Adverse Events of Thiopurine Therapy in Pediatric Inflammatory Bowel Disease and Correlations with Metabolites: A Cohort Study.

BACKGROUND: In the recent era of growing availability of biological agents, the role of thiopurines needs to be reassessed with the focus on toxicity. AIMS: We assessed the incidence and predictive factors of thiopurine-induced adverse events (AE) resulting in therapy cessation in pediatric inflammatory bowel disease (IBD), related to thiopurine metabolites and biochemical abnormalities, and determined overall drug survival.
METHODS: We performed a retrospective, single-center study of children diagnosed with IBD between 2000 and 2019 and treated with thiopurine therapy. The incidence of AE and overall drug survival of thiopurines were evaluated using the Kaplan-Meier method. Correlations between thiopurine metabolites and biochemical tests were computed using Spearman's correlation coefficient.
RESULTS: Of 391 patients with IBD, 233 patients (162 Crohn's disease, 62 ulcerative colitis, and 9 IBD-unclassified) were prescribed thiopurines (230 azathioprine and 3 mercaptopurine), of whom 50 patients (22%) discontinued treatment, at least temporary, due to thiopurine-induced AE (median follow-up 20.7 months). Twenty-six patients (52%) were rechallenged and 18 of them (70%) tolerated this. Sixteen patients (6%) switched to a second thiopurine agent after azathioprine intolerance and 10 of them (63%) tolerated this. No predictive factors for development of AE could be identified. Concentrations of 6-thioguanine nucleotides (6-TGN) were significantly correlated with white blood cell and neutrophil count, 6-methylmercaptopurine (6-MMP) concentrations with alanine aminotransferase and gamma-glutamyltranspeptidase.
CONCLUSIONS: Approximately 20% of pediatric patients with IBD discontinued thiopurine treatment due to AE. A rechallenge or switch to mercaptopurine is an effective strategy after development of AE. Concentrations of 6-TGN and 6-MMP are associated with biochemical abnormalities.

Introduction

The immunomodulating thiopurine drugs, including azathioprine (AZA) and mercaptopurine (MP), are frequently used in pediatric inflammatory bowel disease (IBD), both as maintenance monotherapy and in combination with infliximab to reduce the risk of formation of anti-IFX antibodies, and to increase efficacy [1-3]. Their efficacy in maintaining remission was demonstrated in several observational studies [4, 5] and in one RCT in children with IBD [6]. However, the role of thiopurines has become debatable due to contradictory results on efficacy in adults with Crohn’s disease (CD) on the one hand [7, 8], and safety concerns on the other [1, 2, 9]. In the recent era of growing availability of different biologic agents, there is need for reassessment of thiopurines with the focus on toxicity.

Several studies provide data regarding thiopurine-induced adverse events (AE) in the pediatric IBD population, reporting discontinuation rates due to AE varying between 10 and 22% [5, 10–13]. However, most studies were characterized by a small sample size and the main objective in the majority of these studies was to assess the efficacy, but not safety of this compound. Mercaptopurine may be considered as an alternative thiopurine agent in patients previously intolerant to AZA therapy [14, 15]. Most studies, however, have focused on adults with IBD.

This study aimed to determine incidence of thiopurine-induced AE resulting in cessation of therapy in a real-life pediatric IBD cohort. In addition, we aimed to evaluate the efficacy of rechallenge and switching to a second thiopurine in case of AE. Secondary aims were to identify predictive factors for AE, to assess the correlation between thiopurine metabolites and biochemical tests, and determining overall drug survival of thiopurines.

Materials and Methods

Study Design and Patient Population

This retrospective, single-center cohort study was performed at the Amsterdam University Medical Center (location VUmc), the Netherlands. All children < 18 years of age, diagnosed with IBD between January 1, 2000, and December 31, 2019, and were prescribed thiopurines, including AZA and MP, were included. The diagnosis of IBD (CD, ulcerative colitis (UC) or IBD-unclassified (IBD-U)) was based on endoscopic, radiologic, and histologic findings according to the revised Porto criteria [16] and classified according to the Paris classification [17]. Patients with bone marrow suppression or preexistent liver disease before initiation of thiopurine therapy or a follow-up less than three months were excluded from analysis. Patients were followed for a maximum of eight years or until cessation of thiopurine therapy.

