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Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference

RNAi screens have, to date, identified many genes required for mitotic divisions of Drosophila tissue culture cells. However, the inventory of such genes remains incomplete. We have combined the powers of bioinformatics and RNAi technology to detect novel mitotic genes. We found that Drosophila gene...

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Autores principales: Somma, Maria Patrizia, Ceprani, Francesca, Bucciarelli, Elisabetta, Naim, Valeria, De Arcangelis, Valeria, Piergentili, Roberto, Palena, Antonella, Ciapponi, Laura, Giansanti, Maria Grazia, Pellacani, Claudia, Petrucci, Romano, Cenci, Giovanni, Vernì, Fiammetta, Fasulo, Barbara, Goldberg, Michael L., Di Cunto, Ferdinando, Gatti, Maurizio
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2008
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2537813/
https://www.ncbi.nlm.nih.gov/pubmed/18797514
http://dx.doi.org/10.1371/journal.pgen.1000126
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author Somma, Maria Patrizia
Ceprani, Francesca
Bucciarelli, Elisabetta
Naim, Valeria
De Arcangelis, Valeria
Piergentili, Roberto
Palena, Antonella
Ciapponi, Laura
Giansanti, Maria Grazia
Pellacani, Claudia
Petrucci, Romano
Cenci, Giovanni
Vernì, Fiammetta
Fasulo, Barbara
Goldberg, Michael L.
Di Cunto, Ferdinando
Gatti, Maurizio
author_facet Somma, Maria Patrizia
Ceprani, Francesca
Bucciarelli, Elisabetta
Naim, Valeria
De Arcangelis, Valeria
Piergentili, Roberto
Palena, Antonella
Ciapponi, Laura
Giansanti, Maria Grazia
Pellacani, Claudia
Petrucci, Romano
Cenci, Giovanni
Vernì, Fiammetta
Fasulo, Barbara
Goldberg, Michael L.
Di Cunto, Ferdinando
Gatti, Maurizio
author_sort Somma, Maria Patrizia
collection PubMed
description RNAi screens have, to date, identified many genes required for mitotic divisions of Drosophila tissue culture cells. However, the inventory of such genes remains incomplete. We have combined the powers of bioinformatics and RNAi technology to detect novel mitotic genes. We found that Drosophila genes involved in mitosis tend to be transcriptionally co-expressed. We thus constructed a co-expression–based list of 1,000 genes that are highly enriched in mitotic functions, and we performed RNAi for each of these genes. By limiting the number of genes to be examined, we were able to perform a very detailed phenotypic analysis of RNAi cells. We examined dsRNA-treated cells for possible abnormalities in both chromosome structure and spindle organization. This analysis allowed the identification of 142 mitotic genes, which were subdivided into 18 phenoclusters. Seventy of these genes have not previously been associated with mitotic defects; 30 of them are required for spindle assembly and/or chromosome segregation, and 40 are required to prevent spontaneous chromosome breakage. We note that the latter type of genes has never been detected in previous RNAi screens in any system. Finally, we found that RNAi against genes encoding kinetochore components or highly conserved splicing factors results in identical defects in chromosome segregation, highlighting an unanticipated role of splicing factors in centromere function. These findings indicate that our co-expression–based method for the detection of mitotic functions works remarkably well. We can foresee that elaboration of co-expression lists using genes in the same phenocluster will provide many candidate genes for small-scale RNAi screens aimed at completing the inventory of mitotic proteins.
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spelling pubmed-25378132008-09-17 Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference Somma, Maria Patrizia Ceprani, Francesca Bucciarelli, Elisabetta Naim, Valeria De Arcangelis, Valeria Piergentili, Roberto Palena, Antonella Ciapponi, Laura Giansanti, Maria Grazia Pellacani, Claudia Petrucci, Romano Cenci, Giovanni Vernì, Fiammetta Fasulo, Barbara Goldberg, Michael L. Di Cunto, Ferdinando Gatti, Maurizio PLoS Genet Research Article RNAi screens have, to date, identified many genes required for mitotic divisions of Drosophila tissue culture cells. However, the inventory of such genes remains incomplete. We have combined the powers of bioinformatics and RNAi technology to detect novel mitotic genes. We found that Drosophila genes involved in mitosis tend to be transcriptionally co-expressed. We thus constructed a co-expression–based list of 1,000 genes that are highly enriched in mitotic functions, and we performed RNAi for each of these genes. By limiting the number of genes to be examined, we were able to perform a very detailed phenotypic analysis of RNAi cells. We examined dsRNA-treated cells for possible abnormalities in both chromosome structure and spindle organization. This analysis allowed the identification of 142 mitotic genes, which were subdivided into 18 phenoclusters. Seventy of these genes have not previously been associated with mitotic defects; 30 of them are required for spindle assembly and/or chromosome segregation, and 40 are required to prevent spontaneous chromosome breakage. We note that the latter type of genes has never been detected in previous RNAi screens in any system. Finally, we found that RNAi against genes encoding kinetochore components or highly conserved splicing factors results in identical defects in chromosome segregation, highlighting an unanticipated role of splicing factors in centromere function. These findings indicate that our co-expression–based method for the detection of mitotic functions works remarkably well. We can foresee that elaboration of co-expression lists using genes in the same phenocluster will provide many candidate genes for small-scale RNAi screens aimed at completing the inventory of mitotic proteins. Public Library of Science 2008-07-18 /pmc/articles/PMC2537813/ /pubmed/18797514 http://dx.doi.org/10.1371/journal.pgen.1000126 Text en Somma et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Somma, Maria Patrizia
Ceprani, Francesca
Bucciarelli, Elisabetta
Naim, Valeria
De Arcangelis, Valeria
Piergentili, Roberto
Palena, Antonella
Ciapponi, Laura
Giansanti, Maria Grazia
Pellacani, Claudia
Petrucci, Romano
Cenci, Giovanni
Vernì, Fiammetta
Fasulo, Barbara
Goldberg, Michael L.
Di Cunto, Ferdinando
Gatti, Maurizio
Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference
title Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference
title_full Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference
title_fullStr Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference
title_full_unstemmed Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference
title_short Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference
title_sort identification of drosophila mitotic genes by combining co-expression analysis and rna interference
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2537813/
https://www.ncbi.nlm.nih.gov/pubmed/18797514
http://dx.doi.org/10.1371/journal.pgen.1000126
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