Clinical Applications of Anterior Segment Optical Coherence Tomography: An Updated Review

Since its introduction, optical coherence tomography (OCT) has revolutionized the field of ophthalmology and has now become an indispensable, noninvasive tool in daily practice. Most ophthalmologists are familiar with its use in the assessment and monitoring of retinal and optic nerve diseases. However, it also has important applications in the assessment of anterior segment structures, including the cornea, conjunctiva, sclera, anterior chamber, and iris, and has the potential to transform the clinical examination of these structures. In this review, we aim to provide a comprehensive overview of the potential clinical utility of anterior segment OCT (AS-OCT) for a wide range of anterior segment pathologies, such as conjunctival neoplasia, pterygium, scleritis, keratoconus, corneal dystrophies, and infectious/noninfectious keratitis. In addition, the clinical applications of AS-OCT (including epithelial mapping) in preoperative planning and postoperative monitoring for corneal and refractive surgeries are discussed.


Introduction
Advances in imaging have revolutionized the field of ophthalmology, transforming our understanding, diagnosis, and treatment of ophthalmic pathologies.Among all imaging tools, optical coherence tomography (OCT) represents one of the most significant, groundbreaking advances in ophthalmic imaging.Since its introduction in the late 1980s, OCT has evolved to become an indispensable, noninvasive tool for in vivo imaging of the ocular structures [1].Nowadays, it is considered to be a key instrument in typical clinical settings, ranging from tertiary hospitals to optometry clinics in the community [2].Most ophthalmologists would be familiar with its use in the assessment and monitoring of retinal and optic nerve diseases [3].However, it also has important applications in the assessment of the anterior segment structures including the cornea, anterior chamber, and iris.The clinical importance and applications of anterior segment OCT (AS-OCT) was first described in 1994 by Izatt et al. [4].Since then, AS-OCT has been further developed, with its function extended to a wide range of practical clinical applications.
The aim of this review is to highlight the current clinical applications of commercially available AS-OCT technologies as an integral diagnostic tool for important ocular surface pathologies.As AS-OCT becomes ubiquitous, it has the potential to revolutionize the clinical examination of anterior ocular structures, much like how the introduction of the slit lamp revolutionized the ocular examination in its time.In addition, the clinical applications of AS-OCT to other anterior segment structures such as the sclera and conjunctiva are covered, alongside AS-OCT applications for corneal and refractive surgeries.AS-OCT has also been shown to be a valuable diagnostic tool for assessing the anterior chamber angle, and iris pathologies and morphologies, though this is beyond the scope of our review [5,6].Furthermore, there has been an increasing clinical and research interest in the use of AS-OCT angiography (AS-OCTA) for various pathologies, for which detailed information can be found in recent reviews [7,8].

Technical Aspects of AS-OCT
AS-OCT is a safe imaging modality, with no reported ocular side effects to the best of our knowledge.It creates a composite image from a series of axial scans (A scans) [9].Longer wavelengths (usually around 1310 nm) are typically used for AS-OCT in comparison to retinal imaging (typically between 800 and 1050 nm); however, this varies, as shown in Table 1 below [10,11].The depth of penetration is influenced by the light scattering caused by opaque structures.As there is less scattering at longer wavelengths, the longer the wavelength, the deeper the penetration into deeper tissue structures [9].The axial  1 = 40,000 scans/s 2 = 80,000 scans/s 3 = 27,000 scans/s [5,21] 1 = 30,000 scans/s 2 = 100,000 scans/s [5] 3 = 16,640 scans/s [15] 1 = 52,000 scans/s [16] * Some measurements are specific to the posterior segment used and might vary for anterior segment OCT; ** not documented in the literature; *** technical specifications shown are for the 'Cornea Application'.This table was adapted from Azzopardi et al. [23].

Corneal Anatomy on AS-OCT Imaging
On AS-OCT imaging, the layers of the cornea appear as follows (Figure 1): 1.
The first hyper-reflective band represents the tear film with a thickness of less than 5 µm [24]; 2.
The first hyporeflective band represents the cornea epithelium with a thickness of between 50 and 70 µm; 3.
Bowman's layer (BL) is represented as a linear structure with similar hyper-reflectivity to that of the stroma; 4.
The stroma has variable hyper-reflectivity with a thickness of around 500 µm; 5.

Corneal Anatomy on AS-OCT Imaging
On AS-OCT imaging, the layers of the cornea appear as follows (Figure 1): 1.The first hyper-reflective band represents the tear film with a thickness of less than 5 µm [24]; 2. The first hyporeflective band represents the cornea epithelium with a thickness o between 50 and 70 µm; 3. Bowman's layer (BL) is represented as a linear structure with similar hyper-reflectiv ity to that of the stroma; 4. The stroma has variable hyper-reflectivity with a thickness of around 500 µm; 5.The pre-Descemet's layer (or Dua's layer (PDL)) and Descemet membrane (DM) ar shown as a hyper-reflective band of tissue.In the context of DM detachment (type 2 or mixed), PDL and DM may show as two separate hyper-reflective bands [25].On AS-OCT imaging, the layers of the bulbar conjunctiva appear as follows (Figure 2): 1.
The first hyper-reflective and hyporeflective band both represent the conjunctival epithelium; 2.
The second hyper-reflective band that underlies the conjunctival epithelium is the substantia propria; 3.
The thick hyper-reflective band represents the sclera.On AS-OCT imaging, the layers of the bulbar conjunctiva appear as follows (Figure 2) 1.The first hyper-reflective and hyporeflective band both represent the conjunctival ep ithelium; 2. The second hyper-reflective band that underlies the conjunctival epithelium is th substantia propria; 3. The thick hyper-reflective band represents the sclera.

Conjunctival Benign and Malignant Tumors
Conjunctival melanocytic naevus is the most common tumor of the conjunctiva; it typical features include childhood onset, pigmentation, location within 1 mm of the cor nea limbus in the nasal and temporal bulbar quadrant, and intralesional cysts <100 µm in diameter [26,27].One of the important indicators of benign conjunctival naevus is th presence of intrinsic cysts (Figure 3), although small cysts can be difficult to detect even with other modalities such as ultrasound biomicroscopy, computer tomography, and magnetic resonance imaging (MRI) [28].Studies have shown the superiority of AS-OCT in the provision of high-resolution imaging of conjunctival naevi, especially for the detec tion of intralesional cysts, with a higher sensitivity reported (61.4%) in comparison to tha of slit-lamp (40.3%) and ultrasound biomicroscopy (28.5%) [29,30].

Conjunctival Benign and Malignant Tumors
Conjunctival melanocytic naevus is the most common tumor of the conjunctiva; its typical features include childhood onset, pigmentation, location within 1 mm of the cornea limbus in the nasal and temporal bulbar quadrant, and intralesional cysts <100 µm in diameter [26,27].One of the important indicators of benign conjunctival naevus is the presence of intrinsic cysts (Figure 3), although small cysts can be difficult to detect even with other modalities such as ultrasound biomicroscopy, computer tomography, and magnetic resonance imaging (MRI) [28].Studies have shown the superiority of AS-OCT in the provision of high-resolution imaging of conjunctival naevi, especially for the detection of intralesional cysts, with a higher sensitivity reported (61.4%) in comparison to that of slit-lamp (40.3%) and ultrasound biomicroscopy (28.5%) [29,30].
On the other hand, the top three primary malignancies of the ocular surface and conjunctiva are ocular surface squamous neoplasia (OSSN), melanoma, and lymphoma [31,32].The typical clinical features of ocular surface squamous neoplasia (OSSN) are pearly grey mass with variable pigmentation, vascularity, and leukoplakia.On AS-OCT, the normal conjunctival epithelium can be abruptly disrupted by abnormal epithelium, characterized by thicker hyper-reflective lesions [33] (Figure 4).
In contrast to benign conjunctival naevi, the typical presentation of conjunctival melanoma is a thickened, elevated, pigmented lesion with feeder vessels, together with a surrounding area of melanosis [34,35].It usually presents in adulthood instead of childhood.On AS-OCT, there is usually normal basal epithelium, with abnormal subepithelial hyperreflectivity representing atypical melanocytes [36].In these scenarios, AS-OCT technology is however limited by the challenge of penetrating thick pigmented lesions, given that the abnormality is subepithelial [35].Penetration can be improved through the use of UHR AS-OCT, but this is not usually available outside research facilities [36].On the other hand, the top three primary malignancies of the ocular surface and conjunctiva are ocular surface squamous neoplasia (OSSN), melanoma, and lymphoma [31,32].The typical clinical features of ocular surface squamous neoplasia (OSSN) are pearly grey mass with variable pigmentation, vascularity, and leukoplakia.On AS-OCT, the normal conjunctival epithelium can be abruptly disrupted by abnormal epithelium, characterized by thicker hyper-reflective lesions [33] (Figure 4).On the other hand, the top three primary malignancies of the ocular surface and conjunctiva are ocular surface squamous neoplasia (OSSN), melanoma, and lymphoma [31,32].The typical clinical features of ocular surface squamous neoplasia (OSSN) are pearly grey mass with variable pigmentation, vascularity, and leukoplakia.On AS-OCT, the normal conjunctival epithelium can be abruptly disrupted by abnormal epithelium, characterized by thicker hyper-reflective lesions [33] (Figure 4).Lastly, conjunctival lymphoma is characterized by a conjunctival mass, salmon-pink in color, smooth and multilobulated, with the presence of feeder vessels.It can also sometimes mimic follicular and papillary conjunctivitis [37].On AS-OCT, it shows up as a homogenous, dark subepithelial lesion with smooth borders, containing monomorphic dot-like infiltrates [38] (Figure 5).
anoma is a thickened, elevated, pigmented lesion with feeder vessels, together with a surrounding area of melanosis [34,35].It usually presents in adulthood instead of childhood.On AS-OCT, there is usually normal basal epithelium, with abnormal subepithelial hyperreflectivity representing atypical melanocytes [36].In these scenarios, AS-OCT technology is however limited by the challenge of penetrating thick pigmented lesions, given that the abnormality is subepithelial [35].Penetration can be improved through the use of UHR AS-OCT, but this is not usually available outside research facilities [36].
Lastly, conjunctival lymphoma is characterized by a conjunctival mass, salmon-pink in color, smooth and multilobulated, with the presence of feeder vessels.It can also sometimes mimic follicular and papillary conjunctivitis [37].On AS-OCT, it shows up as a homogenous, dark subepithelial lesion with smooth borders, containing monomorphic dotlike infiltrates [38] (Figure 5).

