Journal article
bioRxiv, 2021
APA
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Yahn, G., Wasek, B. L., Bottiglieri, T., Malysheva, O., Caudill, M., & Jadavji, N. (2021). Dietary vitamin B12 deficiency impairs motor function and changes neuronal survival and choline metabolism after ischemic stroke in middle aged male and female mice. BioRxiv.
Chicago/Turabian
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Yahn, G., Brandi L. Wasek, T. Bottiglieri, O. Malysheva, M. Caudill, and N. Jadavji. “Dietary Vitamin B12 Deficiency Impairs Motor Function and Changes Neuronal Survival and Choline Metabolism after Ischemic Stroke in Middle Aged Male and Female Mice.” bioRxiv (2021).
MLA
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Yahn, G., et al. “Dietary Vitamin B12 Deficiency Impairs Motor Function and Changes Neuronal Survival and Choline Metabolism after Ischemic Stroke in Middle Aged Male and Female Mice.” BioRxiv, 2021.
BibTeX Click to copy
@article{g2021a,
title = {Dietary vitamin B12 deficiency impairs motor function and changes neuronal survival and choline metabolism after ischemic stroke in middle aged male and female mice},
year = {2021},
journal = {bioRxiv},
author = {Yahn, G. and Wasek, Brandi L. and Bottiglieri, T. and Malysheva, O. and Caudill, M. and Jadavji, N.}
}
Nutrition is a modifiable risk factor for ischemic stroke. As people age their ability to absorb some nutrients decreases, a primary example is vitamin B12. Older individuals with a vitamin B12 deficiency are at a higher risk for ischemic stroke and have worse stroke outcome. However, the mechanisms through which these occur remain unknown. The aim of the study was to investigate the role of vitamin B12 deficiency in ischemic stroke outcome and mechanistic changes in a mouse model. Ten-month-old male and female mice were put on control or vitamin B12 deficient diets for 4-weeks prior to and after ischemic stroke to the sensorimotor cortex. Motor function was measured, and tissues were collected to assess potential mechanisms. All deficient mice had increased levels of total homocysteine in plasma and liver tissues. After ischemic stroke, deficient mice had impaired motor function compared to control mice. There was no difference between groups in lesion volume, however, there was an increase in total apoptosis within the ischemic region of brain tissue in male deficient mice. More neuronal survival was present in ischemic brain tissue of the deficient mice compared to controls. Additionally, there were changes in choline metabolites in ischemic brain tissue because of a vitamin B12 deficiency. The data presented in this study confirms that a vitamin B12 deficiency worsens stroke outcome in male and female mice. The mechanisms driving this change may be a result of neuronal survival and compensation in choline metabolism within the damaged brain tissue.