J Rheum Dis 2021; 28(1): 4-16
Published online January 1, 2021
© Korean College of Rheumatology
Correspondence to : Jae Hee Cheon http://orcid.org/0000-0002-2282-8904
Department of Internal Medicine and Institute of Gastroenterology, Yonsei University College of Medicine, 50-1 Yonsei-ro, Seodaemun-gu, Seoul 03722, Korea. E-mail:geniushee@yuhs.ac
Intestinal Behçet’s disease (intestinal BD) is a rare chronic inflammatory disorder of the intestine that is characterized by recurrent intestinal manifestations with other systemic features of BD. Intestinal BD is diagnosed when a typically shaped ulcer is observed in the gastrointestinal tract, and the clinical findings meet the diagnostic criteria for BD. Owing to the small number of patients, intestinal BD is easily underestimated. On the other hand, but it often requires surgical treatment because of severe complications, including intestinal perforations or massive bleeding. The same treatment strategies used for inflammatory bowel diseases, such as Crohn’s disease and ulcerative colitis, are used for intestinal BD. 5-Aminosalicylic acids, corticosteroids, and immunomodulators are considered conventional therapies, but a considerable number of patients eventually become unresponsive to these pharmaceutical treatments. Recently, biologic agents, such as anti-tumor necrosis factor-alpha inhibitors, have also been suggested as a new treatment option for intestinal BD. This article reviews the pathogenesis and diagnosis of intestinal BD and the current treatment strategies that are expected to be useful for rheumatologic specialists.
Keywords Behçet’s disease, Intestinal Behçet’s disease, Therapeutic strategy, Anti-TNF-α inhibitor
Behçet’s disease (BD) is a chronic and relapsing disorder that causes multisystemic inflammation. The disease was named after the Turkish dermatologist Hulûsi Behçet, who described BD for the first time in 1937 in patients with symptoms consisting of aphthous oral ulcers, genital ulcers, and iritis [1]. BD is rare in Western countries but is relatively prevalent in East Asia, Middle East Asia, and the Mediterranean region. In general, BD involves oral and genital ulcers and vascular and ocular manifestations. Occasionally, it can also occur in joints, central nervous system, and gastrointestinal tract. Intestinal BD is defined when a patient diagnosed with BD has prevalent intestinal symptoms and typical ulcerations observed on an endoscopic examination [2,3]. Among patients with BD, up to 5%∼10% are diagnosed with intestinal BD [4,5].
Similar to BD, the causes of intestinal BD are not completely understood, but genetic, immunologic, and environmental factors appear to be associated with the disease. The major symptoms of intestinal BD include abdominal pain, diarrhea, severe hematochezia, and even intestinal perforation. The symptoms and clinical courses are heterogeneous, ranging from mild to severe, and several patients show a poor prognosis. The demand for novel therapy and clinical trials is high because it is currently incurable, but relatively few studies have been conducted because of its low prevalence. Despite this limitation, clinical studies have been conducted [4]. Another aspect of intestinal BD is its similarity to inflammatory bowel disease (IBD). These two diseases share the same genetic background, pathogenesis, treatment strategies, and clinical outcomes. Hence, gastroenterologists often classified them as the same disease entity. Based on studies on the pathogenesis of immune-related diseases and clinical similarity of these two diseases, the therapeutic armamentarium for intestinal BD has been developed in accordance with that for IBD.
On the other hand, there is a critical demand for elaborate therapeutic strategies for intestinal BD because it frequently fails to respond to conventional therapies and is a long-standing disease requiring large amounts of medications. Moreover, BD is handled mainly by rheumatologists, whereas the gastroenterologists have more experience with patients with intestinal involvement of BD. Accordingly, intestinal BD, which has overlapping parts in terms of vasculitis and intestinal pathologies, requires cooperative care that can integrate expertise between rheumatology and gastroenterology under a systemic communication route. This review article provides up-to-date information for rheumatologist readers on the pathogenesis and treatment options for intestinal BD from the perspective of a gastroenterologist.
BD is difficult to confirm because no definitive diagnostic biomarker has been identified, and the related symptoms often develop asynchronously. Moreover, intestinal BD is more complicated because of its similarity to other illnesses, such as Crohn’s disease and intestinal tuberculosis. Thus, a differential diagnosis is important for deciding the therapeutic approach for intestinal BD. The diagnostic criteria for BD recommended by the BD research committee of Japan in 1987 have been used widely and consist of four major and five minor symptoms [6]. In 1990, the International Study Group for Behçet’s Disease also recommended the diagnostic criteria, which include recurrent oral ulceration and the presence of any two of the following clinical manifestations: genital ulcers, skin lesions, eye involvement, and positive pathergy reaction [7]. Traditionally, BD and intestinal BD are diagnosed based on subjective symptom assessments, which are often challenging and dependent on the clinicians’ experience. For a long time, intestinal BD was diagnosed when BD patients with predominantly gastrointestinal symptoms showed intestinal ulcerations on endoscopic and radiological examinations [3].
On the other hand, a delayed diagnosis is prevalent because not all patients with intestinal BD show systemic symptoms at the time of the endoscopic examination [8] because these symptoms may appear several years after the patient’s first experience of intestinal discomfort [9]. To overcome these limitations, novel diagnostic criteria have been recommended by the Korean Association for the Study of Intestinal Diseases using the modified Delphi process, which is now commonly used in clinical trials and patient treatment [10]. In accordance with these criteria, intestinal BD can be diagnosed when ulceration in the terminal ileum or inflammation in the small or large intestine is found along with clinical manifestations that satisfy the diagnostic criteria of BD. These clinical findings are particularly useful for diagnosing patients whose symptoms do not fully meet the diagnostic criteria for systemic BD at the initial presentation. Basically, a diagnosis of intestinal BD relies on a combination of clinical, endoscopic, pathological, and radiological findings [11]. The clinical manifestations are similar to those of IBD, including diarrhea, hematochezia, weight loss, and abdominal pain with tenderness on the affected area [12]. The typical endoscopic features are oval-shaped large intestinal ulcerations in the ileocecal area with deep and discrete borders [8]. These features can vary from aphthous to deep penetrating volcano-shaped ulcerations and ulcerations with a more frequently focal to less frequently diffuse distribution [13]. The pathological findings in patients with intestinal BD are vasculitis involving the small and medium-sized vessels; lymphocyte infiltration in the perivascular space can also be detected [14,15]. Figure 1 presents the recommended diagnostic algorithm, which includes endoscopic observations and systemic BD criteria [10].
In diseases with unknown etiologies and no accurate diagnostic biomarkers, such as BD or IBD, the level of inflammation cannot be easily measured using a single parameter. Hence, a disease activity scoring system is needed to monitor the inflammatory status objectively and confirm the disease severity. The BD activity indices usually include the severity, location, and extent of the disease, and complications [16]. For intestinal BD, a simple and validated measurement tool called the Disease Activity Index of intestinal Behçet’s disease (DAIBD) was proposed in 2011 by the Korean IBD Study Group for an assessment of the disease activity and establishing a therapeutic plan [17]. Before the development of the DAIBD, the Crohn’s disease activity index (CDAI) had been used for intestinal BD owing to the similarities between the two diseases [3]. The DAIBD involves eight categories: general condition, extraintestinal manifestations, fever, abdominal pain, abdominal mass, abdominal tenderness, intestinal complications, and frequent liquid stools. The items are rated, with total scores ranging from 0 to 325. The disease is categorized as quiescent, mild, moderate, and severe disease based on the total score (≤19, 20∼39, 40∼74, and ≥75, respectively). The DAIBD is highly weighted on the general well-being and abdominal pain rather than on the other indices. Although the DAIBD is not correlated significantly with the endoscopic severity [18], it is more responsive and shows a better correlation with the physician’s global assessment score than CDAI. Further studies will be needed in various ethnicities and for the validation of DAIBD regarding whether it can predict the disease course precisely based on endoscopic examinations and clinical symptoms.
