CRISPR-Cas9–based treatment of myocilin-associated glaucoma

Jain, Ankur; Zode, Gulab; Kasetti, Ramesh Babu; Ran, F. Ann; Yan, Wang‐Ji; Sharma, Tasneem Putliwala; Bugge, Kevin; Searby, Charles; Fingert, John H.; Zhang, Feng; Clark, Abbot F.; Sheffield, Val C.

doi:10.1073/pnas.1706193114

Cited by 136 publications

(101 citation statements)

References 45 publications

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“…Adenovirus encoding parts of the CRISPR/Cas9 system have been used to target the myocilin mutations in a murine model and it was found that by targeting the myocilin mutation, the IOP decreased in affected mice and this prevented further damage to the rodent eyes. The same laboratory also looked at the effects of the vector on the trabecular network of ex vivo eyes and reported a decrease in myocilin mRNA . These reports open avenues for translation into clinical trials of early‐onset glaucoma caused by myocilin mutations.…”

Section: Future Directions To Increase Efficacy Of Therapymentioning

confidence: 96%

“…The same laboratory also looked at the effects of the vector on the trabecular network of ex vivo eyes and reported a decrease in myocilin mRNA. 139 These reports open avenues for translation into clinical trials of early-onset glaucoma caused by myocilin mutations.…”

Section: Glaucomamentioning

confidence: 99%

“…Monogenic forms of glaucoma are uncommon and mostly present earlier in life than the typical adult‐onset glaucoma. Myocilin‐dominant gain of function mutations which affect the functioning of the trabecular meshwork, which is responsible for draining aqueous humour from the eye, leads to elevated IOP and have been reported in 10%‐33% of early‐onset glaucoma . Adenovirus encoding parts of the CRISPR/Cas9 system have been used to target the myocilin mutations in a murine model and it was found that by targeting the myocilin mutation, the IOP decreased in affected mice and this prevented further damage to the rodent eyes.…”

Section: Future Directions To Increase Efficacy Of Therapymentioning

confidence: 99%

“…Myocilin-dominant gain of function mutations which affect the functioning of the trabecular meshwork, which is responsible for draining aqueous humour from the eye, leads to elevated IOP and have been reported in 10%-33% of early-onset glaucoma. [139][140][141] Adenovirus encoding parts of the CRISPR/Cas9 system have been used to target the myocilin mutations in a murine model and it was found that by targeting the myocilin mutation, the IOP decreased in affected mice and this prevented further damage to the rodent eyes. The same laboratory also looked at the effects of the vector on the trabecular network of ex vivo eyes and reported a decrease in myocilin mRNA.…”

Section: Glaucomamentioning

confidence: 99%

See 3 more Smart Citations

Gene therapy and the adeno‐associated virus in the treatment of genetic and acquired ophthalmic diseases in humans: Trials, future directions and safety considerations

Ramlogan‐Steel

Murali

Andrzejewski

et al. 2019

Clinical Exper Ophthalmology

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Voretigene neparvovec‐rzyl was recently approved for the treatment of Leber congenital amaurosis, and the use of gene therapy for eye disease is attracting even greater interest. The eye has immune privileged status, is easily accessible, requires a reduced dosage of therapy due to its size and is highly compartmentalized, significantly reducing systemic spread. Adeno‐associated virus (AAV), with its low pathogenicity, prolonged expression profile and ability to transduce multiple cell types, has become the leading gene therapy vector. Target diseases have moved beyond currently untreatable inherited dystrophies to common, partially treatable acquired conditions such as exudative age‐related macular degeneration and glaucoma, but use of the technology in these conditions imposes added obligations for caution in vector design. This review discusses the current status of AAV gene therapy trials in genetic and acquired ocular diseases, and explores new scientific developments, which could help ensure effective and safe use of the therapy in the future.

