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Homocysteine metabolism in renal failure

 

作者: Alessandra Perna,   Diego Ingrosso,   Ersilia Satta,   Cinzia Lombardi,   Filomena Acanfora,   Natale De Santo,  

 

期刊: Current Opinion in Clinical Nutrition and Metabolic Care  (OVID Available online 2004)
卷期: Volume 7, issue 1  

页码: 53-57

 

ISSN:1363-1950

 

年代: 2004

 

出版商: OVID

 

关键词: homocysteine;uraemia;chronic renal failure;cardiovascular disease;uraemic toxicity

 

数据来源: OVID

 

摘要:

Purpose of reviewThis review focuses on recent findings (June 2002-July 2003) on the topic of homocysteine, a sulfur amino acid associated with cardiovascular disease, and its metabolism in renal failure, a condition with a high prevalence of both hyperhomocysteinemia and cardiovascular disease.Recent findingsA large meta-analysis of prospective studies in the general population established that hyperhomocysteinemia is a risk factor for cardiovascular disease. The results of intervention trials, once available, will also have to be tested in a meta-analysis, because of predicted problems with their statistical power. In kidney patients, intervention trials, still in the recruiting stage, target transplant patients, because of their unique characteristics related to folate responsiveness. As for the cause of hyperhomocysteinemia, new findings show that in humans, renal metabolic extraction depends on renal plasma flow in the post-absorptive state. Folate absorption or interconversion seems not to be affected. Riboflavin is a determinant of plasma homocysteine levels in uraemia. The consequences of hyperhomocysteinemia in uraemia are DNA hypomethylation and altered gene expression.SummaryThe causes of hyperhomocysteinemia in renal failure are still not clear. However, the possibilities include defective renal or extrarenal metabolism as a result of uraemic toxicity. Renal plasma flow is important in homocysteine renal metabolism. Among the consequences of hyperhomocysteinemia in renal failure are impaired protein and DNA methylation, with an alteration in the allelic expression of genes regulated through methylation. Intervention trials are under way to test whether hyperhomocysteinemia is causally related to cardiovascular disease in this patient population.

 

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