Accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages

BACKGROUND: Disease severity of autosomal dominant polycystic kidney disease (ADPKD) is influenced by diet. Dietary protein, a recognized cyst-accelerating factor, is catabolized into amino acids (AA) and delivered to the kidney leading to renal hypertrophy. Injury-induced hypertrophic signaling in...

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Autores principales: Sedaka, Randee, Huang, Jifeng, Yamaguchi, Shinobu, Lovelady, Caleb, Hsu, Jung-Shan, Shinde, Sejal, Kasztan, Malgorzata, Crossman, David K., Saigusa, Takamitsu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Medicine
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10394241/
https://www.ncbi.nlm.nih.gov/pubmed/37538309
http://dx.doi.org/10.3389/fmed.2023.1173674
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author Sedaka, Randee
Huang, Jifeng
Yamaguchi, Shinobu
Lovelady, Caleb
Hsu, Jung-Shan
Shinde, Sejal
Kasztan, Malgorzata
Crossman, David K.
Saigusa, Takamitsu
author_facet Sedaka, Randee
Huang, Jifeng
Yamaguchi, Shinobu
Lovelady, Caleb
Hsu, Jung-Shan
Shinde, Sejal
Kasztan, Malgorzata
Crossman, David K.
Saigusa, Takamitsu
author_sort Sedaka, Randee
collection PubMed
description BACKGROUND: Disease severity of autosomal dominant polycystic kidney disease (ADPKD) is influenced by diet. Dietary protein, a recognized cyst-accelerating factor, is catabolized into amino acids (AA) and delivered to the kidney leading to renal hypertrophy. Injury-induced hypertrophic signaling in ADPKD results in increased macrophage (MФ) activation and inflammation followed by cyst growth. We hypothesize that the cystogenesis-prompting effects of HP diet are caused by increased delivery of specific AA to the kidney, ultimately stimulating MФs to promote cyst progression. METHODS: Pkd1(flox/flox) mice with and without Cre (CAGG-ER) were given tamoxifen to induce global gene deletion (Pkd1KO). Pkd1KO mice were fed either a low (LP; 6%), normal (NP; 18%), or high (HP; 60%) protein diet for 1 week (early) or 6 weeks (chronic). Mice were then euthanized and tissues were used for histology, immunofluorescence and various biochemical assays. One week fed kidney tissue was cell sorted to isolate tubular epithelial cells for RNA sequencing. RESULTS: Chronic dietary protein load in Pkd1KO mice increased kidney weight, number of kidney infiltrating and resident MФs, chemokines, cytokines and cystic index compared to LP diet fed mice. Accelerated cyst growth induced by chronic HP were attenuated by liposomal clodronate-mediated MФ depletion. Early HP diet fed Pkd1KO mice had larger cystic kidneys compared to NP or LP fed counterparts, but without increases in the number of kidney MФs, cytokines, or markers of tubular injury. RNA sequencing of tubular epithelial cells in HP compared to NP or LP diet group revealed increased expression of sodium-glutamine transporter Snat3, chloride channel Clcnka, and gluconeogenesis marker Pepck1, accompanied by increased excretion of urinary ammonia, a byproduct of glutamine. Early glutamine supplementation in Pkd1KO mice lead to kidney hypertrophy. CONCLUSION: Chronic dietary protein load-induced renal hypertrophy and accelerated cyst growth in Pkd1KO mice is dependent on both infiltrating and resident MФ recruitment and subsequent inflammatory response. Early cyst expansion by HP diet, however, is relient on increased delivery of glutamine to kidney epithelial cells, driving downstream metabolic changes prior to inflammatory provocation.
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spelling pubmed-103942412023-08-03 Accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages Sedaka, Randee Huang, Jifeng Yamaguchi, Shinobu Lovelady, Caleb Hsu, Jung-Shan Shinde, Sejal Kasztan, Malgorzata Crossman, David K. Saigusa, Takamitsu Front Med (Lausanne) Medicine BACKGROUND: Disease severity of autosomal dominant polycystic kidney disease (ADPKD) is influenced by diet. Dietary protein, a recognized cyst-accelerating factor, is catabolized into amino acids (AA) and delivered to the kidney leading to renal hypertrophy. Injury-induced hypertrophic signaling in ADPKD results in increased macrophage (MФ) activation and inflammation followed by cyst growth. We hypothesize that the cystogenesis-prompting effects of HP diet are caused by increased delivery of specific AA to the kidney, ultimately stimulating MФs to promote cyst progression. METHODS: Pkd1(flox/flox) mice with and without Cre (CAGG-ER) were given tamoxifen to induce global gene deletion (Pkd1KO). Pkd1KO mice were fed either a low (LP; 6%), normal (NP; 18%), or high (HP; 60%) protein diet for 1 week (early) or 6 weeks (chronic). Mice were then euthanized and tissues were used for histology, immunofluorescence and various biochemical assays. One week fed kidney tissue was cell sorted to isolate tubular epithelial cells for RNA sequencing. RESULTS: Chronic dietary protein load in Pkd1KO mice increased kidney weight, number of kidney infiltrating and resident MФs, chemokines, cytokines and cystic index compared to LP diet fed mice. Accelerated cyst growth induced by chronic HP were attenuated by liposomal clodronate-mediated MФ depletion. Early HP diet fed Pkd1KO mice had larger cystic kidneys compared to NP or LP fed counterparts, but without increases in the number of kidney MФs, cytokines, or markers of tubular injury. RNA sequencing of tubular epithelial cells in HP compared to NP or LP diet group revealed increased expression of sodium-glutamine transporter Snat3, chloride channel Clcnka, and gluconeogenesis marker Pepck1, accompanied by increased excretion of urinary ammonia, a byproduct of glutamine. Early glutamine supplementation in Pkd1KO mice lead to kidney hypertrophy. CONCLUSION: Chronic dietary protein load-induced renal hypertrophy and accelerated cyst growth in Pkd1KO mice is dependent on both infiltrating and resident MФ recruitment and subsequent inflammatory response. Early cyst expansion by HP diet, however, is relient on increased delivery of glutamine to kidney epithelial cells, driving downstream metabolic changes prior to inflammatory provocation. Frontiers Media S.A. 2023-07-19 /pmc/articles/PMC10394241/ /pubmed/37538309 http://dx.doi.org/10.3389/fmed.2023.1173674 Text en Copyright © 2023 Sedaka, Huang, Yamaguchi, Lovelady, Hsu, Shinde, Kasztan, Crossman and Saigusa. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Medicine
Sedaka, Randee
Huang, Jifeng
Yamaguchi, Shinobu
Lovelady, Caleb
Hsu, Jung-Shan
Shinde, Sejal
Kasztan, Malgorzata
Crossman, David K.
Saigusa, Takamitsu
Accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages
title Accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages
title_full Accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages
title_fullStr Accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages
title_full_unstemmed Accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages
title_short Accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages
title_sort accelerated cystogenesis by dietary protein load is dependent on, but not initiated by kidney macrophages
topic Medicine
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10394241/
https://www.ncbi.nlm.nih.gov/pubmed/37538309
http://dx.doi.org/10.3389/fmed.2023.1173674
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