Homocysteine in chronic kidney disease: Clinical diagnostic aspects-Reference-Cited by-同舟云学术

Homocysteine in chronic kidney disease: Clinical diagnostic aspects

Published:2023-03-30 Issue:4 Volume: Page:23-29
ISSN:2078-5631
Container-title:Medical alphabet
language:
Short-container-title:Medicinskij alfavit

Author:

Murkamilov I. T.¹^ORCID,Aitbaev K. A.²^ORCID,Fomin V. V.³^ORCID,Murkamilova Zh. A.⁴^ORCID,Kudaibergenova I. O.⁵^ORCID,Yusupov F. A.⁶^ORCID,Aidarov Z. А.⁵^ORCID

Affiliation:

1. Kyrgyz State Medical Academy n. a. I. K. Akhunbaev; Kyrgyz-Russian Slavic University

2. Scientific Research Institute of Molecular Biology and Medicine

3. First Moscow State Medical University n. a. I. M. Sechenov

4. Kyrgyz-Russian Slavic University

5. Kyrgyz State Medical Academy n. a. I. K. Akhunbaev

6. Osh State University

Abstract

Chronic kidney disease (CKD) is one of the most common pathologies worldwide. With CKD, cardiovascular risk increases and mortality rises. The article presents the role of homocysteine as a laboratory marker of renal failure and the development of cardiovascular disease. Homocysteine is a thiol-containing amino acid, which is an intermediate product of methionine metabolism, which is metabolized in two ways: due to the transfer of the sulfate group, which occurs in the presence of vitamin B 6, or remethylation, which occurs in the presence of vitamin B 12 and folic acid. Normally, in an adult, the concentration of total homocysteine in blood plasma does not exceed 15 μmol/L. It has been shown that with CKD, hyperhomocysteinemia is observed at the initial stages and its frequency increases at the pre- and dialysis stages of the disease. Hyperhomocysteinemia provokes endothelial dysfunction, accelerates systemic atherosclerosis, increases the risk of atherothrombotic complications. Evaluation of plasma homocysteine levels may be useful in stratifying nephrocardio- and cerebrovascular risk in CKD.

Publisher

Alfmed LLC

Subject

Materials Chemistry,Economics and Econometrics,Media Technology,Forestry

Reference46 articles.

1. Centers for Disease Control and Prevention. Chronic Kidney Disease in the United States, 2019. Atlanta, GA: US Department of Health and Human Services, Centers for Disease Control and Prevention; 2019.

2. Moiseev VC, Mukhin NA. Cardiovascular risk and chronic kidney disease: cardio- and nephroprotection strategies. Clinical Nephrology. 2014; 2: 4–29 (In Russ).

3. Kamyshnikova LA, Yefremova OA, Pivovar RS. Features of cardiorenal relationships at patients with the chronic disease of kidney. The current state of the problem. Scientific Statements. Series Medicine. Pharmacy. 2017; 5(254): 13–21. (In Russ).

4. Skvortsov YuI, Korolkova AS. Homocysteine as a risk factor of ischemic heart disease development (review). Saratov Journal of Medical Scientific Research. 2011; 7: 3: 619–624. (In Russ).

5. Protopopov AA, Nesterenko OV, Borodulin VB, Shevchenko OV. Hyperhpmocysteinemia as a predictor of chronic pyelonephritis progression. Clinical Nephrology. 2013; 6: 33–36. (In Russ).