Abstract:Purpose
To investigate the expression of corneal epithelium–derived netrin-1 (NTN-1) and its immunoregulatory function in dry eye disease (DED) using a DED mouse model.
Methods
We generated DED mouse models with desiccating stress under scopolamine treatment. RNA sequencing was performed to identify differentially expressed genes (DEGs) in the corneal epithelium of DED mice. NTN-1 expression was analyzed via real-time PCR, immunofluorescence staining, and immunoblotting… Show more
“…Notably, the drug was mainly distributed in the epithelium of the cornea, which may benefit DED therapy as the DED was characterized by the abnormal corneal epithelium. 50 Figure 5 The effects of TAT modification on the retention of drugs in the cornea. ( a ) The changes of MT contents in the cornea, and ( b ) the calculated area under the curve (AUCs).…”
Introduction
Benzalkonium chloride (BAC) is widely employed as a preservative in eye drops, which will cause the death of corneal epithelial cells due to ROS production, DNA strand breakage, and mitochondrial dysfunction, resulting in dry eye disease (DED)-like changes in ocular surface tissues. In this study, Melatonin (MT) liposomes (TAT-MT-LIPs) designed by loading MT into TAT-modified liposomes have been developed, characterized, and used for inhibiting BAC-induced DED (BAC-DED).
Methods
The TAT was chemically grafted onto the Mal-PEG
2000
-DSPE by Michael’s addition between the sulfhydryl group in TAT and the maleimide group in Mal-PEG
2000
-DSPE. TAT-MT-LIPs were prepared using film dispersion followed by the extrusion method and topically treated in rats once a day. BAC-DED was induced in rats by topical administration with 0.2% BAC twice daily. Defects, edema, and inflammation of the corneas, as well as IOP, were examined. Histologic analyses of corneas were performed to assess the change of mitochondrial DNA oxidation and NLRP3/Caspase-1/GSDMD signaling transduction.
Results
After topical administration, TAT-MT-LIPs significantly alleviated DED-clinical symptoms of experimental animals by inhibiting tissue inflammation and preventing the loss of the corneal epithelium and conjunctival goblet cells. Our data suggested continuous ocular surface exposure of BAC-induced NLRP3/Caspase-1/GSDMD mediated corneal epithelium pyroptosis, which was not reported before. BAC caused substantial mt-DNA oxidation, which promoted the transduction of NLRP3/Caspase-1/GSDMD and consequent corneal epithelium pyroptosis. TAT-MT-LIPs could efficiently suppress the BAC-induced corneal epithelium pyroptosis and inflammation by inhibiting mt-DNA oxidation and the subsequent signal transmission.
Conclusion
NLRP3/Caspase-1/GSDMD mediated corneal epithelium pyroptosis is involved in the development of BAC-DED. The present study provided new insights into the adverse effects of BAC, which can serve as a new target for protecting corneal epithelium when applying BAC as a preservative in eye drops. The developed TAT-MT-LIPs can efficiently inhibit BAC-DED and give great potential to be developed as a new DED treatment.
“…Notably, the drug was mainly distributed in the epithelium of the cornea, which may benefit DED therapy as the DED was characterized by the abnormal corneal epithelium. 50 Figure 5 The effects of TAT modification on the retention of drugs in the cornea. ( a ) The changes of MT contents in the cornea, and ( b ) the calculated area under the curve (AUCs).…”
Introduction
Benzalkonium chloride (BAC) is widely employed as a preservative in eye drops, which will cause the death of corneal epithelial cells due to ROS production, DNA strand breakage, and mitochondrial dysfunction, resulting in dry eye disease (DED)-like changes in ocular surface tissues. In this study, Melatonin (MT) liposomes (TAT-MT-LIPs) designed by loading MT into TAT-modified liposomes have been developed, characterized, and used for inhibiting BAC-induced DED (BAC-DED).
Methods
The TAT was chemically grafted onto the Mal-PEG
2000
-DSPE by Michael’s addition between the sulfhydryl group in TAT and the maleimide group in Mal-PEG
2000
-DSPE. TAT-MT-LIPs were prepared using film dispersion followed by the extrusion method and topically treated in rats once a day. BAC-DED was induced in rats by topical administration with 0.2% BAC twice daily. Defects, edema, and inflammation of the corneas, as well as IOP, were examined. Histologic analyses of corneas were performed to assess the change of mitochondrial DNA oxidation and NLRP3/Caspase-1/GSDMD signaling transduction.
Results
After topical administration, TAT-MT-LIPs significantly alleviated DED-clinical symptoms of experimental animals by inhibiting tissue inflammation and preventing the loss of the corneal epithelium and conjunctival goblet cells. Our data suggested continuous ocular surface exposure of BAC-induced NLRP3/Caspase-1/GSDMD mediated corneal epithelium pyroptosis, which was not reported before. BAC caused substantial mt-DNA oxidation, which promoted the transduction of NLRP3/Caspase-1/GSDMD and consequent corneal epithelium pyroptosis. TAT-MT-LIPs could efficiently suppress the BAC-induced corneal epithelium pyroptosis and inflammation by inhibiting mt-DNA oxidation and the subsequent signal transmission.
