GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needs (2025)

Supplement to November/December 2021 FACULTY: GLAUCOMA Nathan M. Radcliffe, MD Jason Bacharach, MD TREATMENTS Murray Fingeret, OD, FAAO Lorraine M. Provencher, MD IN 2021: Personalizing Patient Needs Administered by Supported by A CE/CME activity administered by Evolve Medical Education LLC. This activity is supported by an unrestricted educational grant from Bausch + Lomb.

Glaucoma Treatments in 2021: CME Release Date: November 2021 CME Expiration Date: December 2022 COPE Release Date: November 29, 2021 Personalizing Patient Needs COPE Expiration Date: October 31, 2024 FACULTY NATHAN M. JASON BACHARACH, MD MURRAY FINGERET, LORRAINE M. RADCLIFFE, MD Glaucoma Specialist OD, FAAO PROVENCHER, MD Program Chair Medical Director Optometrist Glaucoma Specialist Glaucoma Specialist North Bay Eye Associates Clinical Professor of Optometry Cincinnati Eye Institute New York Eye Surgery Center Sonoma County, CA State University of New York Cincinnati, OH New York, NY Co-Director of Glaucoma Division College of Optometry California Pacific Medical Center New York, NY San Francisco, CA CONTENT SOURCE GRANTOR STATEMENT This continuing medical education (CE/CME) activity captures This activity is supported by an unrestricted educational grant content from a roundtable in August. from Bausch + Lomb. ACTIVITY DESCRIPTION ACCREDITATION STATEMENT Based on a roundtable held in August, this supplement Evolve Medical Education LLC (Evolve) is accredited by summarizes a discussion of the mechanisms of actions and the Accreditation Council for Continuing Medical Education challenges with currently available and novel therapeutics as well (ACCME) to provide continuing medical education for physicians. as how to personalize glaucoma treatments. CREDIT DESIGNATION STATEMENT TARGET AUDIENCE Evolve Medical Education designates this enduring material for This certified CME/CE activity is designed eye care providers a maximum of 1 AMA PRA Category 1 Credit™. Physicians should involved in the management of glaucoma and associated disorders. claim only the credit commensurate with the extent of their participation in the activity. LEARNING OBJECTIVES Upon completion of this activity, the participant should be able to: Evolve is an approved COPE administrator. • Describe the mechanisms of action of novel therapeutics and classes of drugs for ocular hypertension (OHT) and primary open-angle glaucoma (POAG) • Interpret the challenges and limitations associated with currently available pharmacologic treatment options for OHT and POAG • Evaluate monotherapy and combination regimens and This activity, COPE Activity Number 122971, is accredited by compare which option is most likely to achieve each COPE for continuing education for optometrists for 1.0 hour. individual patient’s goal IOP • Compare and assess the efficacy of novel therapeutics with Course Approval # 75406-GL traditional prostaglandins Activity Approval # 1229712 SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY | NOVEMBER/DECEMBER 2021

TO OBTAIN CREDIT Jason Bacharach, MD, has had a financial agreement or To obtain credit for this activity, you must read the activity affiliation during the past year with the following commercialin its entirety and complete the Pretest/Posttest/Activity interests in the form of Grant/Research: Allergan, Glaukos, Nicox,Evaluation/Satisfaction Measures Form, which consists Ocular Therapeutix, and Santen. Consultant: Aerie Pharmaceuticals,of a series of multiple-choice questions. To answer these Allergan, Bausch + Lomb, Glaukos, and Santen. Speaker’s Bureau:questions online and receive real-time results, please visit Aerie Pharmaceuticals, Allergan, and Bausch + Lomb. Shareholder:http://evolvemeded.com/course/2133-supp. Upon completing the Injectsense.activity and self-assessment test, your certificate will be available.Alternatively, please complete the Posttest/Activity Evaluation/ Murray Fingeret, OD, FAAO, has had a financial agreementSatisfaction Form and mail or fax to Evolve Medical Education or affiliation during the past year with the following commercialLLC, 353 West Lancaster Avenue, Second Floor, Wayne, PA 19087; interests in the form of Consultant: Aerie Pharmaceuticals,Fax: (215) 933-3950. Allergan, Bausch + Lomb, Carl Zeiss Meditec, Heidelberg, and Topcon. Speaker’s Bureau: Aerie Pharmaceuticals.DISCLOSURE POLICY It is the policy of Evolve that faculty and other individuals who Lorraine M. Provencher, MD, has had a financial agreementare in the position to control the content of this activity disclose or affiliation during the past year with the following commercialany real or apparent conflicts of interest relating to the topics of this interests in the form of Consultant: Allergan, Ivantis, and Visus.educational activity. Evolve has full policies in place that will identify Speaker’s Bureau: Allergan and MST.and resolve all conflicts of interest prior to this educational activity. EDITORIAL SUPPORT DISCLOSURES The following faculty/staff members have the following financial The Evolve staff and planners have no financial relationshipsrelationships with commercial interests: with commercial interests. Michelle Dalton, writer, and Nisha Mukherjee, MD, peer reviewer, have no financial relationships with Nathan M. Radcliffe, MD, has had a financial agreement or commercial interests.affiliation during the past year with the following commercial interestsin the form of Consultant: Aerie Pharmaceuticals, Alcon Vision, Alimera OFF-LABEL STATEMENTSciences, Allergan, Bausch + Lomb, Beaver-Visitec International, This educational activity may contain discussion of publishedCarl Zeiss Meditec, CATS, Ellex, ELT Sight, Equinox, Eyepoint and/or investigational uses of agents that are not indicated byPharmaceuticals, Glaukos, Iridex, Ivantis/Kala Pharmaceuticals, Lumenis, the FDA. The opinions expressed in the educational activityNew World Medical, Novartis, Ocular Science, Ocular Therapeutix, are those of the faculty. Please refer to the official prescribingOmeros, Quantel Medical, Reichert, Santen, Shire, Sight Sciences, information for each product for discussion of approved indications,Spyglass, Thea, and ViaLase. Speaker’s Bureau: Aerie Pharmaceuticals, contraindications, and warnings.Alcon Vision, Alimera Sciences, Allergan, Bausch + Lomb, Beaver-Visitec DISCLAIMERInternational, Eyepoint Pharmaceuticals, Glaukos, Iridex, Ivantis\Kala The views and opinions expressed in this educational activity arePharmaceuticals, Lumenis, New World Medical, Novartis, Reichert, and those of the faculty and do not necessarily represent the views ofSight Sciences. Stock/Shareholder: CATS, ELT Sight, Equinox, Ivantis, Evolve, Glaucoma Today, Modern Optometry, or Bausch + Lomb.Sight Sciences, and Spyglass. DIGITAL EDITION To view the online version of the material, go to http://evolvemeded.com/course/2133-supp. NOVEMBER/DECEMBER 2021 | SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY 3