Pterygium, Pinguecula, Pseudopterygium, and Salzmann Nodular Degeneration
Pterygium is one of the commonest ocular surface diseases, resulting from the growth of subepithelial fibrovascular tissue originating from the bulbar conjunctiva, which eventually encroaches on the cornea, and is often associated with UV exposure [40,41].Its prevalence is estimated to be up to 10 percent globally, with significant geographical variations [42].Pinguecula, on the other hand, presents as a raised yellowish growth of the conjunctiva, with deposition of elastic-like material [43].As it encroaches onto the cornea, it can transform into pterygium.The prevalence of pinguecula can be close to 50 percent in some populations [44][45][46][47].Salzmann nodular degeneration (SND) is another slowly progressive, degenerative ocular surface disease characterized by whitish nodule(s) of the corneal subepithelial layer (anterior to the Bowman's layer).
On AS-OCT, pterygium tissues appear as a subepithelial hyper-reflective lesion from the conjunctiva with extension into the cornea, with separation of the cornea epithelium from BM [48].Pinguecula would have a similar appearance, only stopping short at the corneal limbus without extension into the cornea.Similarly, SND appears as a hyper-reflective lesion on the cornea limited to the subepithelial corneal layer (Figure 6).

Pterygium, Pinguecula, Pseudopterygium, and Salzmann Nodular Degeneration
Pterygium is one of the commonest ocular surface diseases, resulting from the growth of subepithelial fibrovascular tissue originating from the bulbar conjunctiva, which eventually encroaches on the cornea, and is often associated with UV exposure [40,41].Its prevalence is estimated to be up to 10 percent globally, with significant geographical variations [42].Pinguecula, on the other hand, presents as a raised yellowish growth of the conjunctiva, with deposition of elastic-like material [43].As it encroaches onto the cornea, it can transform into pterygium.The prevalence of pinguecula can be close to 50 percent in some populations [44][45][46][47].Salzmann nodular degeneration (SND) is another slowly progressive, degenerative ocular surface disease characterized by whitish nodule(s) of the corneal subepithelial layer (anterior to the Bowman's layer).
On AS-OCT, pterygium tissues appear as a subepithelial hyper-reflective lesion from the conjunctiva with extension into the cornea, with separation of the cornea epithelium from BM [48].Pinguecula would have a similar appearance, only stopping short at the corneal limbus without extension into the cornea.Similarly, SND appears as a hyperreflective lesion on the cornea limited to the subepithelial corneal layer (Figure 6).
In contrast with pterygium, pseudopterygium is characterized as a nonprogressive conjunctival adhesion to the peripheral cornea secondary to cornea limbal damage from chemical injury or chronic inflammation [49].It can occur at any conjunctival quadrant, unlike pterygium, which has a predilection to arise from the nasal conjunctiva.Pseudopterygium is usually nonadherent to the limbus and has edges that can be elevated, under which a probe can be passed through.In clinical practice, this test might be difficult to perform due to patient discomfort.On AS-OCT, pseudopterygium is visualized as an overgrowing membrane that is not attached to the underlying cornea [48].In contrast with pterygium, pseudopterygium is characterized as a nonprogressive conjunctival adhesion to the peripheral cornea secondary to cornea limbal damage from chemical injury or chronic inflammation [49].It can occur at any conjunctival quadrant, unlike pterygium, which has a predilection to arise from the nasal conjunctiva.Pseudopterygium is usually nonadherent to the limbus and has edges that can be elevated, under which a probe can be passed through.In clinical practice, this test might be difficult to perform due to patient discomfort.On AS-OCT, pseudopterygium is visualized as an overgrowing membrane that is not attached to the underlying cornea [48].

Episcleritis and Scleritis
Scleritis is a potentially sight-threatening inflammation of the sclera [50].In anterior scleritis, there is involvement of both the superficial and deep episcleral capillary network.Comparatively, episcleritis is typically a self-limiting condition affecting only the superficial capillary network.While pain is the hallmark symptom of scleritis, clinical examination to differentiate between the two can be difficult due to overlapping features [51].A common test used is topical 10% phenylephrine, which causes blanching of the superficial vessels in episcleritis.Other clinical differentiating signs include a distinct red hue in episcleritis versus a bluish-violet hue in scleritis [51].Clinical assessment is however still subjective and not always straightforward.
On AS-OCT, episcleritis tends to appear with increased episcleral and episcleral network thickness, with minimal changes in scleral thickness.However, the total combined thickness of the conjunctiva, episcleral, and sclera can be increased in both episcleritis and scleritis (Figure 7) [52].The key difference that points toward a diagnosis of scleritis is an increase in hyporeflective spaces at variable depths, corresponding to dilated superficial and deep episcleral blood vessels [53].Correlation with clinical exam is important, as greater dilated blood vessels on clinical exam reflect larger hyporeflective spaces on AS-OCT.

Clinical Applications for Scleral Diseases Episcleritis and Scleritis
Scleritis is a potentially sight-threatening inflammation of the sclera [50].In anterior scleritis, there is involvement of both the superficial and deep episcleral capillary network.Comparatively, episcleritis is typically a self-limiting condition affecting only the superficial capillary network.While pain is the hallmark symptom of scleritis, clinical examination to differentiate between the two can be difficult due to overlapping features [51].A common test used is topical 10% phenylephrine, which causes blanching of the superficial vessels in episcleritis.Other clinical differentiating signs include a distinct red hue in episcleritis versus a bluish-violet hue in scleritis [51].Clinical assessment is however still subjective and not always straightforward.
On AS-OCT, episcleritis tends to appear with increased episcleral and episcleral network thickness, with minimal changes in scleral thickness.However, the total combined thickness of the conjunctiva, episcleral, and sclera can be increased in both episcleritis and scleritis (Figure 7) [52].The key difference that points toward a diagnosis of scleritis is an increase in hyporeflective spaces at variable depths, corresponding to dilated superficial and deep episcleral blood vessels [53].Correlation with clinical exam is important, as greater dilated blood vessels on clinical exam reflect larger hyporeflective spaces on AS-OCT.

