Trafficking of the amino acid transporter B0,+ (SLC6A14) to the plasma membrane involves an exclusive interaction with SEC24C for its exit from the endoplasmic reticulum

Kovalchuk, Vasylyna; Samluk, Łukasz; Juraszek, Barbara; Jurkiewicz-Trząska, Dominika; Sučić, Sonja; Freissmuth, Michael; Nałęcz, Katarzyna A.

doi:10.1016/j.bbamcr.2018.11.005

Cited by 16 publications

(18 citation statements)

References 55 publications

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“…In a model structure of LeuT bacterial transporter glycosylation sites were found at the second extracellular loop, a localization confirmed by crystallization of SERT in which N-acetylglucoseamine electron density were found to be linked to Asn moieties of the second extracellular loop (Coleman et al, 2016). As shown by Kovalchuk et al (2019), ATB 0,+ overexpressed in HEK293 cells was sensitive to deglycosylating enzymes: peptide-N 4 -(acetyl-β-glucosaminyl)asparagine amidase (PNGase F, EC 3.5.1.52) and endoglycosidase (Endo H, EC 3.2.1.96), confirming the presence of glycosylated form of the transporter in the plasma membrane.…”

Section: Slc6a14 -A Transporter With Broad Substrate Specificitymentioning

confidence: 75%

“…As shown by Kovalchuk et al (2019), SLC6A14 co-localizes with calnexin, moreover, the core-glycosylated species of the transporter, characterized by lower M r than the fully glycosylated one can be detected by Western blot. Inhibition of SLC6A14 exit from ER results in accumulation of coreglycosylated transporter and directs the protein to ER-associated protein degradation (ERAD) (Kovalchuk et al, 2019). The further glycosylation steps take place in Golgi apparatus and lead to fully glycosylated protein (Moremen et al, 2012) which from trans-Golgi is trafficked in the vesicles to the plasma membrane.…”

Section: Regulation Of Slc6a14mentioning

confidence: 89%

“…The first steps of glycosylation, so called core-glycosylation, take place in the ER lumen: The initial N-glycan: Glc 3 Man 9 GlcNAc 2 (Glc -glucose, Man -mannose, GlcNAc -N-acetylglucosamine) is transferred to a nascent polypeptide from dolichol phosphate linked precursor and, after trimming two glucose residues (Moremen et al, 2012) undergoes a quality check, by two lectin chaperons acting in the ER lumen: soluble calretinin and membrane bound calnexin (Lederkremer, 2009;Chevet et al, 2010). As shown by Kovalchuk et al (2019), SLC6A14 co-localizes with calnexin, moreover, the core-glycosylated species of the transporter, characterized by lower M r than the fully glycosylated one can be detected by Western blot. Inhibition of SLC6A14 exit from ER results in accumulation of coreglycosylated transporter and directs the protein to ER-associated protein degradation (ERAD) (Kovalchuk et al, 2019).…”

Section: Regulation Of Slc6a14mentioning

confidence: 99%

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Amino Acid Transporter SLC6A14 (ATB0,+) – A Target in Combined Anti-cancer Therapy

Nałęcz

2020

Front. Cell Dev. Biol.

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Cancer cells are characterized by quick growth and proliferation, demanding constant supply of various nutrients. Several plasma membrane transporters delivering such compounds are upregulated in cancer. Solute carrier family 6 member 14 (SLC6A14), known as amino acid transporter B 0,+ (ATB 0,+) transports all amino acids with exception of the acidic ones: aspartate and glutamate. Its malfunctioning is correlated with several pathological states and it is upregulated in solid tumors. The high expression of SLC6A14 is prognostic and unfavorable in pancreatic cancer, while in breast cancer it is expressed in estrogen receptor positive cells. As many plasma membrane transporters it resides in endoplasmic reticulum (ER) membrane after translation before further trafficking through Golgi to the cell surface. Transporter exit from ER is strictly controlled. The proper folding of SLC6A14 was shown to be controlled from the cytoplasmic side by heat shock proteins, further exit from ER and formation of coatomer II (COPII) coated vesicles depends on specific interaction with COPII cargo-recognizing subunit SEC24C, phosphorylated by kinase AKT. Inhibition of heat shock proteins, known to be upregulated in cancer, directs SLC6A14 to degradation. Targeting proteins regulating SLC6A14 trafficking is proposed as an additional pharmacological treatment of cancer.

