Evidence for the druggability of aldosterone targets in heart failure: A bioinformatics and data science-driven decision-making approach

Lucas Salgado Rezende de Mendonça; Sergio Senar; Luana Lorena Moreira; José Antônio Silva Júnior; Moni Nader; Luciana Aparecida Campos; Ovidiu Constantin Baltatu

doi:10.1016/j.compbiomed.2024.108124

Evidence for the druggability of aldosterone targets in heart failure: A bioinformatics and data science-driven decision-making approach

Comput Biol Med. 2024 Mar:171:108124. doi: 10.1016/j.compbiomed.2024.108124. Epub 2024 Feb 13.

Authors

Lucas Salgado Rezende de Mendonça¹, Sergio Senar², Luana Lorena Moreira¹, José Antônio Silva Júnior³, Moni Nader⁴, Luciana Aparecida Campos⁵, Ovidiu Constantin Baltatu⁶

Affiliations

¹ Center of Innovation, Technology, and Education (CITE) at Anhembi Morumbi University, Anima Institute, Sao Jose dos Campos Technology Park, Sao Jose dos Campos, Brazil.
² DrTarget, 28806 Madrid, Spain(1).
³ Universidade Nove de Julho (UNINOVE), Sao Paulo, Brazil.
⁴ College of Medicine & Health Sciences, Khalifa University of Science and Technology, Abu Dhabi, United Arab Emirates.
⁵ Center of Innovation, Technology, and Education (CITE) at Anhembi Morumbi University, Anima Institute, Sao Jose dos Campos Technology Park, Sao Jose dos Campos, Brazil. Electronic address: camposbaltatu@gmail.com.
⁶ Center of Innovation, Technology, and Education (CITE) at Anhembi Morumbi University, Anima Institute, Sao Jose dos Campos Technology Park, Sao Jose dos Campos, Brazil. Electronic address: ocbaltatu@gmail.com.

PMID: 38412691
DOI: 10.1016/j.compbiomed.2024.108124

Abstract

Background: Aldosterone plays a key role in the neurohormonal drive of heart failure. Systematic prioritization of drug targets using bioinformatics and database-driven decision-making can provide a competitive advantage in therapeutic R&D. This study investigated the evidence on the druggability of these aldosterone targets in heart failure.

Methods: The target disease predictability of mineralocorticoid receptors (MR) and aldosterone synthase (AS) in cardiac failure was evaluated using Open Targets target-disease association scores. The Open Targets database collections were downloaded to MongoDB and queried according to the desired aggregation level, and the results were retrieved from the Europe PMC (data type: text mining), ChEMBL (data type: drugs), Open Targets Genetics Portal (data type: genetic associations), and IMPC (data type: genetic associations) databases. The target tractability of MR and AS in the cardiovascular system was investigated by computing activity scores in a curated ChEMBL database using supervised machine learning.

Results: The medians of the association scores of the MR and AS groups were similar, indicating a comparable predictability of the target disease. The median of the MR activity scores group was significantly lower than that of AS, indicating that AS has higher target tractability than MR [Hodges-Lehmann difference 0.62 (95%CI 0.53-0.70, p < 0.0001]. The cumulative distributions of the overall multiplatform association scores of cardiac diseases with MR were considerably higher than with AS, indicating more advanced investigations on a wider range of disorders evaluated for MR (Kolmogorov-Smirnov D = 0.36, p = 0.0009). In curated ChEMBL, MR had a higher cumulative distribution of activity scores in experimental cardiovascular assays than AS (Kolmogorov-Smirnov D = 0.23, p < 0.0001). Documented clinical trials for MR in heart failures surfaced in database searches, none for AS.

Conclusions: Although its clinical development has lagged behind that of MR, our findings indicate that AS is a promising therapeutic target for the treatment of cardiac failure. The multiplatform-integrated identification used in this study allowed us to comprehensively explore the available scientific evidence on MR and AS for heart failure therapy.

Keywords: Aldosterone; CYP11B2; Databases; Heart failure; Machine learning; NR3C2; Open access platforms.

MeSH terms

Aldosterone*
Cardiotonic Agents
Computational Biology
Data Science
Enzyme Inhibitors
Heart
Heart Failure* / drug therapy
Humans

Substances

Aldosterone
Enzyme Inhibitors
Cardiotonic Agents