Insights into the roles of genetic and immune responses in disease development or prognosis along with the development of molecular biological research techniques, including the genome-wide association studies (GWASs) and next-genome sequencing (NGS), have changed medical practice significantly [19]. The clinical symptoms and genetic features between intestinal BD and BD or IBD overlap; some genetic features of intestinal BD overlap with IBD, while others overlap with BD. A
Regarding the contribution of the immunological response to triggering inflammation, similar to those in other autoimmune diseases, increased levels of Th1, Th17, CD4+, and CD8+ T cell, and γδ+ T cell activities, as well as IL-12 and tumor necrosis factor alpha (TNF-α) levels, were elevated in patients with BD [27-32]. Most of the proinflammatory cytokines associated with the innate immune system are activated in Crohn’s disease and ulcerative colitis. This finding also applies to intestinal BD and has therapeutic implications. In patients with IBD, increasing numbers or activation of innate immune cells, including neutrophils, macrophages, and natural killer T cells, and adaptive immune cells, such as B and T cells, increase in the levels of TNF-α, IL-1β, interferon (IFN)-γ, and cytokines in the IL-23–Th17 pathway [33]. As with Crohn’s disease, Th1- and Th17-related cytokines (IL-12, IL-23, and IL-27) are also upregulated in BD [34]. A recent study reported that the IL-12B levels correlated with the clinical and endoscopic disease activities of intestinal BD and IBD [35]. Proteomic analysis showed that the IL-1β and serum amyloid A levels were markedly higher in patients with intestinal BD [36]. These explanations of the pathophysiology of intestinal BD and the genetic/clinical overlap between intestinal BD and IBD lead to a wide range of changes in the therapeutic environment of intestinal BD.
Owing to the rarity of intestinal BD, scrutinized or systematic prospective clinical trials have not been prevalently conducted. Empirical and evidence-based therapeutic approaches have been established based on several retrospective studies and the similar pathophysiological background between intestinal BD and Crohn’s disease, but the choice of treatment is still dependent on the physicians’ opinion [4]. In this regard, Japanese researchers published consensus statements for the diagnosis and standard therapy for intestinal BD in 2007 [3]. Revised versions of the statements were published in 2014 [37] and 2020 [38], including the statement that an anti-TNF inhibitor can be considered standard therapy. The treatment algorithm, according to the disease severity, has been proposed based on the accumulated studies and experts’ opinions in 2013 [39]. Considering the latest clinical trials and published data, this paper suggests an up-to-date treatment algorithm as follows (Figure 2). Basically, it is similar to the treatment procedure in the step-up therapy for IBD according to the disease severity (mild to moderate or severe) aiming to achieve and maintain clinical remission [40]. This is a sequential treatment procedure that is usually initiated by generally tolerable medications, such as 5-aminosalicylates, with escalation to the more effective but potentially more toxic drugs, including immunomodulators and biologics, for patients in whom each previous step of therapy has failed. With this algorithm, patients can avoid overtreatment and the unnecessary risk of adverse events, particularly in cases of a tolerable standard therapy. In IBD treatment, the top-down therapy strategy was proposed to induce rapid clinical remission with highly effective medications, such as early biologics, but no such attempts or research studies have been performed for intestinal BD. Surgery should be considered in a timely manner when the patient is suspected of severe complications or does not respond properly to the medical treatment. Complications, even irreversible ones, are likely to occur in accordance with a delayed decision of surgical intervention. Hence, the close discussion between gastroenterologists and surgeons is required. Therefore, a multidisciplinary approach should be available whenever their expertise is demanded in the intestinal BD treatment.
5-Aminosalicylic acids (5-ASA) have a similar mechanism to aspirin or non-steroidal anti-inflammatory drugs, which target the COX-2-inducing immunomodulatory actions to reduce intestinal inflammation [41]. 5-ASA inhibits COX-2 expression resulting from TNF-α/IL-1β [42]. The 5-ASAs used widely for IBD treatment, especially for patients with ulcerative colitis, are mesalamine, mesalazine, or sulfasalazine [43]. The clinical dosages of 5-ASA in patients with intestinal BD usually range from 2 to 4 g/day, while sulfasalazine is generally administered at 3 to 4 g/day [4]. Several clinical studies have obtained inconsistent results regarding the effectiveness of 5-ASA for intestinal BD. A case series study that included patients with intestinal BD reported that 79% patients showed symptomatic or colonoscopic improvement with sulfasalazine therapy [44]. A large-scale retrospective study conducted in 2012 showed that 5-ASA/sulfasalazine monotherapy was effective in maintaining remission, specifically with cumulative relapse rates of 46.7% at 10 years after remission. Younger age, disease severity, and higher C-reactive protein (CRP) level were associated with a poor prognosis with 5-ASA/sulfasalazine therapy [45]. A recent study investigated the induction response rate of oral 5-ASA and showed response and remission rates of 61% and 57%, respectively, at week 8 [46]. Thus, 5-ASA can be recommended as induction and maintenance therapies for relatively mild to moderate intestinal BD. Conclusively, 5-ASA is a substantial therapeutic option that needs to be used in almost all patients with intestinal BD. On the other hand, patients with small bowel involvement are not indicated for sulfasalazine use.
Systemic corticosteroids are used effectively to control flare-ups in patients with moderate to severe BD and IBD in cases of failure of 5-ASA/sulfasalazine treatment [47-49]. Corticosteroids, which are well-known fast-acting anti-inflammatory drugs, are used widely with tapering strategies at a starting dosage of 0.5∼1.0 mg/kg/day [3] that is tapered to 5 mg each week and stopped within three months. Well-designed prospective clinical trials on the effectiveness of corticosteroids in patients with intestinal BD have not been conducted thus far. Some retrospective studies have suggested that corticosteroids are effective in the induction phase of intestinal BD. One retrospective cohort study [50] in Korea that included 54 patients reported that 46.3% (n=25) of patients with active intestinal BD achieved complete remission after one month of treatment, while 42.6% showed partial remission. After three months of treatment, 40.7% of the patients still responded to the corticosteroid treatment. One year after the initiation of corticosteroid administration, 48.1% of the patients remained responsive to the treatment, and 8.1% showed a prolonged response, but 35.2% had corticosteroid dependency, and 7.4% underwent intestinal surgery. Thus, it is recommended for inducing a short-term response in the early phase of the disease course, especially with severe systemic symptoms or severe disease activity. Considering that patients with intestinal BD with high-risk factors, such as gastrointestinal bleeding, mainly use this medication, side effects are the main burden for both physicians and patients because they increase the risk of gastrointestinal bleeding and perforation [51]. In addition, corticosteroid therapy was strongly associated with rebleeding in patients with intestinal BD (hazard ratio [HR], 3.2; 95% confidence interval, 1.070∼9.462; p=0.037) [52]. Therefore, a tapering dose strategy should be maintained, and the prolonged use of prednisolone must not exceed 10 mg/day. Systemic corticosteroids are often used too easily without hesitation, even if there are no symptoms. Moreover, they are often prolonged in clinical practice. Steroid usage should be based rigorously on the overall symptoms, and should not be used unconditionally due only to the presence of intestinal ulcers.
Thiopurine analogs, consisting of 6-mercaptopurine (6-MP) and its derivate, azathioprine (AZA), are functioning antimetabolites of nucleic acids that were introduced to inhibit the growth of rapidly dividing cells in the 1950s [53]. Thiopurines require an extensive metabolism to form thioguanine nucleotides (TGNs) because they are prodrugs that act specifically via the following three pathways: (1) inactivation of 6-MP to thiouric acid by xanthine oxidase and aldehyde oxidase, (2) 6-methyl MP (6-MMP) production by thiopurine methyltransferase (TPMT), (3) conversion of 6-MP to 6-TGN by enzymes, such as TPMT, inosine monophosphate dehydrogenase, and hypoxanthine phosphoribosyl transferase [54,55]. Regarding the mechanism of action of thiopurines, TPMT plays a major role in producing inactive 6-MMP and active 6-TGN by generating 6-methyl MP ribonucleotide (6-MMPR), and can ultimately increase 6-TGN production by converting 6-thioinosine monophosphate to 6-MMR indirectly [56]. The anti-inflammatory action of thiopurine is achieved by 6-TGN. In particular, it is integrated into leukocyte DNA and prevents DNA synthesis, which inhibits downstream T-cell proliferation and immunosuppression [57]. Based on this metabolism, AZA/6-MP is commonly indicated for patients with moderate to severe intestinal BD, specifically those who are refractory or dependent on corticosteroids or show a secondary loss of response to anti-TNF-α agents. The drug is also used to reduce the postoperative recurrence rate after intestinal surgery [58].
