Thiamine and benfotiamine prevent stress-induced suppression of hippocampal neurogenesis in mice exposed to predation without affecting brain thiamine diphosphate levels

Julie Vignisse; Margaux Sambon; Anna Gorlova; Dmitrii Pavlov; Nicolas Caron; Brigitte Malgrange; Elena Shevtsova; Andrey Svistunov; Daniel C. Anthony; Natalyia Markova; Natalyia Bazhenova; Bernard Coumans; Bernard Lakaye; Pierre Wins; Tatyana Strekalova; Lucien Bettendorff

doi:10.1016/j.mcn.2017.05.005

Thiamine and benfotiamine prevent stress-induced suppression of hippocampal neurogenesis in mice exposed to predation without affecting brain thiamine diphosphate levels

Julie Vignisse, Margaux Sambon, Anna Gorlova, Dmitrii Pavlov, Nicolas Caron, Brigitte Malgrange, Elena Shevtsova, Andrey Svistunov, Daniel C. Anthony, Natalyia Markova, Natalyia Bazhenova, Bernard Coumans, Bernard Lakaye, Pierre Wins, Tatyana Strekalova^*, Lucien Bettendorff^*

^*Corresponding author for this work

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

Abstract

Thiamine is essential for normal brain function and its deficiency causes metabolic impairment, specific lesions, oxidative damage and reduced adult hippocampal neurogenesis (AHN). Thiamine precursors with increased bioavailability, especially benfotiamine, exert neuroprotective effects not only for thiamine deficiency (TD), but also in mouse models of neurodegeneration. As it is known that AHN is impaired by stress in rodents, we exposed C57BL6/J mice to predator stress for 5 consecutive nights and studied the proliferation (number of Ki67-positive cells) and survival (number of BrdU-positive cells) of newborn immature neurons in the subgranular zone of the dentate gyrus. In stressed mice, the number of Ki67- and BrdU-positive cells was reduced compared to non stressed animals. This reduction was prevented when the mice were treated (200 mg/kg/day in drinking water for 20 days) with thiamine or benfotiamine, that were recently found to prevent stress-induced behavioral changes and glycogen synthase kinase-3 beta (GSK-3 beta) upregulation in the CNS. Moreover, we show that thiamine and benfotiamine counteract stress-induced bodyweight loss and suppress stress-induced anxiety-like behavior. Both treatments induced a modest increase in the brain content of free thiamine while the level of thiamine di-phosphate (ThDP) remained unchanged, suggesting that the beneficial effects observed are not linked to the role of this coenzyme in energy metabolism. Predator stress increased hippocampal protein carbonylation, an indicator of oxidative stress. This effect was antagonized by both thiamine and benfotiamine. Moreover, using cultured mouse neuroblastoma cells, we show that in particular benfotiamine protects against paraquat-induced oxidative stress. We therefore hypothesize that thiamine compounds may act by boosting anti-oxidant cellular defenses, by a mechanism that still remains to be unveiled. Our study demonstrates, for the first time, that thiamine and benfotiamine prevent stress-induced inhibition of hippocampal neurogenesis and accompanying physiological changes. The present data suggest that thiamine precursors with high bioavailability might be useful as a complementary therapy in several neuropsychiatric disorders. (C) 2017 Elsevier Inc. All rights reserved.

Original language	English
Pages (from-to)	126-136
Number of pages	11
Journal	Molecular and Cellular Neuroscience
Volume	82
DOIs	https://doi.org/10.1016/j.mcn.2017.05.005
Publication status	Published - Jul 2017

Keywords

Thiamine
benfotiamine
predator stress
neurogenesis
survival
oxidative stress
hippocampus
COGNITIVE IMPAIRMENT
ADULT NEUROGENESIS
CELL-PROLIFERATION
OXIDATIVE DAMAGE
DOUBLE-BLIND
DEPRESSION
PROTEIN
MODEL
RATS
DIFFERENTIATION

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Vignisse, J., Sambon, M., Gorlova, A., Pavlov, D., Caron, N., Malgrange, B., Shevtsova, E., Svistunov, A., Anthony, D. C., Markova, N., Bazhenova, N., Coumans, B., Lakaye, B., Wins, P., Strekalova, T., & Bettendorff, L. (2017). Thiamine and benfotiamine prevent stress-induced suppression of hippocampal neurogenesis in mice exposed to predation without affecting brain thiamine diphosphate levels. Molecular and Cellular Neuroscience, 82, 126-136. https://doi.org/10.1016/j.mcn.2017.05.005

