Serum microRNAs as peripheral markers of primary aldosteronism

Primary aldosteronism (PA) is the principal cause of secondary hypertension; it leads to significantly elevated cardiovascular morbidity and mortality, but only a fraction of its cases ever get detected, partially due to diagnostic procedures that are difficult to perform and to interpret. More stra...

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Published inFrontiers in endocrinology (Lausanne) Vol. 16; p. 1511096
Main Authors Makhnov, Nikita, Axling, Fredrik, Barazeghi, Elham, Stålberg, Peter, Åkerström, Tobias, Hellman, Per
Format Journal Article
LanguageEnglish
Published Switzerland Frontiers Media S.A 20.03.2025
Subjects
Adult
Biomarkers - blood
Endocrinology
Female
genetic markers
Humans
hyperaldosteronism
Hyperaldosteronism - blood
Hyperaldosteronism - diagnosis
Hyperaldosteronism - genetics
hypertension
Hypertension - blood
Hypertension - diagnosis
machine learning
Male
Medical Science
Medicinsk vetenskap
microRNAs
MicroRNAs - blood
MicroRNAs - genetics
Middle Aged
serum
microRNAs
diagnostics
primary aldosteronism
hyperaldosteronism
genetic markers
machine learning
serum
hypertension
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Summary:Primary aldosteronism (PA) is the principal cause of secondary hypertension; it leads to significantly elevated cardiovascular morbidity and mortality, but only a fraction of its cases ever get detected, partially due to diagnostic procedures that are difficult to perform and to interpret. More straightforward diagnostic methods are needed. Lateralized, or unilateral PA (uPA), is best treated by surgery. Bilateral PA (bPA) is treated medically. The aim of our study was to explore microRNA (miRNA) in peripheral blood as markers of PA, uPA and bPA. In groups of subjects with primary hypertension (HT, n = 11), bPA (n = 12), and uPA (n = 16), peripheral serum was used for isolation of total RNA, library preparation, and NGS sequencing to achieve a comparative analysis of miRNA expression. Five-fold cross-validation support vector machine learning (ML) models were employed to search for miRNA that could be used as markers of PA and its forms. In our cohort of patients, the discovered combinations of miRNAs could, with a high level of accuracy, sensitivity, and specificity, characterize the difference between HT and PA, as well as between a combined group of HT + bPA vs. uPA. The differentiating parameters were moderately good for comparison of bPA vs. uPA. Within our patient cohort, and using ML, the study identified distinctly different miRNA profiles between HT and PA, as well as between bPA and uPA. Further validation studies may lead to the emergence of a new tool for clinical diagnostics of PA.
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Reviewed by: Antonio Concistrè, Ospedale San Filippo Neri, Italy
Edited by: Mirko Parasiliti-Caprino, University of Turin, Italy
Peter Igaz, Semmelweis University, Hungary
These authors have contributed equally to this work and share first authorship
ISSN:1664-2392
1664-2392
DOI:10.3389/fendo.2025.1511096