PMID- 27149138
OWN - NLM
STAT- MEDLINE
DCOM- 20170331
LR  - 20170331
IS  - 1847-6538 (Electronic)
IS  - 1330-027X (Linking)
VI  - 24
IP  - 1
DP  - 2016 Apr
TI  - Generalized Pyoderma Gangrenosum Associated with Ulcerative Colitis: Successful 
      Treatment with Infliximab and Azathioprine.
PG  - 83-5
AB  - Pyoderma gangrenosum (PG) is a rare ulcerative skin disease, part of the spectrum 
      of neutrophilic and auto-inflammatory dermatoses. Its pathogenesis is unknown, 
      although immune pathways have been implicated. Lesion biopsies show a 
      predominantly neutrophilic infiltrate. The incidence of PG is uncertain, but it 
      is estimated to be 3-10 per million per year, occurring at any age but most 
      commonly between 20 and 50 years with a possible slightly higher incidence in 
      women. Approximately 50% of patients with PG also have another disease associated 
      with PG. The most common is inflammatory bowel disease (IBD), particularly 
      Crohn's and ulcerative colitis (UC). Local treatment may be sufficient for mild 
      cases, while for severe cases systemic immunosuppressants are the mainstay (1,2). 
      We report the case of a patient with bullous PG and UC successfully treated with 
      infliximab and azathioprine. A 32-year-old male Caucasian patient presented with 
      painful violaceous vesicles and enlarging bullae of various sizes and with acute 
      onset, located on the trunk and bilaterally on both the lower and the upper 
      extremities. Lesions on the trunk were composed of hemorrhagic pustules with a 
      surrounding erythematous overhanging border. Some of the lesions had undergone 
      central necrosis and ulceration (Figure 1, a-d). The patient reported of the 
      lesions had appeared one week ago, simultaneously with the exacerbation of a 
      known inflammatory bowel disease with hemorrhagic mucoid diarrhea and fever of up 
      to 38.5 degrees C. The patient's medical history included UC affecting the whole colon 
      (pancolitis), diagnosed 5 months prior to the onset of the epidermal lesions, for 
      which the patient was receiving treatment with oral prednisolone 10 mg/day and 
      mesalazine granules. Blood tests showed severe anemia, leukocytosis, and 
      increased inflammatory markers (C-reactive protein, erythrocyte sedimentation 
      rate). Antinuclear antibodies (ANA), anti-double stranded DNA (anti-dsDNA) 
      andtibodies, antineutrophil cytoplasmic antibodies (cANCA), perinuclear 
      neutrophil antibodies (p-ANCA), antiphospholipid antibodies, and tumor markers 
      were within normal limits. The patient was negative for cryoglobulins, viral 
      hepatitis (B, C) and human immunodeficiency virus (HIV). Blood cultures were 
      negative. Microscopy and cultures for mycobacteria and fungi gave negative 
      results. Stool samples tested negative for infections agents. The Mantoux skin 
      test was negative. Colonoscopy showed severe pancolitis, and biopsies from the 
      rectum and sigmoid colon were consistent with chronic ulcerative colitis. 
      Abdominal ultrasound and chest and abdominal X-rays did not result in significant 
      findings. Because of severe anemia, the patient received 2 blood transfusions. 
      The histopathologic examination carried out on the erythematous border of a 
      lesion on the lower leg showed a neutrophilic infiltrate, confined to the dermis. 
      On the basis of clinical findings, the diagnosis of PG was established. Topical 
      wound care consisted of local wound care and a topical corticosteroid. Systemic 
      therapy was initiated with 40 mg/day methylprednisolone for 7 days, 30 mg/day for 
      7 days, then 25 mg/day, and then tapered down further. The patient received an 
      infusion of infliximab 7.5 mg/kg at weeks 0, 2, and 6 and every 8 weeks 
      thereafter. After week 2, oral azathioprine 2.5 mg/kg daily was added to the 
      treatment. The patient also received mesalazine tablets (2 g x2/day) and 
      mesalazine enema (1-2/day). The patient showed good response to treatment, with 
      clinical remission of skin lesions. Lesions healed with characteristic thin, 
      atrophic scars (Figure 2, a-d). At 7-month follow-up the patient was continuing 
      with infusions of infliximab 7.5 mg/kg and azathioprine 2.5 mg/kg and was still 
      in remission. We reported our experience with a case of generalized bullous 
      pyoderma gangrenosum associated with ulcerative colitis. Generalized pyoderma 
      gangrenosum is very rare. Bullous or atypical PG was first described by Perry and 
      Winklemann in 1972 (1). Brunsting et al. coined the term pyoderma gangrenosum 
      (PG) to describe a series of patients with recurrent ulcerations (3). The 
      incidence of this disease is uncertain. Its pathogenesis is unknown, but an 
      immunological background has been suggested. In approximately 50% of patients, an 
      underlying immunological disease is present, commonly inflammatory bowel disease 
      (IBD) (4-6). In larger series of patients with PG, approximately 50% present with 
      a primary disorder. Ulcerative colitis is found in 10-15% of cases. Crohn's 
      disease is associated with PG closed than UC. Less than 3% of patients with 
      Crohn's disease or UC develop PG (6). PG is characterized by cutaneous 
      ulcerations with mucopurulent or hemorrhagic exudate. It begins as an 
      inflammatory pustule with a surrounding halo that enlarges and begins to 
      ulcerate. These very painful ulcers present with undermined bluish borders with 
      surrounding erythema. The lesions of PG most commonly occur on the legs, but they 
      may occur anywhere on the body. The clinical picture of PG is very 
      characteristic. Therefore the diagnosis of PG is based firstly on clinical signs 
      and on the patient's history of underlying diseases and then supported by biopsy. 