Keratoconus
In 1844, the physician James Pickford wrote, 'There is probably no disease to which the eye is subject, hitherto so rebellious to medicine, so intractable in its natures, and, at the same time, so fatal to vision, as conical cornea…the pathology and treatment of which

Clinical Applications for Corneal Diseases 6.1. Keratoconus
In 1844, the physician James Pickford wrote, 'There is probably no disease to which the eye is subject, hitherto so rebellious to medicine, so intractable in its natures, and, at the same time, so fatal to vision, as conical cornea. ..the pathology and treatment of which are so little understood [54]'.
More than a century and a half later, we understand keratoconus as a noninflammatory bilateral, asymmetric ocular disease that causes astigmatism and impaired vision as a result of progressive corneal thinning and steepening [22,55].Due to substantial global variation, the prevalence of keratoconus is estimated to be between 0.2 and 4790 per 100,000 people, with a predilection for people between their 20s and 30s [55].Variability between different epidemiological studies have been attributed to differences in geography, ethnicity, keratoconus definition and diagnostic criteria, study design, and the age and cohort of subjects assessed [55].
The clinical features of keratoconus on slit-lamp examination have been well chronicled, including numerous clinical/eponymous signs such as a scissoring reflex during retinoscopy, Munson's sign (deformation of the lower eyelid on downgaze due to protrusion of the cornea, Rizzuti's sign (nasal limbus reflection that appears following the direction light at the temporal limbus), Fleischer's ring (subepithelial deposition of iron oxide hemosiderin around the base of the cone), Vogt's striae (vertical stress lines within the posterior stroma of the cornea that disappears with digital pressure), and oil droplet reflex (a dark shadow appearance in the midperiphery of the cornea on retroillumination) [56].
The early detection of keratoconus can lead to improved patient outcomes, with timely reviews to monitor disease progression and appropriate interventions with corneal crosslinking when indicated [57][58][59][60].With certain machines, AS-OCT technology can generate a quantitative pachymetry map with parameters including keratometry, inferior-superior (I-S) dioptric value, and multivariate indexes such as KISA% [61].In keratoconus, the typical characteristics include thinner-than-average corneas with inferior focal thinning [61].The clinical use of AS-OCT-based pachymetry mapping is supported by the good intertest concordance with other modalities, including ultrasound pachymetry and Scheimpflugbased instruments such as the Pentacam (Oculus, Wetzlar, Germany) [62,63].However, AS-OCT has been reported to have a better repeatability of the anterior corneal parameters in mild-to-moderate keratoconus as well as posterior corneal parameters in both normal and keratoconic eyes [64].In addition, AS-OCT-based epithelial mapping has been increasingly shown to be a useful diagnostic test for detecting early keratoconus, as discussed later [63,65].
One of the severe complications of keratoconus is the development of acute corneal hydrops, which is due to a spontaneous break in the PDL/DM, resulting in the imbibition of the anterior chamber aqueous fluid into the cornea stroma [66][67][68][69] (Figure 8).In serious cases of acute corneal hydrops, scar tissue can impair visual acuity and might necessitate treatment with scleral contact lenses or even corneal transplant [70,71].On AS-OCT, the integrity of the PDL/DM can be visualized and characterized based on parameters such as the size of the break, the depth of the detachment (which is the distance between the posterior cornea and detached DM), the corneal thickness, and the varying degree of involvement of the PDL and DM [25,72,73].The capture of these parameters upon initial presentation of acute hydrops might guide further management by corneal specialists, as it has been suggested that eyes with deeper DM detachment, larger breaks, and the presence of large intrastromal clefts have poorer prognosis and require a longer time for the resolution of corneal edema [72,74].
posterior cornea and detached DM), the corneal thickness, and the varying degree of involvement of the PDL and DM [25,72,73].The capture of these parameters upon initial presentation of acute hydrops might guide further management by corneal specialists, as it has been suggested that eyes with deeper DM detachment, larger breaks, and the presence of large intrastromal clefts have poorer prognosis and require a longer time for the resolution of corneal edema [72,74].

Corneal Dystrophy
Corneal dystrophy refers to a group of corneal disease that are typically bilateral, symmetrical, slowly progressive, and independent of environmental and systemic factors [75].It is now classified based on the IC3D classification, with dystrophies classified according to the affected layers, namely, epithelial, subepithelial, BM, stromal, DM, and endothelial dystrophies.These can also be grouped together based on known, common genetic bases [76].
Prior to the development of the slit lamp, the examination of the cornea was limited.Even with the slit lamp, the differential diagnosis of corneal dystrophies is challenging due to similarities in clinical phenotypes.The ability of AS-OCT to discriminate between the corneal layers in almost histological detail marks another potential breakthrough in the diagnosis of corneal dystrophies [77].However, their precise diagnosis still requires significant clinical correlation.

Infectious and Noninfectious Keratitis
Another major application of AS-OCT in clinical practice is the diagnosis and management of keratitis.In keratitis, inflammatory cells infiltrate the different corneal layers in response to noxious stimuli.This is often associated with corneal edema and ciliary congestion and can lead to the suppurative melting of the corneal epithelium and stroma, with the formation of ulcers and the loss of corneal clarity.Corneal opacification is the fifth leading cause of blindness globally, with approximately 6 million people worldwide

Corneal Dystrophy
Corneal dystrophy refers to a group of corneal disease that are typically bilateral, symmetrical, slowly progressive, and independent of environmental and systemic factors [75].It is now classified based on the IC3D classification, with dystrophies classified according to the affected layers, namely, epithelial, subepithelial, BM, stromal, DM, and endothelial dystrophies.These can also be grouped together based on known, common genetic bases [76].
Prior to the development of the slit lamp, the examination of the cornea was limited.Even with the slit lamp, the differential diagnosis of corneal dystrophies is challenging due to similarities in clinical phenotypes.The ability of AS-OCT to discriminate between the corneal layers in almost histological detail marks another potential breakthrough in the diagnosis of corneal dystrophies [77].However, their precise diagnosis still requires significant clinical correlation.