Data Collection

The following patient characteristics were collected: gender, weight, height, IBD type, age at diagnosis, time (in months) since IBD diagnosis until initiation of thiopurine therapy, and small bowel surgery prior to thiopurine treatment. Furthermore, type of thiopurine (AZA or MP), date of initiation of thiopurine, age at initiation of thiopurine, thiopurine dose, and duration of thiopurine use were collected. Thiopurines were prescribed according to the ECCO/ESPGHAN guidelines (AZA dose of 2–2.5 mg/kg or a MP dose of 1–1.5 mg/kg) [1, 2]. Thiopurine methyltransferase (TPMT) genotyping and activity assessments were not routinely assessed. The use of concomitant anti-TNFα agents was documented. Concentrations of 6-thioguanine nucleotides (6-TGN) and 6-methylmercaptopurine (6-MMP) measured routinely 8–16 weeks after initiation of thiopurine therapy, were collected. In patients who ceased therapy due to AE, concentrations of 6-TGN and 6-MMP were collected within the interval of maximum 4 months before cessation.

Adverse Events

An AE was defined as any noxious or unintended response that occurred during the course of treatment, considered to be thiopurine-induced, and resulting in cessation of thiopurine therapy. The decision to stop treatment, rechallenge, or switch to another thiopurine compound was based on the treating physician's judgement, together with the patient and/or the parents. AE were graded in severity according to The Common Terminology Criteria for Adverse Events (CTCAE) (Version 5.0, released November 27, 2017) [18]. The CTCAE are a set of criteria for the standardized classification of AE using a range of grades from 1 to 5 (1: mild, 2: moderate, 3: severe, 4: life-threatening and 5: adverse event-related death). AE were subdivided into leukopenia, neutropenia, thrombocytopenia, myelotoxicity, hepatotoxicity, flu-like symptoms, gastrointestinal symptoms, pancreatitis, and others. Definitions are depicted in Table 1.

Table 1

Definitions of thiopurine-induced adverse events

Adverse Event	Definition
Moderate leukopenia Severe leukopenia	White blood cell count < 3.0 × 109/L White blood cell count < 2.0 × 109/L
Neutropenia	Absolute neutrophil count < 1.5 × 109/L
Thrombocytopenia	Platelet count < 150 × 109/L
Myelotoxicity	Suppression of the bone marrow activity leading to anaemia (hemoglobin concentration < 2.5th percentile for age), leukopenia, and thrombocytopenia
Hepatotoxicity	Twice or more the upper limit of ALT, AST, AP, or GGT
Flu-like symptoms	General malaise, fever, and muscle and joint pain
Gastrointestinal symptoms	Nausea and vomiting
Pancreatitis	Severe abdominal pain accompanied with a rise in serum lipase levels three times above the upper limit of normalcy
Others	Includes infection and nonspecific side effects, such as headache, asthenia, or other symptoms during treatment necessitating cessation of thiopurine therapy

ALT alanine aminotransferase, AST  aspartate aminotransferase, AP alkaline phosphatase, GGT  gamma-glutamyltranspeptidase

Thiopurine Metabolites and Laboratory Measurements

To assess the association between thiopurine metabolites and hematological indices and liver tests, the therapeutic drug monitoring database of the department of clinical pharmacology was scrutinized for available thiopurine metabolite measurements. All laboratory measurements within a timeframe of 3 days before or after thiopurine metabolite measurement were included. The reported laboratory measurements included: hemoglobin concentration (Hb), white blood cell (WBC) count, mean corpuscular volume (MCV), absolute neutrophil count (ANC), platelet count, alanine aminotransferase (ALT), aspartate aminotransferase (AST), alkaline phosphatase (AP), and gamma-glutamyltranspeptidase (GGT). In this sub-analysis, hepatotoxicity was defined as > twice upper limit of ALT, AST, AP, or GGT; myelosuppression as either WBC below 3.0 × 109/L or PC under 150 × 109/L or ANC below 1.5 × 109/L, not necessarily resulting in thiopurine cessation.

