Publications by authors named "E Gomez-G de la Pedrosa"

Introduction: Acute onset of severe psychiatric symptoms or regression may occur in children with premorbid neurodevelopmental disorders, although typically developing children can also be affected. Infections or other stressors are likely triggers. The underlying causes are unclear, but a current hypothesis suggests the convergence of genes that influence neuronal and immunological function.

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Article Synopsis
  • The study looked at how many people got hospital treatment for a type of surgery called sympathectomy in Brazil from 2014 to 2023.
  • It found that fewer people were having these surgeries over the years and that video-assisted surgeries were more common for chest operations but less for lower back ones.
  • Even though video-assisted surgeries were safer, many still chose the older open surgery method, especially for lower back surgeries.
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More than 100 genes have been associated with significantly increased risks of autism spectrum disorders (ASD) with an estimate of ∼1000 genes that may contribute. The new challenge is to investigate the molecular and cellular functions of these genes during neural and brain development, and then even more challenging, to link the altered molecular and cellular phenotypes to the ASD clinical manifestations. In this study, we used single-cell RNA-seq analysis to study one of the top risk genes, , in cerebral organoids, which models early neural development.

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Infective second-stage juveniles (J2) of spp. migrate towards host roots, which depends on several factors, including root exudates and soil temperature. Although is a highly virulent nematode that affects major agricultural crops worldwide, there is limited ecological data about it.

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Genes encoding the KDM5 family of transcriptional regulators are disrupted in individuals with intellectual disability (ID). To understand the link between KDM5 and ID, we characterized five Drosophila strains harboring missense alleles analogous to those observed in patients. These alleles disrupted neuroanatomical development, cognition and other behaviors, and displayed a transcriptional signature characterized by the downregulation of many ribosomal protein genes.

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