SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2947885989> ?p ?o ?g. }

Showing items 1 to 100 of ±155 with 100 items per page.

W2947885989 endingPage "799" @default.
W2947885989 startingPage "784" @default.
W2947885989 abstract "An enigma in studies of neuropsychiatric disorders is how to translate polygenic risk into disease biology. For schizophrenia, where > 145 significant GWAS loci have been identified and only a few genes directly implicated, addressing this issue is a particular challenge. We used a combined cellomics and proteomics approach to show that polygenic risk can be disentangled by searching for shared neuronal morphology and cellular pathway phenotypes of candidate schizophrenia risk genes. We first performed an automated high-content cellular screen to characterize neuronal morphology phenotypes of 41 candidate schizophrenia risk genes. The transcription factors Tcf4 and Tbr1 and the RNA topoisomerase Top3b shared a neuronal phenotype marked by an early and progressive reduction in synapse numbers upon knockdown in mouse primary neuronal cultures. Proteomics analysis subsequently showed that these three genes converge onto the syntaxin-mediated neurotransmitter release pathway, which was previously implicated in schizophrenia, but for which genetic evidence was weak. We show that dysregulation of multiple proteins in this pathway may be due to the combined effects of schizophrenia risk genes Tcf4, Tbr1, and Top3b. Together, our data provide new biological functions for schizophrenia risk genes and support the idea that polygenic risk is the result of multiple small impacts on common neuronal signaling pathways." @default.
W2947885989 created "2019-06-07" @default.
W2947885989 creator A5010890182 @default.
W2947885989 creator A5031107150 @default.
W2947885989 creator A5037003034 @default.
W2947885989 creator A5041708405 @default.
W2947885989 creator A5046661343 @default.
W2947885989 creator A5052016436 @default.
W2947885989 creator A5059328206 @default.
W2947885989 creator A5061802355 @default.
W2947885989 creator A5078688258 @default.
W2947885989 date "2019-05-29" @default.
W2947885989 modified "2023-10-15" @default.
W2947885989 title "Combined cellomics and proteomics analysis reveals shared neuronal morphology and molecular pathway phenotypes for multiple schizophrenia risk genes" @default.
W2947885989 cites W1951724000 @default.
W2947885989 cites W1970654007 @default.
W2947885989 cites W1983194657 @default.
W2947885989 cites W1983241347 @default.
W2947885989 cites W1983719168 @default.
W2947885989 cites W1984940197 @default.
W2947885989 cites W1987336175 @default.
W2947885989 cites W1989596998 @default.
W2947885989 cites W2001275516 @default.
W2947885989 cites W2004341780 @default.
W2947885989 cites W2004575367 @default.
W2947885989 cites W2007731679 @default.
W2947885989 cites W2016532227 @default.
W2947885989 cites W2019761487 @default.
W2947885989 cites W2019799816 @default.
W2947885989 cites W2030430356 @default.
W2947885989 cites W2040863019 @default.
W2947885989 cites W2052326665 @default.
W2947885989 cites W2054091111 @default.
W2947885989 cites W2061608089 @default.
W2947885989 cites W2064234593 @default.
W2947885989 cites W2065909162 @default.
W2947885989 cites W2088067673 @default.
W2947885989 cites W2089216562 @default.
W2947885989 cites W2089397711 @default.
W2947885989 cites W2089927164 @default.
W2947885989 cites W2091446808 @default.
W2947885989 cites W2096173332 @default.
W2947885989 cites W2101357408 @default.
W2947885989 cites W2102722285 @default.
W2947885989 cites W2108329409 @default.
W2947885989 cites W2108994842 @default.
W2947885989 cites W2132244902 @default.
W2947885989 cites W2132297623 @default.
W2947885989 cites W2140484686 @default.
W2947885989 cites W2156548928 @default.
W2947885989 cites W2156825608 @default.
W2947885989 cites W2170349574 @default.
W2947885989 cites W2171063023 @default.
W2947885989 cites W2188528468 @default.
W2947885989 cites W2266116507 @default.
W2947885989 cites W2277462866 @default.
W2947885989 cites W2291183135 @default.
W2947885989 cites W2330845539 @default.
W2947885989 cites W2343234170 @default.
W2947885989 cites W2345884556 @default.
W2947885989 cites W2412282165 @default.
W2947885989 cites W2497081376 @default.
W2947885989 cites W2501689990 @default.
W2947885989 cites W2551102722 @default.
W2947885989 cites W2591119594 @default.
W2947885989 cites W2605379571 @default.
W2947885989 cites W2613466142 @default.
W2947885989 cites W2614844078 @default.
W2947885989 cites W2626815279 @default.
W2947885989 cites W2739134108 @default.
W2947885989 cites W2765389138 @default.
W2947885989 cites W2766489743 @default.
W2947885989 cites W2769377508 @default.
W2947885989 cites W2773146760 @default.
W2947885989 cites W2777388159 @default.
W2947885989 cites W2807744873 @default.
W2947885989 cites W2809398132 @default.
W2947885989 cites W2886690627 @default.
W2947885989 cites W2892227414 @default.
W2947885989 cites W2918086501 @default.
W2947885989 doi "https://doi.org/10.1038/s41380-019-0436-y" @default.
W2947885989 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/7910218" @default.
W2947885989 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31142819" @default.
W2947885989 hasPublicationYear "2019" @default.
W2947885989 type Work @default.
W2947885989 sameAs 2947885989 @default.
W2947885989 citedByCount "19" @default.
W2947885989 countsByYear W29478859892020 @default.
W2947885989 countsByYear W29478859892021 @default.
W2947885989 countsByYear W29478859892022 @default.
W2947885989 countsByYear W29478859892023 @default.
W2947885989 crossrefType "journal-article" @default.
W2947885989 hasAuthorship W2947885989A5010890182 @default.
W2947885989 hasAuthorship W2947885989A5031107150 @default.
W2947885989 hasAuthorship W2947885989A5037003034 @default.
W2947885989 hasAuthorship W2947885989A5041708405 @default.
W2947885989 hasAuthorship W2947885989A5046661343 @default.
W2947885989 hasAuthorship W2947885989A5052016436 @default.