Cargando…
Transcriptome-wide co-expression analysis identifies LRRC2 as a novel mediator of mitochondrial and cardiac function
Mitochondrial dysfunction contributes to myriad monogenic and complex pathologies. To understand the underlying mechanisms, it is essential to define the full complement of proteins that modulate mitochondrial function. To identify such proteins, we performed a meta-analysis of publicly available ge...
| Autores principales: | , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Public Library of Science
2017
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5291451/ https://www.ncbi.nlm.nih.gov/pubmed/28158196 http://dx.doi.org/10.1371/journal.pone.0170458 |
| _version_ | 1782504782380924928 |
|---|---|
| author | McDermott-Roe, Chris Leleu, Marion Rowe, Glenn C. Palygin, Oleg Bukowy, John D. Kuo, Judy Rech, Monika Hermans-Beijnsberger, Steffie Schaefer, Sebastian Adami, Eleonora Creemers, Esther E. Heinig, Matthias Schroen, Blanche Arany, Zoltan Petretto, Enrico Geurts, Aron M. |
| author_facet | McDermott-Roe, Chris Leleu, Marion Rowe, Glenn C. Palygin, Oleg Bukowy, John D. Kuo, Judy Rech, Monika Hermans-Beijnsberger, Steffie Schaefer, Sebastian Adami, Eleonora Creemers, Esther E. Heinig, Matthias Schroen, Blanche Arany, Zoltan Petretto, Enrico Geurts, Aron M. |
| author_sort | McDermott-Roe, Chris |
| collection | PubMed |
| description | Mitochondrial dysfunction contributes to myriad monogenic and complex pathologies. To understand the underlying mechanisms, it is essential to define the full complement of proteins that modulate mitochondrial function. To identify such proteins, we performed a meta-analysis of publicly available gene expression data. Gene co-expression analysis of a large and heterogeneous compendium of microarray data nominated a sub-population of transcripts that whilst highly correlated with known mitochondrial protein-encoding transcripts (MPETs), are not themselves recognized as generating proteins either localized to the mitochondrion or pertinent to functions therein. To focus the analysis on a medically-important condition with a strong yet incompletely understood mitochondrial component, candidates were cross-referenced with an MPET-enriched module independently generated via genome-wide co-expression network analysis of a human heart failure gene expression dataset. The strongest uncharacterized candidate in the analysis was Leucine Rich Repeat Containing 2 (LRRC2). LRRC2 was found to be localized to the mitochondria in human cells and transcriptionally-regulated by the mitochondrial master regulator Pgc-1α. We report that Lrrc2 transcript abundance correlates with that of β-MHC, a canonical marker of cardiac hypertrophy in humans and experimentally demonstrated an elevation in Lrrc2 transcript in in vitro and in vivo rodent models of cardiac hypertrophy as well as in patients with dilated cardiomyopathy. RNAi-mediated Lrrc2 knockdown in a rat-derived cardiomyocyte cell line resulted in enhanced expression of canonical hypertrophic biomarkers as well as increased mitochondrial mass in the context of increased Pgc-1α expression. In conclusion, our meta-analysis represents a simple yet powerful springboard for the nomination of putative mitochondrially-pertinent proteins relevant to cardiac function and enabled the identification of LRRC2 as a novel mitochondrially-relevant protein and regulator of the hypertrophic response. |
| format | Online Article Text |
| id | pubmed-5291451 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2017 |
| publisher | Public Library of Science |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-52914512017-02-17 Transcriptome-wide co-expression analysis identifies LRRC2 as a novel mediator of mitochondrial and cardiac function McDermott-Roe, Chris Leleu, Marion Rowe, Glenn C. Palygin, Oleg Bukowy, John D. Kuo, Judy Rech, Monika Hermans-Beijnsberger, Steffie Schaefer, Sebastian Adami, Eleonora Creemers, Esther E. Heinig, Matthias Schroen, Blanche Arany, Zoltan Petretto, Enrico Geurts, Aron M. PLoS One Research Article Mitochondrial dysfunction contributes to myriad monogenic and complex pathologies. To understand the underlying mechanisms, it is essential to define the full complement of proteins that modulate mitochondrial function. To identify such proteins, we performed a meta-analysis of publicly available gene expression data. Gene co-expression analysis of a large and heterogeneous compendium of microarray data nominated a