Enhanced Model Predictive Control (eMPC) Strategy for Automated Glucose Control

Development of an effective artificial pancreas (AP) controller to deliver insulin autonomously to people with type 1 diabetes mellitus is a difficult task. In this paper, three enhancements to a clinically validated AP model predictive controller (MPC) are proposed that address major challenges fac...

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Bibliographic Details
Published in:Industrial & engineering chemistry research 2016-11, Vol.55 (46), p.11857-11868
Main Authors: Lee, Joon Bok, Dassau, Eyal, Gondhalekar, Ravi, Seborg, Dale E, Pinsker, Jordan E, Doyle, Francis J
Format: Article
Language:English
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Summary:Development of an effective artificial pancreas (AP) controller to deliver insulin autonomously to people with type 1 diabetes mellitus is a difficult task. In this paper, three enhancements to a clinically validated AP model predictive controller (MPC) are proposed that address major challenges facing automated blood glucose control and are then evaluated by both in silico tests and clinical trials. First, the core model of insulin–blood glucose dynamics utilized in the MPC is expanded with a medically inspired personalization scheme to improve controller responses in the face of inter- and intraindividual variations in insulin sensitivity. Next, the asymmetric nature of the short-term consequences of hypoglycemia versus hyperglycemia is incorporated in an asymmetric weighting of the MPC cost function. Finally, an enhanced dynamic insulin-on-board algorithm is proposed to minimize the likelihood of controller-induced hypoglycemia following a rapid rise of blood glucose due to rescue carbohydrate load with accompanying insulin suspension. Each advancement is evaluated separately and in unison through in silico trials based on a new clinical protocol, which incorporates induced hyper- and hypoglycemia to test robustness. The advancements are also evaluated in an advisory mode (simulated) testing of clinical data. The combination of the three proposed advancements show statistically significantly improved performance over the nonpersonalized controller without any enhancements across all metrics, displaying increased time in the 70–180 mg/dL safe glycemic range (76.9% versus 68.8%) and the 80–140 mg/dL euglycemic range (48.1% versus 44.5%), without a statistically significant increase in instances of hypoglycemia. The proposed advancements provide safe control action for AP applications, personalizing and improving controller performance without the need for extensive model identification processes.
ISSN:0888-5885
1520-5045
DOI:10.1021/acs.iecr.6b02718