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Oral Anticoagulants and risk of Type 2 Diabetes among adults with atrial fibrillation in the United Kingdom
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  • Yan-Ling Lu,
  • Emma Powell,
  • Usha Gungabissoon,
  • Ian Douglas,
  • Kevin Wing,
  • Anna Schultze
Yan-Ling Lu
London School of Hygiene & Tropical Medicine Faculty of Epidemiology and Population Health

Corresponding Author:[email protected]

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Emma Powell
London School of Hygiene & Tropical Medicine Faculty of Epidemiology and Population Health
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Usha Gungabissoon
GSK plc
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Ian Douglas
London School of Hygiene & Tropical Medicine Faculty of Epidemiology and Population Health
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Kevin Wing
London School of Hygiene & Tropical Medicine Faculty of Epidemiology and Population Health
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Anna Schultze
London School of Hygiene & Tropical Medicine Faculty of Epidemiology and Population Health
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Abstract

Background: A number of observational studies and small trials have suggested that higher levels of circulating vitamin K1 might improve insulin sensitivity and therefore protect against the development of Type II Diabetes (T2DM). The use of vitamin K-inhibitors, such as warfarin, may lead to an increased risk of developing T2DM compared to alternative oral anticoagulants (OACs). Objective: To compare the risk of developing T2DM among atrial fibrillation patients initiating warfarin vs direct-acting oral anticoagulants (DOACs). Methods: We included AF patients with no history of diabetes newly prescribed OACs in Clinical Practice Research Datalink (CPRD) Aurum between 01.01.2013 to 31.01.2019. Patients were followed from 30 days after the first OAC prescription to 21.01.2020, death, deregistration or the first occurrence of a diagnostic code for T2DM. Potential confounders were identified using a directed acyclic graph, and Cox regression was used to calculate adjusted hazard ratios (aHR), comparing the hazard of T2DM between warfarin and DOAC initiators. We investigated a-priori interactions with sex and age and conducted subgroup analyses according to the type of DOAC. An on-treatment analysis was added post-hoc to take into account treatment switches and discontinuation. Results: A total of 94,394 OAC initiators were included, 46.34% were female, and the average age was 74.78 (SD 11.6) years. After a mean follow-up of 2.77 years (IQR 1.45-4.19), 7,041 patients developed T2DM, with the crude Kaplan-Meier risk slightly lower among DOAC initiators (13.58%, 95%CI=12.89 – 14.31) compared to warfarin initiators (15.53%, 95%CI = 14.99 – 16.09). After adjusting for a-priori identified confounders, a modest protective association between DOACs and incident T2DM was found (aHR=0.90, 95%CI 0.84-0.95; p<0.001). No interaction by age group or sex was observed (p=0.11 and 0.61, respectively). Subgroup analyses were consistent, with potentially somewhat more marked protective effects for initiators of edoxaban and dabigatran compared to warfarin, although confidence intervals were wide [HR=0.82 (95%CI 0.63-1.08) and HR=0.86 (95%CI 0.76-0.96), respectively]. Sensitivity analyses applying a lagged index date (initiation + 180 days) led to consistent results. On-treatment analysis showed a more marked protective effect, with an adjusted HR of 0.69 (0.65, 0.73). Conclusions: Treatment initiation with DOACs compared to warfarin was associated with a relatively modest reduction in the risk of developing T2DM in this cohort. We did not find any evidence that the association differed according to patient sex or age.