A Step Forward: The Latest Developments in Neurotrophic Keratitis

Neurotrophic keratitis (NK) is a degenerative corneal disease caused by damage to the trigeminal nerve.¹ Patients have decreased or no corneal sensation, which results in corneal epithelium breakdown, poor corneal healing, and the eventual development of corneal ulceration, melting, and perforation if left untreated.¹ Due to the desensitization of the corneal nerves, patients don’t experience pain and are likely unware of their disease beyond minor complaints of vision fluctuation. It is therefore critical that eye care clinicians are proactive in screening for, recognizing, and managing NK. Until 2017, there was no specific treatment for NK. That changed with the Food and Drug Administration (FDA) approval of cenegermin. As our experience with cenegermin has deepened, new data on long-term efficacy has also emerged. A modern-day NK classification system has been proposed that outlines the clinical signs and symptoms of early stage disease, empowering clinicians to intervene early on in the disease process when NK is most treatable. The following content summarizes a presentation by experts in NK who discussed clinical evidence on how to differentiate NK from other masquerading ocular surface diseases (OSDs) as well as pearls on diagnosis and management.

— Kelly K. Nichols, OD, MPH, PhD, FAAO, Program Chair

AN INTRODUCTION TO NEUROTROPHIC KERATITIS

Dr. Nichols: NK is considered an orphan disease, which allows new treatments to advance through the FDA approval process a bit more rapidly.² Prevalence is difficult to estimate, and estimations are largely based on other conditions that have NK associated with them. As of right now, we say that there are fewer than 65,000 cases in the United States.³ Some conditions that are associated with NK include herpes simplex keratitis and herpes zoster. About 6% and 12% of patients with herpes simplex and zoster, respectively, will develop NK.³ With zoster, specifically, you’ll see some postsurgical nerve damage. It’s important to note that some of these conditions can overlap making NK much worse.

In terms of differential diagnosis, it’s important to focus on pain and not stain. NK affects the nerves of the eye, and patients experience a loss of corneal sensation. Their clinical presentation may not match their pain level.^1-3 That is very different from neuropathic pain, in which a patient has excessive pain with no clinical signs, like corneal staining.

NK is a degenerative corneal disease where there’s damage to the trigeminal nerve, cranial nerve 5, and the loss of corneal sensation, which, through feedback loop and regulation of the ocular surface, results in a breakdown of corneal epithelium. It can then impact the stroma. You can have stromal melting and a persistent epithelial defect that doesn’t seem to clear or keeps returning.¹

Figure 1 illustrates the feedback loop. When the nerves are damaged, the feedback loop is broken, and the system slowly unravels. There are protective and trophic functions of nerves beyond just sensation that support the epithelial cells and their growth, regeneration, and survival. With a loss of sensation, the cells stop communicating.^2-5

Dr. Nichols: There are also factors associated with neuropeptides, like substance P, that are released when the corneal nerves are normal. This is part of the feedback loop that results in epithelial cell proliferation and migration, allowing them to communicate and touch one another. Blinking also occurs through the nerves, and normal corneal innervation patterns keep the ocular surface healthy. Any breakdown, even if it slowly occurs over time, causes this to worsen with poor healing.¹ Figure 2 shows how impaired corneal trigeminal innervation leads to NK.

Dr. Nichols: Systemic conditions that are associated with NK don’t stop with herpes simplex and herpes zoster. There are many, including diabetes, listed in Table 1. A diet high in sugar and certain medications can also lead to NK. Chronic comorbidities—such as dry eye, blepharitis, exposure keratitis, topical drug toxicity, contact lens-related disorder, and others—can also cofound the diagnosis of NK, increasing the need for a thorough diagnostic workup, including a confirmatory test.² It’s unclear if comorbidities are more likely to result in a recurrence even with treatment, but I would suspect that’s the case.

