Cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / Norhafiza Razali
Glaucoma, a common cause of optic neuropathy, is associated with elevated intraocular pressure (IOP) and is the leading cause of irreversible visual disability. Steroid-induced glaucoma, a common type of secondary glaucoma, is also associated with elevated IOP (steroid-induced ocular hypertension (S...
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my-uitm-ir.185812022-03-08T07:31:40Z Cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / Norhafiza Razali 2016 Razali, Norhafiza Glaucoma, a common cause of optic neuropathy, is associated with elevated intraocular pressure (IOP) and is the leading cause of irreversible visual disability. Steroid-induced glaucoma, a common type of secondary glaucoma, is also associated with elevated IOP (steroid-induced ocular hypertension (SIOH)). SIOH and glaucoma are currently treated with antiglaucoma agents, which often have suboptimal efficacy and are associated with adverse effects. The objective of this study was to determine if topical application of /nms-resveratrol reduces IOP in rats with SIOH and to investigate its mechanisms of action. This study was divided into in vivo and in vitro studies. In the in vivo study, we evaluated the oculohypotensive effects of topical toms-resveratrol in normal and SIOH rats and investigated the role of adenosine receptors (ARs) and transforming growth factor-β (TGF-β) signalling in the IOP lowering effect of fnms-resveratrol. Involvement of AR was studied by observing the IOP changes in response to /rara-resveratrol after pre-treating SIOH animals with AR subtype-specific antagonists. The study also investigated phospholipase C (PLC) activation, extracellular regulated kinase 1/2 (ERK1/2) phosphorylation and increased matrix metalloproteinases (MMPs) secretion in the aqueous humour (AH) as mechanism of resveratrol-induced oculohypotension in SIOH rats. In vitro studies evaluated the effect of frans-resveratrol on cellular signalling pathways of ARs and TGF-β in primary human trabecular meshwork cells (HTMCs). Single drop of all concentrations of toms-resveratrol produced significant oculohypotension in normotensive rats and 0.2% concentration produced maximum IOP reduction. Twicedaily topical application of fnms-resveratrol 0.2% for 21-day in SIOH rats resulted in significant and sustained IOP reduction. This was associated with significantly higher AH MMP-2 level; significantly reduced trabecular meshwork (TM) thickness and increased number of TM cells. Treatment with /raws-resveratrol also significantly increased the ganglion cell survival and reduced retinal oxidative stress. Pretreatment with adenosine Ai receptor antagonist inhibited the oculohypotensive effect of resveratrol. The use of A₁ AR, PLC and ERK 1/2 inhibitors also reduced resveratrolinduced MMP-2 secretion. These results were further supported by in vitro study that demonstrated that ERK1/2, PLC and MMP-2 secretion by HTMC is stimulated after resveratrol treatment and these effects are associated with upregulation of Ai AR gene expression. Topical /r<ms-resveratrol also produced significantly raised plasminogen activator levels and combined TGF-β2+resveratrol treatment caused significant upregulation of inhibitory SMAD7 when compared to TGF-β2-only treated group. Hence, it could be concluded that frvms-resveratrol-induced oculohypotension in SIOH rats involves its agonistic activity at the A₁AR leading to PLC activation, ERK 1/2 phosphorylation and increased MMP-2 secretion. Increased MMP-2 secretion seems to cause changes in TM favourable for AH outflow leading to reduced IOP. 7><ms-resveratrol-induced oculohypotension could also be attributed to increased level of plasminogen activators, which seems to result from increased expression of inhibitory SMAD7, a TGF-β2 signalling molecule. Although current study, for the first time, has clearly demonstrated the significant effects of topical fratts-resveratrol on IOP in rats with SIOH and some of the underlying mechanisms; further investigations are needed to fully understand the mechanisms of action of transresveratrol and to explore its potential as a future antiglaucoma agent. 2016 Thesis https://ir.uitm.edu.my/id/eprint/18581/ https://ir.uitm.edu.my/id/eprint/18581/1/TP_NORHAFIZA%20RAZALI%20MD%2016_5.pdf text en public phd doctoral Universiti Teknologi MARA Faculty of Medicine |
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| description |
