Continuing Education Activity

Anterior ischemic optic neuropathy occurs due to decreased blood supply to the optic nerve head. It is divided into a) Arteritic anterior ischemic optic neuropathy (A-AION) and b) Non-arteritic anterior ischemic optic neuropathy (NAION). These two conditions have entirely different ethology and approach to their diagnosis and management is completely different. This activity will focus on the role of the interprofessional team in the diagnosis and management of NAION.

Objectives:

• Identify the etiology of NAION.
• Summarize the evaluation of NAION.
• Outline the management options available for NAION.
• Discuss interprofessional team strategies for improving care coordination and communication to advance NAION management and improve outcomes.

Introduction

• Non-arteritic anterior ischemic optic neuropathy (NAION) is the most common cause of optic nerve swelling and optic neuropathy in adults over 50 years of age.[1]
• Risk factors that have been strongly associated with NAION include hypertension, hypercholesterolemia, diabetes mellitus, cardio- and cerebrovascular disease, and obstructive sleep apnea.[2]
• While the exact pathogenesis of a NAION has not been elucidated, the prevailing theory is that it is caused by hypoperfusion of the short posterior ciliary arteries supplying the optic nerve, which then causes ischemia which induces swelling of the portion of the optic nerve traveling through the small opening in a scleral canal.[2] This, in turn, leads to the compartment syndrome involving neighboring axons that are now compressed in a space limited by the small opening in the scleral canal, leading to apoptosis and death of the ganglion cells whose axons comprise the optic nerve.
• The natural history of NAION has been elucidated in Ischemic Optic Neuropathy Decompression Trial which demonstrated that about 30% of patients would regain 3 or more lines of vision at 2 years follow up, 20% will lose 3 or more lines of vision and in the majority of patients, the vision will remain unchanged after the onset.[3] In reality, visual acuity will not change in the vast majority of patients after the acute event has resolved, and the ones who are able to see a few lines better likely learned to improve their fixation.

Etiology

The optic nerve head (ONH) can be subdivided into four regions: intra-ocular, prelaminar region, lamina cribrosa, and retrolaminar regions.

• Blood supply to the ONH is primarily via the short posterior ciliary arteries (SPCA).[4] Pial branches and the peripapillary choroid contribute to the retrolaminar region and prelaminar regions, respectively, but significant variation exists.
• The short posterior ciliary arteries are branches of the ophthalmic artery.[5] Multiple branches of short posterior ciliary arteries form the circle of Zinn-Haller, which surrounds the optic nerve at its passage through the sclera via the lamina cribrosa.
• All blood supply, whether from pial branches, choroid or ciliary arteries, is derived from the ophthalmic artery whose branches these smaller vessels represent.

The pathophysiology of NAION is not completely understood, but it is accepted that relative hypoperfusion of the optic nerve head, as well as structural or other factors, lead to edema and infarction of optic nerve fibers, most often in the superior half of the ONH.[6] 

• Several systemic and ocular risk factors are recognized to increase the risk of NAION including small optic nerve cup (representing the so-called "disc at risk"), optic disc drusen, systemic hypertension, diabetes mellitus, obstructive sleep apnea, and the use of phosphodiesterase-5 inhibitors but their exact roles in the mechanism are not yet fully understood.[7]
• Crowded discs or "disc-at-risk" is the strongest risk factor for developing NAION. A disc-at-risk is characterized as ONH that has a small diameter and small cup-to-disc ratio, typically 0.2 or less. In a disc-at-risk, optic nerve head edema induced by ischemic injury is thought to cause compression of the axons within a smaller, rigid scleral tunnel.
• Similarly, optic disc drusen are thought to contribute to axonal compression within the tight confines of the ONH.
• Hypertension, diabetes mellitus, hyperlipidemia, and smoking all contribute to the vascular causes of NAION, including arteriosclerosis of branches of the ophthalmic artery and intimal thickening of sPCAs.[8]
• Obstructive sleep apnea has also been recognized more recently to also be an independent risk factor for NAION, likely due to its effect on nocturnal blood pressure.

