Abstract
SUMMARYPostural orthostatic tachycardia syndrome (POTS) is a common autonomic disorder of largely unknown etiology that presents with sustained tachycardia on standing, syncope and elevated norepinephrine spillover. Some individuals with POTS experience anxiety, depression and cognitive dysfunction. Previously, we identified a mutation, A457P, in the norepinephrine (NE; also known as noradrenaline) transporter (NET; encoded by SLC6A2) in POTS patients. NET is expressed at presynaptic sites in NE neurons and plays a crucial role in regulating NE signaling and homeostasis through NE reuptake into noradrenergic nerve terminals. Our in vitro studies demonstrate that A457P reduces both NET surface trafficking and NE transport and exerts a dominant-negative impact on wild-type NET proteins. Here we report the generation and characterization of NET A457P mice, demonstrating the ability of A457P to drive the POTS phenotype and behaviors that are consistent with reported comorbidities. Mice carrying one A457P allele (NET+/P) exhibited reduced brain and sympathetic NE transport levels compared with wild-type (NET+/+) mice, whereas transport activity in mice carrying two A457P alleles (NETP/P) was nearly abolished. NET+/P and NETP/P mice exhibited elevations in plasma and urine NE levels, reduced 3,4-dihydroxyphenylglycol (DHPG), and reduced DHPG:NE ratios, consistent with a decrease in sympathetic nerve terminal NE reuptake. Radiotelemetry in unanesthetized mice revealed tachycardia in NET+/P mice without a change in blood pressure or baroreceptor sensitivity, consistent with studies of human NET A457P carriers. NET+/P mice also demonstrated behavioral changes consistent with CNS NET dysfunction. Our findings support that NET dysfunction is sufficient to produce a POTS phenotype and introduces the first genetic model suitable for more detailed mechanistic studies of the disorder and its comorbidities.
Highlights
Norepinephrine (NE; known as noradrenaline) is the primary signaling neurotransmitter of the autonomic sympathetic nervous system (SNS), where it acts to control heart rate (HR)
They report that NE transporter (NET) A457P knock-in mice have the Postural orthostatic tachycardia syndrome (POTS) phenotype as well as behaviors consistent with reported co-morbidities
Heterozygote mice carrying one A457P allele (NET+/P) exhibited reduced brain and sympathetic NE transport levels compared with wild-type mice (NET+/+), whereas transport activity in homozygotes (NETP/P) was virtually abolished
Summary
Norepinephrine (NE; known as noradrenaline) is the primary signaling neurotransmitter of the autonomic sympathetic nervous system (SNS), where it acts to control heart rate (HR). Released NE is inactivated through active transport into noradrenergic terminals by the presynaptically localized Na+/Cl–-dependent NE transporter (NET; encoded by SLC6A2; note that throughout this paper the gene is referred to as NET) (Iversen, 1963; Matthies et al, 2009). Altered sympathetic nerve terminal NET uptake sites and/or activity are found in hypertension, diabetes, cardiomyopathy, heart failure and ischemia (Böhm et al, 1998; Merlet et al, 1992; Rumantir et al, 2000; Schnell et al, 1996; Schömig et al, 1991)
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