Glaucoma, a common cause of optic neuropathy, is associated with elevated intraocular pressure (IOP) and is the leading cause of irreversible visual disability. Steroid-induced glaucoma, a common type of secondary glaucoma, is also associated with elevated IOP (steroid-induced ocular hypertension (SIOH)). SIOH and glaucoma are currently treated with antiglaucoma agents, which often have suboptimal efficacy and are associated with adverse effects. The objective of this study was to determine if topical application of /nms-resveratrol reduces IOP in rats with SIOH and to investigate its mechanisms of action. This study was divided into in vivo and in vitro studies. In the in vivo study, we evaluated the oculohypotensive effects of topical toms-resveratrol in normal and SIOH rats and investigated the role of adenosine receptors (ARs) and transforming growth factor-β (TGF-β) signalling in the IOP lowering effect of fnms-resveratrol. Involvement of AR was studied by observing the IOP changes in response to /rara-resveratrol after pre-treating SIOH animals with AR subtype-specific antagonists. The study also investigated phospholipase C (PLC) activation, extracellular regulated kinase 1/2 (ERK1/2) phosphorylation and increased matrix metalloproteinases (MMPs) secretion in the aqueous humour (AH) as mechanism of resveratrol-induced oculohypotension in SIOH rats. In vitro studies evaluated the effect of frans-resveratrol on cellular signalling pathways of ARs and TGF-β in primary human trabecular meshwork cells (HTMCs). Single drop of all concentrations of toms-resveratrol produced significant oculohypotension in normotensive rats and 0.2% concentration produced maximum IOP reduction. Twicedaily topical application of fnms-resveratrol 0.2% for 21-day in SIOH rats resulted in significant and sustained IOP reduction. This was associated with significantly higher AH MMP-2 level; significantly reduced trabecular meshwork (TM) thickness and increased number of TM cells. Treatment with /raws-resveratrol also significantly increased the ganglion cell survival and reduced retinal oxidative stress. Pretreatment with adenosine Ai receptor antagonist inhibited the oculohypotensive effect of resveratrol. The use of A₁ AR, PLC and ERK 1/2 inhibitors also reduced resveratrolinduced MMP-2 secretion. These results were further supported by in vitro study that demonstrated that ERK1/2, PLC and MMP-2 secretion by HTMC is stimulated after resveratrol treatment and these effects are associated with upregulation of Ai AR gene expression. Topical /r<ms-resveratrol also produced significantly raised plasminogen activator levels and combined TGF-β2+resveratrol treatment caused significant upregulation of inhibitory SMAD7 when compared to TGF-β2-only treated group. Hence, it could be concluded that frvms-resveratrol-induced oculohypotension in SIOH rats involves its agonistic activity at the A₁AR leading to PLC activation, ERK 1/2 phosphorylation and increased MMP-2 secretion. Increased MMP-2 secretion seems to cause changes in TM favourable for AH outflow leading to reduced IOP. 7><ms-resveratrol-induced oculohypotension could also be attributed to increased level of plasminogen activators, which seems to result from increased expression of inhibitory SMAD7, a TGF-β2 signalling molecule. Although current study, for the first time, has clearly demonstrated the significant effects of topical fratts-resveratrol on IOP in rats with SIOH and some of the underlying mechanisms; further investigations are needed to fully understand the mechanisms of action of transresveratrol and to explore its potential as a future antiglaucoma agent. |
| format |
Thesis |
| qualification_name |
Doctor of Philosophy (PhD.) |
| qualification_level |
Doctorate |
| author |
Razali, Norhafiza |
| spellingShingle |
Razali, Norhafiza Cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / Norhafiza Razali |
| author_facet |
Razali, Norhafiza |
| author_sort |
Razali, Norhafiza |
| title |
Cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / Norhafiza Razali |
| title_short |
Cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / Norhafiza Razali |
| title_full |
Cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / Norhafiza Razali |
| title_fullStr |
Cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / Norhafiza Razali |
| title_full_unstemmed |
Cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / Norhafiza Razali |
| title_sort |
cellular mechanisms of action of resveratrol in regulation of aqueous humour dynamics / norhafiza razali |
| granting_institution |
Universiti Teknologi MARA |
| granting_department |
Faculty of Medicine |
| publishDate |
2016 |
| url |
https://ir.uitm.edu.my/id/eprint/18581/1/TP_NORHAFIZA%20RAZALI%20MD%2016_5.pdf |
| _version_ |
1783733696739672064 |