Epidemiology

NAION is the most common cause of optic neuropathy in adults over 50 years of age.[1] The prevalence of NAION in the US has been estimated to be anywhere between 2.3 to 10.2 per 100000. It is less common in blacks and is most common in Caucasians presumably because blacks tend to have a larger cup to disc ratio and are thus less likely to have small optic nerve cups, which is the biggest risk factor for developing NAION.

Pathophysiology

As mentioned above, the exact pathophysiology of NAION; however, the main theory is that the hypoperfusion of short posterior ciliary arteries supplying the optic nerve head leads to localized edema of the involved axons.[9] As the scleral canal through which optic nerve passes into its intra-orbital compartment is small, in predisposed individuals (those with small cup-to-disc ratio) localized optic nerve head edema leads to a compartment syndrome where the swelling is propagated by affecting the neighboring axons. This eventually leads to severe axonal swelling/ischemia and apoptosis with loss of function of the involved axons. 

History and Physical

Complete neuro-ophthalmological history should be obtained emphasizing the onset of visual loss (typically sudden in NAION and semi-acute in optic neuritis) and any other associated symptoms (about 10-15% of patients with NAION experience pain in and around the eye but not with eye movements as is typical in optic neuritis).

Typically there usually aren't any other accompanying neurological symptoms.

Medications history with specific attention to the use of PD-5 inhibitors and anti-hypertensive medications, especially the use of these medications at night, as well as the use of amiodarone, which can be associated with the anterior optic neuropathy whose presentation can be similar to NAION.

A complete examination should be performed.

• Visual acuity can vary from 20/15 to no light perception, although very poor vision (hand motions or worse) is not common in NAION.[10]
• The relative afferent pupillary defect should be present in all patients at presentation. All patients must have optic nerve head edema at the time of presentation, which can persist for 4-6 weeks after onset, and while it is present visual acuity can continue to decline due to the compartment syndrome effect.[4]
• Formal visual fields should be performed in each eye: field abnormalities are typically nerve fiber bundle defects with altitudinal defects being particularly common, possibly because of the proposed semicircle organization of short posterior ciliary arteries supplying the optic nerve head.[6]
• Peripapillary optical coherence tomography would invariably demonstrate thickening of the retinal nerve fiber layer. The presence of the so-called "disc at risk," cup to disc ratio of 0.2 or less in the fellow eye, is seen in over 95% of patients with NAION, and if it is not present, the diagnosis should be questioned.

Evaluation

The diagnosis of NAION is a clinical one: all patients must have optic nerve edema at the time of presentation and over 97% of patients would have a disc-at-risk in the fellow eye with the cup to disc ratio of 0.2 or less.

• Patients with NAION might have a variety of visual field defects although many will have an altitudinal defect supporting the notion that there are two separate semicircles of short posterior ciliary arteries supplying the superior and inferior portions of the optic nerve.

• Visual acuity can vary from 20/20 to no light perception although very poor visual acuity is uncommon and should raise the suspicion for giant cell arteritis.[11]

• While most patients with NAION are over 50 years of age, many are younger and young age at presentation does not exclude the diagnosis although demyelinating optic neuritis should be thought of and excluded in younger individuals.[8]

• Typically in demyelinating optic neuritis optic nerve head edema if present is mild and the presence of peripapillary hemorrhages is rare (less than 5% in optic neuritis treatment trial).
• Pain with eye movements is distinctly uncommon in NAION (although pain in and around the eye can be present in up to 10-15% of patients) whether it is present in up to 94% of patients with demyelinating optic neuritis.

• If the differentiation between NAION and other optic neuropathies is difficult, MRI of the orbits with gadolinium can be useful as it should be normal in all patients with NAION and almost always demonstrates enhancement of the optic nerve in post-contrast imaging in patients with inflammatory optic neuropathies.

