Glycemic response trajectories on metformin monotherapy in real-world diabetes care

Objectives: Diabetes affects over 500 million people globally and glycemia is inadequately managed. Metformin is the most frequently prescribed initial treatment for type 2 diabetes globally, yet glycemic response trajectories to metformin in routine real-world care and predictors of treatment response have not been well described. We aimed to identify glycemic response trajectories in adults prescribed metformin monotherapy as initial type 2 diabetes treatment and predictors of poor glycemic response to metformin. Design: Observational cohort study using latent class mixed models to identify hemoglobin A1c (HbA1c) trajectory classes, followed by random forests machine learning to predict trajectory class membership. Setting: US Veterans Affairs Healthcare System Participants: Adults treated with metformin alone for >30 days after diabetes diagnosis with a minimum of two HbA1c measurements from 90 days prior to two years after the first metformin prescription (N=140,413). Exposures: Demographic, laboratory, vital sign, and comorbidity data were included as predictors of metformin response trajectory Main Outcomes and Measures: We included all HbA1c measurements (487,604 total) for two years after metformin initiation to define metformin glycemic response trajectories. Results: We identified three HbA1c trajectories: stably low (89.7% of sample, mean HbA1c decrease from 7.2% to 6.6%), brisk response (7.1% of sample, mean HbA1c decrease from 11.4% to 7.0%), and non-response (3.1% of sample, mean HbA1c increase from 8.9% to 10.8%). Of those in the stably low and brisk response classes at 2 years, 91% maintained HbA1c at approximately 7% on metformin alone for 5 years after drug initiation. Prediction models could accurately predict brisk response (91% accuracy) but not metformin non-response (59% accuracy). Conclusions: Most individuals treated initially with metformin monotherapy have a beneficial and durable glycemic response. Predicting individuals who will not respond to metformin may be challenging but is evident within six months with recommended glycemic surveillance. The findings support current guidelines for HbA1c surveillance when initiating diabetes treatment.