Dr. Nichols: If you see a nonhealing wound, it’s important to ask yourself if there is an association with herpetic corneal disease. Is there damage due to a stroke or a brain injury? Has there been a history of recent surgery or repetitive surgery? Have they had longstanding contact lens wear? Maybe they wore rigid lens for a number of years. Do they use chronic topical medications for glaucoma? When you see something on the cornea that isn’t resolving, you need to be asking these questions and thinking of NK, especially if more than one is present in the patient.

DIAGNOSING NEUROTROPHIC KERATITIS

Walter O. Whitley, OD, MBA, FAAO: Patients with NK have decreased sensation or decreased or no pain whatsoever.⁶ The cornea epithelium will have some irregularities, which you can have with or without an epithelial defect. Is the stroma involved? If it is, it’s usually oval shaped. Patients may also have a corneal ulcer that has led to melting as well as perforation.

When it comes to diagnosing NK, taking a complete history is crucial. Ask patients directly if they’ve had a herpetic eye infection. Ask them about their contact lens wear, if they take glaucoma medication, and if they are on multiple medications. We know preservatives in eye drops can cause toxicity and accumulate within that corneal epithelium leading to dysfunction.⁷ Corneal sensitivity testing is also essential and should be included in every OSD workup. Drs. Mah and Nichols, do you routinely check corneal sensitivity?

Francis S. Mah, MD: Yes. I include corneal sensitivity testing in all my ocular surface referrals and consults. I assess corneal sensitivity on every patient who comes in with any type of OSD.

Dr. Whitley: Corneal sensitivity assessment is part of our workup when someone comes in for dry eye as well. If you see any significant or chronic staining or epithelial defects, you should have NK as a potential differential. You should also be suspicious for NK in patients with diabetes, which we know can overlap with dry eye disease and occurs in about 54% of patients.⁸ Diabetes also affects the peripheral nerve endings, and we know that there are significant nerve endings within the cornea itself. Does the patient have diabetic retinopathy? There are various reports looking at patients with proliferative diabetic retinopathy who had a vitrectomy and also had concurrent NK.^9,10 Table 2 lists diagnostic considerations for NK.

Dr. Whitley: Staining is definitely underutilized, and you want to make sure you’re looking at this—whether it’s fluorescein, lissamine green, or whatever stain you feel most comfortable with—because if you don’t use stain, you will miss some of the subtle clinical findings that are common within NK. Dr. Nichols, how often do you use the Schirmer test?

Dr. Nichols: I think it is important to measure tear production on all new dry eye patients to understand their baseline. For example, could they be at risk for Sjögren syndrome?

Dr. Mah: I’m not doing a whole lot of Schirmer tests. I’ll do them for rheumatology workups, for Sjögren syndrome, and for clinical trials.

Dr. Whitley: In addition to corneal sensitivity testing, I often use Schirmer when I suspect a patient has NK and when I am trying to get medications approved to show insurance a clinical finding. If you’re concerned about an epithelial defect or if the patient has an infectious ulcer, corneal cultures would be indicated. Additionally, in a cornea clinic, we can utilize confocal microscopy and evaluate the sub-basal corneal nerves to see how those have been impacted.

If a patient has nocturnal lagophthalmos, for example, we can put drops on there all day long, but if we’re not finding the underlying etiology and treating that first, it’s not going to get better. In these cases, exposure keratitis as well as NK is going to be our differential. We have to make sure we’re remembering that list whether it’s dry eye, contact lens wear, or chronic medication with preservatives—could this patient have NK?

How to Conduct Corneal Sensitivity Testing

Dr. Whitley: Corneal sensitivity testing is critical to diagnosing NK. Does the patient have normal or reduced sensitivity or is it completely absent? Typically, the greatest sensitivity will be in the central cornea, but in older adults the cornea will be more sensitive in the periphery. Corneal sensation does drop rapidly as the distance increases from the limbus and falls with increasing age. It’s not affected by iris color. Testing can be done with a cotton wisp from a cotton swab, unwaxed dental floss, or tissue tip.⁵ Of course, don’t put anesthetic in the eye beforehand because you want to see how sensitive, not sensitive, or desensitized that cornea is.