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title = "Thiamine and benfotiamine prevent stress-induced suppression of hippocampal neurogenesis in mice exposed to predation without affecting brain thiamine diphosphate levels",

abstract = "Thiamine is essential for normal brain function and its deficiency causes metabolic impairment, specific lesions, oxidative damage and reduced adult hippocampal neurogenesis (AHN). Thiamine precursors with increased bioavailability, especially benfotiamine, exert neuroprotective effects not only for thiamine deficiency (TD), but also in mouse models of neurodegeneration. As it is known that AHN is impaired by stress in rodents, we exposed C57BL6/J mice to predator stress for 5 consecutive nights and studied the proliferation (number of Ki67-positive cells) and survival (number of BrdU-positive cells) of newborn immature neurons in the subgranular zone of the dentate gyrus. In stressed mice, the number of Ki67- and BrdU-positive cells was reduced compared to non stressed animals. This reduction was prevented when the mice were treated (200 mg/kg/day in drinking water for 20 days) with thiamine or benfotiamine, that were recently found to prevent stress-induced behavioral changes and glycogen synthase kinase-3 beta (GSK-3 beta) upregulation in the CNS. Moreover, we show that thiamine and benfotiamine counteract stress-induced bodyweight loss and suppress stress-induced anxiety-like behavior. Both treatments induced a modest increase in the brain content of free thiamine while the level of thiamine di-phosphate (ThDP) remained unchanged, suggesting that the beneficial effects observed are not linked to the role of this coenzyme in energy metabolism. Predator stress increased hippocampal protein carbonylation, an indicator of oxidative stress. This effect was antagonized by both thiamine and benfotiamine. Moreover, using cultured mouse neuroblastoma cells, we show that in particular benfotiamine protects against paraquat-induced oxidative stress. We therefore hypothesize that thiamine compounds may act by boosting anti-oxidant cellular defenses, by a mechanism that still remains to be unveiled. Our study demonstrates, for the first time, that thiamine and benfotiamine prevent stress-induced inhibition of hippocampal neurogenesis and accompanying physiological changes. The present data suggest that thiamine precursors with high bioavailability might be useful as a complementary therapy in several neuropsychiatric disorders. (C) 2017 Elsevier Inc. All rights reserved.",

keywords = "Thiamine, benfotiamine, predator stress, neurogenesis, survival, oxidative stress, hippocampus, COGNITIVE IMPAIRMENT, ADULT NEUROGENESIS, CELL-PROLIFERATION, OXIDATIVE DAMAGE, DOUBLE-BLIND, DEPRESSION, PROTEIN, MODEL, RATS, DIFFERENTIATION",

author = "Julie Vignisse and Margaux Sambon and Anna Gorlova and Dmitrii Pavlov and Nicolas Caron and Brigitte Malgrange and Elena Shevtsova and Andrey Svistunov and Anthony, {Daniel C.} and Natalyia Markova and Natalyia Bazhenova and Bernard Coumans and Bernard Lakaye and Pierre Wins and Tatyana Strekalova and Lucien Bettendorff",

year = "2017",

month = jul,

doi = "10.1016/j.mcn.2017.05.005",

language = "English",

volume = "82",

pages = "126--136",

journal = "Molecular and Cellular Neuroscience",

issn = "1044-7431",

publisher = "Elsevier Science",

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Vignisse, J, Sambon, M, Gorlova, A, Pavlov, D, Caron, N, Malgrange, B, Shevtsova, E, Svistunov, A, Anthony, DC, Markova, N, Bazhenova, N, Coumans, B, Lakaye, B, Wins, P, Strekalova, T & Bettendorff, L 2017, 'Thiamine and benfotiamine prevent stress-induced suppression of hippocampal neurogenesis in mice exposed to predation without affecting brain thiamine diphosphate levels', Molecular and Cellular Neuroscience, vol. 82, pp. 126-136. https://doi.org/10.1016/j.mcn.2017.05.005

Thiamine and benfotiamine prevent stress-induced suppression of hippocampal neurogenesis in mice exposed to predation without affecting brain thiamine diphosphate levels. / Vignisse, Julie; Sambon, Margaux; Gorlova, Anna et al.
In: Molecular and Cellular Neuroscience, Vol. 82, 07.2017, p. 126-136.

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

TY - JOUR

T1 - Thiamine and benfotiamine prevent stress-induced suppression of hippocampal neurogenesis in mice exposed to predation without affecting brain thiamine diphosphate levels

AU - Vignisse, Julie

AU - Sambon, Margaux

AU - Gorlova, Anna

AU - Pavlov, Dmitrii

AU - Caron, Nicolas

AU - Malgrange, Brigitte

AU - Shevtsova, Elena

AU - Svistunov, Andrey

AU - Anthony, Daniel C.