The concentrations of 6-TGN and 6-MMP in our center were determined in red blood cells, using a high-performance liquid chromatography method modified from Dervieux et al. [19]. The lower limit of detection was 30 pmol/8 × 108 RBC for 6-TGN and 15 pmol/8 × 108 RBC for 6-MMP, whereas the lower limit of quantification was 70 and 100 pmol/8 × 108 RBC, respectively. According to hospital guideline, reference values are 300–600 pmol/8 × 108 RBC and < 5700 pmol/8 × 108 RBC for 6-TGN and 6-MMP, respectively (according to the method of Dervieux).

Drug Survival

Drug survival was measured by calculating the number of patients on thiopurine therapy at 3, 6, 12, 24, and 60 months after initiation. Reasons for cessation of therapy were documented, including clinical refractoriness, sustained clinical remission, or at patients’ or parents’ own request. Patients with combination therapy of thiopurines and anti-TNFα agents in context of an anti-TNFα-based top-down approach [1], and patients who ceased thiopurine therapy due to AE, were excluded from this analysis. Fecal calprotectin levels were collected in patients who continued thiopurine monotherapy until the end of follow-up period, to evaluate disease activity. Biochemical remission was defined as fecal calprotectin levels of < 250 μg/mg, in samples available within 3 months from last follow-up visit.

Statistical Analyses

Statistical analyses were performed using the Statistical Package for Social Sciences (SPSS, IBM; v25). P values < 0.05 were considered to be statistically significant. For normally distributed data, both means and standard deviations were calculated, whereas medians and interquartile ranges (IQR) were calculated for data with a non-normal distribution. Data were compared using the Mann–Whitney U test for nonparametric continuous data and the unpaired t test for normally distributed data. Categorical variables were compared using the Chi-square test or Fisher’s exact. The Kaplan–Meier method was used to evaluate the cumulative incidence of AE and overall drug survival. Logistic regression analyses were performed to investigate potential predictive factors for thiopurine-induced AE within 6 months after initiation. Variables reaching statistical significance (p < 0.2) were included in a multivariate regression analysis. The results were expressed as odds ratios (OR) with 95% confidence intervals. Correlations between thiopurine metabolites and laboratory measurements were computed using Spearman rank correlation coefficient.

Results

Patient Population and Baseline Characteristics

A total of 391 pediatric patients were diagnosed with IBD in the predefined study period, and 245 children (62.7%) used thiopurines at any moment following diagnosis. We excluded 12 patients: nine patients due to an insufficient follow-up and three patients refused to participate. The patient characteristics of the 233 included children are depicted in Table 2. The median follow-up was 20.7 months [IQR, 6.0–42.1]. In the group of patients with AZA, the median start dose was 2.3 mg/kg [IQR, 2.1–2.5]. In patients using MP, the median start dose was 1.2 mg/kg [range, 1.2–2.4]. Forty-nine patients (21%) received combination therapy with infliximab and AZA following diagnosis. The concomitant use of infliximab did not affect the thiopurine dose and concentrations of 6-TGN and 6-MMP.

