Identification of Novel Fibrosis Modifiers by In Vivo siRNA Silencing

Fibrotic diseases contribute to 45% of deaths in the industrialized world, and therefore a better understanding of the pathophysiological mechanisms underlying tissue fibrosis is sorely needed. We aimed to identify novel modifiers of tissue fibrosis expressed by myofibroblasts and their progenitors...

Descripción completa

Detalles Bibliográficos
Autores principales: Vollmann, Elisabeth H., Cao, Lizhi, Amatucci, Aldo, Reynolds, Taylor, Hamann, Stefan, Dalkilic-Liddle, Isin, Cameron, Thomas O., Hossbach, Markus, Kauffman, Kevin J., Mir, Faryal F., Anderson, Daniel G., Novobrantseva, Tatiana, Koteliansky, Victor, Kisseleva, Tatiana, Brenner, David, Duffield, Jeremy, Burkly, Linda C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society of Gene & Cell Therapy 2017
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5424569/
https://www.ncbi.nlm.nih.gov/pubmed/28624207
http://dx.doi.org/10.1016/j.omtn.2017.04.014
_version_ 1783235156336705536
author Vollmann, Elisabeth H.
Cao, Lizhi
Amatucci, Aldo
Reynolds, Taylor
Hamann, Stefan
Dalkilic-Liddle, Isin
Cameron, Thomas O.
Hossbach, Markus
Kauffman, Kevin J.
Mir, Faryal F.
Anderson, Daniel G.
Novobrantseva, Tatiana
Koteliansky, Victor
Kisseleva, Tatiana
Brenner, David
Duffield, Jeremy
Burkly, Linda C.
author_facet Vollmann, Elisabeth H.
Cao, Lizhi
Amatucci, Aldo
Reynolds, Taylor
Hamann, Stefan
Dalkilic-Liddle, Isin
Cameron, Thomas O.
Hossbach, Markus
Kauffman, Kevin J.
Mir, Faryal F.
Anderson, Daniel G.
Novobrantseva, Tatiana
Koteliansky, Victor
Kisseleva, Tatiana
Brenner, David
Duffield, Jeremy
Burkly, Linda C.
author_sort Vollmann, Elisabeth H.
collection PubMed
description Fibrotic diseases contribute to 45% of deaths in the industrialized world, and therefore a better understanding of the pathophysiological mechanisms underlying tissue fibrosis is sorely needed. We aimed to identify novel modifiers of tissue fibrosis expressed by myofibroblasts and their progenitors in their disease microenvironment through RNA silencing in vivo. We leveraged novel biology, targeting genes upregulated during liver and kidney fibrosis in this cell lineage, and employed small interfering RNA (siRNA)-formulated lipid nanoparticles technology to silence these genes in carbon-tetrachloride-induced liver fibrosis in mice. We identified five genes, Egr2, Atp1a2, Fkbp10, Fstl1, and Has2, which modified fibrogenesis based on their silencing, resulting in reduced Col1a1 mRNA levels and collagen accumulation in the liver. These genes fell into different groups based on the effects of their silencing on a transcriptional mini-array and histological outcomes. Silencing of Egr2 had the broadest effects in vivo and also reduced fibrogenic gene expression in a human fibroblast cell line. Prior to our study, Egr2, Atp1a2, and Fkbp10 had not been functionally validated in fibrosis in vivo. Thus, our results provide a major advance over the existing knowledge of fibrogenic pathways. Our study is the first example of a targeted siRNA assay to identify novel fibrosis modifiers in vivo.
format Online
Article
Text
id pubmed-5424569
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher American Society of Gene & Cell Therapy
record_format MEDLINE/PubMed
spelling pubmed-54245692017-05-11 Identification of Novel Fibrosis Modifiers by In Vivo siRNA Silencing Vollmann, Elisabeth H. Cao, Lizhi Amatucci, Aldo Reynolds, Taylor Hamann, Stefan Dalkilic-Liddle, Isin Cameron, Thomas O. Hossbach, Markus Kauffman, Kevin J. Mir, Faryal F. Anderson, Daniel G. Novobrantseva, Tatiana Koteliansky, Victor Kisseleva, Tatiana Brenner, David Duffield, Jeremy Burkly, Linda C. Mol Ther Nucleic Acids Original Article Fibrotic diseases contribute to 45% of deaths in the industrialized world, and therefore a better understanding of the pathophysiological mechanisms underlying tissue fibrosis is sorely needed. We aimed to identify novel modifiers of tissue fibrosis expressed by myofibroblasts and their progenitors in their disease microenvironment through RNA silencing in vivo. We leveraged novel biology, targeting genes upregulated during liver and kidney fibrosis in this cell lineage, and employed small interfering RNA (siRNA)-formulated lipid nanoparticles technology to silence these genes in carbon-tetrachloride-induced liver fibrosis in mice. We identified five genes, Egr2, Atp1a2, Fkbp10, Fstl1, and Has2, which modified fibrogenesis based on their silencing, resulting in reduced Col1a1 mRNA levels and collagen accumulation in the liver. These genes fell into different groups based on the effects of their silencing on a transcriptional mini-array and histological outcomes. Silencing of Egr2 had the broadest effects in vivo and also reduced fibrogenic gene expression in a human fibroblast cell line. Prior to our study, Egr2, Atp1a2, and Fkbp10 had not been functionally validated in fibrosis in vivo. Thus, our results provide a major advance over the existing knowledge of fibrogenic pathways. Our study is the first example of a targeted siRNA assay to identify novel fibrosis modifiers in vivo. American Society of Gene & Cell Therapy 2017-04-20 /pmc/articles/PMC5424569/ /pubmed/28624207 http://dx.doi.org/10.1016/j.omtn.2017.04.014 Text en © 2017 The Author(s) http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Article
Vollmann, Elisabeth H.
Cao, Lizhi
Amatucci, Aldo
Reynolds, Taylor
Hamann, Stefan
Dalkilic-Liddle, Isin
Cameron, Thomas O.
Hossbach, Markus
Kauffman, Kevin J.
Mir, Faryal F.
Anderson, Daniel G.
Novobrantseva, Tatiana
Koteliansky, Victor
Kisseleva, Tatiana
Brenner, David
Duffield, Jeremy
Burkly, Linda C.
Identification of Novel Fibrosis Modifiers by In Vivo siRNA Silencing
title Identification of Novel Fibrosis Modifiers by In Vivo siRNA Silencing
title_full Identification of Novel Fibrosis Modifiers by In Vivo siRNA Silencing
title_fullStr Identification of Novel Fibrosis Modifiers by In Vivo siRNA Silencing
title_full_unstemmed Identification of Novel Fibrosis Modifiers by In Vivo siRNA Silencing
title_short Identification of Novel Fibrosis Modifiers by In Vivo siRNA Silencing
title_sort identification of novel fibrosis modifiers by in vivo sirna silencing
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5424569/
https://www.ncbi.nlm.nih.gov/pubmed/28624207
http://dx.doi.org/10.1016/j.omtn.2017.04.014
work_keys_str_mv AT vollmannelisabethh identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT caolizhi identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT amatuccialdo identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT reynoldstaylor identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT hamannstefan identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT dalkilicliddleisin identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT cameronthomaso identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT hossbachmarkus identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT kauffmankevinj identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT mirfaryalf identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT andersondanielg identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT novobrantsevatatiana identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT kotelianskyvictor identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT kisselevatatiana identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT brennerdavid identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT duffieldjeremy identificationofnovelfibrosismodifiersbyinvivosirnasilencing
AT burklylindac identificationofnovelfibrosismodifiersbyinvivosirnasilencing

Ejemplares similares