Integral pharmacological management of bone mineral disorders in chronic kidney disease (part II): from treatment of phosphate imbalance to control of PTH and prevention of progression of cardiovascular calcification

被引:13
作者
Bover, J. [1 ]
Urena-Torres, P. [2 ,3 ]
Lloret, M. J. [1 ]
Ruiz, C. [1 ]
DaSilva, I. [1 ]
Diaz-Encarnacion, M. M. [1 ]
Mercado, C. [1 ]
Mateu, S. [1 ]
Fernandez, E. [4 ]
Ballarin, J. [1 ]
机构
[1] Fundacio Puigvert, Dept Nephrol, IIB St Pau, RedinRen, Barcelona, Spain
[2] Clin Landy, Dept Nephrol, Ramsay Gen Sante, Paris, France
[3] Univ Paris 05, Dept Renal Physiol, Necker Hosp, Paris, France
[4] Hosp Arnau Vilanova, IRB LLeida, RedinRen, Dept Nephrol, Lleida, Spain
关键词
Chronic kidney disease; CKD-MBD; phosphate; secondary hyperparathyroidism; vascular calcification; calcium receptor; vitamin D; paricalcitol; cinacalcet; calcimimetics; etelcalcetide; adynamic bone disease; VITAMIN-D-RECEPTOR; PATIENTS RECEIVING HEMODIALYSIS; CALCIUM-SENSING RECEPTOR; HIGH-DOSE CHOLECALCIFEROL; CINACALCET HCL THERAPY; QUALITY-OF-LIFE; SECONDARY HYPERPARATHYROIDISM; DIALYSIS PATIENTS; PARATHYROID-HORMONE; VASCULAR CALCIFICATION;
D O I
10.1080/14656566.2016.1182985
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Introduction: Chronic kidney disease-mineral and bone disorders (CKD-MBD) are associated with costly complications and dismal hard-outcomes. Areas covered: In two comprehensive articles we review contemporary and future pharmacological options for treatment of phosphate (P) imbalance (part 1) and hyperparathyroidism (this part 2), taking into account CKD-accelerated cardiovascular calcification (CVC) processes. Expert opinion: Improvements in CKD-MBD require an integral approach, addressing all three components of the CKD-MBD triad. Here, initial guidance to control hyperparathyroidism is provided, taking into account the presence/absence of CVC. We include also measures for patients at risk of adynamic bone disease or suffering from calciphylaxis. Many epidemiological studies (relating to vitamin D) and thorough analyses of recent randomized clinical trials (of cinacalcet) point towards benefits of attempting to improve biochemical parameters while trying to, at least, avoid progression of CVC by more rational use of intestinal P-binders and low-dose vitamin D derivatives and/or calcimimetics. This approach does not seem to be far away from significantly improving hard-outcomes, at least in the dialysis population. The availability of new drugs and the performance of randomized clinical trials should ultimately lead to define earlier, clearer, and more cost-effective patient stratification and biochemical targets with consequent significant clinical improvements.
引用
收藏
页码:1363 / 1373
页数:11
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