Pyoderma gangrenosum associated with Wegener's granulomatosis: partial response to mycophenolate mofetil

C. Le Hello, I. Bonte1, J.-J. Mora2, L. Verneuil3, L.-H. Noël4 and L. Guillevin5

Unité de Médecine Vasculaire, Service de Chirurgie Thoracique et Cardiovasculaire, CHU de Caen, avenue de la Côte de Nacre, 14000 Caen,
1 Service de Dermatologie, Hôpital Avicenne, 125, route de Stalingrad, 93009 Bobigny,
2 Service de Rhumatologie, Hôpital de Bayeux, 13, rue de Nesmond, BP 142, 14401 Bayeux,
3 Service de Dermatologie, CHU de Caen, avenue de la Côte de Nacre, 14000 Caen,
4 Inserm U507, Hôpital Necker, 161, rue de Sèvres, 75015 Paris and
5 Service de Médecine Interne, Hôpital Avicenne, 125, route de Stalingrad, 93009 Bobigny, France

SIR, We report the history of a 41-yr-old Caucasian male with systemic Wegener's granulomatosis (WG) associated with pyoderma gangrenosum (PG). Despite attenuation of clinical manifestations of WG, PG did not respond to several immunosuppressants and immunomodulating agents but regressed rapidly, albeit incompletely, under treatment with corticosteroids (CS) and mycophenolate mofetil (MMF).

Since December 1991, this man had suffered from histologically proven WG initially characterized by sinusitis and pulmonary nodules. Antineutrophil cytoplasm antibodies with a cytoplasmic labelling pattern (c-ANCA) were found and enzyme-linked immunosorbent assay (ELISA) detected anti-proteinase 3 (PR3) antibodies. Combining CS with 18 pulses of cyclophosphamide (CYC; cumulative dose 27 g) led to remission. The c-ANCA disappeared. In October 1995, he suffered a relapse characterized by pleuropericarditis, pulmonary nodules, slow atrial flutter, first-degree atrioventricular block, sinusitis and sciatalgia; he was weakly positive for c-ANCA. Combined CS and CYC therapy was reinitiated. CYC (cumulative dose, 18 g) again led to remission but was stopped because of haemorrhagic cystitis. CS were stopped during the summer of 1997. ANCA were undetectable and anti-PR3 were positive by ELISA [60 arbitrary units (AU), threshold for positivity >20 AU]. In September 1997, the patient presented headaches, crusted rhinitis, atrial flutter with complete heart block, interatrial septum nodules and pulmonary hypertension due to compression of pulmonary arteries. He again became weakly positive for c-ANCA and the anti-PR3 level rose (to 73 AU). A dramatic response was obtained under CS (three pulses of 15 mg/kg/day and then 1 mg/kg/day orally) in combination with intravenous immunoglobulins (IV Ig; 2 g/kg every 3 weeks for 8 months). In November 1997, a computed tomography (CT) scan of the chest showed regression of pulmonary and mediastinal abnormalities, and echocardiography showed regression of interatrial septum nodules; tapering of the CS dose was begun. One month later, numerous acneiform papular and pustular lesions of the trunk appeared (CS 0.95 mg/kg/day). They spread and evolved into PG—ulcers with clear-cut margins, deep, irregular, violaceous borders and a necrotic centre and showing chronic discharge. These multiple, painful, deep necrotic ulcers (1–3 cm in diameter) covered the trunk and neck (Fig. 1Go). Microbiological tests performed on histological sections showed no microorganisms, a finding confirmed by negative cultures. A skin biopsy showed an inflammatory suppurative dermal infiltrate harbouring neutrophils, lymphocytes and histiocytes. IV Ig were continued and CS tapered to 0.4 mg/kg/day. In February 1998, the skin area affected by PG decreased under treatment with IV Ig and CS (0.25 mg/kg/day). CS were further tapered (0.2 mg/kg/day). ANCA and anti-PR3 were no longer detectable. Sinusitis with periorbital oedema recurred in March 1998. A skin biopsy from the border of an ulcer showed intense inflammation of the superficial dermis with multinucleated macrophage-like cells. IV Ig was replaced with azathioprine (2 mg/kg/day) in May 1998. Five months later, skin lesions had regressed partially. Azathioprine was increased to 2.5 mg/kg/day but to no avail. Pulmonary nodules, crusted rhinitis and right-sided deafness occurred in April 1999. c-ANCA were detected by immunofluorescence and anti-PR3 by ELISA (66 AU). Azathioprine was stopped, MMF (2 g/day orally) was started and the CS dose was increased to 1 mg/kg/day. For the first time, the PG regressed dramatically; complete healing was obtained within 3 weeks but proved transitory. CS were rapidly tapered (0.5 mg/kg/day at the end of April). No new lesions appeared over the next 2 months but, when CS reached 0.1 mg/kg/day at the end of June, small zones of PG reappeared on the left shoulder. This relapse was controlled by increasing prednisone to 0.15 mg/kg/day and MMF to 3 g/day. No side-effects of MMF were noted. WG was then in remission, with only minor zones of PG on the left shoulder; c-ANCA and anti-PR3 levels were also stable.



