Faster Serotonin Clearance in CA3 Region of Hippocampus and Antidepressant-like Effect of Decynium-22 in Juvenile Mice Are Putatively Linked to Increased Plasma Membrane Monoamine Transporter Function: Implications for Efficacy of Antidepressants in Juveniles

Bowman, Melodi A.; Gómez, Jesús María Fernández; Mitchell, Nathan C.; Wells, Anne M.; Vitela, Melissa; Clarke, Kyra; Horton, Rebecca E.; Koek, Wouter; Daws, Lynette C.

doi:10.3390/cells11152454

Cited by 2 publications

(1 citation statement)

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“…PMAT is a monoamine and organic cation transporter highly expressed in human brain, complementing the activity of high-affinity monoamine transporters such as NET (Duan and Wang, 2010;Vieira and Wang, 2021;Bowman et al, 2022). In healthy tissues and transfected JPET-AR-2023-001672 cell lines, PMAT is localized to the plasma membrane of cells (Engel et al, 2004;Dahlin et al, 2007;Duan and Wang, 2013).…”

Section: Discussionmentioning

confidence: 99%

The Plasma Membrane Monoamine Transporter is Highly Expressed in Neuroblastoma and Functions as an mIBG Transporter

Vieira

Zhang

Quinones

et al. 2023

J Pharmacol Exp Ther

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Neuroblastoma (NB) is a pediatric cancer with low survival rates in high-risk patients. 131 I-mIBG has emerged as a promising therapy for high-risk NB and kills tumor cells by radiation. Consequently, 131 I-mIBG tumor uptake and retention are major determinants for its therapeutic efficacy. mIBG enters NB cells through the norepinephrine transporter (NET), and accumulates in mitochondria through unknown mechanisms. Here we evaluated the expression of monoamine and organic cation transporters in high-risk NB tumors and explored their relationship with MYCN amplification and patient survival. We found that NB mainly expresses NET, the plasma membrane monoamine transporter (PMAT), and the vesicular membrane monoamine transporter 1/2 (VMAT1/2), and that the expression of these transporters is significantly reduced in MYCN-amplified tumor samples. PMAT expression is the highest and correlates with overall survival in high-risk NB patients without MYCN amplification.Immunostaining showed that PMAT resides intracellularly in NB cells and co-localizes with mitochondria. Using cells expressing PMAT, mIBG was identified as a PMAT substrate. In mitochondria isolated from NB cell lines, mIBG uptake was reduced by ~50% by a PMAT inhibitor. Together, our data suggest that PMAT is a previously unrecognized transporter highly expressed in NB and could impact intracellular transport and therapeutic response to 131 I-mIBG.

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