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Original Article

Effect of Pupil Dilation with Tropicamide on Retinal Vascular Caliber

ORCID Icon, , , , , , , , , , & show all
Pages 400-407 | Received 18 Feb 2019, Accepted 29 Jun 2019, Published online: 03 Jul 2019
 

ABSTRACT

Purpose: The retinal blood vessels reflect changes in the brain’s micro-circulation and these changes have been shown to correlate with the incidence of diseases such as stroke, heart disease and Alzheimer’s disease. Studies investigating the retinal vasculature routinely use pupil dilation with tropicamide to optimize image acquisition and quality. The aim of this study was to investigate the effects of tropicamide on retinal vascular parameters using retinal photography.

Methods: The study was performed on 41 healthy young subjects of both sexes, using tropicamide to dilate only the right pupil, leaving the left as a control.

Results: Pupil dilation with tropicamide resulted in reduced retinal vessel width measures based on standardized approaches, particularly reduced arteriolar caliber (p < .0005). However, closer investigation of the images revealed reduced fundus image magnification in the post-tropicamide images, based on reduced optic nerve head diameter (p < .0005) and longitudinal analysis with image registration and affine transformation (p < .0001). No change in vessel width parameters was observed after adjustment for image magnification.

Conclusion: These results suggest that tropicamide does not change the width of the retinal vessels, however width parameters as measured by standard approaches may be reduced due to image magnification changes resulting from cycloplegia. In this study, improved optic nerve head segmentation for image scale conversion removed the magnification error. With this correction, the tropicamide intervention had no effect on vessel width parameters in young healthy people and could be utilized in future without affecting the results of retinal vascular analysis.

Acknowledgments

We thank all the participants who took part in this study and the clinicians who referred participants. The generous research support by the Royal Perth Hospital Medical Research Foundation (MRF) is also acknowledged.

Disclosure statement

None of the authors have any proprietary interests or conflicts of interest related to this submission.

Additional information

Funding

SMF is supported by a National Health and Medical Research Council (NHMRC) Dementia Research Fellowship. MPS is supported by a National Health and Medical Research Council (NHMRC) Senior Research Fellowship.

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