Conclusion
NLRP3/Caspase-1/GSDMD mediated corneal epithelium pyroptosis is involved in the development of BAC-DED. The present study provided new insights into the adverse effects of BAC, which can serve as a new target for protecting corneal epithelium when applying BAC as a preservative in eye drops. The developed TAT-MT-LIPs can efficiently inhibit BAC-DED and give great potential to be developed as a new DED treatment.
“…[ 10 , 43 - 53 ] Numerous in vivo studies have confirmed similar altered status of DCs in cornea, conjunctiva and lacrimal gland, and its plausible contribution or mechanism to disease pathogenesis in DED. [ 54 - 60 ] The clinical relevance of DCs can be appreciated with its strong association with DED clinical parameters in patients and the mechanistic studies in the animal models of DED. As illustrated in Fig.…”
Section: Ocular Surface Immune Cell Profile In Dedmentioning
confidence: 99%
“…T cell subsets that were investigated in animal models of DED include CD4+ T cells,[ 70 , 76 , 82 - 84 ] CD8+ T cells,[ 76 ] central memory T cells,[ 85 ] effector memory T cells,[ 85 ] Th1 cells,[ 38 , 86 - 88 ] Th2 cells,[ 89 ] Th17 cells,[ 38 , 60 , 88 , 90 - 92 ] and T regulatory cells – Tregs. [ 38 , 39 , 86 , 90 , 91 ] Increase in ocular surface CD4+ T cells,[ 70 , 76 , 82 - 84 ] CD8+ T cells,[ 76 ] Th1 cells,[ 86 , 87 ] and Th17 cells,[ 60 , 88 , 90 - 92 ] and a decrease in the ocular surface Tregs,[ 86 , 90 ] have been observed in various DED animal models. Contrary to the observations made in a human study,[ 81 ] a decrease in naïve T cells and central memory, along with an increase in effector memory T cells in the eye tissues of DED animals.…”
Section: Ocular Surface Immune Cell Profile In Dedmentioning
confidence: 99%
“…Topical administration of netrin-1,[ 60 ] PEDF,[ 61 ] COX-2 inhibitor,[ 57 ] and TRPV1 channel blockade[ 65 ] have shown suppression of DC activation, maturation, migration, related ocular surface inflammation, and DED severity. Treatment with resolvin,[ 70 ] PEDF,[ 68 ] CCR7 blockade,[ 67 ] or IL-20 blockade[ 69 ] resulted in the reduction of ocular surface infiltration of macrophages, migration of macrophages to lymph nodes, ocular surface inflammation and DED severity in animal models.…”
Section: Ocular Surface Immune Cell Profile In Dedmentioning
confidence: 99%
“…Anti-TNF,[ 82 ] polyphenols – quercetin and resveratrol,[ 83 ] diquafosol sodium,[ 87 ] dexamethasone,[ 74 ] cyclosporine,[ 106 ] voclosporin, a calcineurin inhibitor,[ 94 ] GW559090, a α4β1 integrin antagonist,[ 73 ] resolvin,[ 70 ] and IL-17 blockade[ 80 ] treatments reduced ocular surface infiltration and activation of T cells in DED animal models. Lifitegrast,[ 105 ] CCL20 neutralization,[ 107 ] erxian decoction,[ 90 ] rebamipide,[ 91 ] and netrin-1[ 60 ] were reported to reduce the infiltration and trafficking of Th17 subsets on to the ocular surface and restored normal ocular surface parameters in various animal models of DED. Studies have also shown the beneficial regulation of Th17 and Treg cells in DED models.…”
Section: Ocular Surface Immune Cell Profile In Dedmentioning
Dry eye disease (DED) is a multifactorial chronic ocular surface inflammatory condition. Disease severity has been directly related to the immuno-inflammatory status of the ocular surface. Any perturbation in the orchestrated functional harmony between the ocular surface structural cells and immune cells, both resident and trafficking ones, can adversely affect ocular surface health. The diversity and contribution of ocular surface immune cells in DED have been of interest for over a couple of decades. As is true with any mucosal tissue, the ocular surface harbors a variety of immune cells of the innate-adaptive continuum and some of which are altered in DED. The current review curates and organizes the knowledge related to the ocular surface immune cell diversity in DED. Ten different major immune cell types and 21 immune cell subsets have been studied in the context of DED in human subjects and in animal models. The most pertinent observations are increased ocular surface proportions of neutrophils, dendritic cells, macrophages, and T cell subsets (CD4+; CD8+; Th17) along with a decrease in T regulatory cells. Some of these cells have demonstrated disease-causal association with ocular surface health parameters such as OSDI score, Schirmer’s test-1, tear break-up time, and corneal staining. The review also summarizes various interventional strategies studied to modulate specific immune cell subsets and reduce DED severity. Further advancements would enable the use of ocular surface immune cell diversity, in patient stratification, i.e. DED-immunotypes, disease monitoring, and selective targeting to resolve the morbidity related to DED.
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