Affiliation:
1. Kabardino-Balkar state University named after Kh. M. Berbekov
2. Republican clinical hospital after Sh. Sh. Ependiev
3. North Caucasus Nephrologycenter LLC
Abstract
BACKGROUND. The increasing prevalence of chronic kidney disease is a global trend as well in general as in terminal kidney failure in particular. Of great interest is the analysis of the impact of mineral and bone disorders on the risk of cardiovascular complications and, first of all, acute myocardial infarction (AMI ). THE AIM: to assess the impact of bone mineral disorders on the risk of AMI in patients with stage 5D chronic kidney disease. PATIENTS AND METHODS. It was conducted a prospective (three-year) cohort study of 85 patients with CKD S5D treated with programmed hemodialysis. At the first stage, it were registered the risk factors and clinical manifestations of CKD 5 St, as well as indicators that characterized bone mineral disorders (levels of blood inorganic phosphate, calcium, parathyroid hormone, 1,25(OH)D, fibroblast growth factor (FGF-23), a-Klotho). Signs of calcification of the heart valves and aortic wall were also determined. The second stage involved a re-examination of patients after 3.1±0.1 years, as well as registration of endpoints, which were identified as cases of fatal and non-fatal AMI. RESULTS. After 3 years of follow-up, the following endpoints were registered: nonfatal AMI - 6 cases, fatal AMI-4 cases. The risk of AMI increased in the presence of initial persistent hyperphosphatemia and 1,25(OH)D3 deficiency, as well as calcification of heart valves and high FGF-23 values, but only in combination with hyperphosphatemia and 1,25(OH)D3 deficiency. Hyperparathyroidism also increased the risk of AMI in conditions of a deficit of 1,25(OH)D3. The risk of nonfatal AMI cases was also increased by the presence of aortic calcification and its severity. The risk of AMI increases in the presence of initial persistent hyperphosphatemia and a deficit of 1.25 (OH)D3, as well as CCS, high FGF-23 values, but only in combination with hyperphosphatemia and a deficit of 1.25(OH)D3. Hyperparathyroidism also increases the risk of AMI in conditions of a deficit of 1.25(OH)D3. The risk of nonfatal cases of AMI also increases the presence of aortic calcification and its severity. CONCLUSION. The risk of AMI increases in the presence of initial persistent hyperphosphatemia and a deficit of 1,25(OH)D3, as well as calcification of the heart valves, high FGF-23 values, but only in combination with hyperphosphatemia and a deficit of 1,25(OH) D3. Hyperparathyroidism also increases the risk of AMI in conditions of a deficit of 1.25(OH)D3. The risk of nonfatal cases of AMI also increases the presence of aortic calcification.
Publisher
Non-profit organization Nephrology
Reference13 articles.
1. Borisov W, Shilov EM. Acute renal failure. Urology 2017;1:11 - 18(ln Russ.), doi: 10.18565/urol.2017.1-supplement.4-10
2. Tomilina NA, AndrusevAM, Peregudova NG, ShinkarevMB. Replacement therapy for terminal chronic kidney failure in the Russian Federation in 2010-2015. Nephrology and Dialysis 2017;19(4):5-111 (In Russ.), doi: 10.28996/1680-4422-2017- 4suppl-1-95
3. Zemchenkov AU. Using the point scales suggested in the European renal best practice clinical guidelines to assess the prognosis in elderly and debilitated patients in the late stages of CKD. Nephrology and Dialysis 2017;19(1):221-225 (In Russ.), doi: 10.28996/1680-4422-2017-1-221-225
4. Vanholder R, Van LaeckeS, GlorieuxG. Deleting Death and Dialysis: Conservative Care of Cardio-Vascular Risk and Kidney Function Loss in Chronic Kidney Disease (CKD). Toxins (Basel) 2018;10(6):237
5. Strokov AG, Gurevich KY) llin IP et al. Treatment of patients with stage 5 chronic kidney disease (CKD 5) by hemodialysis and hemodiafiltration. Clinical recommendations. Nephrology(Saint- Petersnurg) 2017;21(3):92-110 (In Russ.), doi: 10.24884/15616274-2017-3-92-111