I find that tissue paper is easier and quicker than a cotton wisp. I twist the tissue and touch it to the cornea. I always start with the right eye, touching the tip of the twisted tissue to the central, superior, temporal, inferior, and nasal cornea. I record the findings, classifying the corneal sensitivity as normal, reduced, or absent, and then move on to the other eye afterward with a new tissue.

If you want a quantitative number, you can also use the Cochet-Bonnet esthesiometer. If you’re using the Cochet-Bonnet, you extend the retractable nylon monofilament to full length of 6 cm. You then retract that filament incrementally in 0.5 cm steps until the patient feels contact. It will give you a number of how sensitive or desensitized that cornea is, with shorter length indicating decreased sensation. It’s primarily used in clinical research, but you can use it in the clinic as well.

Dr. Mah, what is your corneal sensitivity testing technique?

Dr. Mah: Similarly, I take my cotton wisp and do each eye. Sometimes the cotton wisp will soak up some of the tears if you do it too far inferiorly or if the patient blinks in the middle, especially if they have normal sensation, then you have to start over. It’s not perfect. But again, it’s not quantitative; it’s more qualitative. Then I’ll use a new cotton swab on the other eye. I also record the sensitivity as normal, reduced, or absent.

Dr. Whitley: Do you test various regions or are you only focused on the central cornea?

Dr. Mah: That’s a great question. In our fellowships, we teach testing the central area and the four quadrants. Historically, the reason to check the four quadrants is because of conditions like herpes simplex or zoster, which can have sectoral corneal hypoesthesia or anesthesia. First and foremost, the key is remembering to test. But I do test central as well as the four quadrants.

Dr. Nichols: I focus on the central cornea unless it looks like there is a lesion somewhere. In that case, I test around the cornea or in other areas for comparison.

Dr. Whitley: I agree that the main focus needs to be on testing in the first place. However, as we get used to sensitivity testing, it’s important to test those various areas because it helps narrow down the underlying cause.

Dr. Nichols: As you treat and the patient improves, you might see a different result if you test the four regions. It’s certainly peripherally where you might see some nerve regeneration and then sensation improves. Testing the four quadrants and being able to compare to future tests is valuable.

Dr. Mah: You also need to test the fellow eye, especially in the beginning, to get an idea of what is normal and what is abnormal. Being able to compare eyes is critical.

TRADITIONAL AND MODERN CLASSIFICATIONS OF NK

Mackie Severity Classification

Dr. Whitley: The Mackie Severity Classification of NK was developed several decades ago. It has three stages (Table 3).^2,11

Dr. Whitley: Thankfully, I see a lot of stage 1 patients in my clinic. Patients with stage 1 disease have punctuate epitheliopathy, staining, decreased tear film breakup time, and increased mucus viscosity. They may also have some stromal haze. Stage 1 may resemble dry eye. This is important because we’ve all had the recalcitrant dry eye patient who has been treated with every anti-inflammatory as well as meibomian gland treatment. We may try various other treatment options, and it’s not getting better. That’s when you need to think that there is something else going on. Once you do corneal staining or sensitivity testing, you’re going to find a lot more patients with NK.

In the more advanced or moderate form of NK, patients will have persistent epithelial defect—that oval shape with smooth, rolled edges. Typically, it’s found centrally or in the inferior part of the cornea and will be surrounded by loose epithelium. You may see some stromal swelling with folds in the Descemet membrane. Depending on the defect, an anterior chamber inflammatory reaction may be present. This is stage 2 disease.

In patients with advanced NK, or stage 3 disease, you’ll see stromal thinning and ulceration, which could lead to corneal perforation. In these patients, you’ll want to use lab testing and corneal cultures.

Although Mackie is three stages, there may be some overlap. They’re clustered, with a number of distinct and often nonsequential phases of NK development into broad, nonspecific categories. The recent advent of more effective treatment options necessitates a more highly defined staging system that better reflects the evolution of the disease and alerts clinicians to the earlier stages of NK. Dr. Mah, tell us about this newly proposed way to identify and stage NK.

