Usefulness of orbital colour Doppler ultrasound in vascular-related monocular vision loss

Author:

Ruiz-Ares Gerardo1ORCID,Fuentes Blanca1,Rodríguez-Pardo de Donlebún Jorge1,Alonso de Leciñana Maria1,Gutiérrez-Zúñiga Raquel1,Rigual Ricardo1,Díez-Tejedor Exuperio1

Affiliation:

1. Department of Neurology, Stroke Centre, La Paz University Hospital – IdiPAZ Health Research Institute, Autonoma University of Madrid, Madrid, Spain

Abstract

Acute, painless, monocular vision loss (APMVL) usually has a vascular aetiology. We conducted a prospective observational study from 2011 to 2018 to analyse the added value of colour Doppler imaging to assess orbital vessel blood flow in the diagnosis of APMVL. The study included 67 patients (39 [58.2%] men; mean age, 65.9 years [SD 13.7]) with APMVL evaluated at the Neurosonology Laboratory within the first 5 days of symptom onset, who were classified as having either transient or persistent monocular blindness. The blood flow in the ophthalmic and central retinal arteries was assessed using colour Doppler ultrasound with a linear 7.5-MHz transducer. Thirty-three (49.3%) patients presented transient monocular blindness, with reduced blood flow in either the ophthalmic or central retinal artery. The group with persistent vision loss included 24 cases of central retinal artery occlusion (CRAO) and 10 cases of ischaemic optic neuropathy (35.8% and 14.9%, respectively, of the total sample). These patients were older and had a higher prevalence of hypertension and mild carotid atherosclerosis. Orbital colour Doppler ultrasound (OCDUS) clarified the mechanism/cause of the ischaemia in 11 (16.4%) patients and showed abnormal flow in 46 (68.7%) patients, confirming the vascular origin in 19 (57.6%) of the transient monocular blindness cases. Lower peak systolic velocity was observed in patients with CRAO ( p < 0.001), and a velocity < 10 cm/s in the central retinal artery was independently associated with the diagnosis of CRAO. OCDUS can be helpful in confirming the vascular cause and identifying the aetiology of APMVL.

Publisher

SAGE Publications

Subject

Cardiology and Cardiovascular Medicine

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