show abstract

Section: Future Directions To Increase Efficacy Of Therapymentioning

confidence: 96%

Section: Glaucomamentioning

confidence: 99%

Section: Future Directions To Increase Efficacy Of Therapymentioning

confidence: 99%

Section: Glaucomamentioning

confidence: 99%

See 2 more Smart Citations

Gene therapy and the adeno‐associated virus in the treatment of genetic and acquired ophthalmic diseases in humans: Trials, future directions and safety considerations

Ramlogan‐Steel

Murali

Andrzejewski

et al. 2019

Clinical Exper Ophthalmology

View full text Add to dashboard Cite

show abstract

“…Only until recently, two significant mouse models have been established for studies of TM cell therapies. 83,84 Zhu et al reported that aqueous humour out-flow was restored following transplantation of iPSC-derived TM cells in a transgenic mouse model of glaucoma. 84 Their results suggest that transplantation of iPSC-TM may restore out-flow facility and IOP in aged mice.…”

Section: Current S Tatus Of Cell Ther Apy In Animal or Clini C Al Smentioning

confidence: 99%

Trabecular meshwork cells are a valuable resource for cellular therapy of glaucoma

Sun

Zhu

Guo

et al. 2019

J Cellular Molecular Medi

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Trabecular meshwork ( TM ) contains a subset of adult stem cells or progenitors that can be differentiated into corneal endothelial cells, adipocytes and chondrocytes, but not osteocytes or keratocytes. Accordingly, these progenitors can be utilized as a cell‐based therapy to prevent blindness caused by glaucoma, corneal endothelial dysfunction and other diseases in general. In this review, we review in vitro expansion techniques for TM progenitors, discuss their phenotypic properties, and highlight their potential clinical applications in various ophthalmic diseases.

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Glaucoma in Adults—Screening, Diagnosis, and Management

Stein

Khawaja

Weizer

2021

JAMA

299

193

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ImportanceGlaucoma is the most common cause of irreversible blindness worldwide. Many patients with glaucoma are asymptomatic early in the disease course. Primary care clinicians should know which patients to refer to an eye care professional for a complete eye examination to check for signs of glaucoma and to determine what systemic conditions or medications can increase a patient’s risk of glaucoma. Open-angle and narrow-angle forms of glaucoma are reviewed, including a description of the pathophysiology, risk factors, screening, disease monitoring, and treatment options.ObservationsGlaucoma is a chronic progressive optic neuropathy, characterized by damage to the optic nerve and retinal nerve fiber layer, that can lead to permanent loss of peripheral or central vision. Intraocular pressure is the only known modifiable risk factor. Other important risk factors include older age, nonwhite race, and a family history of glaucoma. Several systemic medical conditions and medications including corticosteroids, anticholinergics, certain antidepressants, and topiramate may predispose patients to glaucoma. There are 2 broad categories of glaucoma, open-angle and angle-closure glaucoma. Diagnostic testing to assess for glaucoma and to monitor for disease progression includes measurement of intraocular pressure, perimetry, and optical coherence tomography. Treatment of glaucoma involves lowering intraocular pressure. This can be achieved with various classes of glaucoma medications as well as laser and incisional surgical procedures.Conclusions and RelevanceVision loss from glaucoma can be minimized by recognizing systemic conditions and medications that increase a patient’s risk of glaucoma and referring high-risk patients for a complete ophthalmologic examination. Clinicians should ensure that patients remain adherent with taking glaucoma medications and should monitor for adverse events from medical or surgical interventions used to treat glaucoma.

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CRISPR-Cas9–based treatment of myocilin-associated glaucoma

Cited by 136 publications

References 45 publications

Gene therapy and the adeno‐associated virus in the treatment of genetic and acquired ophthalmic diseases in humans: Trials, future directions and safety considerations

Gene therapy and the adeno‐associated virus in the treatment of genetic and acquired ophthalmic diseases in humans: Trials, future directions and safety considerations

Trabecular meshwork cells are a valuable resource for cellular therapy of glaucoma

Glaucoma in Adults—Screening, Diagnosis, and Management

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