Analysis of LPI-causing mutations on y+LAT1 function and localization.

Bianca Maria RotoliAmelia BarilliFilippo IngogliaRossana VisigalliMassimiliano G BianchiFrancesca FerrariDiego MartinelliCarlo Dionisi-ViciValeria Dall'Asta

Published in: Orphanet journal of rare diseases (2019)

The three mutations studied of y+LAT1 transporter result in a defective arginine transport both in ex vivo (monocytes) and in vitro (CHO transfected cells) models, likely caused by the retention of the mutated proteins in the cytosol. The different effect of y+LAT1 mutation on arginine transport in monocytes and lymphoblasts is supposed to be due to the different expression of SLC7A7 mRNA in the two models, supporting the hypothesis that the impact of LPI defect largely depends on the relative abundance of LPI target gene in each cell type.

Keyphrases

nitric oxide
induced apoptosis
poor prognosis
dendritic cells
peripheral blood
binding protein
cell cycle arrest
genome wide
copy number
amino acid
endoplasmic reticulum stress
oxidative stress
gene expression
dna methylation
cell proliferation
long non coding rna
genome wide analysis
wild type