Table 2

Characteristics of pediatric patients with IBD managed with thiopurine therapy

	Total (n = 233)
Median age at diagnosis, years [IQR]	13.7 [11.1–15.4]
Male, n (%)	126 (54.1)
Type of disease, n (%)
CD	162 (69.5)
UC	62 (26.6)
IBD-U	9 (3.9)
Paris location of CD patients, n (%)
L1: ileal	32 (19.8)
L2: colonic	46 (28.4)
L3: ileocolonic	79 (48.8)
Upper GI involvement: L4a, L4b	43 (26.5), 2 (1.2)
Paris behavior of CD patients, n (%)
B1: nonstricturing, nonpenetrating	145 (89.5)
B2: stricturing	12 (7.4)
B3: penetrating	2 (1.2)
B2B3: both penetrating and structuring	3 (1.9)
P: perianal disease modifier, n (%)	40 (24.7)
Paris location of UC patients, n (%)
E1: ulcerative proctitis	3 (4.8)
E2: left-sided UC (distal splenic flexure)	5 (8.1)
E3: extensive (hepatic flexure distally)	4 (6.5)
E4: pancolitis (proximal hepatic flexure)	50 (80.6)
First type of thiopurine, n (%)
AZA	230 (98.7)
MP	3 (1.3)
Median time to start thiopurine, days [IQR]	42 [17–153]
Median age at start thiopurine, years [IQR]	14.5 [11.9–15.8]
Small bowel surgery, n (%)	5 (2.1)

CD   crohn's disease, UC ulcerative colitis, IBD-U  IBD-unclassified, GI gastrointestinal, AZA azathioprine, MP mercaptopurine

In total, 50 patients (21.5%) developed thiopurine-induced AE leading to, at least temporary, cessation of therapy (Table 3 and 4). None developed grade 4 or 5 AE (i.e., life-threatening or adverse event-related death), malignancy, lymphoproliferative disorders or hemophagocytic lymphohistiocytosis (HLH). The median time of cessation of therapy due to AE was 57 days [IQR, 21–217] following initiation of thiopurines (Fig. 1).

Table 3

Adverse events (n = 50) leading to cessation of thiopurine therapy, listed, and graded according to the common terminology criteria (CTC)

Adverse event	Grade 1 (mild) n = 12	Grade 2 (moderate) n = 21	Grade 3 (severe) n = 17
Blood, lymphatic and vascular disorders	Myelotoxicity, n = 1	—	Severe leukopenia, n = 2 Myelotoxicity, n = 1 Thrombocytopenia, n = 1
Gastrointestinal disorders	Nausea, n = 5 Vomiting, n = 1	Pancreatitis, n = 1 Vomiting, n = 9	Pancreatitis, n = 7 Vomiting, n = 1
General, neurological, and psychiatric disorders	Flu-like symptoms, n = 2	Flu-like symptoms, n = 7	Flu-like symptoms, n = 3
Hepatobiliary disorders	Hepatotoxicity, n = 1	Hepatotoxicity, n = 2	Hepatotoxicity, n = 2
Infections and infestations	—	Shingles, n = 1	—
Musculoskeletal and skin disorders	Alopecia, n = 2	Rhabdomyolysis, n = 1	—

Table 4

Time of onset of the AE following initiation of thiopurine therapy and restart of thiopurine therapy in patients with thiopurine-induced AE leading to cessation of therapy

Adverse event	Patients, n (%)	Median time with thiopurines, days (IQR)	Rechallenge same thiopurine, n (%)	Reoccurrence AE, n (%)	Rechallenge second thiopurine, n (%)	Reoccurrence AE, n (%)
Severe leukopenia	2 (4.0)	31–514†	1 (50.0)	1 (100)	0	0
Thrombocytopenia	1 (2.0)	161	1 (100)	0	0	0
Myelotoxicity	2 (4.0)	118–399†	0	0	0	0
Hepatotoxicity	5 (10.0)	59 (32–976)	2 (40.0)	0	1 (20.0)	1 (100)
Flu-like symptoms	12 (24.0)	82 (27–181)	10 (83.3)	2 (20.0)	2 (16.7)	2 (100)
GI symptoms	16 (32.0)	40 (14–128)	2 (12.5)	0	5 (31.3)	1 (20.0)
Pancreatitis	8 (16.0)	21 (16–26)	0	0	0	0
Alopecia	2 (4.0)	119–1872†	1 (50.0)	1 (100)	0	0
Shingles	1 (2.0)	321	1 (100)	0	0	0
Rhabdomyolysis	1 (2.0)	409	0	0	0	0

AE  adverse event, GI  gastrointestinal

† Median time is not applicable. The range is used to present the time of onset of severe leukopenia, myelotoxicity and alopecia (n = 2)

