Decreased serotonin transporter activity in the mitral valve contributes to progression of degenerative mitral regurgitation.
Estibaliz CastilleroEmmett FitzpatrickSamuel J KeeneyAlex M D'AngeloBenjamin B PresslyMichael T SimpsonMangesh KuradeW Clinton ErwinVivian MorenoChiara CamilloHalley J ShuklaVaishali V InamdarArbi AghaliJuan B GrauElisa SalvatiItzhak NissimLubica RauovaMark A OyamaStanley J StachelekChase BrownAbba M KriegerRobert J LevyGiovanni FerrariPublished in: Science translational medicine (2023)
Degenerative mitral valve (MV) regurgitation (MR) is a highly prevalent heart disease that requires surgery in severe cases. Here, we show that a decrease in the activity of the serotonin transporter (SERT) accelerates MV remodeling and progression to MR. Through studies of a population of patients with MR, we show that selective serotonin reuptake inhibitor (SSRI) use and SERT promoter polymorphism 5-HTTLPR LL genotype were associated with MV surgery at younger age. Functional characterization of 122 human MV samples, in conjunction with in vivo studies in SERT -/- mice and wild-type mice treated with the SSRI fluoxetine, showed that diminished SERT activity in MV interstitial cells (MVICs) contributed to the pathophysiology of MR through enhanced serotonin receptor (HTR) signaling. SERT activity was decreased in LL MVICs partially because of diminished membrane localization of SERT. In mice, fluoxetine treatment or SERT knockdown resulted in thickened MV leaflets. Similarly, silencing of SERT in normal human MVICs led to up-regulation of transforming growth factor β1 ( TGF β 1 ) and collagen ( COL1A1 ) in the presence of serotonin. In addition, treatment of MVICs with fluoxetine not only directly inhibited SERT activity but also decreased SERT expression and increased HTR2B expression. Fluoxetine treatment and LL genotype were also associated with increased COL1A1 expression in the presence of serotonin in MVICs, and these effects were attenuated by HTR2B inhibition. These results suggest that assessment of both 5-HTTLPR genotype and SERT-inhibiting treatments may be useful tools to risk-stratify patients with MV disease to estimate the likelihood of rapid disease progression.
Keyphrases
- mitral valve
- transforming growth factor
- wild type
- poor prognosis
- minimally invasive
- endothelial cells
- magnetic resonance
- high fat diet induced
- epithelial mesenchymal transition
- left atrial
- induced apoptosis
- binding protein
- signaling pathway
- heart failure
- magnetic resonance imaging
- aortic valve
- quantum dots
- skeletal muscle
- pulmonary hypertension
- long non coding rna
- transcription factor
- cell cycle arrest
- metabolic syndrome
- cell death
- coronary artery disease
- replacement therapy
- transcatheter aortic valve replacement
- clinical evaluation