AZA (25 to 50 mg/day) is effective for both the cellular and humoral immune responses, particularly for the initial dose indication, in patients with intestinal BD. The dose can be increased gradually every 2 to 3 weeks up to 2.0 to 2.5 mg/kg, unless adverse drug reactions occur, such as leukopenia [59]. Although only one retrospective cohort study was conducted in patients with intestinal BD treated with AZA, it established the benefit of AZA as maintenance therapy. Jung et al. [59] evaluated 272 patients with intestinal BD who received thiopurine monotherapy and reported that 58.2% (39/67) of patients who received the first course of thiopurine remained in remission with thiopurine maintenance therapy. In this study, the cumulative relapse rates at 1, 2, 3, and 5 years after remission were 5.8%, 28.7%, 43.7%, and 51.7%, respectively. Younger age (<25 years) at diagnosis and lower hemoglobin level (<11 g/dL) were associated with a poor prognosis.
Similarly, Lee at al. [58] reviewed the postoperative recurrence rate of intestinal BD in patients who received thiopurine treatment, and the cumulative rate of clinical recurrence after surgery was significantly lower in the thiopurine group than in the 5-ASA treatment group (p= 0.050). Moreover, the HR of postoperative thiopurines compared to 5-ASA was 0.636 (range, 0.130∼1.016; p=0.053) for postoperative recurrence. AZA is an effective treatment for intestinal inflammation and can be used stably in the long term unless side effects occur. The most common and serious side effect is leukopenia, which increases the infection risk and even mortality [60]. Thus, the American Gastroenterological Association recommends that patients treated with AZA should be monitored routinely with complete blood counts [61].
With regard to IBD treatment, a genotype-based strategy for thiopurine treatment using the
Methotrexate (MTX) is an analog of folic acid and aminopterin that was first manufactured in 1945 and is a long-standing medication that has been used for patients with cancer since the 1950s [63]. Recently, it has gained renewed attention as a notable therapy for autoimmune diseases. Low-dose MTX (25 mg/day for the induction phase) appears to be effective in the treatment of rheumatoid arthritis, neuro-BD, uveitis, and other types of BD involvement [64-66]. In addition, MTX is used increasingly in combination with biologics owing to the immuno-genicity of anti-TNF inhibitors [67]. The mechanism of immunosuppression by MTX mainly involves the reduction of cell proliferation, an increase in the rate of apoptosis of T-cells, and endogenous adenosine accumul-ation. Hence, it can alter cytokine production, humoral responses, and bone formation, which leads to the deactivation of the immune system [68]. The effectiveness and safety of MTX for intestinal BD have rarely been investigated. A case series of 10 patients with refractory intestinal BD reported improved symptoms and disease-related complications within four weeks of MTX treatment in 2011 [69]. Moreover, the ulcers disappeared in nine of the patients at 12 months.
Park et al. [70] published retrospective data on the efficacy of MTX therapy, specifically MTX monotherapy and combination therapy with MTX and adalimumab (ADA), for intestinal BD in 2018. Among 10 patients, three and five attained steroid-free remission at three and six months, respectively. The serum CRP level, erythrocyte sedimentation rate, and DAIBD score decreased at six months compared to their baseline values, but only the decrease in CRP levels was statistically significant (p= 0.039) [70].
(3) Other immunomodulatorsImmunomodulators, including cyclosporine, tacrolimus, interferon (IFN), and intravenous immunoglobulin (IVIG), are considered alternative therapeutic options for intestinal BD based on their pharmaceutical mechanism. On the other hand, no sufficient scientific evidence exists because of the relatively few cases reported, and no prospective clinical trials of immunomodulators have been conducted in patients with intestinal BD. Cyclosporine, which decreases the levels of inflammatory cytokines in T-lymphocytes by blocking the phosphatase activity of calcineurin [71], is commonly used for autoimmune diseases, such as rheumatoid arthritis, psoriasis, and ocular manifestations of BD [72,73]. According to the updated European League Against Rheumatism guideline, nervous system involvement is not indicated for cyclosporine based on level 3 evidence [74]. Bayraktar et al. [75] and the unpublished experience from Severance Hospital suggest that cyclosporine therapy has no clinical benefit for patients with intestinal BD. Tacrolimus, a macrocyclic lactone with potent immunosuppressive properties [76], is a standard immunosuppressive regimen after renal transplantation [77]. One case was reported, and clinical improvement was observed in patients with intestinal BD refractory to conventional therapies [78]. IFN and IVIG were introduced in the 1950s and have been used for arthritis, BD [79,80], and other autoimmune diseases.
On the other hand, studies examining the role of these therapies in intestinal BD are limited. Therefore, the efficacy of IFN or IVIG for intestinal BD is unclear. A study of patients with BD who were unresponsive to systemic steroids and/or immunosuppressants was conducted using subcutaneous IFN‐α at a dosage of 6×106 IU/day three times per week for two months. In that study, 75% (9/12) of the patients achieved complete remission, 16.6% (2/12) had partial remission, and 8.3% showed no response [81]. In 1998, a 32-year-old Caucasian woman with intestinal BD was treated with IVIG. Her symptoms improved after IVIG treatment initiation, and the intestinal lesions disappeared after six weeks of IVIG therapy at 400 mg/kg/day for five days [82]. Nevertheless, further evidence and clinical trials will be needed to prove their efficacy.
Thalidomide was first used as a sedative in the 1950s and withdrawn from the European pharmaceutical market in the 1960s owing to its teratogenic effects in early pregnancy, including severe birth defects, such as phocomelia [83]. This was defined as a “thalidomide tragedy” and has been a major issue in the history of biomedical ethics and drug safety monitoring. Eventually, it contributed to the approval system and toxicology guidelines of the United States Food and Drug Administration [84,85]. After several clinical trials over a decade, thalidomide has now been approved and used for the treatment of inflammatory diseases, including leprosy, rheumatoid arthritis, BD, and even multiple myeloma or malignant B-cell lymphoma [86-88]. Thalidomide, a synthetic derivative of glutamic acid, was suggested to be effective against the mucocutaneous and follicular lesions of BD based on the results of a randomized, double-blind, placebo-controlled study [89]. A case series of BD with intestinal involvement reported that thalidomide was effective for recurrent perforating intestinal ulcers and led to clinical improvement in terms of corticosteroid-free remission [90,91].
These outcomes were observed consistently in another case series in Korea [92]. Patients with recurrent intestinal BD refractory to conventional treatments, including 5-ASA and immunomodulators, reported a response to thalidomide with clinical and radiological improvement. The major side effects observed were edema, neutropenia, and sepsis. Similarly, a prospective open-label study of patients with IBD treated with thalidomide reported clinical response rates of 83.3% and 100.0% for Crohn’s disease and ulcerative colitis at week 12 [93]. Definitive dose guidelines for intestinal BD are not available. On the other hand, an initial thalidomide dosage of 2 mg/kg/day has been used, and dose adjustment according to the treatment response is needed [90]. In addition, thalidomide appears to exert a selective effect on TNF‐α production by the degradation of its encoding messenger RNA [94]. Thus, the efficacy and safety of anti-TNF inhibitor or thalidomide therapy were investigated in patients with intestinal BD who were refractory to conventional therapies [95]. Of 13 patients, 10 (75%) achieved clinical and endoscopic remission with TNF-α antagonists and/or thalidomide therapy. This result also supports the efficacy of thalidomide as a therapeutic option for intestinal BD. Nevertheless, well-designed prospective trials are still needed, and rigorous monitoring of the side effects is warranted.
