2012
DOI: 10.1681/asn.2012010048
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Targeted Deletion of Klotho in Kidney Distal Tubule Disrupts Mineral Metabolism

Abstract: Renal Klotho controls mineral metabolism by directly modulating tubular reabsorption of phosphate and calcium and by acting as a co-receptor for the phosphaturic and vitamin D-regulating hormone fibroblast growth factor-23 (FGF23). Klotho null mice have a markedly abnormal phenotype. We sought to determine effects of renal-specific and partial deletion of Klotho to facilitate investigation of its roles in health and disease. We generated a mouse model with partial deletion of Klotho in distal tubular segments … Show more

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Cited by 135 publications
(120 citation statements)
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“…18,19 Prior studies in mice show that klotho haplo insufficiency (approximately 50% reduction in klotho) is accompanied by an approximately threefold higher FGF23 concentration, suggesting that FGF23 may be increased in a compensatory fashion to induce its biologic effects when klotho is decreased. 14,15 In this context, our findings could suggest that concurrent high FGF23 and low FePi may be serving as a noninvasive marker of low kidney klotho expression or activity. Future studies with kidney pathology specimens suitable for klotho assays are required to confirm this hypothesis.…”
Section: Discussionmentioning
confidence: 84%
See 1 more Smart Citation
“…18,19 Prior studies in mice show that klotho haplo insufficiency (approximately 50% reduction in klotho) is accompanied by an approximately threefold higher FGF23 concentration, suggesting that FGF23 may be increased in a compensatory fashion to induce its biologic effects when klotho is decreased. 14,15 In this context, our findings could suggest that concurrent high FGF23 and low FePi may be serving as a noninvasive marker of low kidney klotho expression or activity. Future studies with kidney pathology specimens suitable for klotho assays are required to confirm this hypothesis.…”
Section: Discussionmentioning
confidence: 84%
“…In individuals with relative renal tubule resistance to FGF23, serum FGF23 concentrations may be secondarily increased in a feedback loop in an attempt to further increase phosphorus excretion. 14,15 To our knowledge, no prior study has examined the joint relationships of FGF23 concentrations and urine FePi with adverse outcomes. To that end, we evaluated the strength of the associations of serum FGF23 concentrations with mortality and CVD events and determined the extent to which these associations were modified by the degree of renal phosphorus excretion.…”
mentioning
confidence: 99%
“…34 FGF-23 and the associated co-receptor Klotho impinge on the same system. Indeed, Klotho knockout mice 35,36 (i.e., animal models characterized by high plasma levels of FGF-23 37 ) do not express NO synthase in the vascular system and exhibit almost abolished response to acetylcholine, the strongest stimulant of NO activity. 36 Our findings show that ADMA has a variable influence on renal outcomes across the spectrum of FGF-23 values because it is associated with a higher risk for CKD progression only when FGF-23 levels are in the low-normal range (i.e., when the expression of NO synthase is not suppressed by FGF-23-Klotho).…”
Section: Discussionmentioning
confidence: 99%
“…This knockout mouse displays increased protein expression of Npt2a in the proximal tubule as a result of the Klotho deletion, and yet decreased levels of the Npt2a transcript, perhaps in response to the accompanying hyperphosphatemia 56 . Glucocorticoids, known downregulators of sodium-phosphate cotransport in the proximal tubule, have been shown to reduce both Npt2a protein and mRNA expression.…”
Section: Part 4: Effect Of Pth On Npt2a Promoter Activitymentioning
confidence: 98%
“…Conversely, mice with FGF23 gene ablation display increased serum phosphate, increased apical expression of Npt2a, and an accompanying increase in the renal phosphate transport maximum 53 . Distal-tubule-specific deletion of Klotho also produces a phenotype of hyperphosphatemia with abundant Npt2a BBM expression 56 .…”
Section: Regulation Of Serum Phosphorusmentioning
confidence: 99%