PRETEST QUESTIONS PLEASE COMPLETE PRIOR TO ACCESSING THE MATERIAL AND SUBMIT WITH POSTTEST/ACTIVITY EVALUATION/ SATISFACTION MEASURES FOR CE/CME CREDIT.1.Please rate your confidence in your ability to apply updates in 8.Which of the following statements about patient compliance and personalizing glaucoma treatment in the clinic. (Based on a scale of 1 dosing is TRUE? to 5, with 1 being not at all confident and 5 being extremely confident.) a.Compliance decreases with decreased dosage regimen and complexity a. 1 b.Compliance increases with decreased dosage regimen and complexity b. 2 c. Less frequent dosing results in worse compliance c. 3 d.There is more compliance with QID drop regimens than with QD d. 4 drop regimens e. 5 9.When counseling patients on the potential side effects of ROCK2.Sustained-release glaucoma treatments are likely to help which group inhibitors, which of the following talking points should be made? of patients the most? a. Hyperemia is common, is not an allergy, and may improve with time a.Patients with ocular surface disease who are struggling with drop b.Any hyperemia is due to an allergy to the medication, and they will adherence need to discontinue use b. Patients on maximum medical therapy c.Systemic side effects are a concern, and you should not use it if c.Patients with advanced glaucoma who need significant IOP reduction you’re pregnant or thinking of becoming pregnant d.Patients with early stage glaucoma who need moderate IOP d. Verticillata is a potential concern and may impact their vision reduction 10.You are seeing a 53-year-old woman who presents for routine exam. You3.Which of the following nitric oxide-donating moieties improves note high IOP at 28 mm Hg in both eyes. She has an enlarged cup-to-disc trabecular outflow? ratio in both eyes as well as a family history of glaucoma. She desires a. Netarsudil therapy with a drop, and she wants to minimize her dosing schedule. b. Netarsudil and latanoprost Which of the following is a first-line agent for this patient? c. Latanoprostene bunod a. Carbonic anhydrase inhibitor d. Selective laser trabeculoplasty (SLT) b. PGAs c. Latanoprostene bunod4.Which of the following is true about the relationship with corneal d. Alpha-adrenergic agonists hysteresis and risk of glaucoma? a.Lower corneal hysteresis is associated with an increased risk of 11.All of the following are mechanism of actions of netarsudil EXCEPT: glaucoma a. Increased aqueous humor production b.Lower corneal hysteresis is associated with a decreased risk of glaucoma b. Increased trabecular outflow c. Corneal hysteresis is not associated with glaucoma c. Decreased episcleral venous pressure d. Corneal hysteresis is the main predictor of propensity to glaucoma d. Decreased trabecular outflow5.A _______ reduction in IOP is necessary to reduce the risk of 12.Sonia, a 50-year-old newscaster, presents for a routine exam, complaining progression according to the Collaborative Normal Tension of blurry vision. Her IOP is 26 mm Hg in her right eye and 24 mm Hg in her Glaucoma Study. left. She has no family history of glaucoma and normal central corneal a. 5% thickness. Her OCT is unremarkable, but her visual field reveals an b. 20% inferior defect on the macular cube on her right eye. She’s diagnosed with c. 30% glaucoma, with a target pressure in the low teens. Her job is unpredictable, d. 40% causing her to work odd hours, and she is frequently on camera. What first- line treatment might be most appropriate for Sonia?6.According to the real-world MOST study, what percentage of patients a. Latanoprostene bunod will experience hyperemia on ROCK inhibitors? b. Latanoprost a. 5% c. OMNI b. 20% d. SLT c. 30% d. 40% 13.Dan is a 65-year-old man with diabetes, hypertension, and moderate glaucoma. He is on combination netarsudil and latanoprost for IOP control7.Which IOP-lowering therapy targets the uveoscleral outflow? with mixed success. He is not always adherent to therapy, causing his a. SLT pressures to range from 8 mm Hg to 17 mm Hg. He presents complaining b. Minimally invasive glaucoma surgery (MIGS) of reduced visual acuity, which is due to a visually significant cataract. His c. Prostaglandin analogs (PGAs) current pressures are 19 mm Hg in both eyes. What is the next treatment d. ROCK inhibitors step for this patient? e. None of the above a. Cataract extraction, IOL implantation, and MIGS b. SLT c. Sustained-release bimatoprost d. Trabeculectomy 4 SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY | NOVEMBER/DECEMBER 2021

GLAUCOMA TREATMENTS IN 2021: Personalizing Patient NeedsGlaucoma Treatments in 2021:Personalizing Patient NeedsFor the nearly 3 million Americans with primary open-angle glaucoma (POAG), medical therapy is the first-line choice to lower IOP. However,these agents have several limitations and barriers that can include compliance, tolerability, and effectiveness.1 Second- and third-linetreatments for patients on maximum medical treatment are laser and surgical procedures, yet there is increasing evidence that laser treatmentshould have a more prominent role in the first-line setting.2 Further, novel mechanisms of action are changing the pharmacologic landscape asnew agents are approved.3 These new agents provide clinicians with multiple options for POAG management, allowing for a more personalizedcare approach. The following roundtable discussion brings together experts in glaucoma management to discuss the current treatmentlandscape and how to create personalized care plans to optimize the outcomes for our patients with glaucoma. —Nathan M. Radcliffe, MD, Program ChairTHE NEED FOR A PERSONALIZED APPROACH TO with the OCT. Donald C. Hood, PhD, of the Hood Visual ScienceGLAUCOMA MANAGEMENT Lab at Columbia University, has spoken a lot about this. He was the Nathan M. Radcliffe, MD: Glaucoma is a challenging disease first to actually flip the nerve fiber layer and put the temporal areathat requires us to use all of the tools at our disposal. Being a in the middle, which allows better structure/function correlationsglaucoma specialist is a journey of constant learning because we so you can look at the field and nerve and assess the changes andhaven’t yet solved this disease. Patients are still losing vision, and how they correlate.8we know we can do better. We must continue to try to find andimplement the new and best therapies. Dr. Radcliffe: Dr. Fingeret, you bring up a great point about where we are with imaging. As for what causes damage to theQ Dr. Fingeret, you’re an imaging expert. What can you tell us about visual field damage and glaucoma? optic nerve, there are risk factors and modifiable risk factors. There’s data indicating that low cerebral spinal fluid (CSF) Murray Fingeret, OD, FAAO: Glaucoma is often thought of as pressure is associated with nerve damage.9-12 Low ocular profusiona group of progressive optic neuropathies that have in common pressure may also be associated with visual field progression.13a slow progressive degeneration of the retinal ganglion cells andtheir axons.4 This process results in a distinct appearance of thedisc and a concomitant pattern of field loss. Glaucoma diagnosis Q Dr. Provencher, what can you tell us about elevated IOP as both a risk factor and a modifiable risk factor?is still essentially clinical; unlike glucose for diabetes, there’s nomarker to make the diagnosis of glaucoma.1 Lorraine M. Provencher, MD: Glaucoma is definitely a The causes of glaucoma are complex. Although IOP is multifactorial disease.1,4 However, in 2021, we still tend to approachthe mainstay of glaucoma treatment, elevated IOP is not a treatment in a unilateral fashion by lowering IOP.1 As Dr. Radcliffeprerequisite for diagnosis; low levels of IOP can stress the optic mentioned, there’s exciting work being done with intracranialnerve head of connective tissue.1 There are other things occurring, pressure (ICP) indicating that low CSF pressure is an independentsuch as blood flow, ischemia, oxidation, and aging.5 What risk factor for glaucoma.11 We may one day have the ability toseparates the glaucomatous optic neuropathy from the other address ICP, but for now, lowering IOP is the main modifiable riskoptic neuropathies are the specific changes that occur within the factor we have. Fortunately, we have great evidence to back up thisganglion cell layer. The remaining layers of the retina are relatively approach. Multiple, large, randomized clinical trials have establishedintact as glaucoma occurs.6 But with that, there’s an excavation the effectiveness of lowering IOP at reducing the risk of glaucomathat occurs to the optic nerve, the so-called ‘bean potting.’ progression and reducing the risk of conversion to glaucoma in One of the challenges on the optometry side is that optometrists patients with ocular hypertension.14-18 The Ocular Hypertensionare not assessing the optic nerve like they once did. Our reliance on Treatment Study (OHTS) showed that treatment to lower IOP ledoptical coherence tomography (OCT) has caused optometrists to to a reduced risk of developing glaucoma at 5 years from 9.5% topay more attention to the nerve fiber layer and the macular region. 4.5%.15 The Early Manifest Glaucoma Trial (EMGT) found that aOCTs don’t always do as good a job with imaging the optic nerve.7 reduction in pressure by 25% reduced the risk of progression fromThe good news is there’s a host of refinements that are occurring 60% to 45%.14,19,20 It also found that each pressure point matters, NOVEMBER/DECEMBER 2021 | SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY 5

GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needs which has since been backed up with other studies. Along those glaucoma treatment. We can improve the trabecular or uveoscleral same lines, the Collaborative Normal Tension Glaucoma Study outflow or decrease aqueous production. (CNTGS) was able to reduce progression in normal tension glau- Multiple drug classes have either a primary mechanism of coma patients through a 30% reduction in IOP.18 action or a secondary mechanism to increase the trabecular or The Advanced Glaucoma Intervention Study 7 (AGIS-7) conventional outflow. Netarsudil 0.02% was the first Rho-kinase showed that in advanced glaucoma, IOP control over time results (ROCK) inhibitor approved in the United States and second in less visual field deterioration.16 In 2015, the United Kingdom ROCK inhibitor approved in the world.21 PGAs have a second- Glaucoma Treatment Study (UKGTS) compared the use of a ary effect of lowering IOP.17,22 Nitric oxide-donating moieties also prostaglandin analog to placebo, and found that treatment improve trabecular outflow. Right now, we have one available lowered IOP and preserved the visual field out to 2 years.17 All of in the United States, latanoprostene bunod 0.024% linked to a these studies provide convincing evidence that pressure reduction PGA.23 Pilocarpine, which is not widely used but very effective, makes a difference. mechanically opens the trabecular outflow pathway. There are other classes of agents in clinical trials right now that appear Jason Bacharach, MD: I’m glad you brought up EMGT, which to demonstrate improved conventional outflow through the was an interesting, population-based study with 7 to 11 years trabecular pathway (including omidenepag isopropyl24,25 and of follow-up. A total of 255 patients, aged 50 to 80 years, with NCX-47026,27). early-stage glaucoma in at least one eye were randomly assigned The other bucket of outflow activity is uveoscleral outflow, which to initial treatment with a selective beta blocker and argon laser PGAs target. Since the CyPass was pulled off the market, we don’t trabeculoplasty (ALT), or left untreated until signs of progres- have a primary surgical mechanism of action to improve uveoscleral sion appeared.14 There were no target pressures set; you got what outflow28; other MIGS devices and procedures are in clinical trials. you got. The reason they performed ALT was because you knew Finally, the third bucket is aqueous suppression. Multiple agents patients would get therapy, and it took compliance out of the suppress aqueous: alpha agonists, beta blockers, and topical picture. At the time, the beta blocker was one of the better treat- carbonic anhydrase inhibitors.1 The issue with suppressing aqueous ment options available because prostaglandin analogs (PGAs) is that we know the eye relies on aqueous for natural function. weren’t yet available on the market. Patients in the treatment arm Remember, Schlemm canal has blood flow but the trabecular had a 25% reduction in pressure, but still had a high progression meshwork doesn’t. The trabecular meshwork and juxtacanalicular rate of 59% at 9 years.14,19,20 Translating this into clinical practice, tissues get their nutrients through aqueous. In younger individuals when we set target pressure goals, in many cases those goals aren’t with a longer life expectancy, we should consider the potential low enough. long-term impact of aqueous suppression.29 Ultimately, lowering IOP is paramount, but I do think Dr. Fingeret: I look at the EMGT and UKGTS studies as mechanism of action is critical. bookends. EMGT showed how many patients progress and UKGTS showed how quickly they change, which can be 12 to 18 months.17 Dr. Radcliffe: Our three newest medications, latanoprostene You’re right, Dr. Bacharach, we should look at target pressures and bunod, netarsudil, and fixed-dose combination of netarsudil and how we are treating these patients. latanoprost have novel mechanisms of action.3,30 Latanoprostene bunod is a nitric oxide-donating prostaglandin F2-alpha ana- Dr. Provencher: I agree, and it’s not just target pressures, it’s logue, and netarsudil is a ROCK inhibitor.21,23 ROCK inhibitors about custom treatment options for patients over time. enhance trabecular outflow. The rationale for this is that the trabecular meshwork is the primary site responsible for elevated Dr. Radcliffe: EMGT showed that one size doesn’t fit all and that pressure in glaucoma, making it a natural target. Rho-kinase 25% pressure reduction probably isn’t sufficient, on average.14 itself increases trabecular meshwork contraction and fibrosis by contracting the actin-myosin stress fibers in the extracel- THE CURRENT TREATMENT LANDSCAPE lular matrix. ROCK inhibitors inhibit Rho-kinase’s ability to link actin-myosin, thereby inhibiting the ability to form the stress Current pharmacologic therapies and novel mechanisms of action fibers in the trabecular meshwork. That causes trabecular mesh- work relaxation, which can even be visualized as a more relaxed, Q DR. RADCLIFFE: Dr. Bacharach, what is your view of the pharmacologic landscape for glaucoma treatment today? open, and visibly porous trabecular meshwork.31 In addition, ROCK inhibitors have been shown to decrease Dr. Bacharach: For years, the emphasis was on lowering IOP, but episcleral venous pressure by as much as 10% in healthy and whether you looked at pharmacologic, laser, or surgical manage- glaucomatous eyes.32,33 With ROCK inhibitors, we can bring more ment with minimally invasive glaucoma surgery (MIGS), a lot of fluid through the trabecular meshwork into Schlemm canal, but also emphasis has shifted to also considering mechanism of action.1 increase that driving force by lowering the episcleral venous pressure There’s really only three mechanisms of action with pharmacologic and, again, bringing more fluid through the trabecular meshwork.6 SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY | NOVEMBER/DECEMBER 2021

