Lymphoplasmacellular mucositis ameliorated by α4β7 integrin inhibitor vedolizumab in a patient with ulcerative colitis.

Introduction

Idiopathic lymphoplasmacellular mucositis-dermatitis (ILPMD) is a term that encompasses a group of disorders defined histopathologically by a dense infiltrate predominantly of plasma cells and some lymphocytes in the skin and mucosa. Zoon first described a similar process with dense plasma cell infiltrates in the glans penis that was termed plasma cell balanitis. Since then, oral involvement has also been reported and described with multiple terms such as idiopathic plasmacytosis, plasma cell orificial mucositis, and mucous membrane plasmacytosis. However, because all these entities share similar histopathologic features, use of ILPMD as an encompassing diagnosis provides a terminological consolidation. Diagnosis of ILPMD requires exclusion of a wide range of clinical disorders. It exhibits a chronic course and tends to be refractory to treatment. Although several other coincidental autoimmune conditions are reported in patients with ILPMD, an association with inflammatory bowel disease is not established. We report a case of oral ILPMD in a patient with ulcerative colitis (UC). Effectiveness of local treatment of the affected lower lip was significantly enhanced with systemic vedolizumab (Entyvio, Takeda Pharmaceuticals USA, Inc, Deerfield, IL) used to treat UC in this patient.

Case report

A 48-year-old African-American woman with history of UC presented with a crusted lesion on her lower lip that had been waxing and waning for the last 2 years. Examination found a fissured, thickened plaque with yellow-brown hemorrhagic crust covering most of her enlarged, depigmented lower lip (Fig 1, A). The remainder of the skin and mucous membrane examination was unremarkable. She was treated previously for cheilitis with topical steroids with minimal improvement, and her flares coincided with worsening of her UC. Past treatments for UC included mesalamine and adalimumab, both of which failed to control her bowel disease.

Fig 1

A, A broad eroded lesion with thick purulent hemorrhagic scale-crust on the lower lip. B, Complete clearance of the lesion after treatment with vedolizumab.

Punch biopsy found a dense and diffuse inflammatory infiltrate consisting of plasma cells (CD138+), histiocytes (CD68+), T cells (CD3+), B cells (CD20+), and rare CD30+ cells (Figs 2 and 3). No granulomas, keratinocyte atypia, or solar elastosis were observed. Immunohistochemistry showed plasma cells positive for κ and λ light chains as well as IgG4. IgG4-related disease was ruled out because of absence of characteristic histopathologic criteria of storiform fibrosis and venalities in both lip and prior intestinal biopsies. Varicella-zoster and herpes simplex virus tissue polymerase chain reaction tests were negative. Given their association with UC, pyoderma gangrenosum and pyoderma vegetans were considered in the differential diagnoses. However, the lack of a predominantly neutrophilic infiltrate excluded pyoderma gangrenosum and the absence of a pseudocarcinomatous hyperplasia with neutrophilic dermal abscesses ruled out pyoderma vegetans. Given the mucosal ulceration with an underlying dense infiltrate composed predominantly of plasma cells with some neutrophils and lymphocytes, a diagnosis of ILPMD was established.

Fig 2

An ulcer with thick hemorrhagic crust accompanied by a dense infiltrate of inflammatory cells consisting of neutrophils, lymphocytes, histiocytes, and numerous plasma cells. (Hematoxylin-eosin stain; original magnification: ×40; inset: ×100.)

Fig 3

CD138 stain highlighting a dense infiltrate of plasma cells throughout the lesion. (CD138 stain; original magnification: ×40.)

The patient was treated with three 1-mL doses of 10 mg/mL intralesional triamcinolone acetonide, administered every 2 weeks with daily application of triamcinolone acetonide 0.1% dental paste. After 6 weeks of this treatment, she noticed only mild improvement of oral lesions and did not continue with intralesional therapy. At this time, her gastroenterologist started systemic infusions of α4β7 integrin inhibitor vedolizumab to treat her UC. Within 4 weeks of receiving her second dose of monthly infusions, the oral lesions completely resolved and remained in remission (Fig 1, B). Treatment also led to resolution of her UC symptoms. However, when vedolizumab was temporarily discontinued because of logistical issues, her oral lesions flared again only to resolve upon the reinstitution of vedolizumab.

Discussion

No defined guidelines exist for the management of ILPMD. Treatment options include topical, intralesional, and systemic corticosteroids; topical and systemic antibiotics or antifungals; topical cyclosporine; topical tacrolimus; dapsone; isotretinoin; and liquid nitrogen cryotherapy. Spontaneous regression over 6 months has also been observed. Our patient's chronic course of ILPMD remained in remission while on vedolizumab and flared when her vedolizumab dosing was delayed. Vedolizumab is a monoclonal antibody that targets gut-homing molecule α4β7 integrin and exerts anti-inflammatory activity in UC. Plasma cells express α4β7 integrin, and α4β7 ligand, MAdCAM-1, is expressed in oral mucosa. Therefore, plasma cell homing to oral mucosa may be inhibited by vedolizumab in ILPMD. Together, these observations suggest a role for vedolizumab in patients with concurrent ILPMD and inflammatory bowel disease. We conclude that close collaboration between gastroenterologists and dermatologists can lead to selection of a dually effective treatment strategy in these patients.