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      Klotho has dual protective effects on cisplatin-induced acute kidney injury

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          Abstract

          Klotho protects the kidney from ischemia-reperfusion injury, but its effect on nephrotoxins is unknown. Here we determined if Klotho protects the kidney from cisplatin toxicity. Cisplatin increased plasma creatinine and induced tubular injury, which were exaggerated in Klotho haplosufficient ( Kl/+) and ameliorated in transgenic Klotho overexpressing ( Tg-Kl) mice. Neutrophil gelatinase-associated lipocalin and active caspase-3 protein, and number of apoptotic cells in the kidney were higher in Kl/+ and lower in Tg-Kl compared to wild type mice. Klotho suppressed basolateral uptake of cisplatin by the normal rat kidney cell line (NRK); an effect similar to cimetidine, a known inhibitor of organic cation transport (OCT). A decrease in cell surface and total OCT2 protein and OCT activity by Klotho was mimicked by glucuronidase. The Klotho effect was attenuated by glucuronidase inhibition. On the other hand, OCT2 mRNA was reduced by Klotho, but not β-glucuronidase. Moreover, cimetidine inhibited OCT activity but not OCT2 expression. Unlike cimetidine, Klotho reduced cisplatin-induced apoptosis from either the basolateral or apical side, and even when added after NRK cells were already loaded with cisplatin. Thus, Klotho protects the kidney against cisplatin nephrotoxicity by reduction of basolateral uptake of cisplatin by OCT2, and a direct anti-apoptotic effect independent of cisplatin uptake. Klotho may be a useful agent to prevent and treat cisplatin-induced nephrotoxicity.

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          Klotho deficiency causes vascular calcification in chronic kidney disease.

          Ming Hu, Mingjun Shi, Jianning Zhang (2011)
          Soft-tissue calcification is a prominent feature in both chronic kidney disease (CKD) and experimental Klotho deficiency, but whether Klotho deficiency is responsible for the calcification in CKD is unknown. Here, wild-type mice with CKD had very low renal, plasma, and urinary levels of Klotho. In humans, we observed a graded reduction in urinary Klotho starting at an early stage of CKD and progressing with loss of renal function. Despite induction of CKD, transgenic mice that overexpressed Klotho had preserved levels of Klotho, enhanced phosphaturia, better renal function, and much less calcification compared with wild-type mice with CKD. Conversely, Klotho-haploinsufficient mice with CKD had undetectable levels of Klotho, worse renal function, and severe calcification. The beneficial effect of Klotho on vascular calcification was a result of more than its effect on renal function and phosphatemia, suggesting a direct effect of Klotho on the vasculature. In vitro, Klotho suppressed Na(+)-dependent uptake of phosphate and mineralization induced by high phosphate and preserved differentiation in vascular smooth muscle cells. In summary, Klotho is an early biomarker for CKD, and Klotho deficiency contributes to soft-tissue calcification in CKD. Klotho ameliorates vascular calcification by enhancing phosphaturia, preserving glomerular filtration, and directly inhibiting phosphate uptake by vascular smooth muscle. Replacement of Klotho may have therapeutic potential for CKD.
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            Apoptosis and acute kidney injury.

            Andrea Havasi, Steven Borkan (2011)
            Improved mechanistic understanding of renal cell death in acute kidney injury (AKI) has generated new therapeutic targets. Clearly, the classic lesion of acute tubular necrosis is not adequate to describe the consequences of renal ischemia, nephrotoxin exposure, or sepsis on glomerular filtration rate. Experimental evidence supports a pathogenic role for apoptosis in AKI. Interestingly, proximal tubule epithelial cells are highly susceptible to apoptosis, and injury at this site contributes to organ failure. During apoptosis, well-orchestrated events converge at the mitochondrion, the organelle that integrates life and death signals generated by the BCL2 (B-cell lymphoma 2) protein family. Death requires the 'perfect storm' for outer mitochondrial membrane injury to release its cellular 'executioners'. The complexity of this process affords new targets for effective interventions, both before and after renal insults. Inhibiting apoptosis appears to be critical, because circulating factors released by the injured kidney induce apoptosis and inflammation in distant organs including the heart, lung, liver, and brain, potentially contributing to the high morbidity and mortality associated with AKI. Manipulation of known stress kinases upstream of mitochondrial injury, induction of endogenous, anti-apoptotic proteins, and improved understanding of the timing and consequences of renal cell apoptosis will inevitably improve the outcome of human AKI.
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              Augmented Wnt signaling in a mammalian model of accelerated aging.

              Hongjun Liu, Maria Fergusson, Rogerio M. Castilho (2007)
              The contribution of stem and progenitor cell dysfunction and depletion in normal aging remains incompletely understood. We explored this concept in the Klotho mouse model of accelerated aging. Analysis of various tissues and organs from young Klotho mice revealed a decrease in stem cell number and an increase in progenitor cell senescence. Because klotho is a secreted protein, we postulated that klotho might interact with other soluble mediators of stem cells. We found that klotho bound to various Wnt family members. In a cell culture model, the Wnt-klotho interaction resulted in the suppression of Wnt biological activity. Tissues and organs from klotho-deficient animals showed evidence of increased Wnt signaling, and ectopic expression of klotho antagonized the activity of endogenous and exogenous Wnt. Both in vitro and in vivo, continuous Wnt exposure triggered accelerated cellular senescence. Thus, klotho appears to be a secreted Wnt antagonist and Wnt proteins have an unexpected role in mammalian aging.
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                Author and article information

                Journal
                Journal ID (nlm-journal-id): 0323470
                Journal ID (pubmed-jr-id): 5428
                Journal ID (nlm-ta): Kidney Int
                Journal ID (iso-abbrev): Kidney Int.
                Title: Kidney international
                ISSN (Print): 0085-2538
                ISSN (Electronic): 1523-1755
                Publication date Nihms-submitted: 20 December 2013
                Publication date (Electronic): 04 December 2013
                Publication date (Print): April 2014
                Publication date PMC-release: 01 October 2014
                Volume: 85
                Issue: 4
                Pages: 855-870
                Affiliations
                [1 ]Charles and Jane Pak Center for Mineral Metabolism and Clinical Research, University of Texas Southwestern Medical Center, Dallas, TX, USA
                [2 ]Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USA
                [3 ]Department of Physiology, University of Texas Southwestern Medical Center, Dallas, TX, USA
                Author notes
                [* ]Address correspondence to: Ming Chang Hu, MD, PhD, Charles and Jane Pak Center for Mineral Metabolism and Clinical Research, and Department of Internal Medicine, The University of Texas Southwestern Medical Center, 5323 Harry Hines Blvd., Dallas, TX 75390-8885 USA, Tel: 1-214-648-9797;, ming-chang.hu@ 123456utsouthwestern.edu
                Article
                Manuscript ID: NIHMS537210
                DOI: 10.1038/ki.2013.489
                PMC ID: 3972320
                PubMed ID: 24304882
                SO-VID: 85785c31-c6fc-4b59-b9f3-909f50caf733
                History
                Categories
                Subject: Article

                ScienceOpen disciplines: Nephrology
                Keywords: acute kidney injury,cisplatin,glucuronidase,kidney,klotho,nephrotoxicity,organic cation transporter
                Data availability:
                ScienceOpen disciplines: Nephrology
                Keywords: acute kidney injury, cisplatin, glucuronidase, kidney, klotho, nephrotoxicity, organic cation transporter

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