The NK Study Group Classification System

Dr. Mah: The Mackie Classification Dr. Whitley so expertly described is the historic classification, which was updated by the NK Study Group (NKSG) a little more than 2 years ago. The issue we had with the Mackie Classification is that the stages are too broad. We started the NKSG to parse the different aspects and define the earlier stages so we can intervene as quickly as possible. NKSG members wrote a paper discussing this updated staging system including diagnosis, diagnostic techniques, and classifications. The paper has been submitted, and is currently under review. The NKSG proposed classification has 7 stages, which allows for earlier diagnosis as well as accurate monitoring of progression and evolution of recurrence. It really parses out the various different stages in much more distinct, finite sections (Table 4).

Dr. Mah: Stage 0 is altered sensation without keratopathy, which makes these patients difficult to identify. This is probably where things start. Patients typically don’t complain, but they may say they have fluctuating vision. They won’t have corneal findings. Previously, these patients would be classified as normal.

Stage 1 is mild. Patients will have some altered corneal sensation and epitheliopathy. There’s no stromal haze. These are those difficult dry eye cases where you’ve prescribed every treatment possible and can’t get the ocular surface to look normal. They look, for all intents and purposes, like dry eye patients. Stage 2, which is more moderate, is an epitheliopathy with a stromal haze. These patients have a damaged ocular surface, but they don’t have an epithelial defect.

Stage 3 is severe NK. Patients have persistent or recurrent epithelial defects and a persistent breakdown of the epithelium. Persistent means different things to different people—some people say 1 week, some 10 days, some 14 days—as long as it’s persistent, 10 days is what most clinicians accept. Stage 4 is when patients have stromal scarring without corneal ulceration. Stage 5 is corneal ulceration, and stage 6, the final stage, is perforation.

I think the NKSG staging, at least in the beginning, will be a bit academic and research-oriented. Importantly, stage 1 NK can look exactly like a recalcitrant dry eye or unresponsive dry eye. How do you differentiate early NK from dry eye?

Dr. Whitley: For me, it’s important to follow OSD evaluation protocols.¹² At my practice, we start with various questionnaires. We use the SPEED questionnaire to assess dry eye symptoms. Some of these patients may not have symptoms other than the fluctuating vision.¹³ We’ll do matrix metallopeptidase-9, tear osmolarity, meibography, or an imaging of the meibomian glands. Remember, you can’t use anesthetic within the eye if you are going to evaluate corneal sensitivity. I follow that up with staining to evaluate tear film breakup time. As we mentioned with the Mackie Classification stage 1, NK patients will have decreased tear film breakup time.

Dr. Mah: In terms of telling patients apart, one of the big differences between dry eye and NK is corneal versus conjunctival staining. With dry eye, you’ll have a lot more conjunctival staining to begin with that will extend into the cornea. You’ll have both corneal and conjunctival staining.¹³ With NK, you don’t have much conjunctival staining. If you use lissamine green or rose bengal and see conjunctival staining, the patient probably has dry eye and not NK.

The second big differential is complaints of pain and discomfort and a scratchy or foreign body sensation in the eye.¹³ Patients with NK don’t typically have these complaints; they are shockingly comfortable. Their main complaint is fluctuating vision.

Dr. Whitley: It’s also important to look at asymmetry patterns. When we think about one of the common causes of NK, viral infection like herpes simplex or zoster, typically that’s unilateral. If you see significant staining in one eye versus another, that should be a clue. Second, if you have a patient being treated for dry eye and you’ve tried various medications and anti-inflammatories but still see staining, it’s time to start testing corneal sensitivity and consider early-stage NK.

Dr. Mah: It’s very easy to test that cornea as part of a dry eye workup. If you think the patient has dry eye and treatments aren’t working, check the corneal sensitivity. The travesty would be ignoring it and pushing it off. Make the diagnosis. If you don’t feel comfortable, refer the patient or attend more of these sessions and get comfortable with the algorithm to start the process. Grow and learn the different stages. At some point, you’ll learn to incorporate some of these tips even if it’s not all of them.

