RESEARCH ARTICLE


Evaluating Optic Nerve Damage: Pearls and Pitfalls



Paul J. Mackenzie*, Frederick S. Mikelberg
Division of Glaucoma, Department of Ophthalmology and Visual Sciences, University of British Columbia, Vancouver Acute, 2550 Willow St, Vancouver, BC V5Z 3N9, Canada


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Creative Commons License
© Mackenzie and Mikelberg; Licensee Bentham Open.

open-access license: This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by-nc/3.0/), which permits unrestrictive use, distribution, and reproduction in any medium, provided the original work is properly cited.

* Address correspondence to this author at the Division of Glaucoma, Department of Ophthalmology and Visual Sciences, University of British Columbia, Vancouver Acute, 2550 Willow St, Vancouver, BC V5Z 3N9, Canada; E-mail: pmack@interchange.ubc.ca


Abstract

Primary open-angle glaucoma is a progressive optic neuropathy involving loss of retinal ganglion cells and their axons at the level of the optic nerve head. This change manifests as thinning and excavation of the neural tissues and nerve fiber layer. Therefore, it has long been known that the structural appearance of the optic nerve head is paramount to both glaucoma diagnosis and to the detection of progression [1-4]. Quantitative imaging methods such as Heidelberg Retinal Tomography (HRT) and Ocular Coherence Tomography (OCT) show great promise for the diagnosis and management of glaucoma and as these technologies continue to improve, they will become more important in the care of glaucoma. However, these tests cannot replace good clinical examination and indeed they depend upon clinical correlation for correct interpretation. Thus, careful and systematic clinical examination of the optic nerve remains a cornerstone of glaucoma management. In this paper, we outline a few pearls for the examination of the optic nerve and some of the pitfalls to be avoided in optic disc examination.




OPTIC NERVE SIZE

Any clinical assessment of the optic nerve needs to be made with respect to disc size. There is a large degree of variability in the size of the normal optic nerve, varying in area over a sevenfold ratio [5-7]. A large nerve can be expected to have a larger cup to disc ratio can be expected. Fig. (1) illustrates a large nerve with a physiologically large cup. Care must also be used when evaluation small optic nerves: even a small amount of cupping and rim thinning can represent glaucomatous damage.

Fig. (1).

Normal large optic nerve with corresponding physiologic cupping. Follows ISN’T rule.


Fig. (2).

Heidelberg retinal tomography (HRT) output of the optic nerve shown in Fig. (1). See text for discussion of Moorfield’s Regression Analysis abnormality in large optic nerve heads.


Fig. (3).

White on white standard automated perimetry of optic nerve from Fig. (1) and HRT from Fig. (3). Normal visual field test.


Fig. (4).

Large optic nerve with glaucomatous cupping. Note violation of ISN’T rule inferiorly, along with inferior notch and associated nerve fibre layer wedge defect.


Fig. (5).

Glaucomatous optic nerve with optic disc hemorrhage inferiorly, with associated nerve fibre layer defect.


Fig. (6).

Glaucomatous optic nerve in a highly myopic patient. See text for discussion of the clinical features.


MEASUREMENT OF DISC SIZE

Clinically, the optic disc is roughly equal to the small aperture (5 degrees) on the Welch Allan direct ophthalmoscope (or the medium spot size on a direct ophthalmoscope with three aperture sizes). Indirect slit-lamp biomicroscopy allows for measurement of the optic disc size using the vertical light scale on the slit lamp. The average vertical diameter of the optic disc around 1.8 mm; a disc that is measured to be less than 1.5 mm is likely a small disc while one greater than 2.2 mm can be considered abnormally large. A correction factor must be used depending on the indirect lens that is used. For a 60 diopter lens, the correction factor is 1; that is, the measured size corresponds to the actual size. The correction factor is 1.1x and 1.3x respectively for a 78D and 90D lens.

Quantitative measurements of disc size can be obtained with imaging technologies. For example, the Heidelberg Retinal Tomograph (HRT) provides a measurement of disc size along with the determination of whether the optic disc is without or outside of the normal range. Fig. (2) shows HRT output for the optic nerve shown in Fig. (1); while Fig. (3) shows the normal standard automated perimetry (SAP) visual field from the same eye. The size of the optic disc is 4.00 mm2, significantly larger than the upper limit of normal of 2.43 mm2. Note as well that the Moorfield’s Regression Analysis (MRA) suggests that this optic nerve has rim segments that are outside the normal range. Although this may represent early glaucoma, it may also be an example of the known decrease in specificity of the MRA with increasing disc size (and indeed all the statistical methods) [8, 9]. This patient has remained stable with full visual fields off treatment and illustrates the potential pitfall of over-reliance on technology or on one abnormal result. These optic nerve classifiers are meant are best used as part of the clinical context rather than as stand-alone decision-making tools.

NEURORETINAL RIM

The cup to disc ratio is a useful tool for assessing and communicating optic nerve health, but it is the remaining rim and not the cup that should be carefully examined. Focal defects may be present and may indicate glaucoma, even in the presence of a "normal" cup to disc ratio. In order to avoid the pitfall of missing focal defects, the observer must pay attention to the entire circumference of the neuroretinal rim. The ISN'T rule is a useful mnemonic for recalling the expected relative thickness of the optic nerve segments. The Inferior rim should be thickest, followed by the Superior, the Nasal and finally the Temporal rim. Fig. (4) illustrates a glaucomatous optic nerve that violates the ISN’T rule throughout the entire inferior rim, with further partial notching at 6 o’clock with an associated nerve fibre layer defect.

