AI Article Synopsis
- Essential hypertension is a widespread condition linked to high morbidity and mortality, but its underlying genetic mechanisms are not fully understood.
- Recent research highlights how blood pressure (BP) is regulated by a complex interaction of genetic elements, specifically through epistatic relationships among various quantitative trait loci (QTLs).
- This study represents the first analysis of BP QTLs in a mammalian system, aiming to clarify the regulatory dynamics that could lead to improved diagnosis and treatment strategies for essential hypertension.
Article Abstract
Essential hypertension is one of the most common disorders that underpin significant morbidity and mortality; however, underlying mechanisms remain elusive that either dictate the actions of individual quantitative trait loci (QTLs) or engineer the overall genetic architecture from them. Recent experimental evidence has unveiled that the genetic architecture determining blood pressure (BP) is assembled from QTL-building blocks by epistasis into regulatory hierarchies. BP, a polygenic and quantitative trait, is homeostasized via pathways participated by Mendelian constituents that operate distantly from end-phase physiological genes. Epistasis genetics performed in the current article has mechanistically unravelled the order and regulatory relationships between certain BP QTLs, and is the first study ever conducted in a mammalian system in analysing a complex trait. The elucidation of the sequence of event and regulatory hierarchies of QTL actions in these pathways will facilitate mechanism-based diagnoses and cause-driven treatments for essential hypertension.
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| http://dx.doi.org/10.1097/HJH.0000000000000479 | DOI Listing |
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