Ophthalmic Nonsteroidal Anti-Inflammatory Drugs as a Therapy for Corneal Dystrophies Caused by SLC4A11 Mutation

Kumari, Aruna; Casey, Joseph R.

doi:10.1167/iovs.18-24301

Cited by 21 publications

(12 citation statements)

References 50 publications

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“…1B) and PS120 fibroblasts stably transfected with HA-tagged SLC4A11 (Fig. 1C), consistent with previous reports of multiple cytoplasmic locations in addition to the plasma membrane [11,24]. TEM immunochemistry of isolated mitochondria from PS120-hSLC4A11-HA cells (Fig.…”

Section: Resultssupporting

confidence: 89%

Ammonia sensitive SLC4A11 mitochondrial uncoupling reduces glutamine induced oxidative stress

et al. 2019

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SLC4A11 is a NH 3 sensitive membrane transporter with H + channel-like properties that facilitates Glutamine catabolism in Human and Mouse corneal endothelium (CE). Loss of SLC4A11 activity induces oxidative stress and cell death, resulting in Congenital Hereditary Endothelial Dystrophy (CHED) with corneal edema and vision loss. However, the mechanism by which SLC4A11 prevents ROS production and protects CE is unknown. Here we demonstrate that SLC4A11 is localized to the inner mitochondrial membrane of CE and SLC4A11 transfected PS120 fibroblasts, where it acts as an NH 3 -sensitive mitochondrial uncoupler that enhances glutamine-dependent oxygen consumption, electron transport chain activity, and ATP levels by suppressing damaging Reactive Oxygen Species (ROS) production. In the presence of glutamine, Slc4a11 −/− (KO) mouse CE generate significantly greater mitochondrial superoxide, a greater proportion of damaged depolarized mitochondria, and more apoptotic cells than WT. KO CE can be rescued by MitoQ, reducing NH 3 production by GLS1 inhibition or dimethyl αKetoglutarate supplementation, or by BAM15 mitochondrial uncoupling. Slc4a11 KO mouse corneal edema can be partially reversed by αKetoglutarate eye drops. Moreover, we demonstrate that this role for SLC4A11 is not specific to CE cells, as SLC4A11 knockdown in glutamine-addicted colon carcinoma cells reduced glutamine catabolism, increased ROS production, and inhibited cell proliferation. Overall, our studies reveal a unique metabolic mechanism that reduces mitochondrial oxidative stress while promoting glutamine catabolism.

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Section: Resultssupporting

confidence: 89%

Ammonia sensitive SLC4A11 mitochondrial uncoupling reduces glutamine induced oxidative stress

et al. 2019

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“…CA inhibitors applied as eye drops have long been used to treat glaucoma by virtue of their ability to reduce the production of aqueous humor, although even their localized ophthalmic use has been documented to lead to the side-effect of systemic MAc in some prone individuals [144] , [145] . Corneal edema that results from the expression of mutant misfolded SLC4A11 may be amenable to correction by small molecule folding chaperones [146] . NHE1 blockers are cytoprotective in a rat model of diabetic cataract formation and retinopathy [147] .…”

Section: Applications By Organ Systemmentioning

confidence: 99%

The therapeutic importance of acid-base balance

Quade

Parker

Occhipinti

2021

Biochemical Pharmacology

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Baking soda and vinegar have been used as home remedies for generations and today we are only a mouse-click away from claims that baking soda, lemon juice, and apple cider vinegar are miracles cures for everything from cancer to COVID-19. Despite these specious claims, the therapeutic value of controlling acid-base balance is indisputable and is the basis of Food and Drug Administration-approved treatments for constipation, epilepsy, metabolic acidosis, and peptic ulcers. In this narrative review, we present evidence in support of the current and potential therapeutic value of countering local and systemic acid-base imbalances, several of which do in fact involve the administration of baking soda (sodium bicarbonate). Furthermore, we discuss the side effects of pharmaceuticals on acid-base balance as well as the influence of acid-base status on pharmacokinetic properties of drugs. Our review considers all major organs systems as well as information relevant to several clinical specialties such as anesthesiology, infectious disease, oncology, dentistry, and surgery.

