We describe a series of three patients treated with ustekinumab as prophylaxis for POR, all with long-standing CD with a stricturing and/or fistulising pattern, having needed one or more surgical resections, and previous treatment with two anti-TNFs and immunosuppressants as common features.

POR was assessed by: endoscopy, MR-enterography and biomarkers (faecal calprotectin, C-reactive protein, ESR and leucocytes).

A 50-year-old female smoker, with CD A2L1B2 diagnosed 12 years previously. She required her first surgical resection two years after diagnosis. Six years after surgery, she developed endoscopic and clinical POR, receiving treatment with azathioprine and infliximab, and later with adalimumab, but with subsequent loss of response. Eight years after diagnosis, she developed long symptomatic fibrotic strictures and a new surgical resection was performed, after which the decision was made for prophylactic treatment with ustekinumab 260 mg IV induction plus 90 mg SC every eight weeks as maintenance.

A 60-year-old male patient with Crohn's disease f A2B3L1, with two ileal resections. He received treatment with methotrexate, azathioprine and infliximab prior to his first resection, and adalimumab dose intensification prior to the second. In view of the patient's previous history, it was decided to start treatment with USTK to prevent POR, with induction doses of 260 mg IV and 290 mg SC as maintenance.

A 64-year-old male patient with Crohn's disease A2B3L1, operated on three times for fistulising disease and intra-abdominal collections, having received prior treatment with azathioprine, infliximab and adalimumab. After the last resection, it was decided to start prophylactic treatment with ustekinumab 260 mg IV and 90 mg SC every eight weeks, with a good response to date.

In our series, 100% of the patients (3/3) had a good clinical, analytical and endoscopic response in the first year of treatment with ustekinumab as prophylaxis for POR. There have been no treatment-related adverse effects or withdrawals due to poor tolerance.

In 2016, the EMA approved the use of ustekinumab in CD. It is a monoclonal antibody which inhibits the activity of human cytokines IL-12 and IL-23, slowing down the inflammatory cascade responsible for the disease.

To date, there are no clinical trials or case series assessing the use of ustekinumab as a preventive treatment for POR in patients undergoing surgical resections, but it does seem reasonable to use new therapeutic targets in patients with risk factors in whom clinical experience has shown the failure of anti-TNFs and thiopurines. In our series of cases, the patients received treatment with ustekinumab as prophylaxis for POR, all showing normal biochemical parameters and clinical and endoscopic remission after one year of treatment.

Although there is a lack of solid scientific evidence to promote its generalised use, ustekinumab is a promising therapeutic option, particularly in patients with CD and a high risk of POR.

The authors have no sources of funding to declare.

The authors declare that they have no conflicts of interest.