In 2006, we reported the first case of UC exacerbation induced by combination therapy of PEG-IFN and RIB for chronic hepatitis C.10,13 Use of this combination therapy is common in Japan and increasing; therefore, additional cases of development or exacerbation of UC associated with this treatment have been reported. Here, we describe the results of a literature review of cases in which the development or exacerbation of UC was coincident with IFN and/or RIB treatment for chronic hepatitis C. We ACP-196 chemical structure also summarize the results of studies that evaluated the effectiveness of IFN for UC or Crohn’s disease, which were carried out primarily in Europe and the USA.18–24 IFN is an antiviral agent that belongs

to a class of proteins known as cytokines. IFN exerts many effects on the immune system, such as: (i) activating macrophages; (ii) upregulating natural killer cell activity; (iii) stimulating antibody-dependent cellular cytotoxicity; (iv) enhancing the effects of killer T cells; and (v) modulating antibody production.25 Common adverse effects of IFN include: (i) flu-like symptoms, fever, ague, general fatigue, headache, and arthralgia; (ii) gastrointestinal symptoms, such as appetite loss, nausea, vomiting, abdominal pain, diarrhea, and constipation; and (iii) skin eruptions or itching.26 Although the incidence is low, several autoimmune diseases can occur as adverse reactions to IFN. These include:

(i) UC and Crohn’s disease/inflammatory bowel disease (IBD); (ii) interstitial pneumonia; (iii) thyroid function abnormalities;27 (iv) autoimmune hemolytic anemia; (v) systemic lupus erythematosus; and (vi) rheumatoid arthritis. In the reported Proteasome inhibitor nine cases of UC exacerbation induced by IFN therapy in Japan (Table 1), seven were associated with IFN-α,2–8 one with IFN-α2b plus RIB,10 and the other with IFN-β;9 thus cases associated with IFN-α were more common. Many more cases of UC exacerbation induced by

PEG-IFN-α2a or 2b plus RIB are expected to be reported in the future as the use of combination therapy becomes more widespread. However, the number of reported cases of UC induced by IFN and RIB has not increased to date. One case of UC exacerbation induced by IFN-β has been reported in Japan,9 and Rodrigues et al. reported four cases of UC exacerbation induced by IFN-β therapy for multiple sclerosis (MS) in 2010.17 IFN-β has been evaluated as a treatment Paclitaxel research buy for UC in Europe and the USA; however, because IFN-β may cause or exacerbate UC, caution is needed in the design of future studies. The period between the development or exacerbation of UC from the start of IFN treatment ranges from only 1 day to 4.5 years, varying very widely among the nine cases reported in Japan2–10 and seven cases found through a MEDLINE search11–17 (one was a publication also found through a search of Japana Centra Revuo Medicina). The reports have assumed a cause-and-effect correlation between IFN treatment and UC development (Tables 1 and 2).