Infectious and Noninfectious Keratitis
Another major application of AS-OCT in clinical practice is the diagnosis and management of keratitis.In keratitis, inflammatory cells infiltrate the different corneal layers in response to noxious stimuli.This is often associated with corneal edema and ciliary congestion and can lead to the suppurative melting of the corneal epithelium and stroma, with the formation of ulcers and the loss of corneal clarity.Corneal opacification is the fifth leading cause of blindness globally, with approximately 6 million people worldwide thought to suffer from cornea-related moderate or severe visual impairment [78,79].The commonest form of keratitis is infectious keratitis (IK), which is the commonest cause for corneal blindness in both developed and developing countries [80][81][82].Other noninfectious causes of keratitis include inflammation, autoimmune reactions, degeneration, and nutritional deficiencies.
Traditionally, keratitis is diagnosed and monitored using a slit lamp by serially assessing the site and size of infiltrates and stromal ulceration [83].However, evaluation of the depth and extent of pathologic features is subjective and depends significantly on the examiner's experience, therefore limiting the reliability and consistency of the interpretation of disease progression and treatment response.This has been aided in recent years through the increased use of anterior segment serial photography, with a potential role for developing deep learning algorithms in the future [84,85].
AS-OCT has the potential to transform the way we manage IK by providing a more reliable and objective method of quantifying and monitoring the disease process [86].Through the use of caliper tools provided by software, it enables the accurate determination and evaluation of the depth and extent of corneal ulceration, infiltrate (visualized as a hyper-reflective area in the stroma), and haze [5,25,[87][88][89][90][91].This is especially useful in scenarios when necrotic tissues or infiltrate obscure the view of the underlying tissues.The most commonly used measurements are the stromal infiltration thickness (IT) and the corneal thickness (CT).By adhering to the same scanning protocols, serial scans can be taken through the same affected corneal areas, allowing objective monitoring of the CT and IT throughout the disease course.In the initial stages of IK, even mild cases seem to have a thick CT in the infiltrated area, which decreases as the infection resolves, along with the IT.
The infiltration can also be qualitatively assessed using AS-OCT, since the intensity of hyper-reflectivity corresponds to the density of the infiltration on slit lamp.However, it is important to interpret AS-OCT findings in the clinical context, as a decreasing CT might not always mean the resolution of infection.For example, if stromal necrosis occurs, such as with fungal keratitis and chronic bacterial keratitis, severe corneal thinning could be mistaken as an 'improving' CT.This is an ominous sign of impending corneal perforation, and this thinning can be detected on AS-OCT before it is apparent on slit-lamp examination (Figure 9).Furthermore, AS-OCT is also able to detect IT thickening before clinical deterioration, emphasizing that when used appropriately, AS-OCT can provide vital information on not only IK improvement but also on deterioration and the risk of corneal perforation [87].
sessing the site and size of infiltrates and stromal ulceration [83].However, evaluation of the depth and extent of pathologic features is subjective and depends significantly on the examiner's experience, therefore limiting the reliability and consistency of the interpretation of disease progression and treatment response.This has been aided in recent years through the increased use of anterior segment serial photography, with a potential role for developing deep learning algorithms in the future [84,85].
AS-OCT has the potential to transform the way we manage IK by providing a more reliable and objective method of quantifying and monitoring the disease process [86].Through the use of caliper tools provided by software, it enables the accurate determination and evaluation of the depth and extent of corneal ulceration, infiltrate (visualized as a hyper-reflective area in the stroma), and haze [5,25,[87][88][89][90][91].This is especially useful in scenarios when necrotic tissues or infiltrate obscure the view of the underlying tissues.The most commonly used measurements are the stromal infiltration thickness (IT) and the corneal thickness (CT).By adhering to the same scanning protocols, serial scans can be taken through the same affected corneal areas, allowing objective monitoring of the CT and IT throughout the disease course.In the initial stages of IK, even mild cases seem to have a thick CT in the infiltrated area, which decreases as the infection resolves, along with the IT.
The infiltration can also be qualitatively assessed using AS-OCT, since the intensity of hyper-reflectivity corresponds to the density of the infiltration on slit lamp.However, it is important to interpret AS-OCT findings in the clinical context, as a decreasing CT might not always mean the resolution of infection.For example, if stromal necrosis occurs, such as with fungal keratitis and chronic bacterial keratitis, severe corneal thinning could be mistaken as an 'improving' CT.This is an ominous sign of impending corneal perforation, and this thinning can be detected on AS-OCT before it is apparent on slit-lamp examination (Figure 9).Furthermore, AS-OCT is also able to detect IT thickening before clinical deterioration, emphasizing that when used appropriately, AS-OCT can provide vital information on not only IK improvement but also on deterioration and the risk of corneal perforation [87].Additional features of IK that can be captured using AS-OCT include inflammatory cells/fibrin in the anterior chamber (AC), which appear as hyper-reflective cells (Figure 10), and retro-corneal pathology such as endothelial inflammatory plaques, typical of fungal keratitis [88,92,93] (Figure 11).The presence of these plaques often interferes with the accurate identification of the corneal layers and thus IT and CT measurement.However, by using AS-OCT, these plaques can be measured and monitored on serial scans as an alternative indicator of disease evolution.The extent of stromal edema, visualized as diffuse stromal thickening that changes the convexity of the posterior corneal surface, can also be assessed with AS-OCT, along with the presence of DM folds (ruffles in the usually smooth corneal endothelium) [87].All this confirms that serial AS-OCT scans allow objective measurement of the disease and treatment response through both quantitative and qualitative information.
gal keratitis [88,92,93] (Figure 11).The presence of these plaques often interferes with the accurate identification of the corneal layers and thus IT and CT measurement.However, by using AS-OCT, these plaques can be measured and monitored on serial scans as an alternative indicator of disease evolution.The extent of stromal edema, visualized as diffuse stromal thickening that changes the convexity of the posterior corneal surface, can also be assessed with AS-OCT, along with the presence of DM folds (ruffles in the usually smooth corneal endothelium) [87].All this confirms that serial AS-OCT scans allow objective measurement of the disease and treatment response through both quantitative and qualitative information.10), and retro-corneal pathology such as endothelial inflammatory plaques, typical of fungal keratitis [88,92,93] (Figure 11).The presence of these plaques often interferes with the accurate identification of the corneal layers and thus IT and CT measurement.However, by using AS-OCT, these plaques can be measured and monitored on serial scans as an alternative indicator of disease evolution.The extent of stromal edema, visualized as diffuse stromal thickening that changes the convexity of the posterior corneal surface, can also be assessed with AS-OCT, along with the presence of DM folds (ruffles in the usually smooth corneal endothelium) [87].All this confirms that serial AS-OCT scans allow objective measurement of the disease and treatment response through both quantitative and qualitative information.AS-OCT might also be of use in differentiating between different forms of IK [89,94].For example, localized and diffuse stromal cystic spaces caused by stromal necrosis can be observed in fungal keratitis, along with endothelial plaques, as mentioned above [92,95].In Acanthamoeba keratitis (AK), AS-OCT provides detailed visual images of radial keratoneuritis and perineural infiltrates, which appear as hyper-reflective bands in the corneal stroma of varying widths (20-200 µm) and depths (subepithelial to mid-stroma) [23,96,97].AS-OCT also seems to be helpful in differentiating AK from herpetic keratitis, in which these hyper-reflective bands are predominantly observed in the subepithelial zone [97].Furthermore, the common whitish, raised, epithelial lesions of ocular microsporidiosis can also be observed with AS-OCT as hyper-reflective epithelial lesions, rising above the epithelial surface.This aids in the differentiation from adenoviral nummular scars (hyper-reflective lesions starting from the subepithelial corneal layer and extending slightly into the anterior stroma, without elevations above the epithelium) [98,99].Finally, in Cytomegalovirus (CMV) corneal endotheliitis, irregularly thickened hyper-reflective coin-shaped lesions have been observed at the endothelial surface, along with protruding hyper-reflective structures at the posterior cornea with a dendritic, dome-shaped, quadrangular, or saw-tooth appearance [100,101].All these AS-OCT features could be used clinically to aid or confirm diagnosis and monitor response to treatment.
Another important infection that can affect the cornea is viral keratoconjunctivitis, a common, contagious infectious eye disease that is often caused by adenovirus.There are studies that have reported its prevalence to be up to 60% of patients presenting with a diagnosis of infectious keratoconjunctivitis [102,103].One of its sequelae is the presence of nonstaining subepithelial infiltrates, which can persist even after the resolution of the acute episode [104].Subepithelial infiltrates are thought to be due to immune hypersensitivity, which can then persist and form irreversible scars [105].The treatment for this is usually a trial of topical steroids, with some evidence for the use of topical ciclosporin [106].The use of AS-OCT in this clinical circumstance lies in its ability to discern subepithelial infiltrates that are potentially reversible [107].

Corneal Foreign Bodies
Corneal foreign bodies are a common type of ocular injury presenting with eye casualty.In the UK, it is estimated that there are 2.7 cases of corneal foreign body per 1000 population presenting to primary care [108].In certain major industries such as car manufacturing, superficial corneal foreign body accounts for up to 70% of work-related injuries [109].While most corneal foreign bodies are superficial and can be easily removed under a slit lamp, in certain cases, corneal foreign bodies can be deeply embedded and difficult to visualize due to corneal edema.The utility of AS-OCT in these cases would be to correctly identify the depth of the foreign body so that an appropriate removal method can be planned.Celebi et al. documented a case whereby AS-OCT demonstrated shadowing of the corneal layers, denoting the location of the corneal foreign body [110].The corneal foreign body was subsequently removed externally as AS-OCT showed that it was not a full-thickness penetration.There are also studies that have shown that AS-OCT can provide clues about the distinguishing characteristics of foreign bodies, for example, opaque materials such as metal and wood tend to have a hyper-reflective anterior border, with posterior border signals blocked from the shadowing effect.With metal foreign bodies, there is also the appearance of a "mirror effect" with hyper-reflective signals either aligned or inverted with the direction of the foreign body, while transparent materials such as plastic and glass can have both hyper-and hyporeflective signals [111,112].

Epithelial Thickness Mapping in Corneal Disease
The corneal epithelium accounts for 1.03 D of the total corneal refractive power at the central 2 mm zone and 0.85 D of the total corneal refractive power over a 3.6 mm zone, with even the subtlest changes in epithelial thickness (ET) and morphology resulting in significant refractive changes [113].The ET profile is nonuniform, with corneal epithelium being thicker inferiorly than superiorly and nasally than temporally, which is thought to be due to eyelid forces and blinking action on the superior cornea [114,115].
ET and stromal thicknesses (ST) have been measured with several devices, including high-frequency, scanning ultrasound biomicroscopy and in vivo confocal microscopy (IVCM) [116,117].AS-OCT has been shown to provide good, repeatable, and reproducible corneal epithelial thickness mapping (ETM) in both normal and diseased corneas, through all map zones, with newer generations providing ETM over a larger zone [118,119].The corneal ET maps can be subdivided into a total of seventeen zones: one central 2 mm diameter zone, eight 3 mm wide paracentral zones, and eight 1 mm wide outer peripheral zones.Through ETM, AS-OCT is also able to measure various other parameters such as minimum CT, minimum-median CT, inferior-superior ET difference, minimum-maximum ET difference, and standard deviation (SD) of the ET [120].
ETM, through the use of AS-OCT, has a wide range of clinical utility.As mentioned above, ETM can be used to diagnose early, subclinical keratoconus, which can be easily missed.The epithelium thins in the area over the cone and thickens around it (epithelial doughnut pattern), while as the disease progress, excessive epithelial thinning can occur [121].Thus, ETM can be a valuable tool for monitoring progression alongside corneal tomography (such as Pentacam).Similarly, postectasia epithelial changes resemble those seen in keratoconus [120,122].ETM can also help in differentiating contact-lens-induced warpage from keratoconus progression; as the former also leads to inferior steepening, it results in a thicker rather than thinner (as would happen with progressing keratoconus) epithelium [120].
ETM also has diagnostic and monitoring value in various ocular surface diseases.For example, in patients with dry eye disease as well as atopic disease, the ET decreases throughout the cornea, whereas in epithelial basement membrane dystrophy (EBMD), it thickens the central and inferior corneal areas [123][124][125].Limbal stem cell deficiency (LSCD) is another corneal disorder that significantly affects the epithelium.In their study, Levy et al. found that ETM in LSCD was associated with a spoke-wheel pattern, a maximum to minimum ET difference greater than 14 µm, and an ET standard deviation greater than 5 µm [126].
The AS-OCT findings of these ocular surface diseases are also summarized in Table 2.
Table 2. AS-OCT features of various ocular surface diseases.

