Abstract

By the year 2020 the most common form of glaucoma, primary open angle glaucoma, will affect 59 million people causing bilateral blindness in 5.9 million. Decreased drainage through a strainer-like structure called trabecular meshwork is responsible for the elevated eye pressure and worsening, irreversible damage of the optic nerve. This meshwork regulates flow by an unknown mechanism. It is not known whether drainage decreases in glaucoma because of cell loss or because of accumulating material next to these cells. The declining turnover of meshwork cells in glaucoma is poorly understood because tools do not exist to extensively yet selectively ablate these cells to study division and migration. Evidence has emerged that trabecular meshwork stem cells may be directly anterior to this structure and can be activated after injury. The long-term goal behind this application is o develop new therapeutic strategies to address the progressive outflow failure in glaucoma. The objective of this application is to create a de novo outflow structure. The main hypothesis is that outflow failure is primarily of cellular origin and can be corrected by reverse engineering of this structure using stem cells. The ability to lower intraocular pressure by creating a new regulating barrier rather than surgically removing it (destroying the anterior chamber-blood barrier) or shunting fluid into a non-physiological space, has high clinical relevance. As gene transfer, tissue engineering and stem cell technologies have matured, the proposed work has become feasible only now using the following systematic approach. (1) The substrate of outflow resistance will be identified and removed by ablating either the inner or the outer part of the meshwork with a conditionally cytotoxic lentiviral gene therapy vector. The changing outflow will be analyzed. (2) Trabecular meshwork stem cells will be mobilized as ablation will trigger cell division and migration. These stem cells may be of rare, neural crest origin with a unique differentiation potential into highly specialized tissues (sympathetic and parasympathetic nervous systems, cartilage, melanocytes). (3) A de novo meshwork will be engineered by seeding induced pluripotent donor stem cells. These cells may be able to use nanoscale cues of the ablated meshwork to form a new outflow structure. These studies capitalize on the ability to target meshwork cells for ablation and on recent insights into how micro-environmental cues guide differentiation. The results will provide a systematic understanding of trabecular meshwork progenitor cell activation and of requirements for regulated outflow to occur, thereby enabling new therapeutic targets in glaucoma.

Public Health Relevance

Primary open-angle glaucoma is a leading and increasing cause of irreversible blindness, becoming more prevalent with age, and has significant impact on individual quality of life, public well-being, and societal burden. Although the disease is thought to be related to decreased drainage that results in increased eye pressure, the exact cause is still poorly understood. This project aims to identify, remove, and replace the faulty drainage structure using new techniques in gene therapy and stem cell technology.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Clinical Investigator Award (CIA) (K08)
Project #
4K08EY022737-05
Application #
9127956
Study Section
Special Emphasis Panel (ZEY1-VSN (10))
Program Officer
Agarwal, Neeraj
Project Start
2012-09-01
Project End
2017-08-31
Budget Start
2016-09-01
Budget End
2017-08-31
Support Year
5
Fiscal Year
2016
Total Cost
$198,642
Indirect Cost
$14,714

  Institution

Name
University of Pittsburgh
Department
Ophthalmology
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Dang, Yalong; Waxman, Susannah; Wang, Chao et al. (2018) Intraocular pressure elevation precedes a phagocytosis decline in a model of pigmentary glaucoma. F1000Res 7:174
Dang, Yalong; Waxman, Susannah; Wang, Chao et al. (2018) A porcine ex vivo model of pigmentary glaucoma. Sci Rep 8:5468
Waxman, Susannah; Loewen, Ralitsa T; Dang, Yalong et al. (2018) High-Resolution, Three-Dimensional Reconstruction of the Outflow Tract Demonstrates Segmental Differences in Cleared Eyes. Invest Ophthalmol Vis Sci 59:2371-2380
Waxman, Susannah; Wang, Chao; Dang, Yalong et al. (2018) Structure-Function Changes of the Porcine Distal Outflow Tract in Response to Nitric Oxide. Invest Ophthalmol Vis Sci 59:4886-4895
Esfandiari, Hamed; Hassanpour, Kiana; Yaseri, Mehdi et al. (2018) Extended pharmacological miosis is superfluous after glaucoma angle surgery: A retrospective study. F1000Res 7:178
Wang, Chao; Dang, Yalong; Waxman, Susannah et al. (2017) Angle stability and outflow in dual blade ab interno trabeculectomy with active versus passive chamber management. PLoS One 12:e0177238
Dang, Yalong; Loewen, Ralitsa; Parikh, Hardik A et al. (2017) Gene transfer to the outflow tract. Exp Eye Res 158:73-84
Dang, Yalong; Waxman, Susannah; Wang, Chao et al. (2017) Rapid learning curve assessment in an ex vivo training system for microincisional glaucoma surgery. Sci Rep 7:1605
Roy, Pritha; Loewen, Ralitsa T; Dang, Yalong et al. (2017) Stratification of phaco-trabectome surgery results using a glaucoma severity index in a retrospective analysis. BMC Ophthalmol 17:30
Fallano, Katherine; Bussel, Igor; Kagemann, Larry et al. (2017) Training strategies and outcomes of ab interno trabeculectomy with the trabectome. F1000Res 6:67

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