Submitted Successfully!
To reward your contribution, here is a gift for you: A free trial for our video production service.
Thank you for your contribution! You can also upload a video entry or images related to this topic.
Version Summary Created by Modification Content Size Created at Operation
1
Malihe Eskandarpour
 + 1398 word(s) 1398 2021-03-02 09:35:59 |
2 Format correct
Vicky Zhou
 Meta information modification 1398 2021-03-30 03:27:44 | |
3 move into EC
Conner Chen
 Meta information modification 1398 2021-08-04 11:16:37 | |
4 move out from EC
Conner Chen
 Meta information modification 1398 2021-09-22 02:47:17 |

Video Upload Options

We provide professional Video Production Services to translate complex research into visually appealing presentations. Would you like to try it?
No, upload directly Yes

Confirm

Are you sure to Delete?
Yes No
Cite
If you have any further questions, please contact Encyclopedia Editorial Office.
Eskandarpour, M. Retinal Vasculitis. Encyclopedia. Available online: https://encyclopedia.pub/entry/8335 (accessed on 16 November 2024).
Eskandarpour M. Retinal Vasculitis. Encyclopedia. Available at: https://encyclopedia.pub/entry/8335. Accessed November 16, 2024.
Eskandarpour, Malihe. "Retinal Vasculitis" Encyclopedia, https://encyclopedia.pub/entry/8335 (accessed November 16, 2024).
Eskandarpour, M. (2021, March 29). Retinal Vasculitis. In Encyclopedia. https://encyclopedia.pub/entry/8335
Eskandarpour, Malihe. "Retinal Vasculitis." Encyclopedia. Web. 29 March, 2021.
Retinal Vasculitis
Edit
This entry is adapted from the peer-reviewed paper 10.3390/cells10020396

Retinal vascular diseases have distinct, complex and multifactorial pathogeneses yet share several key pathophysiological aspects including inflammation, vascular permeability and neovascularisation. In non-infectious posterior uveitis (NIU), retinal vasculitis involves vessel leakage leading to retinal enlargement, exudation, and macular oedema. Neovascularisation is not a common feature in NIU, however, detection of the major angiogenic factor—vascular endothelial growth factor A (VEGF-A)—in intraocular fluids in animal models of uveitis and patient samples may be an indication for a role for this cytokine in a highly inflammatory condition. Suppression of VEGF-A by directly targeting the leukotriene B4 (LTB4) receptor (BLT1) pathway indicates a connection between leukotrienes (LTs), which have prominent roles in initiating and propagating inflammatory responses, and VEGF-A in retinal inflammatory diseases.

Retinal Vasculitis vessel inflammation inflammation vessel leakage vessel occlusion

1. Introduction

Non-infectious posterior uveitis (NIU) is defined as inflammation of the uveal tract. Approximately 10–15% of blindness affecting young and middle-age people in the West is caused by uveitis [1]. Therapies for posterior uveitis are limited to corticosteroids, cyclosporine and tumour necrosis factor (TNF)-blocking agents as well as off-label use of methotrexate, azathioprine and mycophenolates [2][3]. However, serious side effects (e.g., glaucoma, cataracts, liver failure and immunosuppression) can arise from long-term use of these treatments [4]. Therefore, there is an urgent need for new therapeutic interventions which are more specific, and which cause fewer side effects. To achieve this goal, an improved understanding of disease pathogenesis is needed in particular for the identification of key mediators that may be therapeutic targets.

Experimental Autoimmune Uveitis (EAU) is an animal model of NIU which is induced by CD4+T cell immune responses to retinal antigens. The main features of EAU are retinal and/or choroidal inflammation, retinal vasculitis, photoreceptor destruction and loss of vision, all of which resemble pathological features in human NIU. The model is well-established and commonly used for investigating fundamental mechanisms of retinal immunopathogenesis. EAU can be induced in many species but is most commonly induced in mice and rats by active immunisation with retinal antigens: interphotoreceptor binding protein (IRBP) for mice, and retinal soluble antigen (SAg) for rats [5][6][7].