Pterygium
• Subepithelial hyper-reflective lesion from the conjunctiva with extension into the cornea, with separation of the cornea epithelium from BM [48].

Pinguecula
• Subepithelial hyper-reflective lesion from the conjunctiva without extension into the cornea (stops short at the corneal limbus).

Salzmann nodular degeneration
• Hyper-reflective lesion on the cornea limited to the subepithelial corneal layer.

Pseudopterygium
• Overgrowing membrane that is not attached to the underlying cornea [48].

Scleritis
• Increase in hyporeflective spaces at variable depths, corresponding to dilated superficial and deep episcleral blood vessels [53].

•
Total combined thickness of the conjunctiva, episcleral and sclera can be increased.

Disease AS-OCT Features
Acute corneal hydrops

•
Integrity of the PDL/DM and the break can be visualized and characterized, based on parameters such as the size of the break, the depth of the detachment (which is the distance between the posterior cornea and detached DM), the corneal thickness, and the varying degree of involvement of PDL and DM [25,72,73].
Infectious keratitis

•
Qualitative assessment of infiltrate: intensity of hyper-reflectivity of infiltrate corresponds to the density of the infiltration on slit lamp; infiltrate thickening picked up before clinical deterioration [87].

•
Improving infection with improving infiltrate thickness and corneal thickness.

•
Hyper-reflective inflammatory cells/fibrin in the anterior chamber • Stromal edema, visualized as diffuse stromal thickening that changes the convexity of the posterior corneal surface, along with the presence of DM folds (ruffles in the usually smooth corneal endothelium) [87].
Differentiation of different form of infectious keratitis: • Fungal keratitis-localized and diffuse stromal cystic spaces caused by stromal necrosis, along with endothelial inflammatory plaques [92,95].

•
Adenoviral keratoconjunctivitis-hyper-reflective lesions starting from the subepithelial corneal layer and extending slightly into the anterior stroma, without elevations above the epithelium [98,99].

•
Cytomegalovirus corneal endotheliitis-irregularly thickened hyper-reflective coin-shaped lesions at the endothelial surface, along with protruding hyper-reflective structures at the posterior cornea with a dendritic, dome-shaped, quadrangular, or saw-tooth appearance [100,101].

Corneal foreign body
• Shadowing of the corneal layers denoting the location of the corneal foreign body [110].

•
Clues about the distinguishing characteristics of foreign bodies, for example, opaque materials such as metal and wood tend to have a hyper-reflective anterior border, with posterior border signals blocked from shadowing effect.With metal foreign bodies, there is also the appearance of a 'mirror effect' with hyper-reflective signals either aligned or inverted with the direction of the foreign body, whereas transparent materials such as plastic and glass can have both hyper-and hyporeflective signals [111,112].

Clinical Applications in Corneal and Refractive Surgeries
AS-OCT is playing an increasing role in the preoperative and intraoperative stages of cornea surgery due to its ability to discern the different layers, especially in the context of corneal transplantation [127].The general ophthalmologists and eye care health professionals would most likely encounter postsurgical cornea patients in an urgent care setting, where AS-OCT can be used as an important diagnostic tool.

Keratoplasty
Penetrating keratoplasty (PKP) was until recently the commonest type of corneal transplantation performed in the UK, though there has been a shift toward the less invasive partial thickness or lamellar keratoplasty techniques in recent years [128][129][130][131].In fact, Descemet's stripping automated endothelial keratoplasty (DSAEK) is nowadays considered to be the most common corneal transplantation technique in the UK, accounting for 33% of all cases of corneal transplant in the period of 2019-2020 [132].Other lamellar keratoplasty techniques include deep anterior lamellar keratoplasty (DALK; 9.3% of all cases in 2019-2020) and Descemet membrane endothelial keratoplasty (DMEK; 23.1% of all cases in 2019-2020) [132].
PKP surgery involves the alignment of the host and donor cornea.AS-OCT provides details of the graft-host junction for both the anterior and posterior interface.In a study by Kaiserman et al. using AS-OCT to examine the wound configuration of patients after PKP, up to 60.8% of graft-host junctions had internal graft-host malappositions such as gapes, steps, or protrusions [133].This is despite all the graft-host junction having a continuous smooth epithelial surface.They also observed a correlation between the extent of malapposition and degree of refractive error.Recently, AS-OCT has also been shown to recognize and characterize graft-host ectasia in post-PK eyes.It was found that a ratio of the lowest corneal thickness at the interface to central corneal thickness of ≤0.7 is associated with a significantly higher chance (2.4 times) of clinically detectable ectasia [134].
The leading causes of corneal allograft failure are graft rejection and infection [135][136][137].The clinical signs of corneal graft rejection may include conjunctival injection, epithelial rejection line, nummular subepithelial infiltrates, corneal edema, corneal vascularization, keratic precipitates, endothelial rejection line (Khodadoust line), and/or anterior chamber inflammatory activity [138].With the use of AS-OCT, corneal edema can be monitored objectively using its pachymetry tool.In addition, subepithelial infiltrates, stromal thickening, and keratic precipitates can be directly visualized (Figure 12).There are suggestions that acute graft rejection can present on AS-OCT as stromal thickening and posterior corneal surface undulation [139].Following treatment with topical and systemic steroids, the stromal thickness decreases, with the corresponding resolution of the posterior undulations.In contrast, patients with chronic graft failure are likely to have persistent stromal thickening refractory to steroid therapy, with a smooth posterior corneal surface.
DALK is a form of lamellar keratoplasty that selectively replaces the anterior part of the cornea, sparing the healthy DM and endothelium.This technique relies on the separation of the stroma from the DM, with the big bubble technique developed by Anwar and Teichmann being one of the more popular approaches [140].Following DALK surgery, AS-OCT can provide high-resolution imaging of the graft-host junction as well as the graft-host interface, enabling the assessment of complications such as DM nonattachment.DM nonattachment following DALK (similar to DM detachment) can be difficult to identify accurately on slit lamp due to epithelial and stromal swelling.Advantageously, AS-OCT can provide detailed information such as the configuration of the nonattachment, as well as whether it is local (less than 1/3 of the corneal surface) or extensive (more than 1/3 of the cornea surface) [141].
On the other hand, DSAEK and DMEK are posterior lamellar keratoplasty techniques in which the recipient's diseased DM and endothelium are replaced.In traditional DSAEK, diseased endothelium is replaced with donor tissue comprising a thin layer of posterior stroma, DM, and endothelium.The DSAEK tissue is usually around 150-200 µm, although ultrathin DSAEK can be as thin as ~80 µm [142].Comparatively, DMEK is a newer technique that only transplants the DM and endothelium and is only about 10-15 µm in thickness [143][144][145][146].In both DSAEK and DMEK, one of the potential complications is graft detachment [147][148][149][150][151]. Similar to what we described for DALK above, the status of the donor and host interface has been historically monitored using slit-lamp examination, which can be challenging in the immediate postoperative period due to corneal edema from chronical endothelial failure.The benefit of AS-OCT is that it can visualize the donor-host interface and provide information on donor apposition and the extent of DM detachment, thereby guiding the need and techniques for rebubbling (if indicated) [149,152] (Figure 13).Studies have shown that AS-OCT performed at 1 h and 1 week after DMEK surgery was able to facilitate the visualization of the extent of DMEK graft attachment and the decision making on rebubbling of the graft [153].For instance, the presence of large graft detachment (>33% of the total graft surface) 1 h postoperatively is associated with a 75% chance of persistent large or complete graft detachment at 6 months.DALK is a form of lamellar keratoplasty that selectively replaces the anterior part of the cornea, sparing the healthy DM and endothelium.This technique relies on the separation of the stroma from the DM, with the big bubble technique developed by Anwar and Teichmann being one of the more popular approaches [140].Following DALK surgery, AS-OCT can provide high-resolution imaging of the graft-host junction as well as the graft-host interface, enabling the assessment of complications such as DM nonattachment.DM nonattachment following DALK (similar to DM detachment) can be difficult to identify accurately on slit lamp due to epithelial and stromal swelling.Advantageously, AS-OCT can provide detailed information such as the configuration of the nonattachment, as well as whether it is local (less than 1/3 of the corneal surface) or extensive (more than 1/3 of the cornea surface) [141].
On the other hand, DSAEK and DMEK are posterior lamellar keratoplasty techniques in which the recipient's diseased DM and endothelium are replaced.In traditional DSAEK, diseased endothelium is replaced with donor tissue comprising a thin layer of posterior stroma, DM, and endothelium.The DSAEK tissue is usually around 150-200 µm, although ultrathin DSAEK can be as thin as ~80 µm [142].Comparatively, DMEK is a newer technique that only transplants the DM and endothelium and is only about 10-15 µm in thickness [143][144][145][146].In both DSAEK and DMEK, one of the potential complications is graft detachment [147][148][149][150][151]. Similar to what we described for DALK above, the status of the donor and host interface has been historically monitored using slit-lamp examination, which can be challenging in the immediate postoperative period due to corneal edema from chronical endothelial failure.The benefit of AS-OCT is that it can visualize the donor-host interface and provide information on donor apposition and the extent of DM detachment, thereby guiding the need and techniques for rebubbling (if indicated) [149,152] (Figure 13).Studies have shown that AS-OCT performed at 1 h and 1 week after DMEK surgery was able to facilitate the visualization of the extent of DMEK graft attachment and the decision making on rebubbling of the graft [153].For instance, the presence of large graft detachment (>33% of the total graft surface) 1 h postoperatively is associated with a 75% chance of persistent large or complete graft detachment at 6 months.AS-OCT can also be employed to visualize and monitor the progression of interface infectious keratitis (Figure 14), which is a distinct and challenging clinical entity following lamellar keratoplasty [154][155][156].AS-OCT can also be employed to visualize and monitor the progression of interface infectious keratitis (Figure 14), which is a distinct and challenging clinical entity following lamellar keratoplasty [154][155][156].suturing of the glaucoma tube.
AS-OCT can also be employed to visualize and monitor the progression of interface infectious keratitis (Figure 14), which is a distinct and challenging clinical entity following lamellar keratoplasty [154][155][156].

