Defective<i>Slc7a7</i>transport reduces erythropoietin compromising erythropoiesis and iron homeostasis

Sotillo, Fernando; Giroud-Gerbetant, Judith; Couso, Jorge; Artuch, Rafael; Zorzano, António; Ormazábal, Aída; Sánchez, Mayka; Weiss, Günter; Bodoy, Susanna; Palacı́n, Manuel

doi:10.1101/2021.08.15.456393

2021

DOI: 10.1101/2021.08.15.456393

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DefectiveSlc7a7transport reduces erythropoietin compromising erythropoiesis and iron homeostasis

Fernando Sotillo

Judith Giroud-Gerbetant

Jorge Couso

et al.

Abstract: Slc7a7 encodes for y+LAT1, a transporter of cationic amino acid across the basolateral membrane of epithelial cells. Mutations in SLC7A7 gene give rise to Lysinuric Protein Intolerance (LPI), a rare autosomal recessive disease with wide variability of complications. Intriguingly, y+LAT1 is also involved in arginine transport in non polarized cells such as macrophages. Here we report that complete inducible Slc7a7 ablation in mouse compromises systemic arginine availability that alters proper erythropoiesis and… Show more

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Delayed skeletal development and IGF-1 deficiency in a mouse model of lysinuric protein intolerance

Stroup,

Li,

et al. 2023

Disease Models &Amp; Mechanisms

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SLC7A7 deficiency, or lysinuric protein intolerance (LPI), causes loss of function of the y+LAT1 transporter critical for efflux of arginine, lysine and ornithine in certain cells. LPI is characterized by urea cycle dysfunction, renal disease, immune dysregulation, growth failure, delayed bone age, and osteoporosis. We previously reported that Slc7a7 knockout mice (C57BL/6 x 129/SvEv F2) recapitulate LPI phenotypes, including growth failure. Our main objective was to characterize the skeletal phenotype in these mice. Compared to wild type littermates, juvenile Slc7a7 knockout mice demonstrated 70% lower body weights, 87% lower plasma IGF-1 concentrations, and delayed skeletal development. Because poor survival prevents evaluation of mature knockout mice, we generated a conditional Slc7a7 deletion in mature osteoblasts or mesenchymal cells of the osteo-chondroprogenitor lineage, butno differences in bone architecture were observed. Overall, global Slc7a7 deficiency caused growth failure with low plasma IGF-1 concentrations and delayed skeletal development, but Slc7a7 deficiency in the osteoblastic lineage was not a major contributor to these phenotypes. Future studies utilizing additional tissue-specific Slc7a7 knockout models may help dissect cell autonomous and non-cell autonomous mechanisms underlying phenotypes in LPI.

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Delayed skeletal development and IGF-1 deficiency in a mouse model of lysinuric protein intolerance

Stroup,

Li,

et al. 2023

Disease Models &Amp; Mechanisms

View full text Add to dashboard Cite

show abstract

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DefectiveSlc7a7transport reduces erythropoietin compromising erythropoiesis and iron homeostasis

Cited by 1 publication

References 156 publications

Delayed skeletal development and IGF-1 deficiency in a mouse model of lysinuric protein intolerance

Delayed skeletal development and IGF-1 deficiency in a mouse model of lysinuric protein intolerance

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