Effect of cross-linked chitosan iron (III) on vascular calcification in uremic rats

Author:

de Castro Barbara Bruna Abreu12,do Carmo Wander Barros12,de Albuquerque Suassuna Paulo Giovani12,Carminatti Moises2,Brito Julia Bianchi12,Dominguez Wagner Vasques3,de Oliveira Ivone Braga3,Jorgetti Vanda3,Custodio Melani Ribeiro3,Sanders-Pinheiro Helady12ORCID

Affiliation:

1. Laboratory of Experimental Nephrology (LABNEX) and Interdisciplinary Nucleus of Laboratory Animal Studies (NIDEAL), Reproductive Biology Center (CBR), Federal University of Juiz de Fora (UFJF), Juiz de Fora 36036900, Brazil

2. Interdisciplinary Nucleus for Studies and Research in Nephrology (NIEPEN), Federal University of Juiz de Fora (UFJF), Juiz de Fora 36036330, Brazil

3. Laboratory of Renal Physiopathology, University of São Paulo Medical School, University of São Paulo, São Paulo 01246903, Brazil

Abstract

Cross-linked chitosan iron (III) is a chitin-derived polymer with a chelating effect on phosphorus, but it is untested in vascular calcification. We evaluated this compound's ability to reduce hyperphosphatemia and its effect on vascular calcification in uremic rats using an adenine-based, phosphorus-rich diet for seven weeks. We used a control group to characterize the uremia. Uremic rats were divided according the treatment into chronic kidney disease, CKD-Ch-Fe(III)CL (CKD-Ch), CKD-calcium carbonate, or CKD-sevelamer groups. We measured creatinine, phosphorus, calcium, alkaline phosphatase, phosphorus excretion fraction, parathyroid hormone, and fibroblast growth factor 23. Vascular calcification was assessed using the aortic calcium content, and a semi-quantitative analysis was performed using Von Kossa and hematoxylin–eosin staining. At week seven, rats in the chronic kidney disease group had higher creatinine, phosphorus, phosphorus excretion fraction, calcium, alkaline phosphatase, fibroblast growth factor 23, and aortic calcium content than those in the Control group. Treatments with cross-linked chitosan iron (III) and calcium carbonate prevented phosphorus increase (20%–30% reduction). The aortic calcium content was lowered by 88% and 85% in the CKD-Ch and CKD-sevelamer groups, respectively. The prevalence of vascular changes was higher in the chronic kidney disease and CKD-calcium carbonate (62.5%) groups than in the CKD-Ch group (37.5%). In conclusion, cross-linked chitosan iron (III) had a phosphorus chelating effect similar to calcium carbonate already available for clinical use, and prevented calcium accumulation in the aorta. Impact statement Vascular calcification (VC) is a common complication due to CKD-related bone and mineral disorder (BMD) and is characterized by deposition of calcium in vessels. Effective therapies are not yet available but new phosphorus chelators can prevent complications from CV. We tested the effect of chitosan, a new phosphorus chelator, on the VC of uremic animals. It has recently been proposed that chitosan treatment may be effective in the treatment of hyperphosphataemia. However, its action on vascular calcification has not been investigated yet. In this study, we demonstrated that chitosan reduced the calcium content in the aorta, suggesting that this may be a therapeutic approach in the treatment of hyperphosphatemia by preventing CV.

Publisher

SAGE Publications

Subject

General Biochemistry, Genetics and Molecular Biology

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