2022
DOI: 10.1016/j.exer.2021.108895
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Cathepsin S is a novel target for age-related dry eye

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Cited by 14 publications
(12 citation statements)
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“… 26 , 27 The age-associated increase in inflammation might create a vicious cycle, as inflammatory cytokines like IFN-γ, TNF, and IL-1β are known to upregulate cathepsin S, 28 , 29 which in turn upregulates IL-1β and TNF (TNF is no longer named TNF-α 30 ). In line with this, cathepsin S increases with aging in the retina, brain, and lacrimal gland of mice, 17 , 31 , 32 and we have previously shown that aged tears have high levels of active cathepsin S. 33 …”
supporting
confidence: 66%
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“… 26 , 27 The age-associated increase in inflammation might create a vicious cycle, as inflammatory cytokines like IFN-γ, TNF, and IL-1β are known to upregulate cathepsin S, 28 , 29 which in turn upregulates IL-1β and TNF (TNF is no longer named TNF-α 30 ). In line with this, cathepsin S increases with aging in the retina, brain, and lacrimal gland of mice, 17 , 31 , 32 and we have previously shown that aged tears have high levels of active cathepsin S. 33 …”
supporting
confidence: 66%
“…We previously reported that aged mice have increased cathepsin S activity in tears and Ctss −/− mice have diminished age-related corneal barrier disruption and do not lose goblet cells with age. 33 In this study, we subjected mice aged 15.5 to 17 months to a cathepsin S inhibition diet to investigate if cathepsin S blockade could be used to revert the age-related dry eye phenotype in mice. 10 , 44 Mice show signs of dry eye disease as early as 12 months.…”
Section: Resultsmentioning
confidence: 99%
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“…In particular, for DED, the role of MMP-9 has been widely studied [ 19 ]. Even though the role of other proteases is less well established, there is evidence that serine and cysteine proteases also play a role in the immunity and inflammation of DED [ 37 , 38 ].…”
Section: Introductionmentioning
confidence: 99%
“… 34 , 35 We and others have used aged mice as a model of dry eye disease. As seen in dry eye disease, aged mice have (1) increased corneal permeability, 36 38 (2) conjunctival goblet cell loss, 37 , 39 , 40 (3) increased corneal irregularity, 41 (4) increased immune infiltration in the conjunctiva, 42 (5) meibomian gland disease, 43 48 (6) an altered tear immunoglobulin profile, 49 (7) altered tear cytokines, 40 , 50 , 51 and (8) increased immune infiltration in the lacrimal gland. 36 , 48 , 50 – 54 Corneal aging produces both structural and functional changes that can affect the ability of the organ to refract light, repair itself, and maintain its barrier function.…”
mentioning
confidence: 99%