Magnetic Resonance Imaging and Micro-Computed Tomography reveal brain morphological abnormalities in a mouse model of early moderate prenatal ethanol exposure

Van T. Nguyen; Quang M. Tieng; Karine Mardon; Christine Zhang; Suyinn Chong; Graham J. Galloway; Nyoman D. Kurniawan

doi:10.1016/j.ntt.2019.106849

Magnetic Resonance Imaging and Micro-Computed Tomography reveal brain morphological abnormalities in a mouse model of early moderate prenatal ethanol exposure

Van T. Nguyen, Quang M. Tieng, Karine Mardon, Christine Zhang, Suyinn Chong, Graham J. Galloway, Nyoman D. Kurniawan

Section of Stem Cell Biology

Research output: Contribution to journal › Article › peer-review

2 Scopus citations

Abstract

Background: This study investigated the effects of early moderate prenatal ethanol exposure (PEE) on the brain in a mouse model that mimics a scenario in humans, whereby moderate daily drinking ceases after a woman becomes aware of her pregnancy. Methods: C57BL/6J pregnant mice were given 10% v/v ethanol from gestational day 0–8 in the drinking water. The male offspring were used for imaging. Anatomical and diffusion Magnetic Resonance Imaging were performed in vivo at postnatal day 28 (P28, adolescence) and P80 (adulthood). Micro-Computed Tomography was performed on fixed whole heads at P80. Tensor-based morphometry (TBM) was applied to detect alterations in brain structure and voxel-based morphometry (VBM) for skull morphology. Diffusion tensor and neurite orientation dispersion and density imaging models were used to detect microstructural changes. Neurofilament (NF) immunohistochemistry was used to validate findings by in vivo diffusion MRI. Results: TBM showed that PEE mice exhibited a significantly smaller third ventricle at P28 (family-wise error rate (FWE), p < 0.05). All other macro-structural alterations did not survive FWE corrections but when displayed with an uncorrected p < 0.005 showed multiple regional volume reductions and expansions, more prominently in the right hemisphere. PEE-induced gross volume changes included a bigger thalamus, hypothalamus and ventricles at P28, and bigger total brain volumes at both P28 and P80 (2-sample t-tests). Disproportionately smaller olfactory bulbs following PEE were revealed at both time-points. No alterations in diffusion parameters were detected, but PEE animals exhibited reduced NF positive staining in the thalamus and striatum and greater bone density in various skull regions. Conclusion: Our results show that early moderate PEE can cause alterations in the brain that are detectable during development and adulthood.

Original language	English
Article number	106849
Journal	Neurotoxicology and Teratology
Volume	77
DOIs	https://doi.org/10.1016/j.ntt.2019.106849
State	Published - Jan 1 2020

Keywords

Computed tomography
Fetal alcohol spectrum disorders
MRI
Morphometry
Mouse brain

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10.1016/j.ntt.2019.106849

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title = "Magnetic Resonance Imaging and Micro-Computed Tomography reveal brain morphological abnormalities in a mouse model of early moderate prenatal ethanol exposure",

abstract = "Background: This study investigated the effects of early moderate prenatal ethanol exposure (PEE) on the brain in a mouse model that mimics a scenario in humans, whereby moderate daily drinking ceases after a woman becomes aware of her pregnancy. Methods: C57BL/6J pregnant mice were given 10% v/v ethanol from gestational day 0–8 in the drinking water. The male offspring were used for imaging. Anatomical and diffusion Magnetic Resonance Imaging were performed in vivo at postnatal day 28 (P28, adolescence) and P80 (adulthood). Micro-Computed Tomography was performed on fixed whole heads at P80. Tensor-based morphometry (TBM) was applied to detect alterations in brain structure and voxel-based morphometry (VBM) for skull morphology. Diffusion tensor and neurite orientation dispersion and density imaging models were used to detect microstructural changes. Neurofilament (NF) immunohistochemistry was used to validate findings by in vivo diffusion MRI. Results: TBM showed that PEE mice exhibited a significantly smaller third ventricle at P28 (family-wise error rate (FWE), p < 0.05). All other macro-structural alterations did not survive FWE corrections but when displayed with an uncorrected p < 0.005 showed multiple regional volume reductions and expansions, more prominently in the right hemisphere. PEE-induced gross volume changes included a bigger thalamus, hypothalamus and ventricles at P28, and bigger total brain volumes at both P28 and P80 (2-sample t-tests). Disproportionately smaller olfactory bulbs following PEE were revealed at both time-points. No alterations in diffusion parameters were detected, but PEE animals exhibited reduced NF positive staining in the thalamus and striatum and greater bone density in various skull regions. Conclusion: Our results show that early moderate PEE can cause alterations in the brain that are detectable during development and adulthood.",

keywords = "Computed tomography, Fetal alcohol spectrum disorders, MRI, Morphometry, Mouse brain",

author = "Nguyen, {Van T.} and Tieng, {Quang M.} and Karine Mardon and Christine Zhang and Suyinn Chong and Galloway, {Graham J.} and Kurniawan, {Nyoman D.}",

note = "Funding Information: This study was funded by the Australian National Health and Medical Research Council (grant number APP1003038). Publisher Copyright: {\textcopyright} 2019 Elsevier Inc.",

year = "2020",

month = jan,

day = "1",

doi = "10.1016/j.ntt.2019.106849",

language = "English",

volume = "77",

journal = "Neurotoxicology and Teratology",

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TY - JOUR

T1 - Magnetic Resonance Imaging and Micro-Computed Tomography reveal brain morphological abnormalities in a mouse model of early moderate prenatal ethanol exposure

AU - Nguyen, Van T.