      PG has four distinctive clinical and histological variants. Some have 
      morphological and histological features that overlap with other reactive 
      neutrophilic skin conditions. There are no diagnostic serologic features (6,7). 
      There is no evidence that the efficacy of treatment strategies for PG differs 
      between IBD and non-IBD patients. For patients with a diffuse disease or rapidly 
      progressive process, systemic treatment is essential. Immunosuppression is the 
      mainstay of treatment. Traditionally, the most commonly used drugs with the best 
      clinical experience are systemic corticosteroids. Corticosteroids have been 
      considered as first line treatment (6,8). As reported by the European Crohn's and 
      Colitis Organisation (ECCO) in 2008, an evidence-based consensus on the 
      management of special situations in patients with ulcerative colitis, systemic 
      corticosteroids are recommended (9). Treatment with corticosteroids (e.g. 
      prednisolone 1-2 mg per kg/day or pulse therapy with 1 g of methylprednisolone) 
      aims to prevent progression and rapidly stop inflammation (6). Additional 
      mesalamine and corticosteroids may be effective in patients with bowel disease 
      (10). In recent years, tumor necrosis alpha (TNF-alpha) inhibitors, such as 
      infliximab and adalimumab, were reported to be effective for PG associated with 
      IBD. These drugs block the biological activity of TNF-alpha, which effects regulatory 
      T cells, restoring their capacity to inhibit cytokine production. The TNF-alpha 
      inhibitors thus suppress the inflammatory processes that is involved in the 
      pathogenesis of PG (11). Infliximab, a chimeric monoclonal antibody, is given by 
      infusion at weeks 0, 2, and 6 and then every 8 weeks, usually at a dosage of 5 
      mg/kg. UC of patients with frequent disease relapse or those that are resistant 
      or dependent on corticosteroids is often treated with purine antimetabolites, 
      such as azathioprine (AZA) (10). AZA, a purine antimetabolite (2.5 mg per kg/day) 
      is administered for its steroid-sparing effects. The response occurs after 2 to 4 
      weeks (6, 10). Infliximab can be combined with AZA. Patients with UC treated with 
      infliximab plus AZA were more likely to achieve corticosteroid-free remission at 
      16 weeks than those receiving either monotherapy (10,12).
FAU - Chatzinasiou, Foteini
AU  - Chatzinasiou F
AD  - Foteini Chatzinasiou MD, PhD, 2nd Department of Dermatology and Venereology, 
      ATTIKON University Hospital, Rimini 1, 124 62 Athens, Greece; 
      foteinichatzinasiou@gmail.com.
FAU - Polymeros, Dimitrios
AU  - Polymeros D
FAU - Panagiotou, Maro
AU  - Panagiotou M
FAU - Theodoropoulos, Konstadinos
AU  - Theodoropoulos K
FAU - Rigopoulos, Dimitrios
AU  - Rigopoulos D
LA  - eng
PT  - Case Reports
PT  - Journal Article
PL  - Croatia
TA  - Acta Dermatovenerol Croat
JT  - Acta dermatovenerologica Croatica : ADC
JID - 9433781
RN  - 0 (Dermatologic Agents)
RN  - 0 (Immunosuppressive Agents)
RN  - B72HH48FLU (Infliximab)
RN  - MRK240IY2L (Azathioprine)
SB  - IM
MH  - Adult
MH  - Azathioprine/*therapeutic use
MH  - Colitis, Ulcerative/*complications
MH  - Dermatologic Agents/*therapeutic use
MH  - Humans
MH  - Immunosuppressive Agents/*therapeutic use
MH  - Infliximab/*therapeutic use
MH  - Male
MH  - Pyoderma Gangrenosum/*drug therapy/etiology
EDAT- 2016/05/07 06:00
MHDA- 2017/04/01 06:00
CRDT- 2016/05/06 06:00
PHST- 2016/05/06 06:00 [entrez]
PHST- 2016/05/07 06:00 [pubmed]
PHST- 2017/04/01 06:00 [medline]
PST - ppublish
SO  - Acta Dermatovenerol Croat. 2016 Apr;24(1):83-5.