The amount secreted may not only be derived from valves being cal

The amount secreted may not only be derived from valves being calcified, but also from arteries being calcified. Correlation between MVC and arterial calcification has been previously reported 30, 31 and 32. Data suggest that the inflammatory state may induce overexpression of OPG as has been previously demonstrated in experimental

studies (33) and that valvular endothelial cells unleash the pathway for osteogenic differentiation and calcification of the same. This is supported by the observation that a correlation is found between ΔOPG and Δhs-CRP (r = 0.25, p <0.009). In the multivariate logistic regression, only PTH and ΔPTH remained as independent risk factors, probably due to the strong correlation between variables, as was the case

with ΔiPTH with check details Δserum albumin, (inverse) Δalbumin and Δhs-PCR and Δhs-PCR with Δserum phosphorus. Calcification of the aortic valve is associated with cyclic mechanical stress derived from hemodynamic overwork as well as biochemical alterations. Regarding development of AVC, patients in this group had only small but significantly higher values of serum cholesterol than non-VC group as in another study of non-renal patients (34) and showed significant increments from baseline to final evaluation in BMI, SBP, DBP, sCr, cCa, triglycerides and hs-CRP and decreases were observed in fetuin. In spite of these differences, only PTH was an independent risk factor for AVC, similar to another study for

AVC (10). Patients with rapid progression (>30 mm2) during 1 year of VC were older, had Caspase phosphorylation DM and had high levels of OPG and low levels of albumin and GFR, as reported in others studies 19, 35 and 36. It is interesting to note that elevated concentrations of OPG persist in Tolmetin our patients with VC. Our study has some limitations. It has a small sample derived from stringent selection criteria, as the decision was to include only patients free of detectable valve calcification. However, it should be noted that restrictions allowed us to clarify the beginning of the calcification process. Another limitation refers to the relatively short follow-up time. We should mention that other studies report periods of 16 months, very similar to this study (13). In summary, heart valve calcification is a frequent and rapid phenomenon that seems to affect mitral and aortic valves in different ways and to different magnitudes. Age, diabetes, osteoprotegerin, parathormone and C-reactive protein are risk factors for mitral calcification and iPTH for aortic valve in incident dialysis patients. The results offer a new perspective on knowledge about the pathophysiology of VC in patients on dialysis that may orient towards new prevention and treatment strategies for the cardiovascular complications of chronic kidney disease. The authors want to thank to Monica Ericsson for OPG measurement, Ma.

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