altered tissue redox environments.

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“…53 Interestingly, both lack of and excessive apoptosis have been associated with NTDs in animal models. Alterations in apoptotic genes Casp3 and Apaf1 impair closure at the midbrain and hindbrain; 54,55 however, excessive cell death has also been associated with failure of neural tube closure, highlighting the delicate balance that must be maintained during neurodevelopment. 27,56 Closure Sites in Primary Neurulation Primary neurulation in mammals is discontinuous with the three separate closure locations arising along the developing neural tube, which is in contrast to an older model that describes the neural tube closing in a continuous, zipper-like fashion ( Figure 2).…”

Section: Neural Plate Bendingmentioning

confidence: 99%

Embryology of Spinal Dysraphism and its Relationship to Surgical Treatment

Eagles

Gupta

2020

Can. J. Neurol. Sci.

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Spinal dysraphism is an umbrella term that encompasses a number of congenital malformations that affect the central nervous system. The etiology of these conditions can be traced back to a specific defect in embryological development, with the more disabling malformations occurring at an earlier gestational age. A thorough understanding of the relevant neuroembryology is imperative for clinicians to select the correct treatment and prevent complications associated with spinal dysraphism. This paper will review the neuroembryology associated with the various forms of spinal dysraphism and provide a clinical-pathological correlation for these congenital malformations.

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Insights into the Etiology of Mammalian Neural Tube Closure Defects from Developmental, Genetic and Evolutionary Studies

Cited by 53 publications

References 223 publications

Sonic hedgehog signaling directs patterned cell remodeling during cranial neural tube closure

Sonic hedgehog signaling directs patterned cell remodeling during cranial neural tube closure

Ceramide: a novel inducer for neural tube defects

Embryology of Spinal Dysraphism and its Relationship to Surgical Treatment

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