Refractive Surgery
According to a refractive surgery market report, the global demand for refractive surgical procedures is estimated as growing at a compound rate of 9.6% from 2020 to 2025, with the number of procedures increasing from 3.6 million to 5.8 million [157].
Laser in situ keratomileusis (LASIK) remains one of the most commonly performed corneal refractive procedures [158,159].The LASIK technique involves the creation of a 'hinged' flap before performing excimer laser ablation on the corneal stromal bed [160,161].Although LASIK has a well-documented safety profile, one of the complications is interface fluid syndrome, which is the presence of liquid at the LASIK flap interface [162].This can be associated with steroid-induced raised intraocular pressure, endothelial decompensation, and other pathophysiologic processes, which result in cornea edema and can occur weeks and months after LASIK procedures [162].Clinically, it can be challenging to diagnose due to its appearance as diffuse corneal haze, which can mimic diffuse lamellar keratitis [163].AS-OCT confers the advantage of confirming the diagnosis of interface fluid syndrome by demonstrating hyporeflective fluid at the flap interface [9,164].
Another potential complication of LASIK is flap displacement/dislocation.This can be easily missed on slit-lamp examination due to the difficulty in identifying the flap edge.There have been several case reports that have demonstrated the superiority of AS-OCT in detecting flap gaps [91,165].Ting and Danjoux reported three cases of lateonset (7-14 years postoperatively) traumatic dislocation of LASIK flaps, all with delayed diagnosis and management [91].All three had signs detected on AS-OCT: two with an infolded flap and one with epithelial ingrowth.AS-OCT can also be utilized to identify and monitor the progression and treatment response for epithelial ingrowth [166] (Figure 15).lamellar keratitis [163].AS-OCT confers the advantage of confirming the diagnosis of interface fluid syndrome by demonstrating hyporeflective fluid at the flap interface [9,164].
Another potential complication of LASIK is flap displacement/dislocation.This can be easily missed on slit-lamp examination due to the difficulty in identifying the flap edge.There have been several case reports that have demonstrated the superiority of AS-OCT in detecting flap gaps [91,165].Ting and Danjoux reported three cases of late-onset (7-14 years postoperatively) traumatic dislocation of LASIK flaps, all with delayed diagnosis and management [91].All three had signs detected on AS-OCT: two with an infolded flap and one with epithelial ingrowth.AS-OCT can also be utilized to identify and monitor the progression and treatment response for epithelial ingrowth [166] (Figure 15).Epithelial ingrowth (also termed epithelial downgrowth) is a rare but sight-threatening complication that can also occur after other ocular surgery techniques, including cataract surgery (Figure 16), clear lens exchange, and PKP [167][168][169][170].It is characterized by a translucent sheet of epithelial cells that spreads across anterior chamber tissues.Its incidence is reported to range from 0.08 to 0.12% after extracapsular or intracapsular cataract surgery and around 0.27% after PKP [169,170].It can lead to intractable intraocular inflammation, high intraocular pressure, and glaucoma.
ing complication that can also occur after other ocular surgery techniques, including cataract surgery (Figure 16), clear lens exchange, and PKP [167][168][169][170].It is characterized by a translucent sheet of epithelial cells that spreads across anterior chamber tissues.Its incidence is reported to range from 0.08 to 0.12% after extracapsular or intracapsular cataract surgery and around 0.27% after PKP [169,170].It can lead to intractable intraocular inflammation, high intraocular pressure, and glaucoma.

Epithelial Thickness Mapping and Refractive Surgery
ETM has been increasingly used during preoperative planning of refractive surgery [120].A major issue after refractive surgery is iatrogenic post-LASIK ectasia (PLE), with preoperative subclinical early-stage keratoconus thought to play a major role.PLE is a serious complication characterized by a gradual loss of vision, localized steepening distortion and thinning of the cornea, and progressive irregular astigmatism [171,172].Even though nowadays corneal topography is still considered to be the gold standard for corneal ectasia, there have been reports of eyes with seemingly normal topography and no other known risk factors proceeding to develop PLE [173][174][175].
In refractive surgery, it is essential that the therapeutic profile applied is based on the real shape of the stromal surface in a true stromal surface topography-guided ablation [176].The corneal epithelium is known to remodel as a result of underlying stromal irregularities and helps mask them [177,178].As mentioned above, the epithelium is not evenly distributed over the BL and attempts to smoothen out abrupt changes in the stromal surface by thinning focally over; hills' and thickening locally over the 'valleys' of an irregular stroma [179].Due to this epithelial masking, topography and wavefront measurements may not provide an accurate picture of the underlying irregular stromal surface, leading to suboptimal outcomes as they only correct for the proportion of the stromal irregularity that is not masked by the epithelium [176].This emphasizes the need for precise,

