Urinary phosphate-containing nanoparticle contributes to inflammation and kidney injury in a salt-sensitive hypertension rat model

Qin Wang; Kenichi Ishizawa; Jinping Li; Wataru Fujii; Yoshikazu Nemoto; Osamu Yamazaki; Yoshifuru Tamura; Yutaka Miura; Xuedan Nie; Ryo Abe; Hiroko Segawa; Makoto Kuro-O; Shigeru Shibata

doi:10.1038/s42003-020-01298-1

Urinary phosphate-containing nanoparticle contributes to inflammation and kidney injury in a salt-sensitive hypertension rat model

Qin Wang
, Kenichi Ishizawa
, Jinping Li
, Wataru Fujii
, Yoshikazu Nemoto
, Osamu Yamazaki
, Yoshifuru Tamura
, Yutaka Miura
, Xuedan Nie
, Ryo Abe
, Hiroko Segawa
, Makoto Kuro-O
, Shigeru Shibata

School of Medicine

Teikyo University
Second Affiliated Hospital of Harbin Medical University
Tianjin First Central Hospital
Jichi Medical University
Tokushima University

Research output: Contribution to journal › Article › peer-review

9 Scopus citations

Abstract

Although disturbed phosphate metabolism frequently accompanies chronic kidney disease (CKD), its causal role in CKD progression remains unclear. It is also not fully understood how excess salt induces organ damage. We here show that urinary phosphate-containing nanoparticles promote kidney injury in salt-sensitive hypertension. In Dahl salt-sensitive rats, salt loading resulted in a significant increase in urinary phosphate excretion without altering serum phosphate levels. An intestinal phosphate binder sucroferric oxyhydroxide attenuated renal inflammation and proteinuria in this model, along with the suppression of phosphaturia. Using cultured proximal tubule cells, we confirmed direct pathogenic roles of phosphate-containing nanoparticles in renal tubules. Finally, transcriptome analysis revealed a potential role of complement C1q in renal inflammation associated with altered phosphate metabolism. These data demonstrate that increased phosphate excretion promotes renal inflammation in salt-sensitive hypertension and suggest a role of disturbed phosphate metabolism in the pathophysiology of hypertensive kidney disease and high salt-induced kidney injury.

Original language	English
Article number	575
Journal	Communications Biology
Volume	3
Issue number	1
DOIs	https://doi.org/10.1038/s42003-020-01298-1
State	Published - 1 Dec 2020

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SDG 3 Good Health and Well-being

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Wang, Q., Ishizawa, K., Li, J., Fujii, W., Nemoto, Y., Yamazaki, O., Tamura, Y., Miura, Y., Nie, X., Abe, R., Segawa, H., Kuro-O, M., & Shibata, S. (2020). Urinary phosphate-containing nanoparticle contributes to inflammation and kidney injury in a salt-sensitive hypertension rat model. Communications Biology, 3(1), Article 575. https://doi.org/10.1038/s42003-020-01298-1

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title = "Urinary phosphate-containing nanoparticle contributes to inflammation and kidney injury in a salt-sensitive hypertension rat model",

abstract = "Although disturbed phosphate metabolism frequently accompanies chronic kidney disease (CKD), its causal role in CKD progression remains unclear. It is also not fully understood how excess salt induces organ damage. We here show that urinary phosphate-containing nanoparticles promote kidney injury in salt-sensitive hypertension. In Dahl salt-sensitive rats, salt loading resulted in a significant increase in urinary phosphate excretion without altering serum phosphate levels. An intestinal phosphate binder sucroferric oxyhydroxide attenuated renal inflammation and proteinuria in this model, along with the suppression of phosphaturia. Using cultured proximal tubule cells, we confirmed direct pathogenic roles of phosphate-containing nanoparticles in renal tubules. Finally, transcriptome analysis revealed a potential role of complement C1q in renal inflammation associated with altered phosphate metabolism. These data demonstrate that increased phosphate excretion promotes renal inflammation in salt-sensitive hypertension and suggest a role of disturbed phosphate metabolism in the pathophysiology of hypertensive kidney disease and high salt-induced kidney injury.",

author = "Qin Wang and Kenichi Ishizawa and Jinping Li and Wataru Fujii and Yoshikazu Nemoto and Osamu Yamazaki and Yoshifuru Tamura and Yutaka Miura and Xuedan Nie and Ryo Abe and Hiroko Segawa and Makoto Kuro-O and Shigeru Shibata",

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AU - Wang, Qin

AU - Ishizawa, Kenichi

AU - Li, Jinping

AU - Fujii, Wataru

AU - Nemoto, Yoshikazu

AU - Yamazaki, Osamu

AU - Tamura, Yoshifuru

AU - Miura, Yutaka

AU - Nie, Xuedan

AU - Abe, Ryo

AU - Segawa, Hiroko

AU - Kuro-O, Makoto

AU - Shibata, Shigeru

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Although disturbed phosphate metabolism frequently accompanies chronic kidney disease (CKD), its causal role in CKD progression remains unclear. It is also not fully understood how excess salt induces organ damage. We here show that urinary phosphate-containing nanoparticles promote kidney injury in salt-sensitive hypertension. In Dahl salt-sensitive rats, salt loading resulted in a significant increase in urinary phosphate excretion without altering serum phosphate levels. An intestinal phosphate binder sucroferric oxyhydroxide attenuated renal inflammation and proteinuria in this model, along with the suppression of phosphaturia. Using cultured proximal tubule cells, we confirmed direct pathogenic roles of phosphate-containing nanoparticles in renal tubules. Finally, transcriptome analysis revealed a potential role of complement C1q in renal inflammation associated with altered phosphate metabolism. These data demonstrate that increased phosphate excretion promotes renal inflammation in salt-sensitive hypertension and suggest a role of disturbed phosphate metabolism in the pathophysiology of hypertensive kidney disease and high salt-induced kidney injury.

AB - Although disturbed phosphate metabolism frequently accompanies chronic kidney disease (CKD), its causal role in CKD progression remains unclear. It is also not fully understood how excess salt induces organ damage. We here show that urinary phosphate-containing nanoparticles promote kidney injury in salt-sensitive hypertension. In Dahl salt-sensitive rats, salt loading resulted in a significant increase in urinary phosphate excretion without altering serum phosphate levels. An intestinal phosphate binder sucroferric oxyhydroxide attenuated renal inflammation and proteinuria in this model, along with the suppression of phosphaturia. Using cultured proximal tubule cells, we confirmed direct pathogenic roles of phosphate-containing nanoparticles in renal tubules. Finally, transcriptome analysis revealed a potential role of complement C1q in renal inflammation associated with altered phosphate metabolism. These data demonstrate that increased phosphate excretion promotes renal inflammation in salt-sensitive hypertension and suggest a role of disturbed phosphate metabolism in the pathophysiology of hypertensive kidney disease and high salt-induced kidney injury.

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DO - 10.1038/s42003-020-01298-1

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AN - SCOPUS:85092580802

SN - 2399-3642

VL - 3

JO - Communications Biology

JF - Communications Biology

IS - 1

M1 - 575

ER -

Urinary phosphate-containing nanoparticle contributes to inflammation and kidney injury in a salt-sensitive hypertension rat model

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