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Human Retinal Transmitochondrial Cybrids with J or H mtDNA Haplogroups Respond Differently to Ultraviolet Radiation: Implications for Retinal Diseases

BACKGROUND: It has been recognized that cells do not respond equally to ultraviolet (UV) radiation but it is not clear whether this is due to genetic, biochemical or structural differences of the cells. We have a novel cybrid (cytoplasmic hybrids) model that allows us to analyze the contribution of...

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Autores principales: Malik, Deepika, Hsu, Tiffany, Falatoonzadeh, Payam, Cáceres-del-Carpio, Javier, Tarek, Mohamed, Chwa, Marilyn, Atilano, Shari R., Ramirez, Claudio, Nesburn, Anthony B., Boyer, David S., Kuppermann, Baruch D., Jazwinski, S. Michal, Miceli, Michael V., Wallace, Douglas C., Udar, Nitin, Kenney, M. Cristina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4053329/
https://www.ncbi.nlm.nih.gov/pubmed/24919117
http://dx.doi.org/10.1371/journal.pone.0099003
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author Malik, Deepika
Hsu, Tiffany
Falatoonzadeh, Payam
Cáceres-del-Carpio, Javier
Tarek, Mohamed
Chwa, Marilyn
Atilano, Shari R.
Ramirez, Claudio
Nesburn, Anthony B.
Boyer, David S.
Kuppermann, Baruch D.
Jazwinski, S. Michal
Miceli, Michael V.
Wallace, Douglas C.
Udar, Nitin
Kenney, M. Cristina
author_facet Malik, Deepika
Hsu, Tiffany
Falatoonzadeh, Payam
Cáceres-del-Carpio, Javier
Tarek, Mohamed
Chwa, Marilyn
Atilano, Shari R.
Ramirez, Claudio
Nesburn, Anthony B.
Boyer, David S.
Kuppermann, Baruch D.
Jazwinski, S. Michal
Miceli, Michael V.
Wallace, Douglas C.
Udar, Nitin
Kenney, M. Cristina
author_sort Malik, Deepika
collection PubMed
description BACKGROUND: It has been recognized that cells do not respond equally to ultraviolet (UV) radiation but it is not clear whether this is due to genetic, biochemical or structural differences of the cells. We have a novel cybrid (cytoplasmic hybrids) model that allows us to analyze the contribution of mitochondrial DNA (mtDNA) to cellular response after exposure to sub-lethal dose of UV. mtDNA can be classified into haplogroups as defined by accumulations of specific single nucleotide polymorphisms (SNPs). Recent studies have shown that J haplogroup is high risk for age-related macular degeneration while the H haplogroup is protective. This study investigates gene expression responses in J cybrids versus H cybrids after exposure to sub-lethal doses of UV-radiation. METHODOLOGY/PRINCIPAL FINDINGS: Cybrids were created by fusing platelets isolated from subjects with either H (n = 3) or J (n = 3) haplogroups with mitochondria-free (Rho(0)) ARPE-19 cells. The H and J cybrids were cultured for 24 hours, treated with 10 mJ of UV-radiation and cultured for an additional 120 hours. Untreated and treated cybrids were analyzed for growth rates and gene expression profiles. The UV-treated and untreated J cybrids had higher growth rates compared to H cybrids. Before treatment, J cybrids showed lower expression levels for CFH, CD55, IL-33, TGF-A, EFEMP-1, RARA, BCL2L13 and BBC3. At 120 hours after UV-treatment, the J cybrids had decreased CFH, RARA and BBC3 levels but increased CD55, IL-33 and EFEMP-1 compared to UV-treated H cybrids. CONCLUSION/SIGNIFICANCE: In cells with identical nuclei, the cellular response to sub-lethal UV-radiation is mediated in part by the mtDNA haplogroup. This supports the hypothesis that differences in growth rates and expression levels of complement, inflammation and apoptosis genes may result from population-specific, hereditary SNP variations in mtDNA. Therefore, when analyzing UV-induced damage in tissues, the mtDNA haplogroup background may be important to consider.