Dr. Nichols: There are many practices out there that focus on the ocular surface. Identify that practice, meet them, see what they are doing, and determine if you can use them to help comanage these patients until you feel comfortable.

NK Treatment

Dr. Mah: Treatment for NK is focused on severity-based therapy (Table 5).^4,6 In early Mackie stage 1 disease, treat with preservative-free artificial tears. The preservative-free aspect is important because preservatives such as benzalkonium chloride could be a cause for NK.⁷ Punctal occlusion is beneficial, and large-diameter hydrogel contact lenses can be used for stages 1, 2, and 3. Recombinant human nerve growth factor (NGF), or cenegermin, is FDA approved for stages 1, 2, and 3.¹⁴ If you have access, autologous serum tears (AST) or the platelet-rich plasma (PRP) is beneficial. There are also amniotic extract eye drops, which are beneficial. With the exception of cenegermin, we use all of these tools on severe dry eye patients.

Dr. Mah: For Mackie stage 2 disease, you can use a scleral lens if it’s a chronic issue, AST/PRP, amniotic membranes, and cenegermin. You can also do some type of nonsurgical tarsorrhaphy, which is more chemical, like Botox or super glue. You can also do a suture tarsorrhaphy if the persistent epithelial defect won’t heal.

For Mackie stage 3, which includes ulcerations and stromal melting, cenegermin is approved in this setting. Other options include keratoplasty, scleral lens, tarsorrhaphy, and neurotization. Dr. Whitley, is there anything you like to use for a specific stage of NK?

Dr. Whitley: In stage 1, punctal occlusion is definitely underused and it’s very beneficial. Even though cenegermin is approved for Mackie stage 1 disease, I still go with the amniotic membrane first and step up to cenegermin if they haven’t approved in a month or 2.

Dr. Mah: A preservative-free topical antibiotic should be used if there is an epithelial defect. Moxifloxacin is FDA approved, and I would use it, at minimum, 3 times a day. AST can be difficult to get, but they are effective. At a 20 to 50% concentration, AST have a success rate ranging from 71 to 100% in terms of healing epithelial defects in NK within 90 days.^15-17 There is some evidence that umbilical cord serum may be more effective and has a higher concentration of substance P and NGF than peripheral blood serum.¹⁸ Studies have also shown that plasma-rich platelets and growth factors are also effective, with epithelial defects healed in 97.4% in stage 2 and stage 3 disease after 11 weeks.¹⁹ Finally, silicon hydrogel contact lenses can be safely used in combination with AST; no inflammation or contact lens deposits were observed in a study by Choi et al.²⁰ However, there isn’t any information on how successful that combination was in terms of healing epithelial defects in NK.

Dr. Whitley: Dr. Mah, what concentration of AST do you recommend? At 50%, you’ll have too much transforming growth factor, which may limit epithelial healing. Do you have any comments on that?

Dr. Mah: AST is typically administered in a 20% concentration, but many clinicians are not using 20%; they are using 50 to 70%.²¹ I personally recommend 50% for NK. You’ll get a higher concentration of NGF, but you’re not going to have transforming NGF.

Moving on to amniotic membrane transplant (AMT), this is a little easier to access because they are commercially available. One randomized clinical trial reported on the healing of refractory neurotrophic ulcers with conventional therapy (lubrication plus bandage contact lenses or tarsorrhaphy) compared with AMT and found that the healing rates were similar between the two groups (67% vs 73%, respectively).²² A second study looked at AMT compared with AST in healing neurotrophic ulcers and found similar rates between them as well (73% vs 70%, respectively).²³ There are many studies looking at AMT, either in layers, glued on, or sutured on for NK, and they seem to work well.²⁴ There’s a growing body of literature in the amniotic membranes that we use in the clinic, the freeze dried or the fresh frozen.^25,26 I prefer the fresh frozen, cryopreserved version. I haven’t had as much success with the freeze dried amniotic membrane commercially available products. Dr. Whitley, Dr. Nichols, any comments?

