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LA UDES PUBLICA
Fecha de publicación:
2023-10-01
Tipo:
Article
Número de artículo:
2677
Identificación:
SCOPUS_ID:85175491542
eID:
2-s2.0-85175491542
Nombre de la revista:
Biomedicines
Título del artículo:

Extrapyramidal Side Effects with Chronic Atypical Antipsychotic Can Be Predicted by Labeling Pattern of FosB and phosphoThr34-DARPP-32 in Nucleus Accumbens

Extrapyramidal side effects (EPS) can be induced by neuroleptics that regulate the expression of transcription factor FosB and dopaminergic mediator DARPP-32 in the striatum. However, the long-term neurobiological changes in striatal projection neurons resulting from a cumulative dosage of typical and atypical antipsychotics are poorly understood. The present study aimed to determine the differential and long-lasting changes in FosB distribution and DARPP-32 phosphorylation in the striatum and nucleus accumbens (NAc) associated with chronic antipsychotic-induced EPS. Male C57Bl/6J mice received daily injections of Olanzapine (Olz, 15 mg/kg), Clozapine (Clz, 20 mg/kg), or Haloperidol (Hal, 1 mg/kg), for a period of 11 weeks with a 4-day withdrawal period before the last dosage. Catalepsy for detection of EPS, along with open-field and rotarod tests, were assessed as behavioral correlates of motor responses. Additionally, FosB and phosphorylated-DARPP-32 immunohistochemistry were examined in striatal regions after treatment. All antipsychotics produced catalepsy and reduced open-field exploration, such as impaired rota-rod performance after Olz and Hal. The washout period was critical for Clz-induced side effects reduction. Both Olz and Clz increased FosB in NAc Shell-region, and phosphoThr34-DARPP-32 in NAc. Only Clz reduced phosphoThr75-DARPP-32 in the dorsal striatum and showed FosB/phosphoThr34-Darpp-32-ir in the NAc Core region. This study provides evidence that atypical antipsychotics such as Olz and Clz also give rise to EPS effects frequently associated with a cumulative dosage of typical neuroleptics such as Hal. Nevertheless, FosB/phosphoThr34-Darpp-32-ir in the NAc Core region is associated with hypokinetic movements inhibition.

Autor(es) UDES:
Echeverry M.B.
Otros Autores:
Prieto S.G., Almeida M.C., Silva J.C.S., Del-Bel E.
Autor Principal:
Prieto S.G.
Áreas del conocimiento:
Medicine (miscellaneous), Biochemistry, Genetics and Molecular Biology (all)
Acerca de la revista donde se publicó este artículo:

Biomedicines

Cuartil Q1
Ranking
5011
Tipo
Journal
eISSN
22279059
Región
Western Europe
País
Switzerland
Volumen
11
Cobertura
2013-2022
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