Stanniocalcin-1 (STC-1), a downstream effector molecule in latanoprost signaling, acts independent of the FP receptor for intraocular pressure reduction

Abstract: Prostaglandin F2 alpha (PGF2α) analogues such as latanoprost are common first-line intraocular pressure (IOP) lowering medications. However, their clinical use is limited in some patient populations due to minimal or no IOP lowering response or side effects. In searching for a more targeted approach for IOP reduction, our lab recently identified Stanniocalcin-1 (STC-1) as a molecule that was required for latanoprost-mediated IOP reduction and also acted as a stand-alone IOP lowering agent. In order to determin… Show more

“…The ability of latanoprost to lower IOP depends on its binding to the FP receptor and activation of downstream signaling cascades [ 45 ]. We had previously shown that STC-1 was necessary for latanoprost-mediated IOP reduction [ 38 ] and when applied topically as an eye drop, could lower IOP through an FP receptor independent mechanism [ 39 ] To determine whether sustained IOP reduction following ssAAV2-STC-1-FLAG injection also did not require the FP receptor, we performed intracameral injections of ssAAV2-STC-1-FLAG in one eye and ssAAV2-GFP in the fellow eye of FP receptor knockout mice previously generated by our laboratory [ 28 ]. There was no difference in baseline IOP measurements between fellow eyes (16.3 ± 0.8 vs 16.3 ± 0.9 mmHg, n = 6, P = 0.8, Fig 6A ).…”

“…Three-month-old C57BL/6J wild-type or FP receptor knockout mice previously generated by our laboratory [ 39 ] were anesthetized with an intraperitoneal injection of ketamine/xylazine/acepromazine (80/6/1 mg/kg body weight) for intracameral injections. Mice were subsequently placed on a dissecting microscope to visualize the anterior chamber.…”

“…To determine the effects of ssAAV2-STC-1-FLAG on parameters of aqueous outflow, 3-month-old C57BL/6J mice were separately treated with the following: 1) intracameral ssAAV-STC-1-FLAG (n = 5), 2) intracameral ssAAV2-GFP (n = 5), 3) topical recombinant human STC-1-FLAG (n = 4; Biovender Research and Diagnostic Products, Czech Republic) [ 38 , 39 ], 4) topical LFA (n = 5; Cayman Chemical, Ann Arbor, MI), or 5) untreated mice (n = 4). Mice that received topical treatments were treated with once daily topical doses of STC-1 (5 μl of a 0.5 μg/μl solution) or LFA (10 −4 M) for 5 days prior to aqueous outflow experiments.…”

“…STC-1 was one of the most consistently upregulated molecules following LFA treatment, and later studies revealed that unlike wild-type controls, STC-1 knockout mice were unresponsive to IOP reduction when treated with LFA. Furthermore, topical application of recombinant STC-1 protein lowered IOP in normotensive [ 38 , 39 ] and ocular hypertensive [ 40 ] mice. Finally, topically administered STC-1 showed equivalent IOP reduction as topically administered LFA, but STC-1 did not require the FP receptor for IOP reduction [ 39 ].…”

“…Furthermore, topical application of recombinant STC-1 protein lowered IOP in normotensive [ 38 , 39 ] and ocular hypertensive [ 40 ] mice. Finally, topically administered STC-1 showed equivalent IOP reduction as topically administered LFA, but STC-1 did not require the FP receptor for IOP reduction [ 39 ]. Given these unique features, we hypothesized that transgene expression of STC-1 in the anterior chamber of the mouse eye would provide sustained IOP reduction.…”

Transgene expression of Stanniocalcin-1 provides sustained intraocular pressure reduction by increasing outflow facility

“…The ability of latanoprost to lower IOP depends on its binding to the FP receptor and activation of downstream signaling cascades [ 45 ]. We had previously shown that STC-1 was necessary for latanoprost-mediated IOP reduction [ 38 ] and when applied topically as an eye drop, could lower IOP through an FP receptor independent mechanism [ 39 ] To determine whether sustained IOP reduction following ssAAV2-STC-1-FLAG injection also did not require the FP receptor, we performed intracameral injections of ssAAV2-STC-1-FLAG in one eye and ssAAV2-GFP in the fellow eye of FP receptor knockout mice previously generated by our laboratory [ 28 ]. There was no difference in baseline IOP measurements between fellow eyes (16.3 ± 0.8 vs 16.3 ± 0.9 mmHg, n = 6, P = 0.8, Fig 6A ).…”

“…Three-month-old C57BL/6J wild-type or FP receptor knockout mice previously generated by our laboratory [ 39 ] were anesthetized with an intraperitoneal injection of ketamine/xylazine/acepromazine (80/6/1 mg/kg body weight) for intracameral injections. Mice were subsequently placed on a dissecting microscope to visualize the anterior chamber.…”

“…To determine the effects of ssAAV2-STC-1-FLAG on parameters of aqueous outflow, 3-month-old C57BL/6J mice were separately treated with the following: 1) intracameral ssAAV-STC-1-FLAG (n = 5), 2) intracameral ssAAV2-GFP (n = 5), 3) topical recombinant human STC-1-FLAG (n = 4; Biovender Research and Diagnostic Products, Czech Republic) [ 38 , 39 ], 4) topical LFA (n = 5; Cayman Chemical, Ann Arbor, MI), or 5) untreated mice (n = 4). Mice that received topical treatments were treated with once daily topical doses of STC-1 (5 μl of a 0.5 μg/μl solution) or LFA (10 −4 M) for 5 days prior to aqueous outflow experiments.…”

“…STC-1 was one of the most consistently upregulated molecules following LFA treatment, and later studies revealed that unlike wild-type controls, STC-1 knockout mice were unresponsive to IOP reduction when treated with LFA. Furthermore, topical application of recombinant STC-1 protein lowered IOP in normotensive [ 38 , 39 ] and ocular hypertensive [ 40 ] mice. Finally, topically administered STC-1 showed equivalent IOP reduction as topically administered LFA, but STC-1 did not require the FP receptor for IOP reduction [ 39 ].…”

“…Furthermore, topical application of recombinant STC-1 protein lowered IOP in normotensive [ 38 , 39 ] and ocular hypertensive [ 40 ] mice. Finally, topically administered STC-1 showed equivalent IOP reduction as topically administered LFA, but STC-1 did not require the FP receptor for IOP reduction [ 39 ]. Given these unique features, we hypothesized that transgene expression of STC-1 in the anterior chamber of the mouse eye would provide sustained IOP reduction.…”

Transgene expression of Stanniocalcin-1 provides sustained intraocular pressure reduction by increasing outflow facility

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