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FIG. 1.  Multiple deep necrotic ulcers covering the trunk and neck.

 
Although skin involvement has been observed in 14–47% of patients with WG [14], pyoderma-like ulcers or necrotizing ulcerations resembling PG are rare manifestations [58]. Cutaneous involvement may occur during the course of the disease or be present at onset [57] and may develop on unusual sites, e.g. the trunk [8], neck [5] and face [6], and may indicate an exacerbation of existing WG. Our case is unusual because cutaneous lesions became the predominant symptom, surpassing sinusitis and pulmonary signs at the time of the second relapse, and because of their persistence and spread despite appropriate treatment, including CS, IV Ig and azathioprine. Nowack et al. [9] were the first to report the successful use of MMF, as maintenance therapy after standard induction therapy, in 10 systemic WG patients, of whom four showed skin involvement. They also successfully prescribed MMF as induction treatment to replace CYC in a WG patient [9]. We used MMF because of its strong immunosuppressive effect and lymphocyte-selective mode of action and because it has few side-effects. As illustrated here, alternative treatments to high-dose CS combined with CYC, azathioprine or high-dose IV Ig and/or new drugs should be attempted in the therapeutic strategy of refractory ANCA-related vasculitides.

Notes

Correspondence to: C. Le Hello. Back

References

  1. Fauci AS, Haynes BF, Katz P, Wolff SM. Wegener's granulomatosis: prospective clinical and therapeutic experience with 85 patients for 21 years. Ann Intern Med1983;98:76–85.[ISI][Medline]
  2. Anderson G, Coles ET, Crane M et al. Wegener's granuloma. A series of 265 British cases seen between 1975 and 1985. A report by a sub-committee of the British Thoracic Society Research Committee. Q J Med1992;302:427–38.
  3. Hoffman GS, Kerr GS, Leavitt RY et al. Wegener granulomatosis: an analysis of 158 patients. Ann Intern Med1992;116:488–98.[ISI][Medline]
  4. Francès C, Lê Thi Huong Du, Piette JC et al. Wegener's granulomatosis. Dermatological manifestations in 75 cases with clinicopathologic correlation. Arch Dermatol1994;130:861–7.[Abstract]
  5. Thomas RH, Payne CME, Black MM. Wegener's granulomatosis presenting as pyoderma gangrenosum. Clin Exp Dermatol1982;7:523–7.[ISI][Medline]
  6. Lerner EA, Dover JS. Malignant pyoderma: a manifestation of Wegener's granulomatosis? J Am Acad Dermatol1986;15:1051–2.[ISI][Medline]
  7. Reed WB, Jensen AK, Konwaler BE, Hunter D. The cutaneous manifestations in Wegener's granulomatosis. Acta Derm Venereol (Stockh)1963;43:250–64.[Medline]
  8. Hu CH, O'Loughlin S, Winkelmann RK. Cutaneous manifestations of Wegener granulomatosis. Arch Dermatol1977;113:175–82.[Abstract]
  9. Nowack R, Gobel U, Klooker P, Hergesell O, Andrassy K, van der Woude FJ. Mycophenolate mofetil for maintenance therapy of Wegener's granulomatosis and microscopic polyangiitis: a pilot study in 11 patients with renal involvement. J Am Soc Nephrol1999;10:1965–71.[Abstract/Free Full Text]
Accepted 7 August 2001