TY - JOUR
T1 - Beta-carotene as a novel therapy for the treatment of “Autistic like behavior” in animal models of Autism
AU - Avraham, Yosefa
AU - Berry, Elliot M.
AU - Donskoy, Marina
AU - Ahmad, Wiessam Abu
AU - Vorobiev, Lia
AU - Albeck, Amnon
AU - Mankuta, David
N1 - Publisher Copyright: © 2017 Elsevier B.V.
PY - 2019/5/17
Y1 - 2019/5/17
N2 - Autism-affected individuals are characterized by lower plasma oxytocin and its ectoenzyme regulator CD38. Oxytocin, a hypothalamic hormone secreted upon the release of CD38, plays a role in social behavior and bonding. All-trans retinoic acid is a potent inducer of CD38 and can be used as a novel therapeutic strategy in autism. We investigated the role of beta-carotene in rescuing autistic-like behavior in BALB/c and BTBR mice. Beta-carotene derivatives are preferred as they are neither toxic nor teratogenic. Beta-carotene at 0.1–5.0 mg/kg was administered orally to BALB/c and BTBR newborn mice on days 1–7. They were tested at age 2–3 months for five behavioral tests for “autism”; in addition, brain CD38, oxytocin, oxytocin receptor, Brain Derived Neurotrophic Factor (BDNF) and retinoic acid receptor gene expression, serum oxytocin levels, and neurological score were evaluated. Beta-carotene administered at birth significantly increased T-maze alternations and led to longer time spent with an unfamiliar mouse in the “three-chamber test” and less time spent in the empty chamber. Furthermore, enhanced activity in the open field test; increased time spent in the reciprocal social interaction test; decreased grooming and bedding behaviors; and enhanced brain CD38, oxytocin, oxytocin receptor, BDNF, retinoic acid gene expression, and serum oxytocin levels. No changes in neurological score were observed. Beta-carotene oral supplementation to BALB/c and BTBR mice at birth significantly reduced restricted and stereotyped behaviors and interests, increased social interactions and communication, CD38, and oxytocin, probably by enhancing brain neuroplasticity without toxicity. Thus, beta-carotene administered after birth to newborns of families predisposed to “autism” has the potential to prevent/ameliorate” autistic like behavior”. These results support further clinical studies.
AB - Autism-affected individuals are characterized by lower plasma oxytocin and its ectoenzyme regulator CD38. Oxytocin, a hypothalamic hormone secreted upon the release of CD38, plays a role in social behavior and bonding. All-trans retinoic acid is a potent inducer of CD38 and can be used as a novel therapeutic strategy in autism. We investigated the role of beta-carotene in rescuing autistic-like behavior in BALB/c and BTBR mice. Beta-carotene derivatives are preferred as they are neither toxic nor teratogenic. Beta-carotene at 0.1–5.0 mg/kg was administered orally to BALB/c and BTBR newborn mice on days 1–7. They were tested at age 2–3 months for five behavioral tests for “autism”; in addition, brain CD38, oxytocin, oxytocin receptor, Brain Derived Neurotrophic Factor (BDNF) and retinoic acid receptor gene expression, serum oxytocin levels, and neurological score were evaluated. Beta-carotene administered at birth significantly increased T-maze alternations and led to longer time spent with an unfamiliar mouse in the “three-chamber test” and less time spent in the empty chamber. Furthermore, enhanced activity in the open field test; increased time spent in the reciprocal social interaction test; decreased grooming and bedding behaviors; and enhanced brain CD38, oxytocin, oxytocin receptor, BDNF, retinoic acid gene expression, and serum oxytocin levels. No changes in neurological score were observed. Beta-carotene oral supplementation to BALB/c and BTBR mice at birth significantly reduced restricted and stereotyped behaviors and interests, increased social interactions and communication, CD38, and oxytocin, probably by enhancing brain neuroplasticity without toxicity. Thus, beta-carotene administered after birth to newborns of families predisposed to “autism” has the potential to prevent/ameliorate” autistic like behavior”. These results support further clinical studies.
KW - Animal models
KW - Autism
KW - BDNF
KW - Behavioral studies
KW - Beta-carotene
KW - Brain
KW - CD38
KW - Oxytocin
KW - Retinoic acid receptor
UR - http://www.scopus.com/inward/record.url?scp=85031925530&partnerID=8YFLogxK
U2 - https://doi.org/10.1016/j.bbr.2017.09.041
DO - https://doi.org/10.1016/j.bbr.2017.09.041
M3 - مقالة
C2 - 28963040
SN - 0166-4328
VL - 364
SP - 469
EP - 479
JO - Behavioural Brain Research
JF - Behavioural Brain Research
ER -