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Ganglion Cell – Inner Plexiform Layer Damage in Diabetic Patients: 3-Year Prospective, Longitudinal, Observational Study

Hyung Bin Lim, Yong Il Shin, Min Woo Lee, Hyung‐Moon Koo, Woo Hyuk Lee, Jung‐Yeul Kim

2020Scientific Reports57 citationsDOIOpen Access PDF

Abstract

Diabetes is expected to accelerate age-related ganglion cell-inner plexiform layer (GC-IPL) loss, but there is limited information on the rate of reduction in GC-IPL thicknesses. We aimed to evaluate the reduction rate of GC-IPL thickness in diabetic patients, and to compare the rates between patients without and with diabetic retinopathy (DR). We included 112 eyes of 112 patients with diabetes [49 eyes without DR (no-DR group) and 63 eyes with mild to moderate non-proliferative DR (NPDR group)] and 63 eyes of 63 normal controls (control group) in this study. Macular GC-IPL thickness in all participants was measured for 3 years at 1-year intervals. The reduction rates of GC-IPL thickness were determined by linear mixed models and compared among the three groups. The estimated reduction rates of the average GC-IPL thickness in the no-DR (-0.627 μm/year) and NPDR (-0.987 μm/year) groups were 2.26-fold (p = 0.010) and 3.56-fold (p = 0.001) faster, respectively, than the control group (-0.277 μm/year). Age, duration of diabetes, and baseline average GC-IPL thickness were associated with longitudinal changes in average GC-IPL thickness. The GC-IPL reduction rate was significantly faster in diabetic patients, with and without DR. Physicians should therefore be aware that GC-IPL damage continues even if there is no DR.

Topics & Concepts

MedicineOphthalmologyDiabetic retinopathyInner plexiform layerDiabetes mellitusGanglionObservational studyInternal medicineRetinalEndocrinologyAnatomyGlaucoma and retinal disordersRetinal Diseases and TreatmentsRetinal and Macular Surgery
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