Dr. Whitley: We’ve also had better clinical results anecdotally within our practice with the cryopreserved.

Dr. Nichols: There’s a bit of comfort level associated with each technique as well. It may be easier for someone to start out with one versus the other, so it’s worth trying to go to a session where you can see both in practice.

Dr. Mah: Moving on, the use of scleral lenses was reported several decades ago, and they are beneficial.²⁷ Nonhealing corneal epithelial defects healed in all nine patients treated with the PROSE scleral lens.²⁸ Overnight wear with close monitoring may accelerate healing.²⁹ Scleral lenses are a great technique, but time consuming because they have to be ordered and fitted. You can’t use it emergently or urgently. If the person is relatively stable, it’s a good method.

Corneal neurotization restores corneal sensitivity using a multidisciplinary surgical technique involving an orbital surgeon and a corneal specialist. It is relatively exciting. You take the free sural nerve and attach it end to side with the supratrochlear nerve, which is why you need an orbital surgeon. The distal portion of the nerve is separated into different fascicles and distributed around the limbus, which is why you need a cornea specialist.³⁰

Several groups have reported on the efficacy of corneal neurotization.^31-33 In general, patients have some corneal sensitivity resulting in resolution of the NK and epithelial defects. This is a valid, exciting approach, but reimbursements are poor and it’s a very long procedure.

Cenegermin: A First-in-Class Treatment for NK

Dr. Whitley: Cenegermin is a human NGF that is structurally identical to the NGF protein within the body.^14,34 It was approved by the FDA in 2017 for the treatment of NK. Corneal integrity is maintained by three mechanisms. Endogenous NGF acts through specific high affinity and low affinity NGF receptors in the anterior segment of the eye.¹ If those nerves aren’t functioning properly, then that epithelium is not going to maintain its regularity, which creates a feedback loop. That’s why it’s important for us to address the nerves, to get them to grow, and to improve their function.

When it comes to corneal innervation, NGF plays a role in the function and stimulates the regeneration and survival of the sensory nerves.^6,35 It also stimulates cell proliferation and differentiation and helps with the survival of the corneal epithelial cells.¹ NGF, combined with the receptors on the lacrimal glands, promotes the sensory mediated reflex tearing secretion.³⁶ To make sure we address the feedback loop, we need to address the underlying issue of denervation, which is where cenegermin comes in. Dr. Nichols, please take us through some of the clinical trial data that led to the approval of cenegermin.

Dr. Nichols: The safety and efficacy of cenegermin dosed six times a day was assessed in two trials: NGF0214 (n = 48), which was conducted in the United States, and REPARO (n = 104), which was conducted in Europe.^37,38 Patients were assigned 1:1 to treatment or placebo. At week 8 in NGF0214, 65% of patients were healed with cenegermin versus 16% with placebo (P = .001). This is a 6 times a day treatment, but you’re also applying placebo 6 times a day a well. You will see some beneficial effect of the repeated lubrication over a period of weeks.

REPARO had similar results but in a bit larger of a study, with 72% of patients at 8 weeks treated with cenegermin showing statistically significant clearance with no staining present versus 33% with placebo (P = .001).^37,38 One of the key questions is how long does a single series of treatment last? Do we have enough data to show over time what the trend is? Do you need to do it again? Of that 72% in REPARO who had clearance at 8 weeks, 80% were still clear after a year.

Pooled together, 50 sites across the world were involved. The most common adverse event was eye pain, which is interesting because these patients don’t experience pain; they have decreased sensation.^37,38 Therefore, how does this pain occur? Does it mean they are improving and are starting to feel again? That could be part of it. The other part could be in the vague way questions are asked in clinical trials. A lot of things are lumped into eye pain. If they had irritation in and around the eye, they could call that eye pain. In most instances, the pain was mild and transient. Dr. Mah, in your experience, what do your patients say about the sensations they experience while using this drop?