Rechallenge with the same thiopurine comprises rechallenge with azathioprine in 17 patients and rechallenge with mercaptopurine in one patient. Rechallenge with a second thiopurine comprises a switch to mercaptopurine in six patients and a switch to tioguanine in 2 patients

Fig. 1

Kaplan–Meier curve of patients with IBD who developed AE leading to therapy cessation. The X-axis represents the time in months. The Y-axis represents the probability of discontinuing treatment due to AE. The cumulative incidence of AE was 13.5%, 16.7%, 17.3%, and 21.8% at 3, 6, 12, and 24 months of therapy, respectively

Thiopurine therapy was restarted in 26 patients (52%) who discontinued treatment due to presumed AE. The same thiopurine, mainly AZA, was reintroduced in 18 patients, while a second thiopurine agent was reintroduced in 8 patients (6 MP, 2 tioguanine). Of these 26 patients, eight patients (30.8%) developed the same AE, resulting in complete cessation of therapy (Table 4). Furthermore, 9 out of 233 patients (3.9%) switched directly (without cessation) from AZA to MP due to AE (n = 8) or aberrant metabolite concentrations (n = 1). Amongst these eight patients with AE, reported AE were alopecia (n = 4), gastrointestinal symptoms (n = 2) and others (n = 2). Six of 8 patients (75%) who switched directly from AZA to MP, could continue with MP therapy. In total, 10 out of 16 patients (62.5%) who switched to a second thiopurine agent, did not experience the previously reported AE. Nineteen patients received allopurinol as co-medication, based on elevated 6-MMP concentrations.

Potential Predictive Factors for Adverse Events Leading to Cessation of Therapy

Thirty-eight patients developed grade 1–3 AE within six months after initiation of thiopurines, leading to cessation of therapy. Univariate logistic regression analyses showed no significant effects of age at diagnosis, gender, and disease phenotype between the AE and non-AE group (Online Resource 1). In 16 out of 38 patients (42.1%) who developed an AE within the first 6 months after initiation of thiopurines, versus 40 out of 162 patients (24.7%) with a follow-up of 6 months in the non-AE group, concentrations of 6-TGN and 6-MMP were measured. No significant differences of 6-TGN and 6-MMP concentrations were found between these two groups (Online Resource 1). Since none of the variables reached a statistical significance of p < 0.2, a multivariate regression analysis was not performed.

Effect of Thiopurine Metabolites on Hematological Indices and Liver Tests

Concentrations of 6-TGN and 6-MMP were measured 469 times in 164 unique patients. In 430 measurements, determination of 6-TGN and 6-MMP was combined with assessment of either hematological indices (n = 34) or liver tests (n = 4), or both (n = 382) within predefine time interval. In 10 cases, 6-TGN and 6-MMP concentrations were undetectable and related laboratory measurements were therefore excluded from analysis. The median 6-TGN concentration was 480 pmol/8 × 108 RBC [IQR, 330–690] and the median 6-MMP concentration was 1400 pmol/8 × 108 RBC [IQR, 580–3375]. There was a statistically significant, positive correlation between 6-TGN concentrations and MCV. 6-TGN concentrations were negatively correlated with WBC count and neutrophil count. A weak positive correlation was found between 6-MMP concentrations and ALT and GGT (Table 5).

Table 5

Spearman’s correlations between erythrocyte concentrations of 6-TGN and 6-MMP and hematological indices and liver tests

	6-TGN Correlation [r (p)]	6-MMP Correlation [r (p)]
Hb	0.025 (p = 0.62)	– 0.010 (p = 0.85)
WBC	– 0.168 (p = 0.001)**	– 0.068 (p = 0.18)
MCV	0.417 (p < 0.0005)**	– 0.040 (p = 0.54)
ANC	– 0.177 (p = 0.004)**	– 0.015 (p = 0.81)
PC	– 0.058 (p = 0.25)	0.058 (p = 0.26)
ALT	– 0.099 (p = 0.05)	0.104 (p = 0.049)*
AST	– 0.080 (p = 0.27)	0.113 (p = 0.13)
AP	0.037 (p = 0.68)	– 0.120 (p = 0.20)
GGT	0.115 (p = 0.11)	0.152 (p = 0.040)*

