Abstract
Simple SummaryImprovement in the understanding of the development of primary aldosteronism, the most common cause of endocrine hypertension and mainly caused by aldosterone producing adenomas or hyperplasia, has been continuously accomplished over the past several years. Herein, we summarize the major milestones in the field, including utilization of the newest available molecular techniques to not only shed light on the mechanisms involved in disease development but also to assist in the identification of disease subtypes with distinct laboratory and molecular findings, enabling the personalized treatment of the patients.Introduction: Primary aldosteronism (PA) is the most common cause of endocrine hypertension, mainly caused by aldosterone-producing adenomas or hyperplasia; understanding its pathophysiological background is important in order to provide ameliorative treatment strategies. Over the past several years, significant progress has been documented in this field, in particular in the clarification of the genetic and molecular mechanisms responsible for the pathogenesis of aldosterone-producing adenomas (APAs). Methods: Systematic searches of the PubMed and Cochrane databases were performed for all human studies applying transcriptomic, epigenetic or metabolomic analyses to PA subjects. Studies involving serial analysis of gene expression and microarray, epigenetic studies with methylome analyses and micro-RNA expression profiles, and metabolomic studies focused on improving understanding of the regulation of autonomous aldosterone production in PA were all included. Results: In this review we summarize the main findings in this area and analyze the interplay between primary aldosteronism and several signaling pathways with differential regulation of the RNA and protein expression of several factors involved in, among others, steroidogenesis, calcium signaling, and nuclear, membrane and G-coupled protein receptors. Distinct transcriptomic and metabolomic patterns are also presented herein, depending on the mutational status of APAs. In particular, two partially opposite transcriptional and steroidogenic profiles appear to distinguish APAs carrying a KCNJ5 mutation from all other APAs, which carry different mutations. Conclusions: These findings can substantially contribute to the development of personalized treatment in patients with PA.
Highlights
Primary aldosteronism (PA) is the most common cause of endocrine hypertension, mainly caused by aldosterone-producing adenomas or hyperplasia; understanding its pathophysiological background is important in order to provide ameliorative treatment strategies
aldosteroneproducing adenomas (APAs) carrying KCNJ5 mutations are significantly larger in size, present lower pre-contrast Hounsfield units in abdominal computed tomography (CT) scans, and histologically display predominantly lipid-rich zona fasciculata (ZF)-like cells [21,22,23]
In the present study, we have summarized the main findings of transcriptome, epigenetic and metabolomic studies investigating the pathogenesis of primary aldosteronism
Summary
Primary aldosteronism (PA) is the most common cause of endocrine hypertension, mainly caused by aldosterone-producing adenomas or hyperplasia; understanding its pathophysiological background is important in order to provide ameliorative treatment strategies. There are two main clinical presentations of PA: aldosterone-producing adrenal adenoma (APA), and bilateral adrenal hyperplasia (BAH), whereas the clinical picture can rarely be attributed to an adrenocortical carcinoma [1]. Both somatic and germline mutations have been identified as causative for the development of APAs; these affect the clinical phenotype of the disease. Acting in a similar way, identified mutations in the ATPase Plasma Membrane Ca2+ Transporting 3 (ATP2B3) and the Calcium Voltage-Gated Channel Subunit Alpha D (CACNA1D) genes act by increasing the intracellular Ca2+ and stimulating Cytochrome P450 Family 11 Subfamily B Member 2 (aldosterone synthaseCYP11B2) expression and subsequent aldosterone synthesis [8,9]. Protein Kinase cAMP-Activated Catalytic Subunit Alpha (PRKACA), sporadic Calcium Voltage-Gated Channel Subunit Alpha H (CACNA1H) and Chloride Voltage-Gated Channel 2 (CLCN2) mutations have been identified in sporadic APAs [13,14,15]
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