Dr. Mah: I tell patients they might get pain, which typically begins 2 to 3 weeks after they start treatment. I explain that it’s a good thing because it means that the nerves, which have deadened, are waking up and they are starting to feel again. Invariably at the end of the treatment, it goes away. As long as they know this is normal, most patients will power through it. They don’t discontinue because of pain.

Dr. Nichols: Now that cenegermin is approved, people want to know the long-term effect. What do we know about the continued beneficial effect over 1, 2, or 3 years out? Are we still seeing improvements in sensitivity and best-corrected visual acuity (BCVA)?

Four studies were published in the last year that help answer some of these questions. Bruscolini et al performed a retrospective chart review of 18 patients with Mackie stage 2 or 3 NK with a least 2 years of follow-up.³⁹ Some patients were followed up to 48 months. There were 4 instances of recurrence over the entire period. At 1 year, three patients recurred. The fourth recurrence occurred at month 36. Visual acuity, corneal sensitivity, and tear production had statistically significant differences at 1, 2, and 3 years. The authors concluded that cenegermin does produce lasting results, even with just one treatment.

In a second study, Pedrotti et al performed a prospective case series of 18 patients with 8 months of follow-up.⁴⁰ The majority, 14 of 18 patients, stayed clear at 4 and 8 months. In vivo corneal microscopy was used to evaluate corneal nerve regeneration. Significant peripheral corneal nerve growth and branching was seen at 2 months and central advancement across the 8 months. Corneal sensitivity improved. The nerve regeneration was partially visible at 8 weeks. It continued after treatment with the hypothesis that the initial growth sustained further regeneration because the reestablishing of the connections allows the nerves to continue to regenerate.

Bonzano et al evaluated anterior segment OCT in 16 patients with NK, half of whom were treated with 50% AST and half of whom were treated with cenegermin.⁴¹ The researchers wanted to see what was happening with corneal thickness as healing progressed. Figure 3 shows that there’s a lumpiness that smooths out, which is especially apparent in Figure 3, images F and G.

Dr. Nichols: Researchers compared the differences between AST and cenegermin and found that both were effective but at different time points. Cenegermin was faster than AST, at 3.9 versus 5.9 weeks, respectively. They were particularly interested in looking at the cornea and how quickly it healed the epithelial layer, if they could see the scar tissue, if the scar tissue improved, and what the overall profile of the cornea looked like. Both improved, perhaps a bit quicker than they suspected, which they hypothesized was due to the peripheral nerve regeneration.

Finally, Sacchetti et al evaluated two groups: amniotic membrane transplant (n = 15) and cenegermin (n = 24) with 12 months of follow up.⁴² A total of 13 patients in the AMT group and 23 patients in the cenegermin group cleared. Similar to other studies, there was a 13% recurrence rate, which favored cenegermin. BCVA was statistically significantly improved. Patient satisfaction with treatment and outcomes was higher in the cenegermin group. Now, of course, you’re comparing a surgical technique versus a drop, and so that probably influenced satisfaction.

I will say, too, that if you look at patients in some of these studies, they did treat the patients who recurred. In general, patients who recurred remained clear at least a year, assuming they were followed. A second treatment could be useful if there’s recurrence.

Dr. Mah: This is fantastic. There’s growing evidence of efficacy and a greater understanding of the effect of the drug on the human cornea.

Dr. Nichols: Being able to see the nerve regeneration is fascinating.

Dr. Whitley: The data you showed are impressive, but there is a 13% recurrence rate, meaning some patients may need retreatment. We don’t have enough evidence there. Hopefully some of you can share your experience with another round of cenegermin in your patients. I’ve done it on a couple of patients so far.

Dr. Nichols: One thing we don’t know is if patients who recur are more likely to have more severe disease at enrollment. These sample sizes are too small to say. I think the mounting body of evidence will help guide future decisions. If patients have a certain severity or a cluster of systemic diseases, they may be more likely to need a second treatment. That information helps with setting patient expectations.

