Klotho and Calciprotein Particles As Therapeutic Targets Against Accelerated Ageing

Overview

Journal Clin Sci (Lond)

Specialties Biochemistry
General Medicine
Science

Date 2021 Aug 10

PMID 34374422

Citations 28

Authors

Makoto Kuro-O

Affiliations

Soon will be listed here.

Abstract

The klotho gene, named after a Greek goddess who spins the thread of life, was identified as a putative 'ageing-suppressor' gene. Klotho-deficient mice exhibit complex ageing-like phenotypes including hypogonadism, arteriosclerosis (vascular calcification), cardiac hypertrophy, osteopenia, sarcopenia, frailty, and premature death. Klotho protein functions as the obligate co-receptor for fibroblast growth factor-23 (FGF23), a bone-derived hormone that promotes urinary phosphate excretion in response to phosphate intake. Thus, Klotho-deficient mice suffer not only from accelerated ageing but also from phosphate retention due to impaired phosphate excretion. Importantly, restoration of the phosphate balance by placing Klotho-deficient mice on low phosphate diet rescued them from premature ageing, leading us to the notion that phosphate accelerates ageing. Because the extracellular fluid is super-saturated in terms of phosphate and calcium ions, an increase in the phosphate concentration can trigger precipitation of calcium-phosphate. In the blood, calcium-phosphate precipitated upon increase in the blood phosphate concentration is adsorbed by serum protein fetuin-A to form colloidal nanoparticles called calciprotein particles (CPPs). In the urine, CPPs appear in the renal tubular fluid when FGF23 increases phosphate load excreted per nephron. CPPs can induce cell damage, ectopic calcification, and inflammatory responses. CPPs in the blood can induce arteriosclerosis and non-infectious chronic inflammation, whereas CPPs in the urine can induce renal tubular damage and interstitial inflammation/fibrosis. Thus, we propose that CPPs behave like a pathogen that accelerates ageing and should be regarded as a novel therapeutic target against age-related disorders including chronic kidney disease.

Citing Articles

Proteomic Profiling of Endothelial Cell Secretomes After Exposure to Calciprotein Particles Reveals Downregulation of Basement Membrane Assembly and Increased Release of Soluble CD59.

Stepanov A, Shishkova D, Markova V, Markova Y, Frolov A, Lazebnaya A Int J Mol Sci. 2024; 25(21).

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Phosphorous metabolism and manipulation in chronic kidney disease.

Marando M, Tamburello A, Salera D, Di Lullo L, Bellasi A Nephrology (Carlton). 2024; 29(12):791-800.

PMID: 39433296 PMC: 11579558. DOI: 10.1111/nep.14407.

Oxidative stress and senescence in aging kidneys: the protective role of SIRT1.

Almalki W, Salman Almujri S EXCLI J. 2024; 23:1030-1067.

PMID: 39391060 PMC: 11464868. DOI: 10.17179/excli2024-7519.

Anti-Inflammatory Role of the Klotho Protein and Relevance to Aging.

Prudhomme G, Wang Q Cells. 2024; 13(17.

PMID: 39272986 PMC: 11394293. DOI: 10.3390/cells13171413.

Calciprotein particle counts associate with vascular remodelling in chronic kidney disease.

Feenstra L, Reijrink M, Pasch A, Smith E, Visser L, Bulthuis M Cardiovasc Res. 2024; 120(15):1953-1966.

PMID: 39102822 PMC: 11629976. DOI: 10.1093/cvr/cvae164.

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