2021
DOI: 10.1101/2021.10.11.21264848
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Molecular phenotypes associated with antipsychotic drugs in the human caudate nucleus

Abstract: Antipsychotic drugs are the current first-line of treatment for schizophrenia and other psychotic conditions. However, their molecular effects on the human brain are poorly studied, due to difficulty of tissue access and confounders associated with disease status. Here we examine differences in gene expression and DNA methylation associated with positive antipsychotic drug toxicology status in the human caudate nucleus. We find no genome-wide significant differences in DNA methylation, but abundant differences… Show more

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Cited by 2 publications
(3 citation statements)
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“…S1 and S4), imbalance of medication in the form of neuroleptic drugs could not be avoided, as the use of antipsychotics is standard among the schizophrenia patients and is not encountered in control individuals. To make sure that the patterns of DE are not associated with this medication regiment, we analyzed two bulk RNA datasets of the DLPFC: one large dataset consisting of ~150 human postmortem samples from antipsychotic-positive and antipsychotic-negative patients ( 44 ), and another consisting of ~35 rhesus macaque samples that were treated with the antipsychotic clozapine or haloperidol or with placebo ( 36 ). We overlapped human antipsychotic-associated or macaque drug treatment–associated DEGs with DEGs between control and schizophrenia samples either for all excitatory or inhibitory neurons or for each neuronal subtype in our dataset.…”
Section: Resultsmentioning
confidence: 99%
See 1 more Smart Citation
“…S1 and S4), imbalance of medication in the form of neuroleptic drugs could not be avoided, as the use of antipsychotics is standard among the schizophrenia patients and is not encountered in control individuals. To make sure that the patterns of DE are not associated with this medication regiment, we analyzed two bulk RNA datasets of the DLPFC: one large dataset consisting of ~150 human postmortem samples from antipsychotic-positive and antipsychotic-negative patients ( 44 ), and another consisting of ~35 rhesus macaque samples that were treated with the antipsychotic clozapine or haloperidol or with placebo ( 36 ). We overlapped human antipsychotic-associated or macaque drug treatment–associated DEGs with DEGs between control and schizophrenia samples either for all excitatory or inhibitory neurons or for each neuronal subtype in our dataset.…”
Section: Resultsmentioning
confidence: 99%
“…In addition, a list of DEGs was obtained from a human DLPFC antipsychotic dataset ( 44 ). DEGs were selected the same way as for the rhesus macaque dataset ( P < 0.05).…”
Section: Methodsmentioning
confidence: 99%
“…Additional File 2 shows how you can then load the outputs of BiocMAP and use the data with R and Bioconductor packages such as bsseq [10], ggplot2 [27], and GGally [28] to perform exploratory data analysis as well as downstream statistical analyses. In addition, development versions of BiocMAP were used in other peer reviewed publications [30, 31, 32] that have publicly available R code for several downstream analyses.…”
Section: Discussionmentioning
confidence: 99%