Whilst angiogenesis and ischemia are not a common feature of uveitis, vascular inflammation, tissue damage and retinal complications are involved in vision loss [8][9]. Neovascularisation is a major problem in ocular diseases affecting the retina. The underlying stress leading to the induction of new vessel growth is mainly a result of ischemia but also inflammation, which causes the induction of angiogenic factors, including vascular endothelial growth factor A (VEGF-A), by local tissue resident cells [10]. VEGF-A has been detected in intraocular fluids during EAU and in some cases of NIU [11][12][13]. In this review, VEGF-A is referred to as VEGF unless indicated otherwise.

VEGF expression in inflammatory or ischemic conditions has been of great interest due to the recent success of therapeutic targeting of angiogenic pathways with anti-VEGF antibodies in ocular vascular diseases [14][15]. However, based on experimental approaches, a high level of VEGF does not always lead to angiogenesis and new vessel formation [16]. The reason might be that additional microenvironmental conditions/mediators are needed for angiogenesis. Such mediators may include cytokines, growth factors and bioactive lipids which all have the potential to alter tissue homeostasis, especially in the immune-privileged posterior segment in which the ocular microenvironment provides protection against retinal immune insults. Hence, there is a need to understand the retinal vascular pathways involved in uveitis and in EAU progression.

Leukotrienes (LT) have been shown to be involved in VEGF expression and in inducing angiogenesis whilst causing vascular inflammation [17][18][19]. Recent findings have demonstrated clinical efficacy of targeting the high-affinity LTB4 receptor (BLT1) pathway in EAU by applying a BLT1 antagonist [20] and by capturing LTB4 which prevented tissue damage and retinal complications [21] and suggest that the LTB4 pathway is a promising new therapeutic target in intraocular inflammatory diseases.

2. Retinal Damage Associated with Disease Severity and Potential Treatment

2.1. Retinal Damage Associated with Disease Severity

Neovascularisation at the site of inflammation fuels the ongoing inflammatory process. In several chronic diseases affecting the retina (e.g., diabetic retinopathy, retinal vein occlusion, AMD and chorioretinal vein occlusion), neovascularisation is a major problem. Pathological retinal neovascularisation is characterised by leaky and tuft-like vessels, which are associated with retinal exudates and haemorrhage, leading to retinal damage, retinal detachment, or both [22]. The underlying stress leading to the induction of new vessel growth is mainly ischemia, which causes the induction of VEGF by local cells. However, the impact of inflammation cannot be ruled out since VEGF has been detected in ocular Behçet disease and uveitic macular oedema [11][14]. Besides the hypoxia-regulated growth factors, other non-oxygen-regulated growth factors acting in this function include the Tie (tyrosine kinase with immunoglobulin-like and EGF-like domain)1-Tie2 receptors, the Tie2 ligand angiopoietin 2. Several cytokines, hormones, and growth factors also regulate VEGF gene expression, leading to the release of VEGF [23]. VEGF is the most specific mitogenic factor for vascular endothelial cells. Phenotypical modifications in retinal endothelial cells during EAU progression have been proposed to increase the level of angiogenic factors including VEGF [24]. Its role in the pathogenesis of uveitic complications such as choroidal-retinal neovascularisation has been described [25] and is further supported by the proven efficacy of intravitreal anti-VEGF therapies in uveitis [14][15]. It has been demonstrated that a prolonged duration of the inflammatory condition involves cytokines and IL-6 and TNFα are strongly associated with retinal damage and disease severity [26].

2.2 Potential Treatment Approaches in Targeting LT Pathways in Retinal Vasculitis

Finding and targeting those pathways having the highest impact on disease outcomes is always a huge challenge. The LTB4 pathway is clearly active in numerous disease states including inflammatory diseases and remains a target of interest for therapeutic drug development, especially where new therapeutic indications are supported by more definitive mechanistic biology. Drugs targeting the LTB4 pathway are classified into 2 broad classes: antagonists of the known LTB4 receptors (BLT1 and BLT2) and inhibitors of the enzymes responsible for generation of LTB4 (e.g., TA4H and 5-LOX) [27].