Treatment / Management

While many medications and treatment strategies have been tried over the years, none have been proven to be effective. One of the very few randomized controlled clinical trials in neuro-ophthalmology was done evaluating whether patients with NAION will benefit from optic nerve head decompression via vitrectomy and demonstrated that surgery was not beneficial and potentially harmful.[3]

Intravitreal injections of bevacizumab, as well as triamcinolone, have been tried with disappointing results as well.[12]

Recently, a clinical trial evaluating intravitreal injection of QRK207, a caspase 2 inhibitor preventing apoptosis, in patients with recent (within 14 days from onset) onset of NAION did not demonstrate its efficacy and was stopped early.

Currently, the only clinical trial that is ongoing includes subcutaneous injections of RPh201, an isolated botanical extract of gum mastic, for patients who had an onset of NAION within 1-5 years prior to enrollment.

Differential Diagnosis

• In patients under 50 years of age, the main entity on differential diagnosis is demyelinating optic neuritis and antibody-mediated (Aquaporin-4 and anti-myelin oligodendrocyte glycoprotein antibody) optic neuritis.[13]

• Typically patients with demyelinating optic neuritis have pain on eye movements (present in over 94%), have no peripapillary hemorrhages (present in only 5% of patients with demyelinating optic neuritis), and most importantly, visual function recovers in the vast majority of patients as opposed to patients with NAION where visual acuity and visual field defect remain unchanged.[1]

• Patients with myelin oligodendrocyte glycoprotein (MOG)-associated optic neuritis often do have swollen optic nerve with hemorrhages on presentation, but they also have a good visual prognosis with majority recovering visual function as opposed to patients with NAION.

• All patients should also be asked about their use of amiodarone as well as erectile dysfunction medications as amiodarone can present with simultaneous or sequential optic neuropathy that resembles NAION but can improve the following discontinuation of the drug.

• Use of phosphodiesterase inhibitors (PDI) has been linked with the development of NAION, but this association remains unclear, and recommendation on stopping the use of these medications in patients with NAION should be made individually (i.e., has the onset of NAION been directly linked with PDI, the visual status of the patient, etc.).

• In patients over the age of 50, the main entity on the differential diagnosis is giant cell arteritis, and all patients over the age of 60 presenting with a swollen optic nerve should have the inflammatory markers checked in order to rule out this potentially treatable condition.

• Patients with compressive optic neuropathies can sometimes present with a swollen optic nerve, but they typically have a slow onset of visual loss rather than an acute one, as seen in NAION.

Prognosis

The natural course of the disease in NAION has been elucidated by the results of the optic nerve decompression treatment trial which demonstrated that 1/3 of patients will re-gain 3 or more lines of vision at 2 years follow up, 30% will lose 3 or more lines at 2 years, and the rest will demonstrate unchanged visual acuity.[14] In reality, most patients likely maintain the vision they have after the resolution of acute optic nerve head edema, and the improvement seen was secondary to their learned ability to fixate around their scotomas.

Complications

Ischemic optic neuropathies lead to atrophy to the optic nerve in one or both the eyes and can lead to permanent blindness.

Deterrence and Patient Education

There are several risk factors of anterior ischemic optic neuropathy, which can be modified. Patients are advised to have a sleep study, and if diagnosed with sleep apnea to start treatment for this condition, modifications of vascular risk factors should be recommended to all patients, avoidance of nocturnal hypotension has been suggested by many clinicians to be an important strategy to prevent NAION in the fellow eye as well. The use of phosphodiesterase inhibitors should also be discussed.

Enhancing Healthcare Team Outcomes

The correct diagnosis and management of ischemic optic neuropathies are essential to ensure that all potential risk factors are modified in order to decrease the chance of a patient developing this condition in the fellow eye. The possible associations like diabetes, hypertension, hyperlipidemia, when present, should be managed by the interprofessional team, including endocrinologists and general physicians. The team can also include optometrists, neurologists, and ophthalmologists. The nurses participate in patient education and follow up, informing the ophthalmologist of any new issues.