While recent advances in the novel therapeutic armamentarium, including biologics for autoimmune diseases, have made transformative changes in therapeutic environments. Several biologic agents are now available for patients with autoimmune diseases, particularly those who do not respond to conventional therapies or those who develop serious adverse events. The use of these biologics has also been attempted in patients with intestinal BD. As mentioned previously, the pathogenesis of intestinal BD is related to an abnormal T-cell immune response and cytokines derived from T helper type 1 (Th1) lymphocytes, including TNF-α, IFN-γ, IL-12, and IL-18 [96,97]. The TNF-α expression level in the blood increases, mucosal damage occurs, and clinical symptoms worsen [98]. Therefore, biologics targeting TNF-α have been administered to patients with intestinal BD with these scientific backgrounds. Currently, anti-TNF-α monoclonal antibodies, including infliximab (IFX) and ADA, are considered standard therapies for patients with intestinal BD [37].
(1) InfliximabIFX, a TNF blocker, is indicated for patients with IBD, arthritis, ankylosing spondylitis, and psoriasis, and who have shown an inadequate response to conventional therapy [4]. A dose of 5 mg/kg at zero, two, and six weeks is suggested for induction therapy and then every eight weeks for maintenance therapy. Some adult patients who respond initially to treatment may benefit from increasing the dose to 10 mg/kg if they later become unresponsive to this treatment [37]. The first case report of IFX use for intestinal BD was in 2001, which showed a decreased CDAI score from 270 to 13 points by week two, and endoscopic and histological improvements at week 10 [99]. The following case reports consistently suggested the positive efficacy of IFX for intestinal BD as both induction and maintenance therapy [100,101]. A multicenter retrospective study in patients with moderate to severe intestinal BD reported the results of IFX treatment from 28 patients in Korean tertiary hospitals [102]. The clinical response rates at 2, 4, 30, and 54 weeks were 75%, 64.3%, 50%, and 39.1%, respectively, and the clinical remission rate at week 30 was 46.2%. During the follow-up period, one case of serious infection was observed, but no malignancies or deaths occurred. The efficacy and safety of IFX were investigated in a prospective open-label phase 3 study in 2016, which included 18 patients with BD. Among the patients enrolled, 11 had intestinal involvement and were refractory to conventional therapies [103]. The IFX dose was the same as that for Crohn’s disease and ulcerative colitis. A complete response was observed in 61% (11/18) of patients at weeks 14 and 30, and the patients remained in remission until week 54. The CRP levels were decreased after week two, and most of the subjects showed healed ulcers at week 14. Despite these results, as with patients with IBD, the patients with intestinal BD in this study also showed a primary and secondary loss of response. Hence, the need to increase the dose at week 30 or treatment failure were observed [103]. An interventional, open-label, single-arm, multicenter study of IFX in 33 patients with moderate to severe refractory intestinal BD is ongoing in Korea (ClinicalTrials.gov NCT02505568). This study is expected to provide more scientific evidence for the effectiveness of IFX treatment for patients with intestinal BD. Studies are still lacking, but evidence for the positive efficacy of IFX combination therapy with immunomo-dulators has been reported. In a previous study [69], all 10 patients showed improvement in the intestinal symptoms and complications within four weeks. The rate of disappearance of ileocecal ulcerations was 50% (5/10) and 90% (9/10) at 6 and 12 months, respectively [69]. Combination therapy of biologics with immunomodulators is beneficial for reducing the immunogenicity and increasing the serum levels, but the risks of infection and malignancy need to be considered carefully [104].
(2) AdalimumabADA is a fully human anti-TNF-α monoclonal antibody, whereas IFX is a chimeric monoclonal antibody against TNF-α. The doses for patients with intestinal BD can be used for induction therapy at doses of 160, 80, and 40 mg at week zero (baseline), two, and four subcutaneously, and then 40 mg every other week for responders [105]. De Cassan et al. [106] described their experience with ADA use as the first anti-TNF-α inhibitor in two patients with familial intestinal BD, who were steroid dependent. Rapid clinical remission was observed in the induction phase, which was sustained in the maintenance phase.
The following case report suggested the efficacy of ADA for intestinal BD with myelodysplastic syndrome based on successful improvement in gastrointestinal symptoms, CRP levels, leukocytopenia, and anemia four months after the ADA treatment [107]. After that, a prospective multicenter open-label study was conducted in Japan that involved 20 patients with intestinal BD, who were refractory to conventional therapies, such as corticosteroids or immunomodulators [105]. Nine patients (45%) achieved the primary endpoints after 24 weeks, which were an alleviation of gastrointestinal symptoms and a decrease in the endoscopic assessment score to 1 or lower than the baseline score. In addition, ADA treatment induced complete remission in 20% of patients at week 24, which was maintained until week 52, but no notable safety issues were observed. A recent phase 3 study in Japan evaluated the efficacy and long-term safety profiles of ADA treatment in 20 patients with intestinal BD. Fifteen of the patients remained in the study until 100 weeks of follow-up. Significant improvement, which was defined based on the gastrointestinal symptom and endoscopic scores, was observed in 60% of patients at week 52 and 40% at week 100. Of the patients, 20% and 15% showed clinical remission at weeks 52 and 100, respectively, with tolerable safety profiles [108]. These results played a pivotal role in gaining approval of the use of ADA for intestinal BD treatment in Japan. Combination therapy using ADA with other immunomodulatory medications has not yet been actively investigated. Vitale et al., however, compared the efficacy and safety of ADA monotherapy and combination therapy with disease-modifying antirheumatic drugs. In this study, 100 patients with BD were enrolled; no significant difference in clinical outcomes was observed between the two groups [109].
A study in 2019 examined the effectiveness of anti-TNFs in patients with intestinal BD compared to that of corticosteroids without anti-TNF. Both groups showed improvement in the DAIBD score one year after treatment (85.2±29.6 to 40.5±44.7 in the corticosteroid group and 64.7±34.9 to 21.1±28.9 in the anti-TNF group). Anti-TNF administration was effective in reducing the concomitant steroid dose to <7.5 mg (p=0.0001). Considering that one patient discontinued treatment because of bacterial infection, the potential risk of intestinal perforation or massive bleeding should be considered when using steroids [110]. A recently published study that used real-world data on ADA and IFX for patients with refractory intestinal BD suggested switching from an anti-TNF inhibitor to another if a patient is refractory to the first-line anti-TNF inhibitor [111]. Biologics can be ineffective in cases of urgent patients who require surgical intervention. Therefore, a decision should be made under a multi-disciplinary discussion, including gastroenterologists, rheumatologists, and surgeons, as to whether to discontinue the treatment and perform surgery.
The prevalence of intestinal BD is low in Western countries but relatively high in East Asian countries, including Korea. Thus, there are limited clinical trial data with intestinal BD due to the general lack of disease awareness, small number of cases, and difficulty in subject recruitment. In addition, it is a relapsing, complex systemic inflammatory disease that is often unpredictable and has a “wax and wane” disease course with massive bleeding and perforation. Patients are easily refractory to conventional therapies, which caused new biologics to evolve in the treatment of intestinal BD. Intestinal BD can be treated using the same therapeutic approaches for BD, but the differences in intestinal BD from other types of BD in terms of the intestinal specific pathophysiology and treatment response must be considered. Thus far, the IBD treatment guidelines are effective in the treatment of intestinal BD. Several retrospective studies or clinical trials with a small number of patients have been the mainstay for gathering evidence on intestinal BD treatment. On the other hand, recent prospective and scientifically designed clinical trials specifically for intestinal BD have actively been conducted. Therefore, an effective treatment guideline is expected to be established soon. As for biologics, many novel agents with different targets have emerged for autoimmune diseases, including IL 12/23, Janus kinases, and IL-6 inhibitors. Further clinical research focusing on intestinal BD will be needed to obtain scientific evidence and provide treatment opportunities to the patients. Ultimately, close cooperation between rheumatology, gastroenterology, and colorectal surgery departments as multidisciplinary care is essential for the treatment of intestinal BD.
The author wishes to thank Sinyoung Park, who assisted in collecting and analyzing the related literature, and writing and revising the manuscript.
No potential conflict of interest relevant to this article was reported.
J Rheum Dis 2021; 28(1): 4-16
Published online January 1, 2021 https://doi.org/10.4078/jrd.2021.28.1.4
Copyright © Korean College of Rheumatology.