Some of the BLT receptor antagonists which have reached phase 2 clinical trials are Etalocib (LY293111; Lilly), Amelubant (BIIL 284; Boehringer Ingelheim), Moxilubant (CGS-25019C, LTB-019; Novartis) and CP-105696 (Pfizer). The target diseases have been chronic obstructive pulmonary disease (COPD), asthma, rheumatoid arthritis, cystic fibrosis and cancer. Antagonist LY293111 in asthmatic patients showed that it led to a significant reduction in the number of neutrophils in BAL fluid, but failed to improve respiratory function or airway reactivity after allergen challenge [28][29][30]. However, a study examining the role of the BLT1 antagonist, CP-105696, in monkeys showed that the compound inhibited both LTB4-mediated neutrophil chemotaxis and upregulation of CD11b+ cells [31]. At least six LTA4H inhibitors of the current generation have entered clinical trials and reached phase 2 studies. Of the LTA4H inhibitors, Ubenimex (Bestatin; Nippon-Kayaku, Eiger Biopharmaceuticals), Acebilustat (CTX-4430 Celtaxsys) and Tosedostat (CHR-2797; CTI Biopharma) have been applied in asthma, myelodysplastic syndrome, solid tumours, active cystic fibrosis, acne vulgari, pulmonary arterial hypertension (PAH), atopic dermatitis and allergic conjunctivitis [31][28].

The well-known 5-LOX inhibitor, Zileuton, is already in clinical use for the maintenance treatment of asthma and has been tried in other inflammatory/allergic diseases including atopic dermatitis and allergic conjunctivitis. Zileuton inhibits VEGF-Induced angiogenesis, expression of cell adhesion molecules (VCAM-1, ICAM-1), TNFα secretion and production of NO [18], the latter being required for efficient angiogenesis which is synthesised by endothelial NOS. NO is produced from bone marrow-derived macrophages stimulated with IFNγ and TNFα and is thought to be produced similarly in vivo [32]. The anti-angiogenic effect of Zileuton might also relate to the activation of the large-conductance Ca2+-activated K+ (BK) channel, resulting in activation of pro-apoptotic signalling cascades. Another possible explanation is based on studies which demonstrated that Zileuton was effective in inhibiting biosynthesis of multiple AA metabolites, including 12- and 15-hydroxyeicosatetranolic acid (12-, 15-HETE) in a hamster cheek pouch model of carcinogenesis. 12-HETE is involved in mediating VEGF-induced angiogenesis [18]. Therefore, there is a possibility that the anti-angiogenic effect of Zileuton comes from preventing the 12-LOX, and not the 5-LOX, pathway thereby blocking the production of 12-HETE, the metabolite of the 12-LOX pathway [28].

A new therapeutic approach could be by using more selective inhibitors of LTB4 and BLT1 interactions in affected tissues/organs. Nomacopan is one example of a compound that demonstrates functional selectivity for LTB4 and shows a promising reduction in disease severity in a preclinical uveitis model, a mouse model of Bullous Pemphigoid [33] and is now in phase 2 clinical study for bullous pemphigoid.

