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Gene variant linked to chronic kidney disease
June 15, 2005Two common gene variations are associated with the risk for developing chronic kidney disease, according to a study by researchers at the Johns Hopkins Bloomberg School of Public Health and other institutions. One variant increases risk and the other decreases risk with a similar effect in whites, African-Americans, diabetic and non-diabetic individuals. The study, published in the June 15 edition of JAMA, is the first large-scale investigation of the role Apolipoprotein E (APOE) alleles play in chronic kidney disease. APOE is known to be associated with risk of Alzheimer's disease and heart disease but interestingly, the kidney disease association is in the opposite direction.
Results of the study found that a variant of the APOE gene, the e2 allele, was associated with a moderately increased risk for chronic kidney disease. The study also confirmed that the e4 variant offered protection against the development of chronic kidney disease. The e4 allele is also a known risk factor for Alzheimer's disease and a weaker risk factor for coronary heart disease. The e2 allele is known to be associated with abnormalities in plasma triglycerides, a condition that is also common with kidney disease. Smaller previous studies have suggested that the e2 increased and e4 alleles decreased the risk of kidney disease, but those studies mostly focused on individuals with diabetes.
"Consistency of association across a number of previous studies is important in convincing us this effect is real. However, our large study suggests that the effect of the APOE gene is much weaker than previous smaller studies indicated," said Josef Coresh, MD, PhD, corresponding author and professor of epidemiology, medicine and biostatistics at the Bloomberg School of Public Health. "Our understanding of the biology and genetics of kidney disease is improved, which may point to directions for future improvements in therapy. However, population screening for kidney disease risk is still best focused on diabetes, hypertension and protein in the urine."
The study involved 14,520 middle-aged whites and African Americans enrolled in the Atherosclerosis Risk in Communities study. Participants underwent standardized medical exams every 3 years from 1987 to 1999. None had severe renal disease when they entered the study and 1,060 developed some kidney disease, as indicated by laboratory testing, hospitalization or death certificates, by 2003. Most recent estimates indicate that approximately 400,000 US residents undergo dialysis and approximately 8 million adults have lost half or more of their kidney function, a level diagnostic of chronic kidney disease.
This study sheds light on susceptibility for developing moderate chronic kidney disease while other studies are increasingly focusing on the consequences and complications of chronic kidney disease, which include an increased risk of developing a heart attack, stroke and bone fractures.
Charles C. Hsu, PhD, lead author of the study and an epidemiologist with the Johns Hopkins University School of Medicine said, "The study points to the potential importance of the effects of APOE on cell-to-cell communication and response to injury in the kidney."
"From a genetics perspective, the APOE gene is fascinating. It has several common variants-only half the people have the most common form of the gene. The two other main variants are still quite common and, interestingly, relate to different diseases in different ways. APOE was first appreciated for its role in targeting cholesterol and other fats through the bloodstream. Compared to the most common e3 variant of the gene, the e4 variant clears from the blood more quickly and the e2 clears more slowly," explained co-author Linda Kao, PhD, of the study, a genetic epidemiologist and assistant professor at the Bloomberg School of Public Health. "It was later appreciated that APOE is a key determinant of Alzheimer's disease risk. APOE is important in the formation of brain lesions central to Alzheimer's, but the exact mechanisms still need to be understood. It is intriguing that APOE is now found to relate to chronic kidney disease progression, but its effect on risk is opposite to that of its effect on heart disease and Alzheimer's disease."
Johns Hopkins University Bloomberg School of Publi
The study involved 14,520 middle-aged whites and African Americans enrolled in the Atherosclerosis Risk in Communities study. Participants underwent standardized medical exams every 3 years from 1987 to 1999. None had severe renal disease when they entered the study and 1,060 developed some kidney disease, as indicated by laboratory testing, hospitalization or death certificates, by 2003. Most recent estimates indicate that approximately 400,000 US residents undergo dialysis and approximately 8 million adults have lost half or more of their kidney function, a level diagnostic of chronic kidney disease.
This study sheds light on susceptibility for developing moderate chronic kidney disease while other studies are increasingly focusing on the consequences and complications of chronic kidney disease, which include an increased risk of developing a heart attack, stroke and bone fractures.
Charles C. Hsu, PhD, lead author of the study and an epidemiologist with the Johns Hopkins University School of Medicine said, "The study points to the potential importance of the effects of APOE on cell-to-cell communication and response to injury in the kidney."
"From a genetics perspective, the APOE gene is fascinating. It has several common variants-only half the people have the most common form of the gene. The two other main variants are still quite common and, interestingly, relate to different diseases in different ways. APOE was first appreciated for its role in targeting cholesterol and other fats through the bloodstream. Compared to the most common e3 variant of the gene, the e4 variant clears from the blood more quickly and the e2 clears more slowly," explained co-author Linda Kao, PhD, of the study, a genetic epidemiologist and assistant professor at the Bloomberg School of Public Health. "It was later appreciated that APOE is a key determinant of Alzheimer's disease risk. APOE is important in the formation of brain lesions central to Alzheimer's, but the exact mechanisms still need to be understood. It is intriguing that APOE is now found to relate to chronic kidney disease progression, but its effect on risk is opposite to that of its effect on heart disease and Alzheimer's disease."
Johns Hopkins University Bloomberg School of Publi
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New class of molecules may help prevent fatal complication in patients with kidney disease
Researchers at the University of Maryland School of Medicine have made an important discovery about why potassium builds up to dangerous levels in the bloodstream, a relatively common medical problem that affects about eight percent of hospitalized patients.
Reduction in glycotoxins from heat-processing of foods reduces risk of chronic disease
Researchers from Mount Sinai School of Medicine report that cutting back on the consumption of processed and fried foods, which are high in toxins called Advanced Glycation End products (AGEs), can reduce inflammation and actually help restore the body's natural defenses regardless of age or health status.
Help your kidneys: Pass on salt and diet soda
Individuals who consume a diet high in sodium or artificially sweetened drinks are more likely to experience a decline in kidney function, according to two papers being presented at the American Society of Nephrology's annual meeting in San Diego, California.
Can charcoal fight heart disease in kidney patients?
Charcoal may provide a new approach to managing the high rate of heart disease in patients with advanced kidney disease, according to preliminary research being presented at the American Society of Nephrology's 42nd Annual Meeting and Scientific Exposition in San Diego, CA.
Women with chronic kidney disease more likely than men to go undiagnosed
Woman are at particular risk of their primary care physicians delaying diagnosis of chronic kidney disease (CKD), according to a paper being presented at the American Society of Nephrology's 42nd Annual Meeting and Scientific Exposition in San Diego, California.
For dialysis patients, skinny is dangerous
Dialysis patients with low body fat are at increased risk of death-even compared to patients at the highest level of body fat percentage, according to research being presented at the American Society of Nephrology's 42nd Annual Meeting and Scientific Exposition in San Diego.
Protein critical for insulin secretion may be contributor to diabetes
A cellular protein from a family involved in several human diseases is crucial for the proper production and release of insulin, new research has found, suggesting that the protein might play a role in diabetes.
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