Epithelial Thickness Mapping and Refractive Surgery
ETM has been increasingly used during preoperative planning of refractive surgery [120].A major issue after refractive surgery is iatrogenic post-LASIK ectasia (PLE), with preoperative subclinical early-stage keratoconus thought to play a major role.PLE is a serious complication characterized by a gradual loss of vision, localized steepening distortion and thinning of the cornea, and progressive irregular astigmatism [171,172].Even though nowadays corneal topography is still considered to be the gold standard for corneal ectasia, there have been reports of eyes with seemingly normal topography and no other known risk factors proceeding to develop PLE [173][174][175].
In refractive surgery, it is essential that the therapeutic profile applied is based on the real shape of the stromal surface in a true stromal surface topography-guided ablation [176].The corneal epithelium is known to remodel as a result of underlying stromal irregularities and helps mask them [177,178].As mentioned above, the epithelium is not evenly distributed over the BL and attempts to smoothen out abrupt changes in the stromal surface by thinning focally over; hills' and thickening locally over the 'valleys' of an irregular stroma [179].Due to this epithelial masking, topography and wavefront measurements may not provide an accurate picture of the underlying irregular stromal surface, leading to suboptimal outcomes as they only correct for the proportion of the stromal irregularity that is not masked by the epithelium [176].This emphasizes the need for precise, preoperative, independent imaging and analysis of the corneal epithelium and stroma via AS-OCT.Accurate preoperative analysis of the ET distribution pattern helps guide whether to defer refractive surgery in subclinical cases with suspicious topography, as well as providing the opportunity for appropriate treatment in the form of corneal crosslinking [180].
When planning transepithelial photorefractive keratectomy (trans-PRK) and LASIK flaps, customization of the ablation depth (for trans-PRK) and flap thickness (for LASIK) based on ETM is essential, as undercorrection due to lesser stromal ablation with standard, noncustomized treatment may occur [120].Accurate ET measurement is also important in planning phototherapeutic keratectomy (PTK), which aims to treat opacities and irregularities of the corneal surface using an excimer laser.With accurate ETM, transepithelial PTK can reach the required depth of epithelium and anterior stroma using a stepwise protocol, improving the regularity of the stromal surface, along with the visual acuity [181].
Apart from pre-operative planning of refractive surgery treatment protocols, ETM also has an important role in evaluating post-operative outcomes, since irregular epithelial remodeling post-refractive surgery can lead to regression.Accurate and repeatable measurements of the ET help improve earlier detection of postoperative iatrogenic ectasia [181].Furthermore, it also helps in the planning of recorrection, improving safety and efficacy [182].

Conclusions
The advances and commercialization of AS-OCT since its first introduction in 1994 have led to increased clinical applications, and it is likely to change the way ophthalmologists diagnose and manage anterior segment conditions.While we did not cover this in our review, AS-OCT also has significant applications in glaucoma due to its ability to image the anterior segment angle [183].The rich datasets produced by AS-OCT will likely pave the way for future applications with artificial intelligence as a clinical diagnostic aid [184].Despite the numerous advantages of AS-OCT over slit lamp in certain contexts, the slit lamp will likely continue remaining the default diagnostic equipment due to its ubiquity and versatility in the examination of both the anterior and posterior structures of the eye.However, AS-OCT is increasingly becoming an indispensable tool within the diagnostic armamentarium of the modern ophthalmic examination.

Figure 3 .
Figure 3. Clinico-morphological and AS-OCT features of conjunctival naevi: (A) pigmented lesion without cystic alterations on AS-OCT (B); (C) amelanotic naevus with macroscopically visible cysts, which are confirmed with AS-OCT examination (D); (E) small pigmented conjunctival naevuscystic alterations are not be visible on slit-lamp examination, and intralesional cysts can be detected only with AS-OCT (F); (G) pigmented conjunctival naevus-intralesional cysts can be visualized with both slit-lamp examination and AS-OCT (H).(This figure was adapted from Vizvári et al. [29] and was reproduced unchanged under the terms of the Creative Commons (CC) BY 4.0 license https://creativecommons.org/licenses/by/4.0/,accessed on 28 September 2023).

Figure 3 .
Figure 3. Clinico-morphological and AS-OCT features of conjunctival naevi: (A) pigmented lesion without cystic alterations on AS-OCT (B); (C) amelanotic naevus with macroscopically visible cysts, which are confirmed with AS-OCT examination (D); (E) small pigmented conjunctival naevuscystic alterations are not be visible on slit-lamp examination, and intralesional cysts can be detected only with AS-OCT (F); (G) pigmented conjunctival naevus-intralesional cysts can be visualized with both slit-lamp examination and AS-OCT (H).(This figure was adapted from Vizvári et al. [29] and was reproduced unchanged under the terms of the Creative Commons (CC) BY 4.0 license https://creativecommons.org/licenses/by/4.0/,accessed on 28 September 2023).

Figure 3 .
Figure 3. Clinico-morphological and AS-OCT features of conjunctival naevi: (A) pigmented lesion without cystic alterations on AS-OCT (B); (C) amelanotic naevus with macroscopically visible cysts, which are confirmed with AS-OCT examination (D); (E) small pigmented conjunctival naevuscystic alterations are not be visible on slit-lamp examination, and intralesional cysts can be detected only with AS-OCT (F); (G) pigmented conjunctival naevus-intralesional cysts can be visualized with both slit-lamp examination and AS-OCT (H).(This figure was adapted from Vizvári et al. [29] and was reproduced unchanged under the terms of the Creative Commons (CC) BY 4.0 license https://creativecommons.org/licenses/by/4.0/,accessed on 28 September 2023).

Figure 4 .
Figure 4.A case of conjunctival/corneal intraepithelial neoplasia: (a) slit-lamp photograph demonstrating a white, gelatinous lesion encroaching on the conjunctival, limbal, and peripheral corneal region (red arrow); (b) AS-OCT delineating the thickened epithelium at the conjunctival, limbal, and corneal regions (yellow arrows).

Figure 5 .
Figure 5. Slit-lamp photograph and AS-OCT of conjunctival lymphoma: (a) slit-lamp photograph of conjunctival lymphoma; (b) on AS-OCT, there is a homogeneous, dark, hyporeflective subepithelial lesion with smooth borders and overlying thin epithelium (arrow).The lesion contains monomorphic, stippled, dot-like infiltrates corresponding to the infiltration of monoclonal lymphocytes (this figure was adapted from Venkateswaran et al. [39] and was reproduced unchanged under the terms of the CC BY 4.0 license, https://creativecommons.org/licenses/by/4.0/,accessed on 28 September 2023).

Figure 5 .
Figure 5. Slit-lamp photograph and AS-OCT of conjunctival lymphoma: (a) slit-lamp photograph of conjunctival lymphoma; (b) on AS-OCT, there is a homogeneous, dark, hyporeflective subepithelial lesion with smooth borders and overlying thin epithelium (arrow).The lesion contains monomorphic, stippled, dot-like infiltrates corresponding to the infiltration of monoclonal lymphocytes (this figure was adapted from Venkateswaran et al. [39] and was reproduced unchanged under the terms of the CC BY 4.0 license, https://creativecommons.org/licenses/by/4.0/,accessed on 28 September 2023).

Figure 8 .
Figure 8. Acute corneal hydrops in advanced keratoconus: (a) slit-lamp photograph demonstrating a right acute corneal hydrops, characterized by significant central corneal edema, opacity, and bullae (red arrow); (b) AS-OCT demonstrating significant corneal edema with a break in pre-Descemet layer/Descemet membrane (PDL/DM; yellow arrow) and large type 1 PDL/DM detachment (green arrows).Attachment of posterior stromal fibers to PDL is visible (blue arrow).

Figure 8 .
Figure 8. Acute corneal hydrops in advanced keratoconus: (a) slit-lamp photograph demonstrating a right acute corneal hydrops, characterized by significant central corneal edema, opacity, and bullae (red arrow); (b) AS-OCT demonstrating significant corneal edema with a break in pre-Descemet layer/Descemet membrane (PDL/DM; yellow arrow) and large type 1 PDL/DM detachment (green arrows).Attachment of posterior stromal fibers to PDL is visible (blue arrow).

Figure 9 .
Figure 9. Severe Pseudomonas aeruginosa keratitis with corneal perforation: (a) slit-lamp photograph demonstrating significant corneal infiltrate and stromal melt/threatened perforation (red arrow), with a negative Seidel sign; (b) AS-OCT demonstrating significant corneal melt (yellow arrow) with a very thin residual layer of epithelium and 360-degree iridocorneal touch and absence of anterior

Figure 9 .
Figure 9. Severe Pseudomonas aeruginosa keratitis with corneal perforation: (a) slit-lamp photograph demonstrating significant corneal infiltrate and stromal melt/threatened perforation (red arrow), with a negative Seidel sign; (b) AS-OCT demonstrating significant corneal melt (yellow arrow) with a very thin residual layer of epithelium and 360-degree iridocorneal touch and absence of anterior chamber (blue arrow), indicating the presence of corneal perforation.The absence of anterior chamber resulted in a negative Seidel sign, providing a false reassurance of corneal integrity.

Figure 10 .
Figure 10.Pseudomonas aeruginosa keratitis with severe anterior chamber reaction: (a) slit-lamp photograph demonstrating a central infiltrate (red arrow) with severe anterior chamber reaction and hypopyon (black arrow); (b) AS-OCT demonstrating severe anterior chamber reaction, evidenced by increased hyper-reflective cellular changes in anterior chamber (yellow arrow).