References

  1. Lee, R.W.; Nicholson, L.B.; Sen, H.N.; Chan, C.C.; Wei, L.; Nussenblatt, R.B.; Dick, A.D. Autoimmune and autoinflammatory mechanisms in uveitis. Semin. Immunopathol. 2014, 36, 581–594.
  2. Dick, A.D. Doyne lecture 2016: Intraocular health and the many faces of inflammation. Eye 2017, 31, 87–96.
  3. Merida, S.; Palacios, E.; Navea, A.; Bosch-Morell, F. New Immunosuppressive Therapies in Uveitis Treatment. Int. J. Mol. Sci. 2015, 16, 18778–18795.
  4. LaMattina, K.C.; Goldstein, D.A. Adalimumab for the treatment of uveitis. Expert Rev. Clin. Immunol. 2017, 13, 181–188.
  5. Agarwal, R.K.; Silver, P.B.; Caspi, R.R. Rodent models of experimental autoimmune uveitis. Methods Mol. Biol. 2012, 900, 443–469.
  6. Caspi, R.R.; Silver, P.B.; Luger, D.; Tang, J.; Cortes, L.M.; Pennesi, G.; Mattapallil, M.J.; Chan, C.C. Mouse models of experimental autoimmune uveitis. Ophthalmic Res. 2008, 40, 169–174.
  7. Caspi, R.R.; Roberge, F.G.; Chan, C.C.; Wiggert, B.; Chader, G.J.; Rozenszajn, L.A.; Lando, Z.; Nussenblatt, R.B. A new model of autoimmune disease. Experimental autoimmune uveoretinitis induced in mice with two different retinal antigens. J. Immunol. 1988, 140, 1490–1495.
  8. Patel, A.K.; Newcomb, C.W.; Liesegang, T.L.; Pujari, S.S.; Suhler, E.B.; Thorne, J.E.; Foster, C.S.; Jabs, D.A.; Levy-Clarke, G.A.; Nussenblatt, R.B.; et al. Risk of Retinal Neovascularization in Cases of Uveitis. Ophthalmology 2016, 123, 646–654.
  9. Graham, E.M.; Stanford, M.R.; Shilling, J.S.; Sanders, M.D. Neovascularisation associated with posterior uveitis. Br. J. Ophthalmol. 1987, 71, 826–833.
  10. Storkebaum, E.; Carmeliet, P. VEGF: A critical player in neurodegeneration. J. Clin. Investig. 2004, 113, 14–18.
  11. Weiss, K.; Steinbrugger, I.; Weger, M.; Ardjomand, N.; Maier, R.; Wegscheider, B.J.; Wedrich, A.; El-Shabrawi, Y. Intravitreal VEGF levels in uveitis patients and treatment of uveitic macular oedema with intravitreal bevacizumab. Eye 2009, 23, 1812–1818.
  12. Vinores, S.A.; Chan, C.C.; Vinores, M.A.; Matteson, D.M.; Chen, Y.S.; Klein, D.A.; Shi, A.; Ozaki, H.; Campochiaro, P.A. Increased vascular endothelial growth factor (VEGF) and transforming growth factor beta (TGFbeta) in experimental autoimmune uveoretinitis: Upregulation of VEGF without neovascularization. J. Neuroimmunol. 1998, 89, 43–50.
  13. Fine, H.F.; Baffi, J.; Reed, G.F.; Csaky, K.G.; Nussenblatt, R.B. Aqueous humor and plasma vascular endothelial growth factor in uveitis-associated cystoid macular edema. Am. J. Ophthalmol. 2001, 132, 794–796.
  14. Mackensen, F.; Heinz, C.; Becker, M.D.; Heiligenhaus, A. Intravitreal bevacizumab (avastin) as a treatment for refractory macular edema in patients with uveitis: A pilot study. Retina 2008, 28, 41–45.
  15. Acharya, N.R.; Hong, K.C.; Lee, S.M. Ranibizumab for refractory uveitis-related macular edema. Am. J. Ophthalmol. 2009, 148, 303–309.e302.
  16. Vinores, S.A.; Kuchle, M.; Mahlow, J.; Chiu, C.; Green, W.R.; Campochiaro, P.A. Blood-ocular barrier breakdown in eyes with ocular melanoma. A potential role for vascular endothelial growth factor/vascular permeability factor. Am. J. Pathol. 1995, 147, 1289–1297.
  17. Duah, E.; Teegala, L.R.; Kondeti, V.; Adapala, R.K.; Keshamouni, V.G.; Kanaoka, Y.; Austen, K.F.; Thodeti, C.K.; Paruchuri, S. Cysteinyl leukotriene 2 receptor promotes endothelial permeability, tumor angiogenesis, and metastasis. Proc. Natl. Acad. Sci. USA 2019, 116, 199–204.
  18. Lim, H.J.; Park, J.; Um, J.Y.; Lee, S.S.; Kwak, H.J. Zileuton, a 5-Lipoxygenase Inhibitor, Exerts Anti-Angiogenic Effect by Inducing Apoptosis of HUVEC via BK Channel Activation. Cells 2019, 8, 1182.
  19. Sasaki, F.; Yokomizo, T. The leukotriene receptors as therapeutic targets of inflammatory diseases. Int. Immunol. 2019, 31, 607–615.