sub-population of transcripts that whilst highly correlated with known mitochondrial protein-encoding transcripts (MPETs), are not themselves recognized as generating proteins either localized to the mitochondrion or pertinent to functions therein. To focus the analysis on a medically-important condition with a strong yet incompletely understood mitochondrial component, candidates were cross-referenced with an MPET-enriched module independently generated via genome-wide co-expression network analysis of a human heart failure gene expression dataset. The strongest uncharacterized candidate in the analysis was Leucine Rich Repeat Containing 2 (LRRC2). LRRC2 was found to be localized to the mitochondria in human cells and transcriptionally-regulated by the mitochondrial master regulator Pgc-1α. We report that Lrrc2 transcript abundance correlates with that of β-MHC, a canonical marker of cardiac hypertrophy in humans and experimentally demonstrated an elevation in Lrrc2 transcript in in vitro and in vivo rodent models of cardiac hypertrophy as well as in patients with dilated cardiomyopathy. RNAi-mediated Lrrc2 knockdown in a rat-derived cardiomyocyte cell line resulted in enhanced expression of canonical hypertrophic biomarkers as well as increased mitochondrial mass in the context of increased Pgc-1α expression. In conclusion, our meta-analysis represents a simple yet powerful springboard for the nomination of putative mitochondrially-pertinent proteins relevant to cardiac function and enabled the identification of LRRC2 as a novel mitochondrially-relevant protein and regulator of the hypertrophic response. Public Library of Science 2017-02-03 /pmc/articles/PMC5291451/ /pubmed/28158196 http://dx.doi.org/10.1371/journal.pone.0170458 Text en © 2017 McDermott-Roe 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. |
| spellingShingle | Research Article McDermott-Roe, Chris Leleu, Marion Rowe, Glenn C. Palygin, Oleg Bukowy, John D. Kuo, Judy Rech, Monika Hermans-Beijnsberger, Steffie Schaefer, Sebastian Adami, Eleonora Creemers, Esther E. Heinig, Matthias Schroen, Blanche Arany, Zoltan Petretto, Enrico Geurts, Aron M. Transcriptome-wide co-expression analysis identifies LRRC2 as a novel mediator of mitochondrial and cardiac function |
| title | Transcriptome-wide co-expression analysis identifies LRRC2 as a novel mediator of mitochondrial and cardiac function |
| title_full | Transcriptome-wide co-expression analysis identifies LRRC2 as a novel mediator of mitochondrial and cardiac function |
| title_fullStr | Transcriptome-wide co-expression analysis identifies LRRC2 as a novel mediator of mitochondrial and cardiac function |
| title_full_unstemmed | Transcriptome-wide co-expression analysis identifies LRRC2 as a novel mediator of mitochondrial and cardiac function |
| title_short | Transcriptome-wide co-expression analysis identifies LRRC2 as a novel mediator of mitochondrial and cardiac function |
| title_sort | transcriptome-wide co-expression analysis identifies lrrc2 as a novel mediator of mitochondrial and cardiac function |
| topic | Research Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5291451/ https://www.ncbi.nlm.nih.gov/pubmed/28158196 http://dx.doi.org/10.1371/journal.pone.0170458 |
| work_keys_str_mv | AT mcdermottroechris transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT leleumarion transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT roweglennc transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT palyginoleg transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT bukowyjohnd transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT kuojudy transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT rechmonika transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT hermansbeijnsbergersteffie transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT schaefersebastian transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT adamieleonora transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT creemersesthere transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT heinigmatthias transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT schroenblanche transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT aranyzoltan transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT petrettoenrico transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction AT geurtsaronm transcriptomewidecoexpressionanalysisidentifieslrrc2asanovelmediatorofmitochondrialandcardiacfunction |