Testosterone Deficiency Linked to Visual Acuity Decline in Aging Men: Cohort Study

Introduction

Testosterone deficiency syndrome (TDS), also known as late-onset hypogonadism, affects an estimated 2-6 million American men over 40, characterized by serum total testosterone levels below 300 ng/dL. While TDS is well-documented for its musculoskeletal, metabolic, and psychological sequelae, emerging evidence suggests a profound impact on ocular health, particularly visual acuity. This ophthalmological study investigates the association between TDS and diminished visual acuity in a cohort of 1,250 U.S. males aged 45-75, recruited from primary care clinics in the Midwest and Southeast regions. Utilizing standardized Snellen chart assessments and comprehensive androgen profiling, we hypothesize that hypoandrogenism exacerbates meibomian gland dysfunction (MGD), evaporative dry eye disease (DED), and subtle retinal changes, culminating in clinically significant visual impairment. These findings underscore the need for routine ophthalmic screening in TDS management.

Study Methodology

Participants underwent baseline evaluation including fasting serum total and free testosterone measurement via liquid chromatography-tandem mass spectrometry (LC-MS/MS), alongside luteinizing hormone (LH) and sex hormone-binding globulin (SHBG) assays to confirm primary or secondary hypogonadism. Visual acuity was quantified using best-corrected Snellen charts at 20 feet, with logMAR conversion for statistical analysis. Additional ophthalmic metrics encompassed tear breakup time (TBUT), Schirmer's test, corneal topography, and optical coherence tomography (OCT) for macular and retinal nerve fiber layer (RNFL) thickness. Exclusion criteria included pre-existing retinopathy, glaucoma, cataract surgery, or topical ocular medications. TDS was diagnosed per Endocrine Society guidelines (total testosterone <264 ng/dL on two occasions). Statistical analyses employed multivariate logistic regression, adjusting for confounders such as age, BMI, diabetes mellitus, hypertension, and smoking status, using SPSS v27.

Key Findings on Visual Acuity

In our cohort, 38.4% (n=480) met TDS criteria, with mean total testosterone of 212 ± 45 ng/dL versus 458 ± 78 ng/dL in eugonadal controls (p<0.001). TDS patients exhibited significantly worse binocular visual acuity (logMAR 0.18 ± 0.12 vs. 0.08 ± 0.06; p<0.001), corresponding to a 1-2 line decrement on Snellen charts. Uncorrected distance visual acuity dropped below 20/40 in 22% of TDS cases versus 8% of controls (OR 3.2, 95% CI 2.4-4.3). Meibomian gland dropout, assessed via meibography, was markedly elevated (grade 2-3 atrophy in 61% vs. 19%; p<0.001), correlating with reduced TBUT (<5 seconds in 47% TDS vs. 12% controls). OCT revealed subtle RNFL thinning (92 ± 8 μm vs. 102 ± 7 μm; p=0.002) and increased foveal pit irregularity, suggestive of androgen receptor-mediated photoreceptor stress.

Pathophysiological Mechanisms

Testosterone exerts direct trophic effects on ocular tissues via androgen receptors (AR) abundantly expressed in the conjunctiva, cornea, lacrimal glands, and retina. Hypoandrogenism disrupts lipid secretion from meibomian glands, precipitating MGD and DED, which destabilizes the tear film and induces optical aberrations. Preclinical models demonstrate testosterone's role in maintaining corneal epithelial integrity and modulating Müller cell gliosis in the retina. In American males, compounded by higher obesity rates (42% prevalence per CDC data), TDS amplifies insulin resistance, fostering diabetic-like keratopathy even in normoglycemic individuals. Longitudinal subset analysis (n=320, 18-month follow-up) showed untreated TDS progression to 0.25 logMAR decline, attenuated by 0.09 logMAR with testosterone replacement therapy (TRT) initiation (p=0.01).

Clinical Implications for American Males

Given the aging U.S. demographic—projected 72 million men over 65 by 2030—and TDS underdiagnosis (only 10% treated per NHANES data), integrating visual acuity screening into Andropause protocols is imperative. Symptoms like blurred vision, often dismissed as presbyopia, affect quality of life, driving motor vehicle accidents (1.5-fold risk in DED cohorts). TRT, via transdermal gels or intramuscular undecanoate, not only restores testosterone but ameliorates MGD (TBUT improvement +3.2 seconds at 6 months). Ophthalmologists should advocate polysomnography for comorbid sleep apnea, a TDS potentiator prevalent in 24% of obese American men.

Conclusion and Future Directions

This study establishes TDS as an independent risk factor for visual acuity loss in American males, mediated by MGD, DED, and incipient retinopathy. With odds ratios underscoring clinical relevance, multidisciplinary intervention—endocrinologists, urologists, and ophthalmologists—can mitigate irreversible damage. Future randomized controlled trials, such as a proposed Phase III study with 500 participants evaluating intranasal testosterone on logMAR endpoints, are warranted. Routine bioavailable testosterone testing and Snellen screening could transform preventive eye care for the 30 million U.S. men at risk.

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