RETINAL NERVE FIBRE LAYER EVALUATION

The normal nerve fibre layer (NFL) can be visualized clinically, photographically or with optic nerve head analyzers such as ocular coherence tomography (OCT). The NFL can be detected clinically in most individuals, and is best appreciated using the red-free setting on the ophthalmoscope or slit-lamp. The NFL can be difficult to appreciate in the blond fundus. It appears as fine white striations radiating outwards from the optic nerve head and is normally most visible inferotemporally and superotemporally. It obscures details of the peripapillary retinal vasculature, particularly along the edges of vessels. A generalized thinning of the NFL can be best appreciated by comparison with the other half of the same fundus and with the other fundus; as well, generalized thinning can be detected by a greater prominence of the blood vessels, with sharper well-demarcated transition between vessel edge and retinal tissue. Localized NFL defects are easier to appreciate and can appear as the earliest sign of glaucomatous damage [10,11]. Although a NFL defect is not specific for glaucoma, it is pathological; therefore the presence of such a defect in an ocular hypertensive is fairly suggestive of glaucomatous damage [12].

DISC HEMORRHAGES

It is important to look for splinter or flame-shaped hemorrhages at or around the optic nerve head as a sign of glaucomatous damage [13]. Fig. (5) illustrates a glaucomatous nerve with a disc hemorrhage with associated nerve fibre layer defect. On some occasions, disc hemorrhages have been shown to precede structural changes to the disc or nerve fibre layer by a period of weeks to months [14]. However, the Ocular Hypertensive Treatment Study found that although some disc hemorrhages predict progression, most (87%) do not [15]. In addition, the Early Manifest Glaucoma Trial (EMGT) found that lowering IOP did not alter the rate of disc hemorrhage, suggesting that the presence of disc hemorrhage, rather than indicating insufficient IOP lowering, may indicate a less IOP-dependent form of glaucoma [16]. Taken together, these results again support the theme that a single individual finding cannot be interpreted without reference to the overall clinical context. For example, the presence of a disc hemorrhage would justify treating a normotensive patient with a full visual field and healthy appearing optic nerve. On the other hand, in a patient with significant glaucoma who is being followed with borderline intraocular pressures, the appearance of a disc hemorrhage might tip the balance in favor of advancing therapy.

OPTIC NERVE PALLOR

In most situations, there are clear differences between the clinical features of glaucoma and other optic neuropathies. However, on occasion, it is possible to be fooled into misdiagnosing non-glaucomatous insult, such as a compressive optic neuropathy, as glaucoma. Greenfield et al. [17]. have proposed the following criteria as suspicious for non-glaucomatous cupping in patients with pressures in the normal range: age less than 50 years, visual acuity less than 20/40, optic nerve pallor in excess of cupping, and vertically aligned visual field defects. However, Ahmed et al. [18] have reported that 6.5% of consecutive patients with what appeared to be clinically typical normal tension glaucoma were found to have a compressive optic neuropathy. They suggested that the Greenfield criteria, while specific for non-glaucomatous optic neuropathy may lack sensitivity. We apply these results in the following way. If a patient has one or more of the Greenfield criteria, they should undergo neuroimaging. However, the absence of these criteria does not rule out the presence of non-glaucomatous cupping and while we do not image everyone, we readily order neuroimaging if there is something unusual about the patient’s glaucoma, including progression at very low apparent intraocular pressures.

MYOPIA

There are several potential pitfalls with respect to evaluating glaucoma in myopes, particularly high myopes. Myopic nerves are difficult to interpret, due to optic nerve tilt that makes evaluation of the temporal nerve, as well as the superior and inferior poles, difficult. However, usually some judgement can be made about the presence or absence of rim tissue at the superior and inferior poles and a nerve with no or little tissue present superiorly or inferiorly should not be disregarded as a myopic tilted nerve. Fig. (6) illustrates a glaucomatous nerve from a highly myopic patient. Although the inferior neuroretinal rim is somewhat obscured due to the tilt, the profile of the retinal vein as it courses inferiorly suggests excavation of rim tissue. An associated nerve fibre layer defect seen clinically and on OCT imaging, along with a corresponding superior arcuate defect on the visual field lend support to the diagnosis of glaucoma.

Peripapillary atrophy can make determination of the optic disc margin difficult and can be misinterpreted as neuroretinal rim. In addition, glaucomatous cupping can be shallow and easily overlooked in a high myope. As well, the normalized databases for both visual fields and imaging technologies do not apply. Furthermore, other conditions such as myopic macular degeneration can complicate interpretation of visual fields. Finally, there are several arguments to suggest that highly myopic discs may be more susceptible to glaucomatous damage [19].

SUMMARY

Clinical evaluation of the optic nerve remains at the heart of glaucoma management, both for glaucoma diagnosis and for monitoring progression. Careful and systematic evaluation of the optic nerve is required in order to avoid potential pitfalls involving optic nerve size, focal rim defects, disc hemorrhages, and nerve fibre layer abnormalities. The reader is directed to the Jonas et al. major review of optic nerve evaluation for more detail [14]. Non-glaucomatous causes of optic neuropathy must always be considered. Finally, decisions should be based on the entire clinical picture and not on one isolated clinical or testing abnormality.

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