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Glutamine Uptake via SNAT6 and Caveolin Regulates Glutamine–Glutamate Cycle

SLC38A6 (SNAT6) is the only known member of the SLC38 family that is expressed exclusively in the excitatory neurons of the brain. It has been described as an orphan transporter with an unknown substrate profile, therefore very little is known about SNAT6. In this study, we addressed the substrate s...

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Autores principales: Gandasi, Nikhil R., Arapi, Vasiliki, Mickael, Michel E., Belekar, Prajakta A., Granlund, Louise, Kothegala, Lakshmi, Fredriksson, Robert, Bagchi, Sonchita
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7865731/
https://www.ncbi.nlm.nih.gov/pubmed/33503881
http://dx.doi.org/10.3390/ijms22031167
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author Gandasi, Nikhil R.
Arapi, Vasiliki
Mickael, Michel E.
Belekar, Prajakta A.
Granlund, Louise
Kothegala, Lakshmi
Fredriksson, Robert
Bagchi, Sonchita
author_facet Gandasi, Nikhil R.
Arapi, Vasiliki
Mickael, Michel E.
Belekar, Prajakta A.
Granlund, Louise
Kothegala, Lakshmi
Fredriksson, Robert
Bagchi, Sonchita
author_sort Gandasi, Nikhil R.
collection PubMed
description SLC38A6 (SNAT6) is the only known member of the SLC38 family that is expressed exclusively in the excitatory neurons of the brain. It has been described as an orphan transporter with an unknown substrate profile, therefore very little is known about SNAT6. In this study, we addressed the substrate specificity, mechanisms for internalization of SNAT6, and the regulatory role of SNAT6 with specific insights into the glutamate–glutamine cycle. We used tritium-labeled amino acids in order to demonstrate that SNAT6 is functioning as a glutamine and glutamate transporter. SNAT6 revealed seven predicted transmembrane segments in a homology model and was localized to caveolin rich sites at the plasma membrane. SNAT6 has high degree of specificity for glutamine and glutamate. Presence of these substrates enables formation of SNAT6-caveolin complexes that aids in sodium dependent trafficking of SNAT6 off the plasma membrane. To further understand its mode of action, several potential interacting partners of SNAT6 were identified using bioinformatics. Among them where CTP synthase 2 (CTPs2), phosphate activated glutaminase (Pag), and glutamate metabotropic receptor 2 (Grm2). Co-expression analysis, immunolabeling with co-localization analysis and proximity ligation assays of these three proteins with SNAT6 were performed to investigate possible interactions. SNAT6 can cycle between cytoplasm and plasma membrane depending on availability of substrates and interact with Pag, synaptophysin, CTPs2, and Grm2. Our data suggest a potential role of SNAT6 in glutamine uptake at the pre-synaptic terminal of excitatory neurons. We propose here a mechanistic model of SNAT6 trafficking that once internalized influences the glutamate–glutamine cycle in presence of its potential interacting partners.
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spelling pubmed-78657312021-02-07 Glutamine Uptake via SNAT6 and Caveolin Regulates Glutamine–Glutamate Cycle Gandasi, Nikhil R. Arapi, Vasiliki Mickael, Michel E. Belekar, Prajakta A. Granlund, Louise Kothegala, Lakshmi Fredriksson, Robert Bagchi, Sonchita Int J Mol Sci Article SLC38A6 (SNAT6) is the only known member of the SLC38 family that is expressed exclusively in the excitatory neurons of the brain. It has been described as an orphan transporter with an unknown substrate profile, therefore very little is known about SNAT6. In this study, we addressed the substrate specificity, mechanisms for internalization of SNAT6, and the regulatory role of SNAT6 with specific insights into the glutamate–glutamine cycle. We used tritium-labeled amino acids in order to demonstrate that SNAT6 is functioning as a glutamine and glutamate transporter. SNAT6 revealed seven predicted transmembrane segments in a homology model and was localized to caveolin rich sites at the plasma membrane. SNAT6 has high degree of specificity for glutamine and glutamate. Presence of these substrates enables formation of SNAT6-caveolin complexes that aids in sodium dependent trafficking of SNAT6 off the plasma membrane. To further understand its mode of action, several potential interacting partners of SNAT6 were identified using bioinformatics. Among them where CTP synthase 2 (CTPs2), phosphate activated glutaminase (Pag), and glutamate metabotropic receptor 2 (Grm2). Co-expression analysis, immunolabeling with co-localization analysis and proximity ligation assays of these three proteins with SNAT6 were performed to investigate possible interactions. SNAT6 can cycle between cytoplasm and plasma membrane depending on availability of substrates and interact with Pag, synaptophysin, CTPs2, and Grm2. Our data suggest a potential role of SNAT6 in glutamine uptake at the pre-synaptic terminal of excitatory neurons. We propose here a mechanistic model of SNAT6 trafficking that once internalized influences the glutamate–glutamine cycle in presence of its potential interacting partners. MDPI 2021-01-25 /pmc/articles/PMC7865731/ /pubmed/33503881 http://dx.doi.org/10.3390/ijms22031167 Text en © 2021 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Gandasi, Nikhil R.
Arapi, Vasiliki
Mickael, Michel E.
Belekar, Prajakta A.
Granlund, Louise
Kothegala, Lakshmi
Fredriksson, Robert
Bagchi, Sonchita
Glutamine Uptake via SNAT6 and Caveolin Regulates Glutamine–Glutamate Cycle
title Glutamine Uptake via SNAT6 and Caveolin Regulates Glutamine–Glutamate Cycle
title_full Glutamine Uptake via SNAT6 and Caveolin Regulates Glutamine–Glutamate Cycle
title_fullStr Glutamine Uptake via SNAT6 and Caveolin Regulates Glutamine–Glutamate Cycle
title_full_unstemmed Glutamine Uptake via SNAT6 and Caveolin Regulates Glutamine–Glutamate Cycle
title_short Glutamine Uptake via SNAT6 and Caveolin Regulates Glutamine–Glutamate Cycle
title_sort glutamine uptake via snat6 and caveolin regulates glutamine–glutamate cycle
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7865731/
https://www.ncbi.nlm.nih.gov/pubmed/33503881
http://dx.doi.org/10.3390/ijms22031167
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