Figure 11 .
Figure 11.Candida keratitis with retrocorneal plaque: (a) slit-lamp photograph demonstrating a deep stromal infiltrate (red arrow) with extension into the anterior chamber; (b) AS-OCT demonstrating a posterior stromal infiltrate with a homogeneous increased hyper-reflectivity (yellow arrow) between posterior stroma and pre-Descemet layer/Descemet membrane (blue arrows), and hyper-reflectivity in anterior chamber (green arrow), suggesting an extension of fungal infection into the anterior chamber.

Figure 10 .
Figure 10.Pseudomonas aeruginosa keratitis with severe anterior chamber reaction: (a) slit-lamp photograph demonstrating a central infiltrate (red arrow) with severe anterior chamber reaction and hypopyon (black arrow); (b) AS-OCT demonstrating severe anterior chamber reaction, evidenced by increased hyper-reflective cellular changes in anterior chamber (yellow arrow).

Figure 10 .
Figure 10.Pseudomonas aeruginosa keratitis with severe anterior chamber reaction: (a) slit-lamp photograph demonstrating a central infiltrate (red arrow) with severe anterior chamber reaction and hypopyon (black arrow); (b) AS-OCT demonstrating severe anterior chamber reaction, evidenced by increased hyper-reflective cellular changes in anterior chamber (yellow arrow).

Figure 11 .
Figure 11.Candida keratitis with retrocorneal plaque: (a) slit-lamp photograph demonstrating a deep stromal infiltrate (red arrow) with extension into the anterior chamber; (b) AS-OCT demonstrating a posterior stromal infiltrate with a homogeneous increased hyper-reflectivity (yellow arrow) between posterior stroma and pre-Descemet layer/Descemet membrane (blue arrows), and hyper-reflectivity in anterior chamber (green arrow), suggesting an extension of fungal infection into the anterior chamber.

Figure 11 .
Figure 11.Candida keratitis with retrocorneal plaque: (a) slit-lamp photograph demonstrating a deep stromal infiltrate (red arrow) with extension into the anterior chamber; (b) AS-OCT demonstrating a posterior stromal infiltrate with a homogeneous increased hyper-reflectivity (yellow arrow) between posterior stroma and pre-Descemet layer/Descemet membrane (blue arrows), and hyperreflectivity in anterior chamber (green arrow), suggesting an extension of fungal infection into the anterior chamber.

Figure 12 .
Figure 12.Corneal endothelial graft rejection: (a) slit-lamp photography demonstrating a mild corneal endothelial graft rejection with keratic precipitates (red arrows) in an eye with previous penetrating keratoplasty for keratoconus; (b) AS-OCT showing keratic precipitates as mild excrescences on the corneal endothelium (yellow arrows).Considerable graft-host ectasia (green arrows) is also noted.

Figure 12 .
Figure 12.Corneal endothelial graft rejection: (a) slit-lamp photography demonstrating a mild corneal endothelial graft rejection with keratic precipitates (red arrows) in an eye with previous penetrating keratoplasty for keratoconus; (b) AS-OCT showing keratic precipitates as mild excrescences on the corneal endothelium (yellow arrows).Considerable graft-host ectasia (green arrows) is also noted.

Figure 13 .
Figure 13.Descemet stripping automated endothelial keratoplasty in an aphakic eye with previous glaucoma tube drainage surgery: (a) AS-OCT demonstrating complete graft detachment postoperatively (red arrow); (b) complete graft attachment was achieved (yellow arrow) after rebubbling and suturing of the glaucoma tube.

Figure 13 .
Figure 13.Descemet stripping automated endothelial keratoplasty in an aphakic eye with previous glaucoma tube drainage surgery: (a) AS-OCT demonstrating complete graft detachment postoperatively (red arrow); (b) complete graft attachment was achieved (yellow arrow) after rebubbling and suturing of the glaucoma tube.

Figure 14 .
Figure 14.A case of interface infectious keratitis (IIK) following Descemet stripping automated endothelial keratoplasty (DSAEK): (A) slit-lamp photography demonstrating an inflamed right eye with diffused stromal haze in a crisscross pattern at the graft-host interface (blue arrows), consistent with a diagnosis of IIK.The edge of the DSAEK graft is visible (yellow arrow); (B) hyper-reflective changes at the graft-host interface (red arrows) are clearly delineated on AS-OCT, highlighting the value of AS-OCT in facilitating the assessment of infectious keratitis; (C) slit-lamp photography demonstrating complete resolution of the IIK following intensive topical antifungal treatment, evidenced by the disappearance of the stromal haze on slit-lamp photograph; (D) this corresponds to the disappearance of the hyper-reflective changes at the graft-host interface on AS-OCT (this figure was adapted from Song et al. [155] and was reproduced unchanged under the terms of the CC BY 4.0 license, https://creativecommons.org/licenses/by/4.0/,accessed on 5 November 2023).

Figure 14 .
Figure 14.A case of interface infectious keratitis (IIK) following Descemet stripping automated endothelial keratoplasty (DSAEK): (A) slit-lamp photography demonstrating an inflamed right eye with diffused stromal haze in a crisscross pattern at the graft-host interface (blue arrows), consistent with a diagnosis of IIK.The edge of the DSAEK graft is visible (yellow arrow); (B) hyper-reflective changes at the graft-host interface (red arrows) are clearly delineated on AS-OCT, highlighting the value of AS-OCT in facilitating the assessment of infectious keratitis; (C) slit-lamp photography demonstrating complete resolution of the IIK following intensive topical antifungal treatment, evidenced by the disappearance of the stromal haze on slit-lamp photograph; (D) this corresponds to the disappearance of the hyper-reflective changes at the graft-host interface on AS-OCT (this figure was adapted from Song et al. [155] and was reproduced unchanged under the terms of the CC BY 4.0 license, https://creativecommons.org/licenses/by/4.0/,accessed on 5 November 2023).

Figure 15 .
Figure 15.Late-onset traumatic dislocation of LASIK flap: (A,B) slit-lamp photos revealing a right hazy and thickened corneal flap, central epithelial ingrowth (red arrow), superior-nasal corneal neovascularization, and a large area of nasal corneal flap folded and tucked under the central flap (green arrows-edge of the original nasal flap; blue arrows-edge of the fold); (C) AS-OCT delineating the extent of the infolded flap (red arrows); (D) Scheimpflug corneal tomography showing significant corneal flattening nasally with irregular astigmatism and steeping centrally; (E) slit-lamp photo showing a clear cornea with an area of very mild interface haze (blue arrow) following the repositioning of the dislocated LASIK flap and removal of epithelial ingrowth; (F) AS-OCT demonstrating a small hole within the LASIK flap postoperatively (red arrow); (G) mild recurrence of epithelial ingrowth (blue, left arrow) was noted 9 months postoperatively; (H) corneal tomography showing significant improvement in the anterior corneal curvature and irregular astigmatism 9 months post-operation (this figure was adapted from Ting et al. [91] with permission from the

Figure 15 .
Figure 15.Late-onset traumatic dislocation of LASIK flap: (A,B) slit-lamp photos revealing a right hazy and thickened corneal flap, central epithelial ingrowth (red arrow), superior-nasal corneal neovascularization, and a large area of nasal corneal flap folded and tucked under the central flap (green arrows-edge of the original nasal flap; blue arrows-edge of the fold); (C) AS-OCT delineating the extent of the infolded flap (red arrows); (D) Scheimpflug corneal tomography showing significant corneal flattening nasally with irregular astigmatism and steeping centrally; (E) slit-lamp photo showing a clear cornea with an area of very mild interface haze (blue arrow) following the repositioning of the dislocated LASIK flap and removal of epithelial ingrowth; (F) AS-OCT demonstrating a small hole within the LASIK flap postoperatively (red arrow); (G) mild recurrence of epithelial ingrowth (blue, left arrow) was noted 9 months postoperatively; (H) corneal tomography showing significant improvement in the anterior corneal curvature and irregular astigmatism 9 months post-operation (this figure was adapted from Ting et al. [91] with permission from the licensor Springer Nature, https://link.springer.com/article/10.1007/s10792-018-0946-7#Fig1,accessed on 14 November 2023).

Figure 16 .
Figure 16.Epithelial ingrowth postcataract surgery: (a,b) AS-OCT showing a hyper-reflective layer of presumed epithelial cells (red arrows) extending through the previous paracentesis (yellow arrows); (c-e) slit-lamp images showing the corresponding area of epithelial ingrowth.

Figure 16 .
Figure 16.Epithelial ingrowth postcataract surgery: (a,b) AS-OCT showing a hyper-reflective layer of presumed epithelial cells (red arrows) extending through the previous paracentesis (yellow arrows); (c-e) slit-lamp images showing the corresponding area of epithelial ingrowth.