  20. Liao, T.; Ke, Y.; Shao, W.H.; Haribabu, B.; Kaplan, H.J.; Sun, D.; Shao, H. Blockade of the interaction of leukotriene b4 with its receptor prevents development of autoimmune uveitis. Investig. Ophthalmol. Vis. Sci. 2006, 47, 1543–1549.
  21. Eskandarpour, M.; Chen, Y.H.; Nunn, M.A.; Coupland, S.E.; Weston-Davies, W.; Calder, V.L. Leukotriene B4 and Its Receptor in Experimental Autoimmune Uveitis and in Human Retinal Tissues: Clinical Severity and LTB4 Dependence of Retinal Th17 Cells. Am. J. Pathol. 2020.
  22. Al-Latayfeh, M.; Silva, P.S.; Sun, J.K.; Aiello, L.P. Antiangiogenic therapy for ischemic retinopathies. Cold Spring Harb. Perspect. Med. 2012, 2, a006411.
  23. Sun, Y.; Smith, L.E.H. Retinal Vasculature in Development and Diseases. Annu. Rev. Vis. Sci. 2018, 4, 101–122.
  24. Lipski, D.A.; Foucart, V.; Dewispelaere, R.; Caspers, L.E.; Defrance, M.; Bruyns, C.; Willermain, F. Retinal endothelial cell phenotypic modifications during experimental autoimmune uveitis: A transcriptomic approach. BMC Ophthalmol. 2020, 20, 106.
  25. Mirando, A.C.; Lima, E.S.R.; Chu, Z.; Campochiaro, P.A.; Pandey, N.B.; Popel, A.S. Suppression of Ocular Vascular Inflammation through Peptide-Mediated Activation of Angiopoietin-Tie2 Signaling. Int. J. Mol. Sci. 2020, 21, 5142.
  26. Silveira, R.C.; Procianoy, R.S. High plasma cytokine levels, white matter injury and neurodevelopment of high risk preterm infants: Assessment at two years. Early Hum. Dev. 2011, 87, 433–437.
  27. Rossi, A.; Pergola, C.; Koeberle, A.; Hoffmann, M.; Dehm, F.; Bramanti, P.; Cuzzocrea, S.; Werz, O.; Sautebin, L. The 5-lipoxygenase inhibitor, zileuton, suppresses prostaglandin biosynthesis by inhibition of arachidonic acid release in macrophages. Br. J. Pharmacol. 2010, 161, 555–570.
  28. Bhatt, L.; Roinestad, K.; Van, T.; Springman, E.B. Recent advances in clinical development of leukotriene B4 pathway drugs. Semin. Immunol. 2017, 33, 65–73.
  29. Gronke, L.; Beeh, K.M.; Cameron, R.; Kornmann, O.; Beier, J.; Shaw, M.; Holz, O.; Buhl, R.; Magnussen, H.; Jorres, R.A. Effect of the oral leukotriene B4 receptor antagonist LTB019 on inflammatory sputum markers in patients with chronic obstructive pulmonary disease. Pulm. Pharmacol. Ther. 2008, 21, 409–417.
  30. Konstan, M.W.; Doring, G.; Heltshe, S.L.; Lands, L.C.; Hilliard, K.A.; Koker, P.; Bhattacharya, S.; Staab, A.; Hamilton, A.; Investigators; et al. A randomized double blind, placebo controlled phase 2 trial of BIIL 284 BS (an LTB4 receptor antagonist) for the treatment of lung disease in children and adults with cystic fibrosis. J. Cyst. Fibros. 2014, 13, 148–155.
  31. Jo-Watanabe, A.; Okuno, T.; Yokomizo, T. The Role of Leukotrienes as Potential Therapeutic Targets in Allergic Disorders. Int. J. Mol. Sci. 2019, 20, 3580.
  32. Robertson, M.J.; Erwig, L.P.; Liversidge, J.; Forrester, J.V.; Rees, A.J.; Dick, A.D. Retinal microenvironment controls resident and infiltrating macrophage function during uveoretinitis. Investig. Ophthalmol. Vis. Sci. 2002, 43, 2250–2257.
  33. Sezin, T.; Murthy, S.; Attah, C.; Seutter, M.; Holtsche, M.M.; Hammers, C.M.; Schmidt, E.; Meshrkey, F.; Mousavi, S.; Zillikens, D.; et al. Dual inhibition of complement factor 5 and leukotriene B4 synergistically suppresses murine pemphigoid disease. JCI Insight 2019, 4.
More
© Text is available under the terms and conditions of the Creative Commons Attribution (CC BY) license; additional terms may apply. By using this site, you agree to the Terms and Conditions and Privacy Policy.
Upload a video for this entry
Information
Subjects: Ophthalmology
Contributor MDPI registered users' name will be linked to their SciProfiles pages. To register with us, please refer to https://encyclopedia.pub/register :
Malihe Eskandarpour
View Times: 606
Revisions: 4 times (View History)
Update Date: 22 Sep 2021
Table of Contents
    1000/1000
    Hot Most Recent
    ScholarVision Creations
    Feedback