Alcohol exposure during the first two trimesters-equivalent alters the development of corpus callosum projection neurons in the rat

Livy, Daniel J.; Elberger, Andrea J.

doi:10.1016/j.alcohol.2008.04.002

Cited by 20 publications

(16 citation statements)

References 47 publications

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“…Midline callosal hypoplasia was detected in both P0 and P20 PrEE mice, consistent with previous studies in both human and mouse that demonstrate an association between PrEE and shape abnormalities with volumetric changes in the CC (Gautam et al., ; Livy and Elberger, ). Our results show an initial thinning of the CC at birth, lasting through P20, due to PrEE.…”

Section: Discussionsupporting

confidence: 90%

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The Impact of Prenatal Ethanol Exposure on Neuroanatomical and Behavioral Development in Mice

Abbott

Kozanian

Kanaan

et al. 2016

Alcoholism Clin & Exp Res

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Background In utero alcohol, or ethanol, exposure produces developmental abnormalities in the brain of the fetus, which can result in lifelong behavioral abnormalities. Fetal alcohol spectrum disorders (FASD) is a term used to describe a range of adverse developmental conditions caused by ethanol exposure during gestation. Children diagnosed with FASD potentially exhibit a host of phenotypes including growth retardation, facial dysmorphology, central nervous system anomalies, abnormal behavior and cognitive deficits. Previous research suggests that abnormal gene expression and circuitry in the neocortex may underlie reported disabilities of learning, memory, and behavior resulting from early exposure to alcohol (El Shawa et al., 2013). Methods Here, we utilize a mouse model of FASD to examine effects of prenatal ethanol exposure, or PrEE, on brain anatomy in newborn (P0), weanling (P20) and early adult (P50) mice. We correlate abnormal cortical and subcortical anatomy with atypical behavior in adult P50 PrEE mice. In this model, experimental dams self-administered a 25% ethanol solution throughout gestation (gestational day, GD, 0 to 19, day of birth), generating the exposure to the offspring. Results Results from these experiments reveal long-term alterations to cortical anatomy, including atypical developmental cortical thinning, and abnormal subcortical development as a result of in utero ethanol exposure. Furthermore, offspring exposed to ethanol during the prenatal period performed poorly on behavioral tasks measuring sensorimotor integration and anxiety. Conclusions Insight from this study will help provide new information on developmental trajectories of prenatal ethanol exposure and the biological etiologies of abnormal behavior in people diagnosed with FASD.

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Section: Discussionsupporting

confidence: 90%

“…Other studies have identified noncortical damage to the developing nervous system from PrEE. For example, West and colleagues described abnormal development in the hippocampus, cerebellum, and CC following PrEE in a rat model of FASD (Livy and Elberger, ; Livy et al., ; Maier and West, ).…”

mentioning

confidence: 99%

The Impact of Prenatal Ethanol Exposure on Neuroanatomical and Behavioral Development in Mice

Abbott

Kozanian

Kanaan

et al. 2016

Alcoholism Clin & Exp Res

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“…Conventional neuroanatomical methods applied to postmortem human or animal tissue have provided evidence that the ADD changes in neurological conditions such as amyotrophic lateral sclerosis (ALS) (Cluskey and Ramsden, 2001) and multiple sclerosis (MS) (Trapp et al, 1998; Evangelou et al, 2001; Lovas et al, 2000). In addition, several pathologies, including autism (Hughes, 2007), dyslexia (Njiokiktjien et al, 1994), schizophrenia (Randall, 1983), and even alcoholism (Livy and Elberger, 2008), have been associated with changes in the distribution of axon size. Changes in the number of axons and their diameters also take place throughout normal development accompanying the period of dynamic behavioral, cognitive, and emotional changes in childhood and adolescence (Yakovlev, 1967; Pfefferbaum et al, 1994; Gregg et al, 2007; Barnea-Goraly et al, 2005; Schlaug et al, 2009).…”

Section: Introductionmentioning

confidence: 99%

White matter microstructure from nonparametric axon diameter distribution mapping

et al. 2016

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We report the development of a double diffusion encoding (DDE) MRI method to estimate and map the axon diameter distribution (ADD) within an imaging volume. A variety of biological processes, ranging from development to disease and trauma, may lead to changes in the ADD in the central and peripheral nervous systems. Unlike previously proposed methods, this ADD experimental design and estimation framework employs a more general, nonparametric approach, without a priori assumptions about the underlying form of the ADD, making it suitable to analyze abnormal tissue. In the current study, this framework was used on an ex vivo ferret spinal cord, while emphasizing the way in which the ADD can be weighted by either the number or the volume of the axons. The different weightings, which result in different spatial contrasts, were considered throughout this work. DDE data were analyzed to derive spatially resolved maps of average axon diameter, ADD variance, and extra-axonal volume fraction, along with a novel sub-micron restricted structures map. The morphological information contained in these maps was then used to segment white matter into distinct domains by using a proposed k-means clustering algorithm with spatial contiguity and left–right symmetry constraints, resulting in identifiable white matter tracks. The method was validated by comparing histological measures to the estimated ADDs using a quantitative similarity metric, resulting in good agreement. With further acquisition acceleration and experimental parameters adjustments, this ADD estimation framework could be first used preclinically, and eventually clinically, enabling a wide range of neuroimaging applications for improved understanding of neurodegenerative pathologies and assessing microstructural changes resulting from trauma.

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“…Studies conducted primarily in rodent have reported ethanol-induced impairments in neurogenesis (Goodlett and Horn, 2001), neuronal migration (Aronne et al, 2011) and axonal outgrowth (Granato et al, 2003; Lindsley et al, 2003; Livy and Elberger, 2008). Regarding the latter, low (12.5 mM) concentrations of ethanol impair growth cone responses to guidance cues, including semaphorins and netrins (Sepulveda et al, 2011), known to regulate axonal growth and targeting (Behar et al, 1996; Luo et al, 1995; Serafini et al, 1994; Steup et al, 2000).…”

Section: Introductionmentioning

confidence: 99%

Ethanol-induced disruption of Golgi apparatus morphology, primary neurite number and cellular orientation in developing cortical neurons

Powrozek¹,

Olson²

2012

Alcohol

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Alcohol exposure during the first two trimesters-equivalent alters the development of corpus callosum projection neurons in the rat

Cited by 20 publications

References 47 publications

The Impact of Prenatal Ethanol Exposure on Neuroanatomical and Behavioral Development in Mice

The Impact of Prenatal Ethanol Exposure on Neuroanatomical and Behavioral Development in Mice

White matter microstructure from nonparametric axon diameter distribution mapping

Ethanol-induced disruption of Golgi apparatus morphology, primary neurite number and cellular orientation in developing cortical neurons

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