Ocular Surface Diseases Induced by Dupilumab in Severe Atopic Dermatitis

Clinical characteristics of AD in this small series are comparable to those of clinical trials [3]. In the LIBERTY AD CAFÉ study, which included severe AD with an inadequate response or intolerance to cyclosporine, incidence of conjunctivitis was up to 28% in dupilumab-treated patients [4]. The incidence of conjunctivitis confirmed by ophthalmologists in real life seems to be greater, namely 25% in our center and in 23% in another report [5].

We summarized dupilumab-induced ocular surface disease reported in the literature in Table S2 (supplementary material). We also found two types of dupilumab-induced ocular surface disease: a mild non-specific conjunctivitis and keratitis with dry eyes and a more specific dupilumab-induced follicular conjunctivitis and limbitis. Most cases were mild or moderate [6]. Most of the patients did not have any history of conjunctivitis. This conjunctivitis was associated with blepharitis in 50–77% of cases or punctual stenosis leading to severe tearing and ectropion in some cases [5‐9]. The follicular conjunctivitis occurred despite antihistamine and hyaluronic acid drops as previously described [6]. Treatment of this follicular conjunctivitis depends on the severity of inflammation, varying from local steroid (fluorometholone 1%, dexamethasone 0.1%, prednisolone) which was tapered from 2 to 4 weeks, associated with tacrolimus eye ointment 0.03% or cyclosporine eye drops [6]. In rare cases (0.2–0.4%), ocular inflammation did not respond to any drops, requiring discontinuation of dupilumab therapy [7, 10, 11]. Blepharoconjunctivitis may be responsible for subepithelial fibrosis, suggesting a potential severity if inflammation is not controlled [12].

In our experience, 64% of DA patients had abnormal ocular surface with posterior blepharitis, evaporative dry eyes, conjunctivitis, keratitis, and limbal neovascularization without any ocular complaints at baseline. We would suggest referral at initiation of dupilumab to classify ocular surface inflammation, preventive treatment of meibomian gland dysfunction, moisture of ocular surface with unpreserved artificial tears, and referral to an ophthalmologist for evaluation and appropriate treatment if follicular conjunctivitis occurred.

The underlying mechanism for the development of conjunctivitis seems to be inflammatory and specific to AD since this side effect was not noted in patients with asthma or nasal polyposis on dupilumab [13]. Frustratingly, severe conjunctivitis occurred in AD patients who responded to dupilumab in our series [10].

Histological findings in conjunctivitis induced by dupilumab reported by Bakker et al. [5] revealed focal scarcity of intra-epithelial goblet cells, which is different from the histopathology of allergic conjunctivitis. This explains mucin deficiency which affects the stability of the tear film. We used a combination of trehalose/hyaluronate since it has effects on ocular surface inflammatory markers, mucin expression (decrease in IL-1β, IL-6, and IL-8 tear levels), and goblet cell density recovery, targeting the mechanism of dupilumab-induced ocular surface disease [5]. Topical cyclosporine eye drops could be combined with dupilumab treatment in case of severe dermatitis. In fact, cyclosporine, as suggested by Shen et al., is a T cell-mediated immune response via decreased expression of IL-4 for the follicular conjunctivitis. Both tacrolimus and cyclosporine are ophthalmic calcineurin inhibitors that inhibit T cell-mediated immune response [8]. While steroid drops can cause serious side effects (infections, glaucoma, or cataracts), cyclosporine does not enter the anterior chamber and has good immunomodulatory effect on the ocular surface. It can also be administered four times a day at 2% as a low-cost galenic product for the patients. Its only side effect is a burning sensation which occurs occasionally on the application of eye drops. By suppressing inflammation, cyclosporine is also considered capable of increasing conjunctival goblet cell density and decreasing corneal cells apoptosis. The therapeutic effects of cyclosporine drops in the treatment of eyes affected by several keratoconjunctivitis have been proven in numerous studies in children and adults [14, 15].

Dupilumab blocks signaling both IL-4 and IL-13, which are Th2-mediated inflammation cytokines. Consequently, the upregulation leading to an increase of Th1 response and IFN-γ-mediated inflammation is also a possible mechanism. The pro-inflammatory IFN-γ has been proven as a biomarker for evaporative dry eye disease [16] and cell-mediated immune response in the mucosal immune compartment leading to a variety of dupilumab-induced inflammation spectrum: blepharitis, tear film instability, meibomian gland dysfunction, goblet cell deficiency, exposure keratopathy, follicular conjunctivitis and limbitis, punctual stenosis, and periocular dermatitis.

Further elucidation of dupilumab’s immunologic effect of the tear film is needed to better understand the underlying mechanism of the ocular and periocular side effects and the Th1/Th2 paradigm in ocular allergy.