A decision support system based on artificial intelligence and systems biology for the simulation of pancreatic cancer patient status

Author:

Junet Valentin12ORCID,Matos‐Filipe Pedro13ORCID,García‐Illarramendi Juan Manuel12ORCID,Ramírez Esther4,Oliva Baldo3ORCID,Farrés Judith1ORCID,Daura Xavier256ORCID,Mas José Manuel1,Morales Rafael7

Affiliation:

1. Anaxomics Biotech SL Barcelona Spain

2. Institute of Biotechnology and Biomedicine Universitat Autònoma de Barcelona Cerdanyola del Vallès Spain

3. Structural Bioinformatics (GRIB‐IMIM), Departament de Ciències Experimentals i de la Salut Universitat Pompeu Fabra Barcelona Spain

4. Iteraset Solutions SL Barcelona Spain

5. Catalan Institution for Research and Advanced Studies (ICREA) Barcelona Spain

6. Biomedical Research Networking Center in Bioengineering, Biomaterials and Nanomedicine (CIBER‐BBN) Instituto de Salud Carlos III Cerdanyola del Vallès Spain

7. Hospital La Mancha Centro Alcázar de San Juan Spain

Abstract

AbstractOncology treatments require continuous individual adjustment based on the measurement of multiple clinical parameters. Prediction tools exploiting the patterns present in the clinical data could be used to assist decision making and ease the burden associated to the interpretation of all these parameters. The goal of this study was to predict the evolution of patients with pancreatic cancer at their next visit using information routinely recorded in health records, providing a decision‐support system for clinicians. We selected hematological variables as the visit's clinical outcomes, under the assumption that they can be predictive of the evolution of the patient. Multivariate models based on regression trees were generated to predict next‐visit values for each of the clinical outcomes selected, based on the longitudinal clinical data as well as on molecular data sets streaming from in silico simulations of individual patient status at each visit. The models predict, with a mean prediction score (balanced accuracy) of 0.79, the evolution trends of eosinophils, leukocytes, monocytes, and platelets. Time span between visits and neutropenia were among the most common factors contributing to the predicted evolution. The inclusion of molecular variables from the systems‐biology in silico simulations provided a molecular background for the observed variations in the selected outcome variables, mostly in relation to the regulation of hematopoiesis. In spite of its limitations, this study serves as a proof of concept for the application of next‐visit prediction tools in real‐world settings, even when available data sets are small.

Publisher

Wiley

Subject

Pharmacology (medical),Modeling and Simulation

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