GLAUCOMA TREATMENTS IN 2021: Personalizing Patient NeedsThis begs the question, could there be a benefit to bringing more redness, that it is normal, and that it may resolve after a couplefluid through the trabecular meshwork that is more lasting? I hope of days. Hyperemia from netarsudil and latanoprostene bunod isfuture investigations look at that important topic. The mechanism is typically mild, but in some cases, it can be significant. For thoseconceptually appealing because you’re addressing outflow. few cases, the hyperemia is not going to get much better. Then it Nitric oxide has a few different roles and many different becomes a game of managing the redness.functions in the human body, throughout the respiratory,urogenital, cardiovascular, and cerebrovascular systems.34 Nitric Dr. Bacharach: In the MERCURY studies, 58% of patients onoxide can be added to a PGA, such as latanoprost using the fixed-combination netarsudil/latanoprost had hyperemia butbunod modification, which allows the PGA to release nitric oxide most of it was graded as mild. The discontinuation rate was 5%.39as it enters the eye.35 With latanoprostene bunod, we have a In the MERCURY trials, subjects were washed out at baseline, anddrug that releases latanoprost acid and nitric oxide in the eye. they had relatively clear eyes. If you take a drug that you know isThat gives us the uveoscleral outflow and also the effects of nitric going to dilate the episcleral venous bed, you would expect someoxide.3 By way of background, nitric oxide is reduced in patients redness particularly from a baseline of very clear eyes. To contrast,with open-angle glaucoma, so it makes sense that you may be a phase 4 study, (MOST) which enrolled 261 real-world patientstreating a deficiency by replenishing nitric oxide in eyes with already on a variety of topical therapies, there was a hyperemiaelevated pressure.36 Although nitric oxide is a ROCK inhibitor, it rate of 20%.42 For me, the take-home message is that we shouldhas its own effect on soluble guanylyl cyclase and cyclic guanosine prepare patients for the possibility of redness during induction,monophosphate (cGMP) that inhibits calcium signaling and but they should not stop the medication if it’s tolerable and mild.release from the cellular stores.37 This has a similar effect in terms The hyperemia tends to wax and wane and it was rarely presentof trabecular meshwork relaxation as was previously discussed. at two visits in a row during the approval studies. We shouldWe now have nitric oxide working directly through cGMP and encourage our patients to stay on the drug and see if they can getthrough Rho-kinase. There’s evidence in animals that nitric oxide through that initiation period. Remember the hyperemia is not anmodulates episcleral venous pressure.38 Although this has not allergy but due to the drugs effect on the episcleral venous bed.been conclusively demonstrated in humans, there is some reasonto be hopeful that it may have that mechanism. Dr. Provencher: I tell my patents to prepare for their eyes to be very red. It is important to set this expectation. I also stress that it Dr. Provencher: The refocus on trabecular outflow needs to be is normal and not an allergy. I explain that we’ll bring them backemphasized. We now have the ability to treat at the site of the in a couple of weeks to assess its effectiveness and then decide ifpathology, ie, conventional outflow, as opposed to uveoscleral the redness is bothersome enough to discontinue the medication.outflow or aqueous suppression. We don’t fully understand what The vast majority of patients do just fine and don’t mind the mildthe long-term use of aqueous suppression or PGA use does to hyperemia, especially when they see the drug is working.conventional outflow. Could it actually shut down what residualtrabecular meshwork-based outflow our patients have? Could Dr. Radcliffe: Setting expectations is a great approach, andtreating to improve trabecular outflow instead have a positive I agree that many patients think the redness is an acceptableeffect over time? This is an exciting concept to consider. trade-off for keeping their vision. Patient perception varies. Some patients are very red and they don’t perceive it as that bad; other Dr. Radcliffe: Although we don’t yet know if these new patients are only mildly red and they think it’s extreme. We don’ttreatments are disease modifying, it makes sense that this is the want to assume the patient is unhappy and then plant that seedtissue you’d want to go after to have some sort of self-propagating in their mind. I try to be mindful not to have my perceptionbenefit. I think it’s also important to mention that both netarsudil negatively impact their care because I want every patient who canand latanoprostene bunod are once-daily dosing, which is the be helped by these drugs to have their chance. It’s important tosecret to patient adherence. With latanoprostene bunod, you’re find a way through the hyperemia when the patient’s vision is ongetting two mechanisms in one bottle: uveoscleral outflow and the line.trabecular outflow. With ROCK inhibitors, you’re similarly gettingmultiple mechanisms with episcleral venous pressure reduction Selective laser trabeculoplasty as a first-line treatmentas well as trabecular outflow.3 The once-daily dosing makespharmacologic treatment manageable. Dr. Radcliffe: The European LiGHT trial randomly assigned 718 treatment-naïve patients with open-angle glaucoma to initialQ yperemia is a well-known side effect of these H agents;39-41 how do you prepare patients for that potential selective laser trabeculoplasty (SLT; n = 356) or medical therapy (n = 362).2 The trial was designed to establish if SLT is a superior side effect? first-line treatment compared with medical management. Target Dr. Fingeret: Hyperemia is pervasive with all of these IOP was set based on disease severity. The primary outcome wasmedications. I explain to my patients that you may see some eye health-related quality of life at 3 years. Secondary outcomes were NOVEMBER/DECEMBER 2021 | SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY 7

GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needs cost-effectiveness, disease-specific health-related quality of life, because, as Dr. Bacharach mentioned, it works better the earlier effectiveness, and safety. At 36 months, no significant difference you use it. That has also reinforced my thinking that trabecular in quality of life was seen between the two groups (difference, meshwork agents should be used early on as well. If laser is most 0.012; 95% CI -0.007 - 0.031; P = .23). However, more patients efficacious before the disease has progressed to the distal outflow in the SLT group maintained target IOP and avoided glaucoma pathway, then perhaps pharmacologically treating patients with surgery compared with the medical management group. Disease outflow agents earlier could have a similar benefit. also progressed in a lower proportion of patients in the SLT group compared with the medical management group. Dr. Bacharach: That is an interesting point. Moster et al showed that success with an SLT might predict how well some of these Q S LT is becoming a first-line treatment for glaucoma. Where does SLT fit in your practice? new outflow agents might work.49-52 I think they play on each other in terms of mechanism of action. Dr. Provencher: I offer first-line SLT to patients with ocular hypertension, POAG, or secondary open-angle glaucomas. I Dr. Fingeret: I’d like to present a different view of SLT. My present it to them as an equal option to medication. I’ll use SLT experience has been that SLT does not provide the extent of anywhere in the treatment algorithm, but the results from the IOP reduction that we get with some of the newer medications. LiGHT trial moved SLT further up in my algorithm. The LiGHT To me, SLT is clearly an initial modality, but we must carefully trial showed us that, not only is SLT effective from a pressure monitor the patient and intervene if we start to see IOP creep up. reduction standpoint, but it is very safe and can improve adherence issues, which are a huge hurdle in glaucoma care.43,44 Minimally invasive glaucoma surgery (MIGS) The Travatan Dosing Aid Study found that even when patients knew they were being monitored electronically and provided free Dr. Radcliffe: In the past decade, MIGS procedures have medication, 45% of patients used their drops less than 75% of emerged as a surgical alternative to traditional glaucoma surgery. the time.43 Once daily dosing helps, but there are still significant MIGS includes a group of ab interno procedures that have a bet- adherence barriers even with the reduced drop burden.45 SLT ter safety profile than filtration surgery because they spare the patients also get better day-to-day and diurnal control. conjunctiva and have fewer complications.53,54 I’ll also add that it is critical to learn how to present and explain SLT to patients so they are not turned off by the sound of laser. I explain that SLT is not a cure and ongoing follow-up will be Q What is your approach to MIGS in 2021? Where is MIGS headed? needed. My SLT patients are typically very happy they chose laser, Dr. Provencher: The recurring theme from this discussion is and they still continue to follow-up, even off of medications. personalized care. But a second common theme is addressing traditional outflow sooner rather than later. We know MIGS Dr. Radcliffe: That’s such a great myth to dispel. Most doctors are safe and minimally disruptive. They should be performed would select SLT for themselves if they had glaucoma, but we ab interno, and they are easy for the physician to perform and still struggle with ways to present it to our patients as a first-line recovery is generally easier for patients. For these reasons, I think option. We all have patients who are on drops and don’t come MIGS can be offered, with confidence, earlier in the treatment back. Adherence is a problem whether someone has had laser or algorithm. I always consider MIGS when the patient has a visually not. At least with laser, I’ve given them the best chance of saving significant cataract and needs cataract surgery. It’s a great oppor- their sight if they fall off therapy. tunity to improve IOP and reduce medications. I will also consider MIGS as a standalone option when a patient is uncontrolled on Dr. Bacharach: Most clinical studies comparing SLT to medications with a MIGS-range IOP target, intolerant to medica- medication have found that SLT is as efficacious as our best tions, or has poor adherence. For standalone cases, I typically per- medicines.46,47 The LiGHT study was conducted in England and form a 180° goniotomy or use the OMNI Surgical System, which demonstrated a cross-benefit with first-line SLT.2 That was an allows for combined ab interno trabeculotomy and transluminal important demonstrable endpoint. I present SLT as a first-line viscoelastic delivery for up to 360°. This device targets multiple option to my patients, but I don’t push it. Many people will points of aqueous humor outflow resistance: the trabecular choose SLT as a second option if they don’t do well with drops. meshwork, Schlemm canal, and distal collector channels.55-57 MIGS You can use SLT anywhere along the algorithm, but I’ve found it is another opportunity for us to delay invasive procedures. We’re tends to work better the earlier you use it and there is good effica- detecting glaucoma earlier and treating it earlier. We’re also trying cy after the second treatment as well.48 SLT is an excellent option to focus on things like quality of life, and I think MIGS fits perfectly for many patients. with that ethos by reducing the treatment burden for the patient. Dr. Radcliffe: I’ve finally come to totally embrace SLT in my Dr. Radcliffe: Recently, I had a patient who could tolerate almost practice. I use it the most in the first- and second-line settings no drops, but I was still uncomfortable offering MIGS. Are we at8 SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY | NOVEMBER/DECEMBER 2021

GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needsthe point where we consider MIGS by themselves to be acceptable for patients who are poorly tolerant, poorly adherent to medica-options for people who are sensitive to topical agents? tions, or patients who desire independence from topical media- tions. In my experience, the bimatoprost implantation is simple Dr. Bacharach: MIGS have been an incredible advance in surgical for the clinician and well-tolerated by patients. I look forwardtreatment for glaucoma patients. It’s revolutionized my surgical to the expansion of this “fourth pillar,” particularly longer-termtreatment options to offer patients. When I look at my surgeries, options and delivery of additional drug classes.eight out of 10 cataract surgeries will have some type of MIGSassociated with it. As for freestanding MIGS, Sight Sciences, the Dr. Bacharach: I also agree with Dr. Radcliffe. Sustained-releasemanufacturer of the OMNI, has just received on-label approval for drug delivery has already become an important consideration inthe procedure itself, goniotomy and viscocanalostomy, without treatment options for patients. The successful implementationcataract.56,58 Others are in the pipeline. For example, Glaukos has of bimatoprost in our clinical practice has been very exciting.recently submitted a supplemental premarket approval application Sustained-release drug delivery is poised to create a paradigm shiftfor iStent infinite. Hopefully, we’ll soon have a multitude of options in glaucoma management.of freestanding MIGS, and we’ll gain more clinical experience. Dr. Fingeret: Drug delivery systems will become an important Dr. Radcliffe: I agree. It’s challenging and probably not as simple part of glaucoma care, the question is when. One issue is thatas doing standalone MIGS all the time. It’s different to get patients the current techniques are invasive with significant expense andinto the operating room for something that won’t improve their potential complications. Noninvasive delivery devices, such asvision like cataract surgery. contact lenses or the ring when they become available (and that is a big question) will allow optometry to this provide this methodNovel drug-delivery systems of care. Dr. Radcliffe: In light of our recognition of the challenges of CASE 1: THE DANGERS OF UNDERTREATINGtopical therapy, including adherence with once-daily drops,45 the "GREEN DISEASE" IN A YOUNG PATIENTfield of sustained delivery promises to offer agents typically placed Dr. Bacharach: Our first case is a 56-year-old white womaninside of the eye that can lower the pressure without the use of with mildly asymmetric cupping that is worse in the right eyetopical agents for months or even years. than left. Her mother had glaucoma and past medical history is Recently, the US Food and Drug Administration approved sus- noncontributory. She’s on no systemic medicines. She’s a long-timetained-release bimatoprost as a single injection.59,60 Bimatoprost triathlete and in excellent physical condition. Her VA is 20/20 OU,can lower IOP for a period of time between 4 months to 2 years and her slit-lamp exam was within normal limits. Her tonometryafter one administration.61 My clinical experience with bimato- was 26 OU at 8 AM and 19 OU at 4 PM. Her pachymetry readingsprost sustained release has been outstanding. Although these were 540 and 535. Figure 1 shows her imaging. You can see thedelivery systems require more discussion with the patient and optic nerve cupping and a Drance hemorrhage OD. Figure 2 showsconsideration of corneal status and anterior chamber narrowing, her OCT evaluation, which was essentially normal in terms of thethe therapy has provided tremendous value to my patients strug- temporal-superior-nasal-inferior-temporal (TSNIT) and gangliongling with adherence due to ocular surface disease. cell complex, although if you look closely, you can see there is actu- The travoprost intraocular implant is in the pipeline.62,63 ally some intra-eye asymmetry. Although it was still in the greenSustained-release travoprost promises an even longer duration level in most of the parameters, the TSNIT did demonstrate someof action with a drug-elutingimplant placed in the anteriorchamber drainage angle in a OD OSminor surgical procedure. It’sexciting to see that we have anout-of-the-box solution to use.I’ve even referred to sustaineddelivery in glaucoma as thefourth pillar of glaucoma care,sitting alongside topical drops,laser, and incisional surgery. Dr. Provencher: I agree withDr. Radcliffe. Sustained drugdelivery provides a nice option Figure 1. The patient’s baseline imaging. NOVEMBER/DECEMBER 2021 | SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY 9

GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needs that you also see a superior change in the ganglion cell area that is extending almost onto the nasal side. To me, this is no longer a mild defect. We’re getting into moderate defects because of the fairly significant field defect that would force a low target pressure. Dr. Radcliffe: We tend to understage glaucoma. We tend to see a visual field defect like this and assume early glaucoma, but this is at least moderate disease. I bet if you look a little closer, you could find a defect within 10° fixation and classify it as severe. The point is we need to be aggressive in treating these cases. If we aren’t careful with our staging, we may mistake this for early disease. Figure 2. The patient’s baseline OCT results. Dr. Fingeret: The field defect is ominous. There’s probably central loss and a case that requires more than simply a first-level PGA. Dr. Provencher: That’s a great catch on an OCT and a lesson in and of itself. In a way, green disease is worse than red disease. You don’t want to miss early glaucoma, and it’s almost better to overtreat red than undertreat green. We must know how to read an OCT. I agree that this case is scary. This patient is young. I’d check the gonioscopy to ensure her angles are open given the degree of disease at this young age. I’m glad you have a morning IOP check and an afternoon IOP check. If you had only Figure 3. The patient’s baseline visual field imaging. seen her in the afternoon when her pres- sures were 19 mm Hg, there wasn’t a disc thinning of the superior nerve in the right eye. I would call this hemorrhage, and her OCT looked pretty normal at quick glance, ‘green disease’ in the right eye. She had a concomitant visual field one could easily miss the diagnosis without a visual field. defect in the right eye and inferior hemiquadrant (Figure 3). I would target my treatment to lower IOP and minimize the fluctuation she’s having throughout the day. Given that she’s physi- Dr. Fingeret: The asymmetry in the right eye is clear when cally fit, she may have a low blood pressure (BP) at baseline and, compared to the left. That’s a big drop. It looks like it may be a despite likely great cardiovascular output, I’d still worry that her BP little greater superiorly. It is significant in that you can see the area dips low. I’d like to put her on something that flattens diurnal fluc- on the symmetry plot that it is flagged in that so-called red zone. tuation and is nighttime friendly. I’d probably offer a PGA or SLT. I can’t quite make out the average retinal nerve fiber layer (RNFL), As for her target pressure, I want to reduce her IOP by at least 30%, but this field defect is almost classic partial arcuate scotoma putting her target pressure in the mid-teens. You might be able inferiorly that correlates with that. That tells you how deep the to get there with a PGA or SLT alone, but something that reduces RNFL drop-out is. Typically, we don’t see field defects that deep episcleral venous pressure or improves trabecular outflow would be until the RNFL is close to being in the 70s. What’s interesting is nice to add.10 SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY | NOVEMBER/DECEMBER 2021
GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needs Dr. Radcliffe: We want to get to OD OSknow this patient and individualizethe therapy. I want to talk to her andassess her expectations. That can helpguide your therapy choice, whetherit’s SLT, netarsudil, or latanoprostenebunod. It is nice that we have variousoptions to capture different elementsof the efficacy and risk-tolerabilityprofile of the patient. Dr. Provencher: If you’re thinkingbetween something like a PGA or aROCK inhibitor, both have differentcosmetic side-effect profiles.64 For a Figure 4. The patient’s baseline imaging.56-year-old woman who might be onthis for a long time, a PGA may not showing up on the deviation map as well as the quadrant andbe the best option for her cosmetically. We need to get to know the clock hour.her and determine if a little hyperemia might be more desirable Figure 6 shows the combined ganglion cell analysis and RNFLlong-term than say periorbitopathy,65 for example. deviation map for both eyes. I like to use this because it combines the macula and the nerve fiber layer so you get an idea of the Dr. Bacharach: On the diagnostic side, we should consider the gestalt of how most defects are a continuum. Figure 7 shows theOCT as another tool, not the be all, end all. On the therapeutic visual field results from both eyes. This person clearly has POAG,side, we should individualize treatment to a particular patient’s with the right eye having more disease than the left. This personneeds and desires. This patient happens to be in the public eye, is young, and the field defect is nearing the central area. Thereso cosmetic side effects are important, but she was willing andunderstood the gravity of the situation. Her mom has glaucomaand has been taking drops successfully for many years. Thispatient also wanted to try a drop first rather than SLT. I starteda trial of latanoprostene bunod as an initial treatment. She didvery well. The pressure dropped into the 16 mm Hg range, whichwas my initial target goal. Obviously, that’s an adjustable num-ber. Maybe it’s not enough; maybe she’ll need more, but for nowwe continue to manage her on monotherapy.CASE 2: GLAUCOMA MANAGEMENT IN A YOUNGPATIENT WITH DIABETES Dr. Fingeret: Our second case is a 54-year-old black man withdiabetes who presented for a comprehensive eye exam. He ison metformin for HbA1c control, and his HbA1c is 8.3%. He hashigh blood pressure and elevated cholesterol. His last eye examwas 9 years ago, which was negative for glaucoma. His pressureat this exam is 19 mm Hg in each eye, with a corneal thickness of536 and 528. Figure 4 shows his optic nerve in his right and lefteyes. You can see several RNFL defects, both superior and infe-rior. The red tissue also looks extremely suspicious. When you look at the top corner of the left eye on the RNFLthickness map (Figure 5), you can see the areas of blue thatshow the nerve fiber layer defects. Although they don’t showup in the deviation map or in either of the quadrants or clockhours, we do see it. That’s a very good way to see defects rightin that thickness map. On the other side of the right eye, thedefects show up even more. Because they’re denser, they’re also Figure 5. The patient’s ONH and RNFL analysis. NOVEMBER/DECEMBER 2021 | SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY 11
GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needs Dr. Bacharach: Dr. Radcliffe, you bring up an interesting point. You mentioned that most classes of agents work better from a higher starting pressure. The one exception would be netarsudil. ROCK inhibitors seem to work regardless of the starting pressure, whereas most other classes of medicines work about a half millimeter less well for every mil- limeter of lower starting pressure. Netarsudil was the perfect drug to use in this patient because the pressures weren’t that high to start. When you look at the data from the netarsudil/latanoprost fixed-combination study, researchers were able to triple the per- centage of eyes reaching 14 mm Hg or below over the latanoprost arm.39 If you use clinical trials as a guide to treatment and then indi- vidualize that treatment to the patient, netar- sudil was the optimal choice. Figure 6. The patient’s PanoMap analysis. Dr. Radcliffe: Excellent comments. I’d like to thank the faculty for their insights on per- sonalizing glaucoma treatment in 2021. n 1. Gedde SJ, Vinod K, Wright MM, et al. Primary open-angle glaucoma preferred practice pattern. Ophthalmology. 2021;128:P71-P150. 2. Gazzard G, Konstantakopoulou E, Garway-Heath D, et al. Selective laser trabeculoplasty versus eye drops for first-line treatment of ocular hypertension and glaucoma (Light): A Multicentre Randomised Controlled Trial. Lancet. 2019;393:1505-16. 3. Mehran NA, Sinha S, Razeghinejad R. New glaucoma medications: latanoprostene bunod, netarsudil, and fixed combination netarsudil-latanoprost. Eye. 2020;34:72-88. 4. Weinreb RN, Aung T, Medeiros FA. The pathophysiology and treatment of glaucoma: a review. JAMA. 2014;311:1901-11. 5. Grzybowski A, Och M, Kanclerz P, Leffler C, Moraes CG. Primary open angle glaucoma and vascular risk factors: a review of population based studies from 1990 to 2019. J Clin Med. 2020;9. 6. Tan O, Chopra V, Lu AT, et al. Detection of macular ganglion cell loss in glaucoma by Fourier- Domain optical coherence tomography. Ophthalmology. 2009;116:2305-14.e1-2. 7. Hood DC. Imaging glaucoma. Annu Rev Vis Sci. 2015;1:51-72. 8. Hood DC, Zemborain ZZ, Tsamis E, De Moraes CG. Improving the detection of glaucoma and its progression: a topographical approach. J Glaucoma. 2020;29:613-21. 9. Jonas JB, Wang N. Association between arterial blood pressure, cerebrospinal fluid pressure and intraocular pressure in the pathophysiology of optic nerve head diseases. Clin Exp Ophthalmol. 2012;40:e233-4. 10. Jonas JB. Role of cerebrospinal fluid pressure in the pathogenesis of glaucoma. Acta Ophthalmol. 2011;89:505-14. Figure 7. The patient’s visual field analysis. 11. Jonas JB, Wang N. Cerebrospinal fluid pressure and glaucoma. J Ophthalmic Vis Res. 2013;8:257-63. 12. Knier CG, Fleischman D, Hodge DO, Berdahl JP, Fautsch MP. Three-decade evaluation of may even be the beginning of field loss in both hemifields, which cerebrospinal fluid pressure in open-angle glaucoma at a tertiary care center. J Ophthalmol. 2020;2020:7487329. would be even more bothersome. This patient needs significant 13. Leske MC, Heijl A, Hyman L, et al. Predictors of long-term progression in the early manifest glaucoma trial. Ophthalmology. 2007;114:1965-72. IOP reduction. I offered him SLT, but he wanted to try medical 14. Heijl A, Leske MC, Bengtsson B, et al. Reduction of intraocular pressure and glaucoma progression: results from the early manifest management first. We started him on latanoprost, but we quickly glaucoma trial. Arch Ophthalmol. 2002;120:1268-79. escalated to adding netarsudil. We were able to bring down the 15. Kass MA, Heuer DK, Higginbotham EJ, et al. The ocular hypertension treatment study: a randomized trial determines that topical ocular hypotensive medication delays or prevents the onset of primary open-angle glaucoma. Arch Ophthalmol. 2002;120:701-13; discussion 829-30. pressures in both eyes to the low teens. 16. The Advanced Glaucoma Intervention Study (Agis): 7. The relationship between control of intraocular pressure and visual field deterioration.the agis investigators. Am J Ophthalmol. 2000;130:429-40. 17. Garway-Heath DF, Crabb DP, Bunce C, et al. Latanoprost for open-angle glaucoma (ukgts): a randomised, multicentre, placebo- Dr. Radcliffe: One thing that jumps out to me here is that I controlled trial. Lancet. 2015;385:1295-304. don’t think SLT is a great option. All agents work better at higher 18. Anderson DR. Collaborative normal tension glaucoma study. Curr Opin Ophthalmol. 2003;14:86-90. 19. Leske MC, Heijl A, Hussein M, Bengtsson B, Hyman L, Komaroff E. Factors for glaucoma progression and the effect of treatment: the early pressures, but SLT has a bit of a floor. I find these two trabecular manifest glaucoma trial. Arch Ophthalmol. 2003;121:48-56. agents to be great at driving pressures into the low teens from the 20. Leske MC, Heijl A, Hyman L, Bengtsson B, Dong L, Yang Z. Predictors of long-term progression in the early manifest glaucoma trial. Ophthalmology. 2007;114:1965-72. mid-teens. I think there you have two just very good options in a 21. Kopczynski CC, Heah T. Netarsudil ophthalmic solution 0.02% for the treatment of patients with open-angle glaucoma or ocular case like this. hypertension. Drugs Today. (Barcelona, Spain: 1998) 2018;54:467-78.12 SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY | NOVEMBER/DECEMBER 2021
GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needs22. Li T, Lindsley K, Rouse B, et al. Comparative effectiveness of first-line medications for primary open-angle glaucoma: a systematic 45. Tapply I, Broadway DC. Improving Adherence to topical medication in patients with glaucoma. Patient Prefer Adher. 2021;15:1477-89.review and network meta-analysis. Ophthalmology. 2016;123:129-40. 46. Katz LJ, Steinmann WC, Kabir A, et al. Selective laser trabeculoplasty versus medical therapy as initial treatment of glaucoma: a23. Hoy SM. Latanoprostene Bunod ophthalmic solution 0.024%: a review in open-angle glaucoma and ocular hypertension. Drugs. prospective, randomized trial. J Glaucoma. 2012;21:460-8.2018;78:773-80. 47. McIlraith I, Strasfeld M, Colev G, Hutnik CM. Selective laser trabeculoplasty as initial and adjunctive treatment for open-angle24. Duggan S. Omidenepag isopropyl ophthalmic solution 0.002%: first global approval. Drugs. 2018;78:1925-29. glaucoma. J Glaucoma. 2006;15:124-30.25. Aihara M, Lu F, Kawata H, Iwata A, Odani-Kawabata N, Shams NK. Omidenepag isopropyl versus latanoprost in primary open-angle 48. Francis BA, Loewen N, Hong B, et al. Repeatability of selective laser trabeculoplasty for open-angle glaucoma. BMC Ophthalmol.glaucoma and ocular hypertension: the phase 3 AYAME study. Am J Ophthalmol. 2020;220:53-63. 2016;16:128.26. Impagnatiello F, Bastia E, Almirante N, et al. Prostaglandin analogues and nitric oxide contribution in the treatment of ocular hyperten- 49. Lin MM, Moster SJ, Zheng CX, et al. Netarsudil's effect in eyes with a history of selective laser trabeculoplasty. Ophthalmol Glaucoma.sion and glaucoma. Br J Pharmacol. 2019;176:1079-89. 2020;3:306-8.27. Impagnatiello F, Toris CB, Batugo M, et al. Intraocular pressure-lowering activity of ncx 470, a novel nitric oxide-donating bimatoprost 50. Garg A, Vickerstaff V, Nathwani N, et al. Efficacy of repeat selective laser trabeculoplasty in medication-naive open-angle glaucomain preclinical models. Invest Ophthalmol Vis Sci. 2015;56:6558-64. and ocular hypertension during the LIGHT trial. Ophthalmology. 2020;127:467-76.28. Alcon. Cypass® Micro-Stent Market Withdrawal. https://www.alcon.com/cypass-recall-information, 2019. 