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9 results on '"Aradottir, Tinna"'

1. Identification of PK-PD Insulin Models using Experimental GIR Data

Author

Freil, Kirstine Sylvest, Fritzen, Liv Olivia, Boiroux, Dimitri, Aradottir, Tinna B., and Jørgensen, John Bagterp

Subjects
Quantitative Biology - Quantitative Methods
Abstract

We present a method to estimate parameters in pharmacokinetic (PK) and pharmacodynamic (PD) models for glucose insulin dynamics in humans. The method combines 1) experimental glucose infusion rate (GIR) data from glucose clamp studies and 2) a PK-PD model to estimate parameters such that the model fits the data. Assuming that the glucose clamp is perfect, we do not need to know the details of the controller in the clamp, and the GIR can be computed directly from the PK-PD model. To illustrate the procedure, we use the glucoregulatory model developed by Hovorka and modify it to have a smooth non-negative endogeneous glucose production (EGP) term. We estimate PK-PD parameters for rapid-acting insulin analogs (Fiasp and NovoRapid). We use these PK-PD parameters to illustrate GIR for insulin analogs with 30% and 50% faster absorption time than currently available rapid-acting insulin analogs. We discuss the role of system identification using GIR data from glucose clamp studies and how such identified models can be used in automated insulin dosing (AID) systems with ultra rapid-acting insulin., Comment: Submitted to be presented at a conference, 6 pages, 10 figures, 1 table

Published
2024

2. Estimating a Personalized Basal Insulin Dose from Short-Term Closed-Loop Data in Type 2 Diabetes

Author

Engell, Sarah Ellinor, Aradóttir, Tinna Björk, Ritschel, Tobias K. S., Bengtsson, Henrik, and Jørgensen, John Bagterp

Subjects
Electrical Engineering and Systems Science - Systems and Control
Abstract

In type 2 diabetes (T2D) treatment, finding a safe and effective basal insulin dose is a challenge. The dose-response is highly individual and to ensure safety, people with T2D titrate by slowly increasing the daily insulin dose to meet treatment targets. This titration can take months. To ease and accelerate the process, we use short-term artificial pancreas (AP) treatment tailored for initial titration and apply it as a diagnostic tool. Specifically, we present a method to automatically estimate a personalized daily dose of basal insulin from closed-loop data collected with an AP. Based on AP-data from a stochastic simulation model, we employ the continuous-discrete extended Kalman filter and a maximum likelihood approach to estimate parameters in a simple dose-response model for 100 virtual people. With the identified model, we compute a daily dose of basal insulin to meet treatment targets for each individual. We test the personalized dose and evaluate the treatment outcomes against clinical reference values. In the tested simulation setup, the proposed method is feasible. However, more extensive tests will reveal whether it can be deemed safe for clinical implementation., Comment: 6 pages, 4 figures, 1 table. Accepted for publication in Proceedings of the 2022 61st IEEE Conference on Decision and Control (CDC)

Published
2022

8. A New Stochastic Approach for Modeling Glycemic Disturbances in Type 2 Diabetes

Author

Clausen, Henrik, Knudsen, Torben, Al Ahdab, Mohamad, Aradottir, Tinna, Schmidt, Signe, Nørgaard, Kirsten, Leth, John, Clausen, Henrik, Knudsen, Torben, Al Ahdab, Mohamad, Aradottir, Tinna, Schmidt, Signe, Nørgaard, Kirsten, and Leth, John

Abstract

OBJECTIVE: To improve insulin treatment in type 2 diabetes (T2D) using model-based control techniques, the underlying model needs to be individualized to each patient. Due to the impact of unknown meals, exercise and other factors on the blood glucose, it is difficult to utilize available data from continuous glucose monitors (CGMs) for model fitting and parameter estimation purposes.METHODS: To overcome this problem, we propose a novel method for modeling the glycemic disturbances as a stochastic process. To differentiate meals from other glycemic disturbances, we model the meal intake as a separate stochastic process while encompassing all other disturbances in another stochastic process. Using particle filtering, we validate the model on simulations as well as on clinical data.RESULTS: Based on simulated CGM data, the residuals generated by the particle filter are white, indicating a good model fit. For the clinical data, we use parameter values estimated based on fasting glucose data. The residuals obtained from clinical CGM data contain correlations up to lag 5.CONCLUSION: The proposed model is shown to adequately describe the meal-induced glucose fluctuations in simulated CGM data while validations on clinical CGM data show promising results as well.SIGNIFICANCE: The proposed model may lay the grounds for new ways of utilizing available CGM data, including CGM-based parameter estimation and stochastic optimal control.

Published
2021

9. A Model-free Approach to Automatic Dose Guidance in Long Acting Insulin Treatment of Type 2 Diabetes

Author

Krishnamoorthy, Dinesh, Boiroux, Dimitri, Aradottir, Tinna Bjork, Engell, Sarah Ellinor, Jørgensen, John Bagterp, Krishnamoorthy, Dinesh, Boiroux, Dimitri, Aradottir, Tinna Bjork, Engell, Sarah Ellinor, and Jørgensen, John Bagterp

Abstract

This paper presents a model-free insulin titration algorithm for patients with type 2 diabetes that automatically finds and maintains the optimal insulin dosage in order to maintain the blood glucose concentration at desired levels. The proposed method is based on recursive least square based extremum seeking control. Since the proposed method does not require a detailed model, it can be applied on a wide population of patients without the need to identify and adapt models to the patient data. We demonstrate the effectiveness of the proposed method using in silico simulations, which are benchmarked against two standard-of-care approaches. We also show that the proposed method can handle intra-patient metabolic variations and non-adherence to the treatment regimen. Finally, using a population of 50 virtual patients, we show that the proposed method is able to handle inter-patient variations.

Published
2021

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