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Researchers have found that corneal epithelial thickness measurements may be useful in detecting actively progressing versus stable keratoconus (KC). This work builds on previous research that showed epithelial analysis can increase the sensitivity for early diagnosis of KC.1,2
“With comprehensive mapping through spectral-domain (SD) OCT, it is possible to reproducibly measure parameters of epithelial thickness,” said Marcony Santhiago, MD, PhD, at the University of São Paulo in Brazil.
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MIN-MAX. KC progression documented in one year. Red arrow = high variability of the min-max parameters.
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Study details. The researchers enrolled 50 patients with progressive KC (maximum keratometry [Kmax] increase of 1 D per year), 50 with stable KC, and 50 healthy controls. All individuals underwent SD-OCT imaging to obtain epithelial thickness maps and pachymetry. Minimum and maximum epithelial thicknesses of the map and the difference between the thicknesses (min-max) were compared between the groups. “We aimed to identify measures of corneal epithelium that behave differently in stable keratoconus from those in progression,” Dr. Santhiago said.
Results. Epithelium min-max was the only epithelial parameter with a statistically significant difference between the stable and progressive KC groups. Eyes with stable KC presented min-max mean values of –18.2 ± 6.6 μm. In contrast, progressing KC eyes presented mean values of –23.4 ± 10.3 μm (p < .0001).
Findings assessed. “We found that epithelial measures are useful to identify eyes with progressing KC and that the variation between the minimum and maximum epithelial points was significantly greater in progressing KC eyes,” said Dr. Santhiago. “A possible explanation for the min-max difference in progression is that the corneal epithelium has rapid cell turnover and is highly reactive to asymmetries in the shape of the underlying stromal surface.”
In addition, he said, “This study confirms that metrics associated with the asymmetric reactive capacity of the epithelium are capable of detecting subtle differences between groups,” which he described as “more meaningful than values such as epithelial thinnest point.”
A substantial aspect of the research team’s methodology is that “we identified eyes that have progressed based on the limits that would make them candidates for corneal crosslinking (1 D over a year), regardless of their final KC stage,” Dr. Santhiago noted. “Only grouping these eyes in stages, regardless of progression, creates a bias for analyzing any variable role in relevant KC progression.”
Next steps. An important part of the group’s research involves the identification of inflammatory biomarkers possibly correlated with structural impairment in eyes with KC, Dr. Santhiago said. Their next step: publishing their latest work, which “showed that progressing KC eyes have a higher concentration of interleukin 6 [IL-6] and cortisol” versus that observed in eyes with stable KC, he said. He added, “There is a significant correlation between increased IL-6 and cortisol with corneal structural change in keratometry and pachymetry.”
Takeaway for clinicians. “Combined with the topography of the cornea, the epithelial map helps to understand structural alterations that represent the disease,” Dr. Santhiago said. “It can be a promising complementary tool both in the follow-up of a patient with KC and in the preoperative course of a patient who is a candidate for refractive surgery. In this group, we want to identify KC in its early forms.”
—Patricia Weiser, PharmD
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1 Santhiago M et al. Ophthalmol Science. 2023;3:100256.
2 Wang Y et al. J Refrac Surg. 2018;34(3):201-211.
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Relevant financial disclosures: Dr. Santhiago—None.
For full disclosures and the disclosure key, see below.
Full Financial Disclosures
Dr. Chaudhary Bayer: C,L,S; Boehringer Ingelheim: C; Novartis: C,S; Roche: L,S.
Dr. Santhiago Alcon: C; Ziemer: C.
Dr. Skowronska-Krawczyk Visgenx: C.
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