Statistically significant at the level p < 0.05

**Statistically significant at the level p < 0.01

6-TGN 6-thioguanine nucleotides, 6-MMP 6-methylmercaptopurine, Hb haemoglobin, WBC white blood cell, MCV mean corpuscular volume, ANC absolute neutrophil count, PC platelet count, ALT alanine aminotransferase, AST aspartate aminotransferase, AP alkaline phosphatase, GGT gamma-glutamyltranspeptidase

Laboratory data regarding WBC, PC or ANC were available in 412 out of 420 measurements (98%). In 17 cases with myelosuppression, concentrations of 6-TGN (median 530 vs. 480 pmol/8 × 108 RBC, p = 0.33) and concentrations of 6-MMP (median 1900 vs. 1400 pmol/8 × 108 RBC, p = 0.20) were slightly higher in patients with myelosuppression as compared to patients without myelosuppression, however this difference did not reach statistical significance. Incidence of myelosuppression was not significantly higher in the group with 6-TGN concentrations outside the therapeutic range (> 600 pmol/8 × 108 RBC) as compared to patients with 6-TGN concentrations within the therapeutic range (Table 6).

Table 6

Incidence of myelosuppression across reference values of 6-TGN and 6-MMP concentrations

Thiopurine metabolites	Myelosuppression (n = 17)	No myelosuppression (n = 375)†
6-MMP (n = 392)
6-MMP > 5700 pmol/8 × 108 RBC (n = 41)	12.2% (n = 5)	87.8% (n = 36)
6-MMP < 5700 pmol/8 × 108 RBC (n = 351)	3.4% (n = 12)	96.6% (n = 339)
p-value	0.023
6-TGN (n = 411)
6-TGN > 600 pmol/8 × 108 RBC (n = 140)	5.7% (n = 8)	94.3% (n = 132)
6-TGN < 600 pmol/8 × 108 RBC (n = 271)	3.3% (n = 9)	96.7% (n = 262)
p value	0.30
6-TGN/6-MMP both abnormal (n = 15)	20.0% (n = 3)	80.0% (n = 12)
‡6-TGN/6-MMP normal (n = 377)	3.7% (n = 14)	96.3% (n = 363)
p value	0.022

6-TGN 6-thioguanine nucleotides, 6-MMP 6-methylmercaptopurine, RBC red blood cell

†392 available 6-MMP or 6-TGN/6-MMP measurements, no myelosuppression: n = 375

411 available 6-TGN measurements, no myelosuppression: n = 394

‡6-TGN > 600 pmol/8 × 108 RBC and 6-MMP > 5700 pmol/8 × 108 RBC

Liver tests were available in 386 measurements (92%). Hepatotoxicity was observed in 20 cases (5%). In these patients, there were no differences in median 6-MMP concentrations (p = 0.65) or 6-TGN concentrations (p = 0.70) as compared to patients without hepatotoxicity. In all patients with hepatotoxicity, 6-MMP concentrations were below the toxic reference value (< 5700 pmol/8 × 108 RBC). Amongst the patients with 6-MMP concentrations exceeding the reference value (> 5700 pmol/8 × 108 RBC), the incidence of myelosuppression was significantly higher compared with patients with 6-MMP concentrations below the toxic reference value. The incidence of myelosuppression across reference values of 6-TGN and 6-MMP concentrations is depicted in Table 6.