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Section: Slc6a14 -A Transporter With Broad Substrate Specificitymentioning

confidence: 75%

Section: Regulation Of Slc6a14mentioning

confidence: 89%

Section: Regulation Of Slc6a14mentioning

confidence: 99%

See 1 more Smart Citation

Amino Acid Transporter SLC6A14 (ATB0,+) – A Target in Combined Anti-cancer Therapy

Nałęcz

2020

Front. Cell Dev. Biol.

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“…In the endoplasmic reticulum, the quality control of SLC6A14 folding involves interactions with the heat shock proteins HSP70 and HSP90 [20]. SLC6A14 trafficking from the endoplasmic reticulum to the Golgi apparatus depends on its interaction with the cargo-recognizing protein SEC24 isoform C and the coatomer II (COPII) complex [21]. Further studies are needed to fully understand the mechanisms allowing SLC6A14 trafficking to the plasma membrane.…”

Section: Slc6a14 Expression and Regulation In The Lung And Gastrointementioning

confidence: 99%

Update on SLC6A14 in lung and gastrointestinal physiology and physiopathology: focus on cystic fibrosis

Ruffin

Mercier

Calmel

et al. 2020

Cell. Mol. Life Sci.

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The solute carrier family 6 member 14 (SLC6A14) protein imports and concentrates all neutral amino acids as well as the two cationic acids lysine and arginine into the cytoplasm of different cell types. Primarily described as involved in several cancer and colonic diseases physiopathological mechanisms, the SLC6A14 gene has been more recently identified as a genetic modifier of cystic fibrosis (CF) disease severity. It was indeed shown to have a pleiotropic effect, modulating meconium ileus occurrence, lung disease severity, and precocity of P. aeruginosa airway infection. The biological mechanisms explaining the impact of SLC6A14 on intestinal and lung phenotypes of CF patients are starting to be elucidated. This review focuses on SLC6A14 in lung and gastrointestinal physiology and physiopathology, especially its involvement in the pathophysiology of CF disease.

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“…In the latter, one possible explanation may be the involvement of Wfs1 in ER stress (Yamada et al 2006;Fonseca et al 2010;Cagalinec et al 2016), associated with the unfolded protein response where Wfs1 may influence protein synthesis and folding of the plasmalemmal NCX1. Supporting this concept, trafficking of the amino acid transporter B 0,+ (SLC6A14) to the plasma membrane involves an exclusive interaction with SEC24C for its exit from the ER (Kovalchuk et al 2019), where the Wfs1 also may be a part of this pathway. More focused to the cardiac myocytes and ion transporters, group of Wang et al (2018) has demonstrated recently, that protein MOG1 is involved in the regulation of the ER exit of cardiac sodium channel Na v 1.5 in neonatal rat cardiomyocytes.…”

mentioning

confidence: 99%

Lack of functional wolframin causes drop in plasmalemmal sodium-calcium exchanger type 1 expression at early stage in rat model of Wolfram syndrome

Kureková

Plaas²,

Cagalinec³

2020

gpb

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In previously introduced rat model of Wolfram syndrome, we have shown that in cardiac myocytes lacking functional wolframin protein the calcium transients and contractile response are significantly changed. Therefore, in this model, we evaluated protein and mRNA expression levels of following proteins involved in cardiac myocytes calcium homeostasis: the ryanodine receptor type 2, calsequestrin type 2, the junctophilin type 2 and plasmalemmal sodium-calcium exchanger type 1 (NCX1). For NCX1 we detected a significant decrease in expression both on protein and mRNA level. Thus, beyond its impact on endoplasmic reticulum stress, calcium, and mitochondria, wolframin influences processes in the myocyte plasma membrane.

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Trafficking of the amino acid transporter B0,+ (SLC6A14) to the plasma membrane involves an exclusive interaction with SEC24C for its exit from the endoplasmic reticulum

Cited by 16 publications

References 55 publications

Amino Acid Transporter SLC6A14 (ATB0,+) – A Target in Combined Anti-cancer Therapy

Amino Acid Transporter SLC6A14 (ATB0,+) – A Target in Combined Anti-cancer Therapy

Update on SLC6A14 in lung and gastrointestinal physiology and physiopathology: focus on cystic fibrosis

Lack of functional wolframin causes drop in plasmalemmal sodium-calcium exchanger type 1 expression at early stage in rat model of Wolfram syndrome

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