Department of Internal Medicine and Institute of Gastroenterology, Yonsei University College of Medicine, Seoul, Korea
Correspondence to:Jae Hee Cheon http://orcid.org/0000-0002-2282-8904
Department of Internal Medicine and Institute of Gastroenterology, Yonsei University College of Medicine, 50-1 Yonsei-ro, Seodaemun-gu, Seoul 03722, Korea. E-mail:geniushee@yuhs.ac
Intestinal Behçet’s disease (intestinal BD) is a rare chronic inflammatory disorder of the intestine that is characterized by recurrent intestinal manifestations with other systemic features of BD. Intestinal BD is diagnosed when a typically shaped ulcer is observed in the gastrointestinal tract, and the clinical findings meet the diagnostic criteria for BD. Owing to the small number of patients, intestinal BD is easily underestimated. On the other hand, but it often requires surgical treatment because of severe complications, including intestinal perforations or massive bleeding. The same treatment strategies used for inflammatory bowel diseases, such as Crohn’s disease and ulcerative colitis, are used for intestinal BD. 5-Aminosalicylic acids, corticosteroids, and immunomodulators are considered conventional therapies, but a considerable number of patients eventually become unresponsive to these pharmaceutical treatments. Recently, biologic agents, such as anti-tumor necrosis factor-alpha inhibitors, have also been suggested as a new treatment option for intestinal BD. This article reviews the pathogenesis and diagnosis of intestinal BD and the current treatment strategies that are expected to be useful for rheumatologic specialists.
Keywords: Behç,et&rsquo,s disease, Intestinal Behç,et&rsquo,s disease, Therapeutic strategy, Anti-TNF-&alpha, inhibitor
Behçet’s disease (BD) is a chronic and relapsing disorder that causes multisystemic inflammation. The disease was named after the Turkish dermatologist Hulûsi Behçet, who described BD for the first time in 1937 in patients with symptoms consisting of aphthous oral ulcers, genital ulcers, and iritis [1]. BD is rare in Western countries but is relatively prevalent in East Asia, Middle East Asia, and the Mediterranean region. In general, BD involves oral and genital ulcers and vascular and ocular manifestations. Occasionally, it can also occur in joints, central nervous system, and gastrointestinal tract. Intestinal BD is defined when a patient diagnosed with BD has prevalent intestinal symptoms and typical ulcerations observed on an endoscopic examination [2,3]. Among patients with BD, up to 5%∼10% are diagnosed with intestinal BD [4,5].
Similar to BD, the causes of intestinal BD are not completely understood, but genetic, immunologic, and environmental factors appear to be associated with the disease. The major symptoms of intestinal BD include abdominal pain, diarrhea, severe hematochezia, and even intestinal perforation. The symptoms and clinical courses are heterogeneous, ranging from mild to severe, and several patients show a poor prognosis. The demand for novel therapy and clinical trials is high because it is currently incurable, but relatively few studies have been conducted because of its low prevalence. Despite this limitation, clinical studies have been conducted [4]. Another aspect of intestinal BD is its similarity to inflammatory bowel disease (IBD). These two diseases share the same genetic background, pathogenesis, treatment strategies, and clinical outcomes. Hence, gastroenterologists often classified them as the same disease entity. Based on studies on the pathogenesis of immune-related diseases and clinical similarity of these two diseases, the therapeutic armamentarium for intestinal BD has been developed in accordance with that for IBD.
On the other hand, there is a critical demand for elaborate therapeutic strategies for intestinal BD because it frequently fails to respond to conventional therapies and is a long-standing disease requiring large amounts of medications. Moreover, BD is handled mainly by rheumatologists, whereas the gastroenterologists have more experience with patients with intestinal involvement of BD. Accordingly, intestinal BD, which has overlapping parts in terms of vasculitis and intestinal pathologies, requires cooperative care that can integrate expertise between rheumatology and gastroenterology under a systemic communication route. This review article provides up-to-date information for rheumatologist readers on the pathogenesis and treatment options for intestinal BD from the perspective of a gastroenterologist.
BD is difficult to confirm because no definitive diagnostic biomarker has been identified, and the related symptoms often develop asynchronously. Moreover, intestinal BD is more complicated because of its similarity to other illnesses, such as Crohn’s disease and intestinal tuberculosis. Thus, a differential diagnosis is important for deciding the therapeutic approach for intestinal BD. The diagnostic criteria for BD recommended by the BD research committee of Japan in 1987 have been used widely and consist of four major and five minor symptoms [6]. In 1990, the International Study Group for Behçet’s Disease also recommended the diagnostic criteria, which include recurrent oral ulceration and the presence of any two of the following clinical manifestations: genital ulcers, skin lesions, eye involvement, and positive pathergy reaction [7]. Traditionally, BD and intestinal BD are diagnosed based on subjective symptom assessments, which are often challenging and dependent on the clinicians’ experience. For a long time, intestinal BD was diagnosed when BD patients with predominantly gastrointestinal symptoms showed intestinal ulcerations on endoscopic and radiological examinations [3].
On the other hand, a delayed diagnosis is prevalent because not all patients with intestinal BD show systemic symptoms at the time of the endoscopic examination [8] because these symptoms may appear several years after the patient’s first experience of intestinal discomfort [9]. To overcome these limitations, novel diagnostic criteria have been recommended by the Korean Association for the Study of Intestinal Diseases using the modified Delphi process, which is now commonly used in clinical trials and patient treatment [10]. In accordance with these criteria, intestinal BD can be diagnosed when ulceration in the terminal ileum or inflammation in the small or large intestine is found along with clinical manifestations that satisfy the diagnostic criteria of BD. These clinical findings are particularly useful for diagnosing patients whose symptoms do not fully meet the diagnostic criteria for systemic BD at the initial presentation. Basically, a diagnosis of intestinal BD relies on a combination of clinical, endoscopic, pathological, and radiological findings [11]. The clinical manifestations are similar to those of IBD, including diarrhea, hematochezia, weight loss, and abdominal pain with tenderness on the affected area [12]. The typical endoscopic features are oval-shaped large intestinal ulcerations in the ileocecal area with deep and discrete borders [8]. These features can vary from aphthous to deep penetrating volcano-shaped ulcerations and ulcerations with a more frequently focal to less frequently diffuse distribution [13]. The pathological findings in patients with intestinal BD are vasculitis involving the small and medium-sized vessels; lymphocyte infiltration in the perivascular space can also be detected [14,15]. Figure 1 presents the recommended diagnostic algorithm, which includes endoscopic observations and systemic BD criteria [10].
In diseases with unknown etiologies and no accurate diagnostic biomarkers, such as BD or IBD, the level of inflammation cannot be easily measured using a single parameter. Hence, a disease activity scoring system is needed to monitor the inflammatory status objectively and confirm the disease severity. The BD activity indices usually include the severity, location, and extent of the disease, and complications [16]. For intestinal BD, a simple and validated measurement tool called the Disease Activity Index of intestinal Behçet’s disease (DAIBD) was proposed in 2011 by the Korean IBD Study Group for an assessment of the disease activity and establishing a therapeutic plan [17]. Before the development of the DAIBD, the Crohn’s disease activity index (CDAI) had been used for intestinal BD owing to the similarities between the two diseases [3]. The DAIBD involves eight categories: general condition, extraintestinal manifestations, fever, abdominal pain, abdominal mass, abdominal tenderness, intestinal complications, and frequent liquid stools. The items are rated, with total scores ranging from 0 to 325. The disease is categorized as quiescent, mild, moderate, and severe disease based on the total score (≤19, 20∼39, 40∼74, and ≥75, respectively). The DAIBD is highly weighted on the general well-being and abdominal pain rather than on the other indices. Although the DAIBD is not correlated significantly with the endoscopic severity [18], it is more responsive and shows a better correlation with the physician’s global assessment score than CDAI. Further studies will be needed in various ethnicities and for the validation of DAIBD regarding whether it can predict the disease course precisely based on endoscopic examinations and clinical symptoms.