To determine the overall drug survival, we excluded 92 patients: 50 patients who ceased thiopurine therapy due to AE, and 42 patients with combination therapy of thiopurines and anti-TNFα agents in context of top-down treatment strategy. Amongst the remaining 141 patients who tolerated thiopurine therapy, 57.4% (n = 81) ceased thiopurines, median duration of therapy was 23.4 months [IQR, 11.0–40.9]. Reasons for cessation included clinical refractoriness (53.1%), sustained clinical remission (14.8%), at patients’ or parents’ own request (22.2%), or others reasons such as pregnancy (6.2%). In three patients, the reason for cessation was unknown. The calculated drug survival is depicted in Fig. 2. In the group of patients who ceased thiopurine therapy due to clinical refractoriness (n = 43), infliximab was initiated as additional therapy in 13 patients (30.2%). These patients received a combination of infliximab and thiopurines, until thiopurine therapy was routinely ceased after 6–12 months. Amongst the 31 patients who continued thiopurine monotherapy until the end of follow-up, fecal calprotectin levels were available in 16 out of 31 patients (51.6%) within 3 months of the last follow-up visit. Twelve out of 16 patients (75%) were considered in biochemical remission, based on a fecal calprotectin value of < 250 μg/mg.

Fig. 2

Kaplan–Meier curve of ongoing thiopurine use in the patients who tolerated thiopurine therapy. The Y-axis represents the percentage of patients still using thiopurines at different time points. The percentage of patients still using thiopurines was 97.8%, 92.0%, 84.3%, 69.2%, and 37.0% at 3, 6, 12, 24, and 60 months following initiation, respectively

Discussion

The present study aimed to determine incidence of thiopurine-induced AE resulting in cessation of therapy in a large cohort of children. Of 233 included pediatric patients, 22% discontinued thiopurine therapy due to thiopurine-induced AE. Approximately 50% of patients were rechallenged and 70% of these patients tolerated this. Only 37% of children were still on thiopurines after 5 years.

Around 20% of patients developed grade 1–3 AE in our cohort, which is comparable to rates reported in other pediatric studies (15–22%) [10-12]. In a study by Hindorf et al. [10], including 79 pediatric patients with IBD, 15% had thiopurine-induced AE leading to therapy cessation or dose reduction. The reported lower percentage might be explained by possible limited access to alternative therapeutic options for pediatric IBD in that study period (1997–2003). Nowadays, treating physicians might opt for an earlier switch to anti-TNFα agents, even in case of mild thiopurine-induced AE. A more recent study in pediatric patients with IBD (n = 216) [12], showed a discontinuation rate of 22% due to thiopurine-induced adverse effects, which is consistent with our findings.

In the present study, 70% tolerated a rechallenge with thiopurines after discontinuation of treatment due to AE. A study by Chaparro et al. [20], found a comparable success percentage following rechallenge of 60% in adults with IBD. In addition, 7% of our pediatric IBD cohort switched from AZA to a second thiopurine agent due to AE, and 63% of these patients tolerated this. Percentages varying between 42 and 73% were reported regarding adults with IBD who tolerated MP after AZA intolerance [14, 15, 21–23]. Mercaptopurine tolerance was observed in adults with IBD with previously reported gastrointestinal intolerance, hepatotoxicity, flu-like symptoms and arthralgia/myalgia (during AZA treatment) [14, 15, 21, 23]. In our cohort, MP was not prescribed in patients with AZA-induced pancreatitis, since we considered this a contraindication for another thiopurine agent. Previous case series in children with CD [24, 25], however, have described MP tolerance after AZA-induced pancreatitis, challenging the assumption that this is an absolute contraindication. It has been hypothesized that the AZA imidazole component, which is released when AZA is converted to MP, is partly responsible for early intolerance [26]. An explanation for the high success rates following rechallenge might be that mild AE, including gastrointestinal intolerance and flu-like symptoms, are transient and could resolve without any intervention. Gastrointestinal symptoms and flu-like symptoms could also be a consequence of unrecognized infections. Additionally, gastrointestinal intolerance, flu-like symptoms, and alopecia, often considered as thiopurine-induced AE, could also be due to IBD disease activity.

