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A portable BRCA1-HAC (human artificial chromosome) module for analysis of BRCA1 tumor suppressor function

BRCA1 is involved in many disparate cellular functions, including DNA damage repair, cell-cycle checkpoint activation, gene transcriptional regulation, DNA replication, centrosome function and others. The majority of evidence strongly favors the maintenance of genomic integrity as a principal tumor...

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Autores principales: Kononenko, Artem V., Bansal, Ruchi, Lee, Nicholas C.O., Grimes, Brenda R., Masumoto, Hiroshi, Earnshaw, William C., Larionov, Vladimir, Kouprina, Natalay
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4245969/
https://www.ncbi.nlm.nih.gov/pubmed/25260588
http://dx.doi.org/10.1093/nar/gku870
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author Kononenko, Artem V.
Bansal, Ruchi
Lee, Nicholas C.O.
Grimes, Brenda R.
Masumoto, Hiroshi
Earnshaw, William C.
Larionov, Vladimir
Kouprina, Natalay
author_facet Kononenko, Artem V.
Bansal, Ruchi
Lee, Nicholas C.O.
Grimes, Brenda R.
Masumoto, Hiroshi
Earnshaw, William C.
Larionov, Vladimir
Kouprina, Natalay
author_sort Kononenko, Artem V.
collection PubMed
description BRCA1 is involved in many disparate cellular functions, including DNA damage repair, cell-cycle checkpoint activation, gene transcriptional regulation, DNA replication, centrosome function and others. The majority of evidence strongly favors the maintenance of genomic integrity as a principal tumor suppressor activity of BRCA1. At the same time some functional aspects of BRCA1 are not fully understood. Here, a HAC (human artificial chromosome) module with a regulated centromere was constructed for delivery and expression of the 90 kb genomic copy of the BRCA1 gene into BRCA1-deficient human cells. A battery of functional tests was carried out to demonstrate functionality of the exogenous BRCA1. In separate experiments, we investigated the role of BRCA1 in maintenance of heterochromatin integrity within a human functional kinetochore. We demonstrated that BRCA1 deficiency results in a specific activation of transcription of higher-order alpha-satellite repeats (HORs) assembled into heterochromatin domains flanking the kinetochore. At the same time no detectable elevation of transcription was observed within HORs assembled into centrochromatin domains. Thus, we demonstrated a link between BRCA1 deficiency and kinetochore dysfunction and extended previous observations that BRCA1 is required to silence transcription in heterochromatin in specific genomic loci. This supports the hypothesis that epigenetic alterations of the kinetochore initiated in the absence of BRCA1 may contribute to cellular transformation.
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spelling pubmed-42459692015-03-17 A portable BRCA1-HAC (human artificial chromosome) module for analysis of BRCA1 tumor suppressor function Kononenko, Artem V. Bansal, Ruchi Lee, Nicholas C.O. Grimes, Brenda R. Masumoto, Hiroshi Earnshaw, William C. Larionov, Vladimir Kouprina, Natalay Nucleic Acids Res Methods Online BRCA1 is involved in many disparate cellular functions, including DNA damage repair, cell-cycle checkpoint activation, gene transcriptional regulation, DNA replication, centrosome function and others. The majority of evidence strongly favors the maintenance of genomic integrity as a principal tumor suppressor activity of BRCA1. At the same time some functional aspects of BRCA1 are not fully understood. Here, a HAC (human artificial chromosome) module with a regulated centromere was constructed for delivery and expression of the 90 kb genomic copy of the BRCA1 gene into BRCA1-deficient human cells. A battery of functional tests was carried out to demonstrate functionality of the exogenous BRCA1. In separate experiments, we investigated the role of BRCA1 in maintenance of heterochromatin integrity within a human functional kinetochore. We demonstrated that BRCA1 deficiency results in a specific activation of transcription of higher-order alpha-satellite repeats (HORs) assembled into heterochromatin domains flanking the kinetochore. At the same time no detectable elevation of transcription was observed within HORs assembled into centrochromatin domains. Thus, we demonstrated a link between BRCA1 deficiency and kinetochore dysfunction and extended previous observations that BRCA1 is required to silence transcription in heterochromatin in specific genomic loci. This supports the hypothesis that epigenetic alterations of the kinetochore initiated in the absence of BRCA1 may contribute to cellular transformation. Oxford University Press 2014-12-01 2014-09-26 /pmc/articles/PMC4245969/ /pubmed/25260588 http://dx.doi.org/10.1093/nar/gku870 Text en Published by Oxford University Press on behalf of Nucleic Acids Research 2014. This work is written by (a) US Government employee(s) and is in the public domain in the US.
spellingShingle Methods Online
Kononenko, Artem V.
Bansal, Ruchi
Lee, Nicholas C.O.
Grimes, Brenda R.
Masumoto, Hiroshi
Earnshaw, William C.
Larionov, Vladimir
Kouprina, Natalay
A portable BRCA1-HAC (human artificial chromosome) module for analysis of BRCA1 tumor suppressor function
title A portable BRCA1-HAC (human artificial chromosome) module for analysis of BRCA1 tumor suppressor function
title_full A portable BRCA1-HAC (human artificial chromosome) module for analysis of BRCA1 tumor suppressor function
title_fullStr A portable BRCA1-HAC (human artificial chromosome) module for analysis of BRCA1 tumor suppressor function
title_full_unstemmed A portable BRCA1-HAC (human artificial chromosome) module for analysis of BRCA1 tumor suppressor function
title_short A portable BRCA1-HAC (human artificial chromosome) module for analysis of BRCA1 tumor suppressor function
title_sort portable brca1-hac (human artificial chromosome) module for analysis of brca1 tumor suppressor function
topic Methods Online
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4245969/
https://www.ncbi.nlm.nih.gov/pubmed/25260588
http://dx.doi.org/10.1093/nar/gku870
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