51. Wang P, Akkach S, Andrew NH, Wells AP. Selective Laser trabeculoplasty: outcomes of multiple repeat treatments. Ophthalmol29. Kiland JA, Gabelt BT, Kaufman PL. Studies on the mechanism of action of timolol and on the effects of suppression and redirection of Glaucoma. 2021.aqueous flow on outflow facility. Exp Eye Res. 2004;78:639-51. 52. Kuley B, Zheng CX, Zhang QE, et al. Predictors of success in selective laser trabeculoplasty. Ophthalmol Glaucoma. 2020;3:97-102.30. Ostler E, Rhee D, Burney E, Sozeri Y. Advances in medical therapy for glaucoma. Curr Opin Ophthalmol. 2021;32:129-33. 53. Mathew DJ, Buys YM. Minimally invasive glaucoma surgery: a critical appraisal of the literature. Annu Rev Vis Sci. 2020;6:47-89.31. Tanna AP, Johnson M. Rho kinase inhibitors as a novel treatment for glaucoma and ocular hypertension. Ophthalmology. 2018;125:1741-56. 54. Lavia C, Dallorto L, Maule M, Ceccarelli M, Fea AM. Minimally-invasive glaucoma surgeries (MIGS) for open angle glaucoma: a32. Kazemi A, McLaren JW, Kopczynski CC, Heah TG, Novack GD, Sit AJ. The effects of netarsudil ophthalmic solution on aqueous humor systematic review and meta-analysis. PLoS One. 2017;12:e0183142.dynamics in a randomized study in humans. J Ocul Pharmacol Ther. 2018;34:380-86. 55. Brown RH, Tsegaw S, Dhamdhere K, Lynch MG. Viscodilation of schlemm canal and trabeculotomy combined with cataract surgery for33. Sit AJ, Gupta D, Kazemi A, et al. Netarsudil improves trabecular outflow facility in patients with primary open angle glaucoma or ocular reducing intraocular pressure in open-angle glaucoma. J Cataract Refract Surg. 2020;46:644-45.hypertension: a phase 2 study. Am J Ophthalmol. 2021;226:262-69. 56. Klabe K, Kaymak H. Standalone trabeculotomy and viscodilation of schlemm's canal and collector channels in open-angle glaucoma34. Rosselli M, Keller PJ, Dubey RK. Role of nitric oxide in the biology, physiology and pathophysiology of reproduction. Hum Reprod Update. using the OMNI Surgical System: 24-month outcomes. Clin Ophthalmol. (Auckland, NZ) 2021;15:3121-29.1998;4:3-24. 57. Vold SD, Williamson BK, Hirsch L, et al. Canaloplasty and Trabeculotomy with the OMNI system in pseudophakic patients with open-35. Cavet ME, Vittitow JL, Impagnatiello F, Ongini E, Bastia E. Nitric Oxide (No): An emerging target for the treatment of glaucoma. Invest angle glaucoma: the ROMEO study. Ophthalmol Glaucoma. 2021;4:173-81.Ophthalmol Vis Sci. 2014;55:5005-15. 58. Sight Sciences Inc. Sight Sciences receives FDA clearance for expanded indication for OMNI Surgical System. https://www.prnewswire.36. Doganay S, Evereklioglu C, Turkoz Y, Er H. Decreased nitric oxide production in primary open-angle glaucoma. Eur J Ophthalmol. com/news-releases/sight-sciences-receives-fda-clearance-for-expanded-indication-for-omni-surgical-system-301241080.html, 2021.2002;12:44-8. 59. Shirley M. Bimatoprost implant: first approval. Drugs & Aging. 2020;37:457-62.37. Arnold WP, Mittal CK, Katsuki S, Murad F. Nitric oxide activates guanylate cyclase and increases guanosine 3':5'-cyclic monophosphate 60. Allergan. Allergan receives FDA approval for Durysta™ (bimatoprost implant) the first and only intracameral biodegradable sustained-levels in various tissue preparations. Proc Natl Acad Sci USA. 1977;74:3203-7. release implant to lower intraocular pressure in open-angle glaucoma or ocular hypertension patients. https://news.abbvie.com/news/38. Zamora DO, Kiel JW. Episcleral venous pressure responses to topical nitroprusside and n-nitro-l-arginine methyl ester. Invest press-releases/therapeutic-area/eye-care/allergan-receives-fda-approval-for-durysta-bimatoprost-implant-first-and-only-intracameral-Ophthalmol Vis Sci. 2010;51:1614-20. biodegradable-sustained-release-implant-to-lower-intraocular-pressure-in-open-angle-glaucoma-or-ocular-hypertension-patients.htm, 2020.39. Walters TR, Ahmed IIK, Lewis RA, et al. Once-daily netarsudil/latanoprost fixed-dose combination for elevated intraocular pressure in 61. Craven ER, Walters T, Christie WC, et al. 24-month phase i/ii clinical trial of bimatoprost sustained-release implant (bimatoprost sr) inthe randomized phase 3 Mercury-2 study. Ophthalmol Glaucoma. 2019;2:280-89. glaucoma patients. Drugs. 2020;80:167-79.40. Bacharach J, Dubiner HB, Levy B, Kopczynski C, Novack GD, AR-13324-CS202 Study Group. Double-masked, randomized, dose-response 62. Glaukos. Glaukos’ Idose® Tr demonstrates sustained iop reduction and favorable safety profile over 24 months in phase 2b study.study of ar-13324 versus latanoprost in patients with elevated intraocular pressure. Ophthalmology. 2015;122:302-7. http://investors.glaukos.com/investors/press-releases/press-release-details/2021/Glaukos-iDose-TR-Demonstrates-Sustained-IOP-41. Serle JB, Katz LJ, McLaurin E, et al. Two phase 3 clinical trials comparing the safety and efficacy of netarsudil to timolol in patients with Reduction-and-Favorable-Safety-Profile-Over-24-Months-in-Phase-2b-Study/default.aspx, 2021.elevated intraocular pressure: rho kinase elevated iop treatment trial 1 and 2 (Rocket-1 and Rocket-2). Am J Ophthalmol. 2018;186:116-27. 63. Glaukos. Glaukos achieves pipeline milestone with completion of patient enrollment in U.S. NDA phase 3 clinical trials for Idose® TR.42. Zaman F, Gieser SC, Schwartz GF, Swan C, Williams JM. A multicenter, open-label study of netarsudil for the reduction of elevated intra- http://investors.glaukos.com/investors/press-releases/press-release-details/2021/Glaukos-Achieves-Pipeline-Milestone-with-Completion-ocular pressure in patients with open-angle glaucoma or ocular hypertension in a real-world setting. Curr Med Res Opin. 2021;37:1011-20. of-Patient-Enrollment-in-U.S.-NDA-Phase-3-Clinical-Trials-for-iDose-TR/default.aspx, 2021.43. Okeke CO, Quigley HA, Jampel HD, et al. Adherence with Topical glaucoma medication monitored electronically the travatan dosing aid 64. Alm A, Grierson I, Shields MB. Side effects associated with prostaglandin analog therapy. Surv Ophthalmol. 2008;53 Suppl1:S93-105.study. Ophthalmology. 2009;116:191-9. 65. Kucukevcilioglu M, Bayer A, Uysal Y, Altinsoy HI. Prostaglandin Associated periorbitopathy in patients using bimatoprost, latanoprost44. Kholdebarin R, Campbell RJ, Jin YP, Buys YM. Multicenter Study of compliance and drop administration in glaucoma. Can J Ophthalmol. and travoprost. Clin Exp Ophthalmol. 2014;42:126-31.2008;43:454-61. NOVEMBER/DECEMBER 2021 | SUPPLEMENT TO GLAUCOMA TODAY & MODERN OPTOMETRY 13
GLAUCOMA TREATMENTS IN 2021: Personalizing Patient Needs (2025)

References

Top Articles
Latest Posts
Recommended Articles
Article information

Author: Reed Wilderman

Last Updated:

Views: 6223

Rating: 4.1 / 5 (52 voted)

Reviews: 83% of readers found this page helpful

Author information

Name: Reed Wilderman

Birthday: 1992-06-14

Address: 998 Estell Village, Lake Oscarberg, SD 48713-6877

Phone: +21813267449721

Job: Technology Engineer

Hobby: Swimming, Do it yourself, Beekeeping, Lapidary, Cosplaying, Hiking, Graffiti

Introduction: My name is Reed Wilderman, I am a faithful, bright, lucky, adventurous, lively, rich, vast person who loves writing and wants to share my knowledge and understanding with you.