CASE 1: LASIK-INDUCED NK

Dr. Mah: Our first case is a 53-year-old woman who works at a computer all day. She had a history of LASIK in April 2017, but she also had a history of right-sided trigeminal neuralgia, at least it was diagnosed as such. It was pain on the right side of her face. In June 2017, she had a rhizotomy as a potential treatment for the trigeminal neuralgia and the pain. It did not resolve the facial pain and resulted in right-sided facial and eye numbness. Although this is not a common complication of rhizotomy, it can happen.

Her current complaint is decreased vision. She doesn’t have pain. As the day progresses, her central more than her peripheral vision becomes hazy in that right eye. She uses artificial tears and was referred by a neuro-ophthalmologist for an epithelial defect. The neuro-ophthalmologist started her on ciprofloxacin three or four times a day. Figure 4 shows her right eye when she came to me. She was 20/40 in her right eye with no improvement. She was 20/40 with 20/20 pinhole in the left eye.

Dr. Mah: I healed her up using ointment four times a day. Remember, this case is from 2017 and 2018 before we had cenegermin. The problem was, over the next 12 months, every time she stopped the ointment another abrasion or epithelial defect formed. She didn’t like the ointment because it blurred her vision, and she works in front of a computer. She developed an abrasion four times within a year. We tried self-retaining AMT. We used ointment, but she kept breaking down when she decreased the ointment use. She was fitted for a scleral lens, but she just couldn’t tolerate it. She finally had a tarsorrhaphy and hated it, but it kept her intact. Cenegermin was launched in early 2019, and I prescribed it immediately. After an 8-week course, 6 times a day, she was healed. She has remained healed just using preservative-free artificial tears. Her vision is 20/25.

CASE 2: NK With History of Herpes Zoster and LASIK

Dr. Mah: Case 2 is a 75-year-old man with a 3- to 4-month nonhealing epithelial defect. He has a history of bilateral LASIK, herpes zoster, and a previous corneal abrasion about a year prior that healed after 2 weeks of aggressive lubrication antibiotic eye drops. Previous treatments include bandage contact lens, two rounds of self-retained AMT, and AST. At the time of referral, he was on antibiotic eye drops, artificial tears, and valacyclovir. Corneal sensitivity was tested and it was complexly absent. He had > 5 mm central abrasion. The diagnosis was nonhealing neurotrophic corneal epithelial defect. He was started on cenegermin, and 4 weeks later half way through treatment, the > 5 mm central abrasion was a small epithelial defect (Figure 5). It completely resolved at week 8, with the patient only reporting a slight bit of haze.

Case 3: OSD or NK?

Dr. Whitley: Our last case is an 84-year-old woman referred for an ocular surface evaluation. She has a 10-year history of dry eye syndrome, a history of herpes stromal keratitis, anterior scleritis, and previous glaucoma medication (eg, chronic preservatives). She has diabetes and seasonal allergies, which she has treated with topical allergy drops. Those have preservatives as well. Previous treatments include punctal cautery and two rounds of cryopreserved, self-retaining AMT. She’s currently on preservative-free artificial tears and cyclosporine twice a day in both eyes. I checked her corneal sensitivity and it was centrally absent. I diagnosed her with a nonhealing punctate keratopathy, which is stage 1 NK. I treated her with 8 weeks of cenegermin. Her ocular surface improved, the nerves regenerated, and the epithelial cells healed.

Dr. Nichols: Any final words on setting expectations with patients treated with cenegermin?

Dr. Mah: I am very happy with cenegermin in terms of effectiveness and durability. The side effect profile is tolerable as well, but I do tell patients to expect some pain. I’ve also been pretty happy with the ability of my patients to access cenegermin. It’s relatively expensive, but the pharmaceutical company has been good about getting patients access.

Dr. Nichols: Thank you all for an excellent discussion on diagnosing and managing patients with NK. 

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