Translational Psychiatry / S100B dysregulation during brain development affects synaptic SHANK protein networks via alteration of zinc homeostasis

Autor: Daini, Eleonora, Hagmeyer, Simone, De Benedictis, Chiara A., Cristóvão, Joana S., Bodria, Martina, Ross, Aisling M., Raab, Andrea, Boeckers, Tobias M., Feldmann, Jörg, Gomes, Cláudio M., Zoli, Michele, Vilella, Antonietta, Grabrucker, Andreas M.
Jazyk: angličtina
Rok vydání: 2021
Předmět:
Autism Spectrum Disorders (ASD) are caused by a combination of genetic predisposition and nongenetic factors. Among the nongenetic factors
maternal immune system activation and zinc deficiency have been proposed. Intriguingly
as a genetic factor
copy-number variations in S100B
a pro-inflammatory damage-associated molecular pattern (DAMP)
have been associated with ASD
and increased serum S100B has been found in ASD. Interestingly
it has been shown that increased S100B levels affect zinc homeostasis in vitro. Thus
here
we investigated the influence of increased S100B levels in vitro and in vivo during pregnancy in mice regarding zinc availability
the zinc-sensitive SHANK protein networks associated with ASD
and behavioral outcomes. We observed that S100B affects the synaptic SHANK2 and SHANK3 levels in a zinc-dependent manner
especially early in neuronal development. Animals exposed to high S100B levels in utero similarly show reduced levels of free zinc and SHANK2 in the brain. On the behavioral level
these mice display hyperactivity
increased stereotypic and abnormal social behaviors
and cognitive impairment. Pro-inflammatory factors and zinc-signaling alterations converge on the synaptic level revealing a common pathomechanism that may mechanistically explain a large share of ASD cases
DOI: 10.1038/s41398-021-01694-z
Popis: Autism Spectrum Disorders (ASD) are caused by a combination of genetic predisposition and nongenetic factors. Among the nongenetic factors, maternal immune system activation and zinc deficiency have been proposed. Intriguingly, as a genetic factor, copy-number variations in S100B, a pro-inflammatory damage-associated molecular pattern (DAMP), have been associated with ASD, and increased serum S100B has been found in ASD. Interestingly, it has been shown that increased S100B levels affect zinc homeostasis in vitro. Thus, here, we investigated the influence of increased S100B levels in vitro and in vivo during pregnancy in mice regarding zinc availability, the zinc-sensitive SHANK protein networks associated with ASD, and behavioral outcomes. We observed that S100B affects the synaptic SHANK2 and SHANK3 levels in a zinc-dependent manner, especially early in neuronal development. Animals exposed to high S100B levels in utero similarly show reduced levels of free zinc and SHANK2 in the brain. On the behavioral level, these mice display hyperactivity, increased stereotypic and abnormal social behaviors, and cognitive impairment. Pro-inflammatory factors and zinc-signaling alterations converge on the synaptic level revealing a common pathomechanism that may mechanistically explain a large share of ASD cases. Version of record
Databáze: OpenAIRE