Insights into the roles of genetic and immune responses in disease development or prognosis along with the development of molecular biological research techniques, including the genome-wide association studies (GWASs) and next-genome sequencing (NGS), have changed medical practice significantly [19]. The clinical symptoms and genetic features between intestinal BD and BD or IBD overlap; some genetic features of intestinal BD overlap with IBD, while others overlap with BD. A
Regarding the contribution of the immunological response to triggering inflammation, similar to those in other autoimmune diseases, increased levels of Th1, Th17, CD4+, and CD8+ T cell, and γδ+ T cell activities, as well as IL-12 and tumor necrosis factor alpha (TNF-α) levels, were elevated in patients with BD [27-32]. Most of the proinflammatory cytokines associated with the innate immune system are activated in Crohn’s disease and ulcerative colitis. This finding also applies to intestinal BD and has therapeutic implications. In patients with IBD, increasing numbers or activation of innate immune cells, including neutrophils, macrophages, and natural killer T cells, and adaptive immune cells, such as B and T cells, increase in the levels of TNF-α, IL-1β, interferon (IFN)-γ, and cytokines in the IL-23–Th17 pathway [33]. As with Crohn’s disease, Th1- and Th17-related cytokines (IL-12, IL-23, and IL-27) are also upregulated in BD [34]. A recent study reported that the IL-12B levels correlated with the clinical and endoscopic disease activities of intestinal BD and IBD [35]. Proteomic analysis showed that the IL-1β and serum amyloid A levels were markedly higher in patients with intestinal BD [36]. These explanations of the pathophysiology of intestinal BD and the genetic/clinical overlap between intestinal BD and IBD lead to a wide range of changes in the therapeutic environment of intestinal BD.
Owing to the rarity of intestinal BD, scrutinized or systematic prospective clinical trials have not been prevalently conducted. Empirical and evidence-based therapeutic approaches have been established based on several retrospective studies and the similar pathophysiological background between intestinal BD and Crohn’s disease, but the choice of treatment is still dependent on the physicians’ opinion [4]. In this regard, Japanese researchers published consensus statements for the diagnosis and standard therapy for intestinal BD in 2007 [3]. Revised versions of the statements were published in 2014 [37] and 2020 [38], including the statement that an anti-TNF inhibitor can be considered standard therapy. The treatment algorithm, according to the disease severity, has been proposed based on the accumulated studies and experts’ opinions in 2013 [39]. Considering the latest clinical trials and published data, this paper suggests an up-to-date treatment algorithm as follows (Figure 2). Basically, it is similar to the treatment procedure in the step-up therapy for IBD according to the disease severity (mild to moderate or severe) aiming to achieve and maintain clinical remission [40]. This is a sequential treatment procedure that is usually initiated by generally tolerable medications, such as 5-aminosalicylates, with escalation to the more effective but potentially more toxic drugs, including immunomodulators and biologics, for patients in whom each previous step of therapy has failed. With this algorithm, patients can avoid overtreatment and the unnecessary risk of adverse events, particularly in cases of a tolerable standard therapy. In IBD treatment, the top-down therapy strategy was proposed to induce rapid clinical remission with highly effective medications, such as early biologics, but no such attempts or research studies have been performed for intestinal BD. Surgery should be considered in a timely manner when the patient is suspected of severe complications or does not respond properly to the medical treatment. Complications, even irreversible ones, are likely to occur in accordance with a delayed decision of surgical intervention. Hence, the close discussion between gastroenterologists and surgeons is required. Therefore, a multidisciplinary approach should be available whenever their expertise is demanded in the intestinal BD treatment.
5-Aminosalicylic acids (5-ASA) have a similar mechanism to aspirin or non-steroidal anti-inflammatory drugs, which target the COX-2-inducing immunomodulatory actions to reduce intestinal inflammation [41]. 5-ASA inhibits COX-2 expression resulting from TNF-α/IL-1β [42]. The 5-ASAs used widely for IBD treatment, especially for patients with ulcerative colitis, are mesalamine, mesalazine, or sulfasalazine [43]. The clinical dosages of 5-ASA in patients with intestinal BD usually range from 2 to 4 g/day, while sulfasalazine is generally administered at 3 to 4 g/day [4]. Several clinical studies have obtained inconsistent results regarding the effectiveness of 5-ASA for intestinal BD. A case series study that included patients with intestinal BD reported that 79% patients showed symptomatic or colonoscopic improvement with sulfasalazine therapy [44]. A large-scale retrospective study conducted in 2012 showed that 5-ASA/sulfasalazine monotherapy was effective in maintaining remission, specifically with cumulative relapse rates of 46.7% at 10 years after remission. Younger age, disease severity, and higher C-reactive protein (CRP) level were associated with a poor prognosis with 5-ASA/sulfasalazine therapy [45]. A recent study investigated the induction response rate of oral 5-ASA and showed response and remission rates of 61% and 57%, respectively, at week 8 [46]. Thus, 5-ASA can be recommended as induction and maintenance therapies for relatively mild to moderate intestinal BD. Conclusively, 5-ASA is a substantial therapeutic option that needs to be used in almost all patients with intestinal BD. On the other hand, patients with small bowel involvement are not indicated for sulfasalazine use.
Systemic corticosteroids are used effectively to control flare-ups in patients with moderate to severe BD and IBD in cases of failure of 5-ASA/sulfasalazine treatment [47-49]. Corticosteroids, which are well-known fast-acting anti-inflammatory drugs, are used widely with tapering strategies at a starting dosage of 0.5∼1.0 mg/kg/day [3] that is tapered to 5 mg each week and stopped within three months. Well-designed prospective clinical trials on the effectiveness of corticosteroids in patients with intestinal BD have not been conducted thus far. Some retrospective studies have suggested that corticosteroids are effective in the induction phase of intestinal BD. One retrospective cohort study [50] in Korea that included 54 patients reported that 46.3% (n=25) of patients with active intestinal BD achieved complete remission after one month of treatment, while 42.6% showed partial remission. After three months of treatment, 40.7% of the patients still responded to the corticosteroid treatment. One year after the initiation of corticosteroid administration, 48.1% of the patients remained responsive to the treatment, and 8.1% showed a prolonged response, but 35.2% had corticosteroid dependency, and 7.4% underwent intestinal surgery. Thus, it is recommended for inducing a short-term response in the early phase of the disease course, especially with severe systemic symptoms or severe disease activity. Considering that patients with intestinal BD with high-risk factors, such as gastrointestinal bleeding, mainly use this medication, side effects are the main burden for both physicians and patients because they increase the risk of gastrointestinal bleeding and perforation [51]. In addition, corticosteroid therapy was strongly associated with rebleeding in patients with intestinal BD (hazard ratio [HR], 3.2; 95% confidence interval, 1.070∼9.462; p=0.037) [52]. Therefore, a tapering dose strategy should be maintained, and the prolonged use of prednisolone must not exceed 10 mg/day. Systemic corticosteroids are often used too easily without hesitation, even if there are no symptoms. Moreover, they are often prolonged in clinical practice. Steroid usage should be based rigorously on the overall symptoms, and should not be used unconditionally due only to the presence of intestinal ulcers.
Thiopurine analogs, consisting of 6-mercaptopurine (6-MP) and its derivate, azathioprine (AZA), are functioning antimetabolites of nucleic acids that were introduced to inhibit the growth of rapidly dividing cells in the 1950s [53]. Thiopurines require an extensive metabolism to form thioguanine nucleotides (TGNs) because they are prodrugs that act specifically via the following three pathways: (1) inactivation of 6-MP to thiouric acid by xanthine oxidase and aldehyde oxidase, (2) 6-methyl MP (6-MMP) production by thiopurine methyltransferase (TPMT), (3) conversion of 6-MP to 6-TGN by enzymes, such as TPMT, inosine monophosphate dehydrogenase, and hypoxanthine phosphoribosyl transferase [54,55]. Regarding the mechanism of action of thiopurines, TPMT plays a major role in producing inactive 6-MMP and active 6-TGN by generating 6-methyl MP ribonucleotide (6-MMPR), and can ultimately increase 6-TGN production by converting 6-thioinosine monophosphate to 6-MMR indirectly [56]. The anti-inflammatory action of thiopurine is achieved by 6-TGN. In particular, it is integrated into leukocyte DNA and prevents DNA synthesis, which inhibits downstream T-cell proliferation and immunosuppression [57]. Based on this metabolism, AZA/6-MP is commonly indicated for patients with moderate to severe intestinal BD, specifically those who are refractory or dependent on corticosteroids or show a secondary loss of response to anti-TNF-α agents. The drug is also used to reduce the postoperative recurrence rate after intestinal surgery [58].
