Mitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescence

Ageing is a risk factor for the development of cardiovascular disease. In particular, senescent vascular smooth muscle cells (VSMCs) have been observed within atherosclerotic plaques. Oxidants are widely implicated in vascular ageing and cardiovascular disease with evidence of oxidative stress in ce...

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Main Author: Sanusi, Morufat Olayide Abisola
Other Authors: Herbert, Karl ; Goodall, Alison
Published: University of Leicester 2016
Online Access:http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.692499
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spelling ndltd-bl.uk-oai-ethos.bl.uk-6924992017-08-30T03:23:27ZMitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescenceSanusi, Morufat Olayide AbisolaHerbert, Karl ; Goodall, Alison2016Ageing is a risk factor for the development of cardiovascular disease. In particular, senescent vascular smooth muscle cells (VSMCs) have been observed within atherosclerotic plaques. Oxidants are widely implicated in vascular ageing and cardiovascular disease with evidence of oxidative stress in cells undergoing senescence. Our previous data showed that Angiotensin II caused stress induced premature senescence (SIPS) in primary human VSMC via oxidant generation. Prevention of senescence with a mitochondria targeted antioxidant, Mito-TEMPO, suggested the mechanism was dependent on mitochondrial superoxide. The current study aimed to investigate if modulation of mitochondrial reactive oxygen species signalling is a general mechanism for senescence induction in human VSMC. The electron transport chain inhibitors Antimycin A and rotenone and the mitochondrial redox cycler, MitoParaquat all stimulated SIPS in VSMC. Interestingly, Antimycin A and rotenone also lead to a reduction in overall H₂O₂ levels suggesting a possible protective mechanism and highlighting the complexity of the signalling mechanism involving mitochondrial oxidants. qPCR Analysis suggested that changes in antioxidant gene expression do not account for the reduction in peroxide levels. Although there was no evidence that Angiotensin II induced senescence in human coronary artery SMC, there was evidence for enhanced mitochondrial hydrogen peroxide production. Senescent cells acquire a senescence associated secretory phenotype (SASP). To determine the composition of VSMC SASP, the tryptically digested secretome of conditioned media was analysed by LC-MS/MS. Bioinformatic analysis identified the NRF2-mediated oxidative stress response pathway and several endogenous antioxidants as amongst the affected responses in the aged VSMC secretome. These new data suggest that senescent VSMC produce a SASP that has multiple effects on neighbouring cell types including the induction of cell senescence and death; but also elements that might serve to preserve cell integrity and function and may limit the expression of a pro-inflammatory phenotype.University of Leicesterhttp://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.692499http://hdl.handle.net/2381/37968Electronic Thesis or Dissertation
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description Ageing is a risk factor for the development of cardiovascular disease. In particular, senescent vascular smooth muscle cells (VSMCs) have been observed within atherosclerotic plaques. Oxidants are widely implicated in vascular ageing and cardiovascular disease with evidence of oxidative stress in cells undergoing senescence. Our previous data showed that Angiotensin II caused stress induced premature senescence (SIPS) in primary human VSMC via oxidant generation. Prevention of senescence with a mitochondria targeted antioxidant, Mito-TEMPO, suggested the mechanism was dependent on mitochondrial superoxide. The current study aimed to investigate if modulation of mitochondrial reactive oxygen species signalling is a general mechanism for senescence induction in human VSMC. The electron transport chain inhibitors Antimycin A and rotenone and the mitochondrial redox cycler, MitoParaquat all stimulated SIPS in VSMC. Interestingly, Antimycin A and rotenone also lead to a reduction in overall H₂O₂ levels suggesting a possible protective mechanism and highlighting the complexity of the signalling mechanism involving mitochondrial oxidants. qPCR Analysis suggested that changes in antioxidant gene expression do not account for the reduction in peroxide levels. Although there was no evidence that Angiotensin II induced senescence in human coronary artery SMC, there was evidence for enhanced mitochondrial hydrogen peroxide production. Senescent cells acquire a senescence associated secretory phenotype (SASP). To determine the composition of VSMC SASP, the tryptically digested secretome of conditioned media was analysed by LC-MS/MS. Bioinformatic analysis identified the NRF2-mediated oxidative stress response pathway and several endogenous antioxidants as amongst the affected responses in the aged VSMC secretome. These new data suggest that senescent VSMC produce a SASP that has multiple effects on neighbouring cell types including the induction of cell senescence and death; but also elements that might serve to preserve cell integrity and function and may limit the expression of a pro-inflammatory phenotype.
author2 Herbert, Karl ; Goodall, Alison
author_facet Herbert, Karl ; Goodall, Alison
Sanusi, Morufat Olayide Abisola
author Sanusi, Morufat Olayide Abisola
spellingShingle Sanusi, Morufat Olayide Abisola
Mitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescence
author_sort Sanusi, Morufat Olayide Abisola
title Mitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescence
title_short Mitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescence
title_full Mitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescence
title_fullStr Mitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescence
title_full_unstemmed Mitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescence
title_sort mitochondrial reactive oxygen species signalling and vascular smooth muscle cell senescence
publisher University of Leicester
publishDate 2016
url http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.692499
work_keys_str_mv AT sanusimorufatolayideabisola mitochondrialreactiveoxygenspeciessignallingandvascularsmoothmusclecellsenescence
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