Clinical utility of thiopurine metabolite monitoring in inflammatory bowel disease and its impact on healthcare utilization in Singapore

Jia Qi Yeo; Hua Heng McVin Cheen; Amanda Wong; Teong Guan Lim; Balram Chowbay; Wai Fook Leong; Chunyan Wang; Ennaliza Salazar; Webber Pak Wo Chan; San Choon Kong; Wan Chee Ong

doi:10.1002/jgh3.12798

Clinical utility of thiopurine metabolite monitoring in inflammatory bowel disease and its impact on healthcare utilization in Singapore

JGH Open. 2022 Aug 1;6(10):658-666. doi: 10.1002/jgh3.12798. eCollection 2022 Oct.

Authors

Jia Qi Yeo¹, Hua Heng McVin Cheen², Amanda Wong², Teong Guan Lim², Balram Chowbay^{3

4

5}, Wai Fook Leong⁵, Chunyan Wang⁶, Ennaliza Salazar⁷, Webber Pak Wo Chan⁷, San Choon Kong⁸, Wan Chee Ong²

Affiliations

¹ National Healthcare Group Pharmacy Singapore.
² Department of Pharmacy Singapore General Hospital Singapore.
³ Clinical Pharmacology Laboratory National Cancer Centre Singapore Singapore.
⁴ Centre for Clinician-Scientist Development Duke-NUS Medical School Singapore.
⁵ Singapore Immunology Network (SIgN) ASTAR (Agency for Science, Technology and Research), Biopolis Singapore.
⁶ Clinical Pharmacology SingHealth Singapore.
⁷ Department of Gastroenterology and Hepatology Singapore General Hospital Singapore.
⁸ Department of Gastroenterology and Hepatology Sengkang General Hospital Singapore.

Abstract

Background and aim: Thiopurines are recommended for maintenance of steroid-free remission (SFR) in inflammatory bowel disease (IBD). Thiopurine metabolite monitoring (MM) is increasingly used in the West but remains novel in Singapore, with limited information on its therapeutic and economic benefits. Hence, this study aims to investigate MM's clinical utility and its impact on healthcare resource utilization in Singaporean IBD patients.

Methods: A retrospective observational study was conducted at Singapore General Hospital outpatient IBD Centre. Patients with IBD, baseline MM during 2014-2017, and weight-based thiopurine doses for ≥4 weeks were followed up for 1 year. Actions were taken to optimize therapy, and metabolite levels before and after the first action were documented. Outcomes assessed included SFR, no therapy escalation or surgery, healthcare resource utilization, and direct healthcare costs.

Results: Ninety IBD patients (50 Crohn's disease, 40 ulcerative colitis) were included. Among them, 40% had baseline metabolite levels within therapeutic range, 31.1% sub-therapeutic, 21.1% supra-therapeutic, and 7.8% shunters. Repeated MM with subsequent dose optimization helped 67.2% of patients achieve therapeutic levels after 1 year. Overall, 87.8% of patients achieved SFR and 90% had no therapy escalation or surgery. Despite greater outpatient visits and laboratory investigations with MM, the median total healthcare costs at 1 year only increased marginally (S$6407.66 [shunters] vs S$5215.20 [supra-therapeutic] vs S$4970.80 [sub-therapeutic] vs S$4370.48 [control (within therapeutic range)], P = 0.592).

Conclusion: MM guided timely therapy escalation for non-responders, identification of non-adherence, and reversal of shunting. Therefore, it is a useful clinical tool to optimize thiopurines without significantly increasing healthcare costs.

Keywords: Crohn's disease; inflammatory bowel disease; metabolite monitoring; thiopurine; ulcerative colitis.