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“…Approximately 94 SLC4A11 mutations have been identified in individuals with CHED. 4,6,9,[31][32][33][34][35][36][37][38][39][40][41][42][43][44][45][46][47][48] Although a large number of these mutations result in SLC4A11 protein misfolding and failure to mature to the plasma membrane, 5,6,[49][50][51] some mutations affect SLC4A11 transporter function without impacting membrane trafficking 17,52,53 or cause aberrant SLC4A11 pre-mRNA splicing and subsequent reduced SLC4A11 expression. 47 Collectively, these observations support the hypothesis that loss of SLC4A11 function is the primary pathogenetic mechanism in CHED rather than mutant SLC4A11 protein misfolding/mislocalization in the endoplasmic reticulum (ER).…”

mentioning

confidence: 99%

Energy Shortage in Human and Mouse Models ofSLC4A11-Associated Corneal Endothelial Dystrophies

Zhang

Frausto

Chung

et al. 2020

Invest. Ophthalmol. Vis. Sci.

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To elucidate the molecular events in solute carrier family 4 member 11 (SLC4A11)-deficient corneal endothelium that lead to the endothelial dysfunction that characterizes the dystrophies associated with SLC4A11 mutations, congenital hereditary endothelial dystrophy (CHED) and Fuchs endothelial corneal dystrophy 4. METHODS. Comparative transcriptomic analysis (CTA) was performed in primary human corneal endothelial cells (pHCEnC) and murine corneal endothelial cells (MCEnC) with normal and reduced levels of SLC4A11 (SLC4A11 KD pHCEnC) and Slc4a11 (Slc4a11 −/− MCEnC), respectively. Validation of differentially expressed genes was performed using immunofluorescence staining of CHED corneal endothelium, as well as western blot and quantitative PCR analysis of SLC4A11 KD pHCEnC and Slc4a11 −/− MCEnC. Functional analyses were performed to investigate potential functional changes associated with the observed transcriptomic alterations. RESULTS. CTA revealed inhibition of cell metabolism and ion transport function as well as mitochondrial dysfunction, leading to reduced adenosine triphosphate (ATP) production, in SLC4A11 KD pHCEnC and Slc4a11 −/− MCEnC. Co-localization of SNARE protein STX17 with mitochondria marker COX4 was observed in CHED corneal endothelium, as was activation of AMPK-p53/ULK1 in both SLC4A11 KD pHCEnC and Slc4a11 −/− MCEnC, providing additional evidence of mitochondrial dysfunction and mitophagy. Reduced Na +-dependent HCO 3 − transport activity and altered NH 4 Cl-induced membrane potential changes were observed in Slc4a11 −/− MCEnC. CONCLUSIONS. Reduced steady-state ATP levels and subsequent activation of the AMPK-p53 pathway provide a link between the metabolic functional deficit and transcriptome alterations, as well as evidence of insufficient ATP to maintain the Na + /K +-ATPase corneal endothelial pump as the cause of the edema that characterizes SLC4A11associated corneal endothelial dystrophies.

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Ophthalmic Nonsteroidal Anti-Inflammatory Drugs as a Therapy for Corneal Dystrophies Caused by SLC4A11 Mutation

Cited by 21 publications

References 50 publications

Ammonia sensitive SLC4A11 mitochondrial uncoupling reduces glutamine induced oxidative stress

Ammonia sensitive SLC4A11 mitochondrial uncoupling reduces glutamine induced oxidative stress

The therapeutic importance of acid-base balance

Energy Shortage in Human and Mouse Models ofSLC4A11-Associated Corneal Endothelial Dystrophies

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