In this study, 6-TGN concentrations were negatively correlated with WBC count and neutrophil count and positively correlated with MCV, while 6-MMP concentrations were positively correlated with ALT and GGT. These findings probably reflect the association between myelosuppression and high concentrations of 6-TGN [1], as well as the association between elevated 6-MMP and hepatotoxicity [27]. However, in our cohort, we did not observe a correlation between 6-MMP concentrations exceeding the toxic reference value (> 5700 pmol/8 × 108 RBC) and hepatotoxicity. A previous study in pediatric patients with IBD did also not find 6-MMP concentrations exceeding the toxic reference value in patients with hepatotoxicity [28]. In contrast to a previous published finding [27], we did not observe an association between myelosuppression and higher 6-TGN concentrations. The lack of association between 6-TGN and 6-MMP concentrations and the adverse effects of myelosuppression and hepatotoxicity may relate to the small number of patients with these events. On the contrary, a study by Duley et al. [29], revealed the problems in measuring 6-TGN in erythrocytes which is not the ideal cell, and technical concerns about the validity of acid hydrolysis method of Dervieux. This may also explain why drop-out of patients due to myelosuppression could not be predicted by measuring 6-TGN concentrations. In the present study, we observed that the incidence of myelosuppression was significantly higher (12% vs. 3%) in the cases with 6-MMP concentrations > 5700 pmol/8 × 108 RBC compared to 6-MMP concentrations below this reference value, respectively. This is in line with a previous study by Wong et al. [30], showing that the predictive value for developing leukopenia of 6-MMP metabolites is similar to that of 6-TGN metabolites. Additionally, they found an increased risk of leukopenia in patients with both 6-MMP and 6-TGN concentrations exceeding the defined threshold, comparable to our findings. These data suggest that 6-MMP and its ribonucleotides can inhibit purine de novo synthesis, resulting in inhibition of DNA formation [31].

In our cohort of pediatric patients, only 37% of patients still used thiopurine therapy after 5 years. Approximately 50% ceased therapy due to clinical refractoriness, and in 30% of these patients, infliximab was already administered. A previous study by van Hoeve et al. [11], showed that only 32% of children with IBD treated with immunosuppressive agents, mainly thiopurines, remained free of biologics or surgery 5-years after diagnosis. Around 20% of patients ceased thiopurine therapy at patients’ or parents’ own request, mostly due to non-adherence. Non-adherence to oral medication is a well-known problem in adolescents, with non-adherence prevalence rates ranging from 2 to 93% [32].

The strength of this study is that we report on the largest pediatric IBD cohort so far regarding incidence of thiopurine-induced AE, related to thiopurine metabolites and biochemical abnormalities. The most important limitation is the retrospective design of this study, and consequently lack of standardization of collected data. Consequently, any potential AE not resulting in cessation of thiopurine therapy has not been recorded in a standardized matter in patients’ files, possibly leading to bias, and therefore not included in this study. Since metabolite measurement was not performed in a standardized matter, timing and reason for measuring metabolites may have led to selection bias. Additionally, TPMT genotyping and activity assessments were not routinely assessed prior to initiation of thiopurines. Another limitation might be the drug interactions between thiopurines and other co-administered drugs that were not analyzed. Patients with reintroduction of thiopurine therapy in case of AE probably infer a selection bias, as there were no standardized criteria for reintroduction of thiopurine therapy after AE. Reintroduction was commonly performed in mild AE and mainly dependent on physician’s judgement, possibly resulting in an overestimated success percentage of rechallenge following AE, however, these data reflect general practice.

In conclusion, in a real-life pediatric IBD cohort, 22% discontinued thiopurines due to AE. A rechallenge or switch to MP can be an effective strategy after AE. This was not studied, however, in patients with pancreatitis and severe myelotoxicity. Thiopurine metabolite concentrations significantly affect hematological indices and liver tests and they should therefore not exceed reference values. Only 37% of children were still on thiopurines after 5 years, illustrating that efficacy of thiopurines as long-term maintenance therapy seems limited in clinical practice. A reassessment of the use of thiopurines, including pre-exposure genotyping and tight monitoring of metabolites, in pediatric IBD is warranted.

Below is the link to the electronic supplementary material.

Supplementary file1 (DOCX 18 kb)