AZA (25 to 50 mg/day) is effective for both the cellular and humoral immune responses, particularly for the initial dose indication, in patients with intestinal BD. The dose can be increased gradually every 2 to 3 weeks up to 2.0 to 2.5 mg/kg, unless adverse drug reactions occur, such as leukopenia [59]. Although only one retrospective cohort study was conducted in patients with intestinal BD treated with AZA, it established the benefit of AZA as maintenance therapy. Jung et al. [59] evaluated 272 patients with intestinal BD who received thiopurine monotherapy and reported that 58.2% (39/67) of patients who received the first course of thiopurine remained in remission with thiopurine maintenance therapy. In this study, the cumulative relapse rates at 1, 2, 3, and 5 years after remission were 5.8%, 28.7%, 43.7%, and 51.7%, respectively. Younger age (<25 years) at diagnosis and lower hemoglobin level (<11 g/dL) were associated with a poor prognosis.
Similarly, Lee at al. [58] reviewed the postoperative recurrence rate of intestinal BD in patients who received thiopurine treatment, and the cumulative rate of clinical recurrence after surgery was significantly lower in the thiopurine group than in the 5-ASA treatment group (p= 0.050). Moreover, the HR of postoperative thiopurines compared to 5-ASA was 0.636 (range, 0.130∼1.016; p=0.053) for postoperative recurrence. AZA is an effective treatment for intestinal inflammation and can be used stably in the long term unless side effects occur. The most common and serious side effect is leukopenia, which increases the infection risk and even mortality [60]. Thus, the American Gastroenterological Association recommends that patients treated with AZA should be monitored routinely with complete blood counts [61].
With regard to IBD treatment, a genotype-based strategy for thiopurine treatment using the
Methotrexate (MTX) is an analog of folic acid and aminopterin that was first manufactured in 1945 and is a long-standing medication that has been used for patients with cancer since the 1950s [63]. Recently, it has gained renewed attention as a notable therapy for autoimmune diseases. Low-dose MTX (25 mg/day for the induction phase) appears to be effective in the treatment of rheumatoid arthritis, neuro-BD, uveitis, and other types of BD involvement [64-66]. In addition, MTX is used increasingly in combination with biologics owing to the immuno-genicity of anti-TNF inhibitors [67]. The mechanism of immunosuppression by MTX mainly involves the reduction of cell proliferation, an increase in the rate of apoptosis of T-cells, and endogenous adenosine accumul-ation. Hence, it can alter cytokine production, humoral responses, and bone formation, which leads to the deactivation of the immune system [68]. The effectiveness and safety of MTX for intestinal BD have rarely been investigated. A case series of 10 patients with refractory intestinal BD reported improved symptoms and disease-related complications within four weeks of MTX treatment in 2011 [69]. Moreover, the ulcers disappeared in nine of the patients at 12 months.
Park et al. [70] published retrospective data on the efficacy of MTX therapy, specifically MTX monotherapy and combination therapy with MTX and adalimumab (ADA), for intestinal BD in 2018. Among 10 patients, three and five attained steroid-free remission at three and six months, respectively. The serum CRP level, erythrocyte sedimentation rate, and DAIBD score decreased at six months compared to their baseline values, but only the decrease in CRP levels was statistically significant (p= 0.039) [70].
(3) Other immunomodulatorsImmunomodulators, including cyclosporine, tacrolimus, interferon (IFN), and intravenous immunoglobulin (IVIG), are considered alternative therapeutic options for intestinal BD based on their pharmaceutical mechanism. On the other hand, no sufficient scientific evidence exists because of the relatively few cases reported, and no prospective clinical trials of immunomodulators have been conducted in patients with intestinal BD. Cyclosporine, which decreases the levels of inflammatory cytokines in T-lymphocytes by blocking the phosphatase activity of calcineurin [71], is commonly used for autoimmune diseases, such as rheumatoid arthritis, psoriasis, and ocular manifestations of BD [72,73]. According to the updated European League Against Rheumatism guideline, nervous system involvement is not indicated for cyclosporine based on level 3 evidence [74]. Bayraktar et al. [75] and the unpublished experience from Severance Hospital suggest that cyclosporine therapy has no clinical benefit for patients with intestinal BD. Tacrolimus, a macrocyclic lactone with potent immunosuppressive properties [76], is a standard immunosuppressive regimen after renal transplantation [77]. One case was reported, and clinical improvement was observed in patients with intestinal BD refractory to conventional therapies [78]. IFN and IVIG were introduced in the 1950s and have been used for arthritis, BD [79,80], and other autoimmune diseases.
On the other hand, studies examining the role of these therapies in intestinal BD are limited. Therefore, the efficacy of IFN or IVIG for intestinal BD is unclear. A study of patients with BD who were unresponsive to systemic steroids and/or immunosuppressants was conducted using subcutaneous IFN‐α at a dosage of 6×106 IU/day three times per week for two months. In that study, 75% (9/12) of the patients achieved complete remission, 16.6% (2/12) had partial remission, and 8.3% showed no response [81]. In 1998, a 32-year-old Caucasian woman with intestinal BD was treated with IVIG. Her symptoms improved after IVIG treatment initiation, and the intestinal lesions disappeared after six weeks of IVIG therapy at 400 mg/kg/day for five days [82]. Nevertheless, further evidence and clinical trials will be needed to prove their efficacy.
Thalidomide was first used as a sedative in the 1950s and withdrawn from the European pharmaceutical market in the 1960s owing to its teratogenic effects in early pregnancy, including severe birth defects, such as phocomelia [83]. This was defined as a “thalidomide tragedy” and has been a major issue in the history of biomedical ethics and drug safety monitoring. Eventually, it contributed to the approval system and toxicology guidelines of the United States Food and Drug Administration [84,85]. After several clinical trials over a decade, thalidomide has now been approved and used for the treatment of inflammatory diseases, including leprosy, rheumatoid arthritis, BD, and even multiple myeloma or malignant B-cell lymphoma [86-88]. Thalidomide, a synthetic derivative of glutamic acid, was suggested to be effective against the mucocutaneous and follicular lesions of BD based on the results of a randomized, double-blind, placebo-controlled study [89]. A case series of BD with intestinal involvement reported that thalidomide was effective for recurrent perforating intestinal ulcers and led to clinical improvement in terms of corticosteroid-free remission [90,91].
These outcomes were observed consistently in another case series in Korea [92]. Patients with recurrent intestinal BD refractory to conventional treatments, including 5-ASA and immunomodulators, reported a response to thalidomide with clinical and radiological improvement. The major side effects observed were edema, neutropenia, and sepsis. Similarly, a prospective open-label study of patients with IBD treated with thalidomide reported clinical response rates of 83.3% and 100.0% for Crohn’s disease and ulcerative colitis at week 12 [93]. Definitive dose guidelines for intestinal BD are not available. On the other hand, an initial thalidomide dosage of 2 mg/kg/day has been used, and dose adjustment according to the treatment response is needed [90]. In addition, thalidomide appears to exert a selective effect on TNF‐α production by the degradation of its encoding messenger RNA [94]. Thus, the efficacy and safety of anti-TNF inhibitor or thalidomide therapy were investigated in patients with intestinal BD who were refractory to conventional therapies [95]. Of 13 patients, 10 (75%) achieved clinical and endoscopic remission with TNF-α antagonists and/or thalidomide therapy. This result also supports the efficacy of thalidomide as a therapeutic option for intestinal BD. Nevertheless, well-designed prospective trials are still needed, and rigorous monitoring of the side effects is warranted.