AU - Markova, Natalyia

AU - Bazhenova, Natalyia

AU - Coumans, Bernard

AU - Lakaye, Bernard

AU - Wins, Pierre

AU - Strekalova, Tatyana

AU - Bettendorff, Lucien

PY - 2017/7

Y1 - 2017/7

N2 - Thiamine is essential for normal brain function and its deficiency causes metabolic impairment, specific lesions, oxidative damage and reduced adult hippocampal neurogenesis (AHN). Thiamine precursors with increased bioavailability, especially benfotiamine, exert neuroprotective effects not only for thiamine deficiency (TD), but also in mouse models of neurodegeneration. As it is known that AHN is impaired by stress in rodents, we exposed C57BL6/J mice to predator stress for 5 consecutive nights and studied the proliferation (number of Ki67-positive cells) and survival (number of BrdU-positive cells) of newborn immature neurons in the subgranular zone of the dentate gyrus. In stressed mice, the number of Ki67- and BrdU-positive cells was reduced compared to non stressed animals. This reduction was prevented when the mice were treated (200 mg/kg/day in drinking water for 20 days) with thiamine or benfotiamine, that were recently found to prevent stress-induced behavioral changes and glycogen synthase kinase-3 beta (GSK-3 beta) upregulation in the CNS. Moreover, we show that thiamine and benfotiamine counteract stress-induced bodyweight loss and suppress stress-induced anxiety-like behavior. Both treatments induced a modest increase in the brain content of free thiamine while the level of thiamine di-phosphate (ThDP) remained unchanged, suggesting that the beneficial effects observed are not linked to the role of this coenzyme in energy metabolism. Predator stress increased hippocampal protein carbonylation, an indicator of oxidative stress. This effect was antagonized by both thiamine and benfotiamine. Moreover, using cultured mouse neuroblastoma cells, we show that in particular benfotiamine protects against paraquat-induced oxidative stress. We therefore hypothesize that thiamine compounds may act by boosting anti-oxidant cellular defenses, by a mechanism that still remains to be unveiled. Our study demonstrates, for the first time, that thiamine and benfotiamine prevent stress-induced inhibition of hippocampal neurogenesis and accompanying physiological changes. The present data suggest that thiamine precursors with high bioavailability might be useful as a complementary therapy in several neuropsychiatric disorders. (C) 2017 Elsevier Inc. All rights reserved.

AB - Thiamine is essential for normal brain function and its deficiency causes metabolic impairment, specific lesions, oxidative damage and reduced adult hippocampal neurogenesis (AHN). Thiamine precursors with increased bioavailability, especially benfotiamine, exert neuroprotective effects not only for thiamine deficiency (TD), but also in mouse models of neurodegeneration. As it is known that AHN is impaired by stress in rodents, we exposed C57BL6/J mice to predator stress for 5 consecutive nights and studied the proliferation (number of Ki67-positive cells) and survival (number of BrdU-positive cells) of newborn immature neurons in the subgranular zone of the dentate gyrus. In stressed mice, the number of Ki67- and BrdU-positive cells was reduced compared to non stressed animals. This reduction was prevented when the mice were treated (200 mg/kg/day in drinking water for 20 days) with thiamine or benfotiamine, that were recently found to prevent stress-induced behavioral changes and glycogen synthase kinase-3 beta (GSK-3 beta) upregulation in the CNS. Moreover, we show that thiamine and benfotiamine counteract stress-induced bodyweight loss and suppress stress-induced anxiety-like behavior. Both treatments induced a modest increase in the brain content of free thiamine while the level of thiamine di-phosphate (ThDP) remained unchanged, suggesting that the beneficial effects observed are not linked to the role of this coenzyme in energy metabolism. Predator stress increased hippocampal protein carbonylation, an indicator of oxidative stress. This effect was antagonized by both thiamine and benfotiamine. Moreover, using cultured mouse neuroblastoma cells, we show that in particular benfotiamine protects against paraquat-induced oxidative stress. We therefore hypothesize that thiamine compounds may act by boosting anti-oxidant cellular defenses, by a mechanism that still remains to be unveiled. Our study demonstrates, for the first time, that thiamine and benfotiamine prevent stress-induced inhibition of hippocampal neurogenesis and accompanying physiological changes. The present data suggest that thiamine precursors with high bioavailability might be useful as a complementary therapy in several neuropsychiatric disorders. (C) 2017 Elsevier Inc. All rights reserved.

KW - Thiamine

KW - benfotiamine

KW - predator stress

KW - neurogenesis

KW - survival

KW - oxidative stress

KW - hippocampus

KW - COGNITIVE IMPAIRMENT

KW - ADULT NEUROGENESIS

KW - CELL-PROLIFERATION

KW - OXIDATIVE DAMAGE

KW - DOUBLE-BLIND

KW - DEPRESSION

KW - PROTEIN

KW - MODEL

KW - RATS

KW - DIFFERENTIATION

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DO - 10.1016/j.mcn.2017.05.005

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JO - Molecular and Cellular Neuroscience

JF - Molecular and Cellular Neuroscience

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