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Review
. 2024 Mar:99:101245.
doi: 10.1016/j.preteyeres.2024.101245. Epub 2024 Jan 17.

Mechanisms of blood-retinal barrier disruption related to intraocular inflammation and malignancy

Affiliations
Free article
Review

Mechanisms of blood-retinal barrier disruption related to intraocular inflammation and malignancy

Oren Tomkins-Netzer et al. Prog Retin Eye Res. 2024 Mar.
Free article

Abstract

Blood-retinal barrier (BRB) disruption is a common accompaniment of intermediate, posterior and panuveitis causing leakage into the retina and macular oedema resulting in vision loss. It is much less common in anterior uveitis or in patients with intraocular lymphoma who may have marked signs of intraocular inflammation. New drugs used for chemotherapy (cytarabine, immune checkpoint inhibitors, BRAF inhibitors, EGFR inhibitors, bispecific anti-EGFR inhibitors, MET receptor inhibitors and Bruton tyrosine kinase inhibitors) can also cause different types of uveitis and BRB disruption. As malignant disease itself can cause uveitis, particularly from breast, lung and gastrointestinal tract cancers, it can be clinically difficult to sort out the cause of BRB disruption. Immunosuppression due to malignant disease and/or chemotherapy can lead to infection which can also cause BRB disruption and intraocular infection. In this paper we address the pathophysiology of BRB disruption related to intraocular inflammation and malignancy, methods for estimating the extent and effect of the disruption and examine why some types of intraocular inflammation and malignancy cause BRB disruption and others do not. Understanding this may help sort and manage these patients, as well as devise future therapeutic approaches.

Keywords: Blood-retinal barrier; Cytokines; Fluorescein angiography; Lymphoma; Uveitis; Vascular endothelial growth factor.

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Conflict of interest statement

Declaration of competing interest The authors make the following declaration of interest: OTN is on the advisory board of AbbVie inc. and Roche inc. RN is a consultant for GSK. JG is a scientific founder and member of the scientific advisory board of a company spun out by UCL Business to commercialise a LRG1 function-blocking therapeutic antibody developed through the UK Medical Research Council DPFS funding scheme. He is also a shareholder of this company and named inventor on three patents related to LRG1 as a therapeutic target. The authors have no other relevant competing interest to declare.