While recent advances in the novel therapeutic armamentarium, including biologics for autoimmune diseases, have made transformative changes in therapeutic environments. Several biologic agents are now available for patients with autoimmune diseases, particularly those who do not respond to conventional therapies or those who develop serious adverse events. The use of these biologics has also been attempted in patients with intestinal BD. As mentioned previously, the pathogenesis of intestinal BD is related to an abnormal T-cell immune response and cytokines derived from T helper type 1 (Th1) lymphocytes, including TNF-α, IFN-γ, IL-12, and IL-18 [96,97]. The TNF-α expression level in the blood increases, mucosal damage occurs, and clinical symptoms worsen [98]. Therefore, biologics targeting TNF-α have been administered to patients with intestinal BD with these scientific backgrounds. Currently, anti-TNF-α monoclonal antibodies, including infliximab (IFX) and ADA, are considered standard therapies for patients with intestinal BD [37].
(1) InfliximabIFX, a TNF blocker, is indicated for patients with IBD, arthritis, ankylosing spondylitis, and psoriasis, and who have shown an inadequate response to conventional therapy [4]. A dose of 5 mg/kg at zero, two, and six weeks is suggested for induction therapy and then every eight weeks for maintenance therapy. Some adult patients who respond initially to treatment may benefit from increasing the dose to 10 mg/kg if they later become unresponsive to this treatment [37]. The first case report of IFX use for intestinal BD was in 2001, which showed a decreased CDAI score from 270 to 13 points by week two, and endoscopic and histological improvements at week 10 [99]. The following case reports consistently suggested the positive efficacy of IFX for intestinal BD as both induction and maintenance therapy [100,101]. A multicenter retrospective study in patients with moderate to severe intestinal BD reported the results of IFX treatment from 28 patients in Korean tertiary hospitals [102]. The clinical response rates at 2, 4, 30, and 54 weeks were 75%, 64.3%, 50%, and 39.1%, respectively, and the clinical remission rate at week 30 was 46.2%. During the follow-up period, one case of serious infection was observed, but no malignancies or deaths occurred. The efficacy and safety of IFX were investigated in a prospective open-label phase 3 study in 2016, which included 18 patients with BD. Among the patients enrolled, 11 had intestinal involvement and were refractory to conventional therapies [103]. The IFX dose was the same as that for Crohn’s disease and ulcerative colitis. A complete response was observed in 61% (11/18) of patients at weeks 14 and 30, and the patients remained in remission until week 54. The CRP levels were decreased after week two, and most of the subjects showed healed ulcers at week 14. Despite these results, as with patients with IBD, the patients with intestinal BD in this study also showed a primary and secondary loss of response. Hence, the need to increase the dose at week 30 or treatment failure were observed [103]. An interventional, open-label, single-arm, multicenter study of IFX in 33 patients with moderate to severe refractory intestinal BD is ongoing in Korea (ClinicalTrials.gov NCT02505568). This study is expected to provide more scientific evidence for the effectiveness of IFX treatment for patients with intestinal BD. Studies are still lacking, but evidence for the positive efficacy of IFX combination therapy with immunomo-dulators has been reported. In a previous study [69], all 10 patients showed improvement in the intestinal symptoms and complications within four weeks. The rate of disappearance of ileocecal ulcerations was 50% (5/10) and 90% (9/10) at 6 and 12 months, respectively [69]. Combination therapy of biologics with immunomodulators is beneficial for reducing the immunogenicity and increasing the serum levels, but the risks of infection and malignancy need to be considered carefully [104].
(2) AdalimumabADA is a fully human anti-TNF-α monoclonal antibody, whereas IFX is a chimeric monoclonal antibody against TNF-α. The doses for patients with intestinal BD can be used for induction therapy at doses of 160, 80, and 40 mg at week zero (baseline), two, and four subcutaneously, and then 40 mg every other week for responders [105]. De Cassan et al. [106] described their experience with ADA use as the first anti-TNF-α inhibitor in two patients with familial intestinal BD, who were steroid dependent. Rapid clinical remission was observed in the induction phase, which was sustained in the maintenance phase.
The following case report suggested the efficacy of ADA for intestinal BD with myelodysplastic syndrome based on successful improvement in gastrointestinal symptoms, CRP levels, leukocytopenia, and anemia four months after the ADA treatment [107]. After that, a prospective multicenter open-label study was conducted in Japan that involved 20 patients with intestinal BD, who were refractory to conventional therapies, such as corticosteroids or immunomodulators [105]. Nine patients (45%) achieved the primary endpoints after 24 weeks, which were an alleviation of gastrointestinal symptoms and a decrease in the endoscopic assessment score to 1 or lower than the baseline score. In addition, ADA treatment induced complete remission in 20% of patients at week 24, which was maintained until week 52, but no notable safety issues were observed. A recent phase 3 study in Japan evaluated the efficacy and long-term safety profiles of ADA treatment in 20 patients with intestinal BD. Fifteen of the patients remained in the study until 100 weeks of follow-up. Significant improvement, which was defined based on the gastrointestinal symptom and endoscopic scores, was observed in 60% of patients at week 52 and 40% at week 100. Of the patients, 20% and 15% showed clinical remission at weeks 52 and 100, respectively, with tolerable safety profiles [108]. These results played a pivotal role in gaining approval of the use of ADA for intestinal BD treatment in Japan. Combination therapy using ADA with other immunomodulatory medications has not yet been actively investigated. Vitale et al., however, compared the efficacy and safety of ADA monotherapy and combination therapy with disease-modifying antirheumatic drugs. In this study, 100 patients with BD were enrolled; no significant difference in clinical outcomes was observed between the two groups [109].
A study in 2019 examined the effectiveness of anti-TNFs in patients with intestinal BD compared to that of corticosteroids without anti-TNF. Both groups showed improvement in the DAIBD score one year after treatment (85.2±29.6 to 40.5±44.7 in the corticosteroid group and 64.7±34.9 to 21.1±28.9 in the anti-TNF group). Anti-TNF administration was effective in reducing the concomitant steroid dose to <7.5 mg (p=0.0001). Considering that one patient discontinued treatment because of bacterial infection, the potential risk of intestinal perforation or massive bleeding should be considered when using steroids [110]. A recently published study that used real-world data on ADA and IFX for patients with refractory intestinal BD suggested switching from an anti-TNF inhibitor to another if a patient is refractory to the first-line anti-TNF inhibitor [111]. Biologics can be ineffective in cases of urgent patients who require surgical intervention. Therefore, a decision should be made under a multi-disciplinary discussion, including gastroenterologists, rheumatologists, and surgeons, as to whether to discontinue the treatment and perform surgery.
The prevalence of intestinal BD is low in Western countries but relatively high in East Asian countries, including Korea. Thus, there are limited clinical trial data with intestinal BD due to the general lack of disease awareness, small number of cases, and difficulty in subject recruitment. In addition, it is a relapsing, complex systemic inflammatory disease that is often unpredictable and has a “wax and wane” disease course with massive bleeding and perforation. Patients are easily refractory to conventional therapies, which caused new biologics to evolve in the treatment of intestinal BD. Intestinal BD can be treated using the same therapeutic approaches for BD, but the differences in intestinal BD from other types of BD in terms of the intestinal specific pathophysiology and treatment response must be considered. Thus far, the IBD treatment guidelines are effective in the treatment of intestinal BD. Several retrospective studies or clinical trials with a small number of patients have been the mainstay for gathering evidence on intestinal BD treatment. On the other hand, recent prospective and scientifically designed clinical trials specifically for intestinal BD have actively been conducted. Therefore, an effective treatment guideline is expected to be established soon. As for biologics, many novel agents with different targets have emerged for autoimmune diseases, including IL 12/23, Janus kinases, and IL-6 inhibitors. Further clinical research focusing on intestinal BD will be needed to obtain scientific evidence and provide treatment opportunities to the patients. Ultimately, close cooperation between rheumatology, gastroenterology, and colorectal surgery departments as multidisciplinary care is essential for the treatment of intestinal BD.
The author wishes to thank Sinyoung Park, who assisted in collecting and analyzing the related literature, and writing and revising the manuscript.
No potential conflict of interest relevant to this article was reported.