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spelling pubmed-40533292014-06-18 Human Retinal Transmitochondrial Cybrids with J or H mtDNA Haplogroups Respond Differently to Ultraviolet Radiation: Implications for Retinal Diseases Malik, Deepika Hsu, Tiffany Falatoonzadeh, Payam Cáceres-del-Carpio, Javier Tarek, Mohamed Chwa, Marilyn Atilano, Shari R. Ramirez, Claudio Nesburn, Anthony B. Boyer, David S. Kuppermann, Baruch D. Jazwinski, S. Michal Miceli, Michael V. Wallace, Douglas C. Udar, Nitin Kenney, M. Cristina PLoS One Research Article BACKGROUND: It has been recognized that cells do not respond equally to ultraviolet (UV) radiation but it is not clear whether this is due to genetic, biochemical or structural differences of the cells. We have a novel cybrid (cytoplasmic hybrids) model that allows us to analyze the contribution of mitochondrial DNA (mtDNA) to cellular response after exposure to sub-lethal dose of UV. mtDNA can be classified into haplogroups as defined by accumulations of specific single nucleotide polymorphisms (SNPs). Recent studies have shown that J haplogroup is high risk for age-related macular degeneration while the H haplogroup is protective. This study investigates gene expression responses in J cybrids versus H cybrids after exposure to sub-lethal doses of UV-radiation. METHODOLOGY/PRINCIPAL FINDINGS: Cybrids were created by fusing platelets isolated from subjects with either H (n = 3) or J (n = 3) haplogroups with mitochondria-free (Rho(0)) ARPE-19 cells. The H and J cybrids were cultured for 24 hours, treated with 10 mJ of UV-radiation and cultured for an additional 120 hours. Untreated and treated cybrids were analyzed for growth rates and gene expression profiles. The UV-treated and untreated J cybrids had higher growth rates compared to H cybrids. Before treatment, J cybrids showed lower expression levels for CFH, CD55, IL-33, TGF-A, EFEMP-1, RARA, BCL2L13 and BBC3. At 120 hours after UV-treatment, the J cybrids had decreased CFH, RARA and BBC3 levels but increased CD55, IL-33 and EFEMP-1 compared to UV-treated H cybrids. CONCLUSION/SIGNIFICANCE: In cells with identical nuclei, the cellular response to sub-lethal UV-radiation is mediated in part by the mtDNA haplogroup. This supports the hypothesis that differences in growth rates and expression levels of complement, inflammation and apoptosis genes may result from population-specific, hereditary SNP variations in mtDNA. Therefore, when analyzing UV-induced damage in tissues, the mtDNA haplogroup background may be important to consider. Public Library of Science 2014-06-11 /pmc/articles/PMC4053329/ /pubmed/24919117 http://dx.doi.org/10.1371/journal.pone.0099003 Text en © 2014 Malik 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
Malik, Deepika
Hsu, Tiffany
Falatoonzadeh, Payam
Cáceres-del-Carpio, Javier
Tarek, Mohamed
Chwa, Marilyn
Atilano, Shari R.
Ramirez, Claudio
Nesburn, Anthony B.
Boyer, David S.
Kuppermann, Baruch D.
Jazwinski, S. Michal
Miceli, Michael V.
Wallace, Douglas C.
Udar, Nitin
Kenney, M. Cristina
Human Retinal Transmitochondrial Cybrids with J or H mtDNA Haplogroups Respond Differently to Ultraviolet Radiation: Implications for Retinal Diseases
title Human Retinal Transmitochondrial Cybrids with J or H mtDNA Haplogroups Respond Differently to Ultraviolet Radiation: Implications for Retinal Diseases
title_full Human Retinal Transmitochondrial Cybrids with J or H mtDNA Haplogroups Respond Differently to Ultraviolet Radiation: Implications for Retinal Diseases
title_fullStr Human Retinal Transmitochondrial Cybrids with J or H mtDNA Haplogroups Respond Differently to Ultraviolet Radiation: Implications for Retinal Diseases
title_full_unstemmed Human Retinal Transmitochondrial Cybrids with J or H mtDNA Haplogroups Respond Differently to Ultraviolet Radiation: Implications for Retinal Diseases
title_short Human Retinal Transmitochondrial Cybrids with J or H mtDNA Haplogroups Respond Differently to Ultraviolet Radiation: Implications for Retinal Diseases
title_sort human retinal transmitochondrial cybrids with j or h mtdna haplogroups respond differently to ultraviolet radiation: implications for retinal diseases
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4053329/
https://www.ncbi.nlm.nih.gov/pubmed/24919117
http://dx.doi.org/10.1371/journal.pone.0099003
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