AU - Tieng, Quang M.

AU - Mardon, Karine

AU - Zhang, Christine

AU - Chong, Suyinn

AU - Galloway, Graham J.

AU - Kurniawan, Nyoman D.

PY - 2020/1/1

Y1 - 2020/1/1

N2 - Background: This study investigated the effects of early moderate prenatal ethanol exposure (PEE) on the brain in a mouse model that mimics a scenario in humans, whereby moderate daily drinking ceases after a woman becomes aware of her pregnancy. Methods: C57BL/6J pregnant mice were given 10% v/v ethanol from gestational day 0–8 in the drinking water. The male offspring were used for imaging. Anatomical and diffusion Magnetic Resonance Imaging were performed in vivo at postnatal day 28 (P28, adolescence) and P80 (adulthood). Micro-Computed Tomography was performed on fixed whole heads at P80. Tensor-based morphometry (TBM) was applied to detect alterations in brain structure and voxel-based morphometry (VBM) for skull morphology. Diffusion tensor and neurite orientation dispersion and density imaging models were used to detect microstructural changes. Neurofilament (NF) immunohistochemistry was used to validate findings by in vivo diffusion MRI. Results: TBM showed that PEE mice exhibited a significantly smaller third ventricle at P28 (family-wise error rate (FWE), p < 0.05). All other macro-structural alterations did not survive FWE corrections but when displayed with an uncorrected p < 0.005 showed multiple regional volume reductions and expansions, more prominently in the right hemisphere. PEE-induced gross volume changes included a bigger thalamus, hypothalamus and ventricles at P28, and bigger total brain volumes at both P28 and P80 (2-sample t-tests). Disproportionately smaller olfactory bulbs following PEE were revealed at both time-points. No alterations in diffusion parameters were detected, but PEE animals exhibited reduced NF positive staining in the thalamus and striatum and greater bone density in various skull regions. Conclusion: Our results show that early moderate PEE can cause alterations in the brain that are detectable during development and adulthood.

AB - Background: This study investigated the effects of early moderate prenatal ethanol exposure (PEE) on the brain in a mouse model that mimics a scenario in humans, whereby moderate daily drinking ceases after a woman becomes aware of her pregnancy. Methods: C57BL/6J pregnant mice were given 10% v/v ethanol from gestational day 0–8 in the drinking water. The male offspring were used for imaging. Anatomical and diffusion Magnetic Resonance Imaging were performed in vivo at postnatal day 28 (P28, adolescence) and P80 (adulthood). Micro-Computed Tomography was performed on fixed whole heads at P80. Tensor-based morphometry (TBM) was applied to detect alterations in brain structure and voxel-based morphometry (VBM) for skull morphology. Diffusion tensor and neurite orientation dispersion and density imaging models were used to detect microstructural changes. Neurofilament (NF) immunohistochemistry was used to validate findings by in vivo diffusion MRI. Results: TBM showed that PEE mice exhibited a significantly smaller third ventricle at P28 (family-wise error rate (FWE), p < 0.05). All other macro-structural alterations did not survive FWE corrections but when displayed with an uncorrected p < 0.005 showed multiple regional volume reductions and expansions, more prominently in the right hemisphere. PEE-induced gross volume changes included a bigger thalamus, hypothalamus and ventricles at P28, and bigger total brain volumes at both P28 and P80 (2-sample t-tests). Disproportionately smaller olfactory bulbs following PEE were revealed at both time-points. No alterations in diffusion parameters were detected, but PEE animals exhibited reduced NF positive staining in the thalamus and striatum and greater bone density in various skull regions. Conclusion: Our results show that early moderate PEE can cause alterations in the brain that are detectable during development and adulthood.

KW - Computed tomography

KW - Fetal alcohol spectrum disorders

KW - MRI

KW - Morphometry

KW - Mouse brain

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DO - 10.1016/j.ntt.2019.106849

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C2 - 31838218

AN - SCOPUS:85076692710

SN - 0892-0362

VL - 77

JO - Neurotoxicology and Teratology

JF - Neurotoxicology and Teratology

M1 - 106849

ER -

Magnetic Resonance Imaging and Micro-Computed Tomography reveal brain morphological abnormalities in a mouse model of early moderate prenatal ethanol exposure

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