Overlap between common genetic polymorphisms underpinning kidney traits and cardiovascular disease phenotypes: the CKDGen consortium

Chronic kidney disease is associated with cardiovascular disease. We tested for evidence of a shared genetic basis to these traits. We conducted 2 targeted analyses. First, we examined whether known single-nucleotide polymorphisms (SNPs) underpinning kidney traits were associated with a series of va...

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Vydáno v:	American journal of kidney diseases Ročník 61; číslo 6; s. 889
Hlavní autoři:	Olden, Matthias, Teumer, Alexander, Bochud, Murielle, Pattaro, Cristian, Köttgen, Anna, Turner, Stephen T, Rettig, Rainer, Chen, Ming-Huei, Dehghan, Abbas, Bastardot, Francois, Schmidt, Reinhold, Vollenweider, Peter, Schunkert, Heribert, Reilly, Muredach P, Fornage, Myriam, Launer, Lenore J, Verwoert, Germaine C, Mitchell, Gary F, Bis, Joshua C, O'Donnell, Christopher J, Cheng, Ching-Yu, Sim, Xueling, Siscovick, David S, Coresh, Josef, Kao, W H Linda, Fox, Caroline S, O'Seaghdha, Conall M
Médium:	Journal Article
Jazyk:	angličtina
Vydáno:	United States 01.06.2013
Témata:	Adaptor Proteins, Signal Transducing Adult Aged Blood Pressure - genetics Cardiovascular Diseases - genetics Carotid Intima-Media Thickness Female Genome-Wide Association Study Glomerular Filtration Rate - genetics Humans Intracellular Signaling Peptides and Proteins Male Middle Aged Polymorphism, Single Nucleotide Proteins - genetics Renal Insufficiency, Chronic - genetics
ISSN:	1523-6838, 1523-6838
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Abstract	Chronic kidney disease is associated with cardiovascular disease. We tested for evidence of a shared genetic basis to these traits. We conducted 2 targeted analyses. First, we examined whether known single-nucleotide polymorphisms (SNPs) underpinning kidney traits were associated with a series of vascular phenotypes. Additionally, we tested whether vascular SNPs were associated with markers of kidney damage. Significance was set to 1.5×10(-4) (0.05/325 tests). Vascular outcomes were analyzed in participants from the AortaGen (20,634), CARDIoGRAM (86,995), CHARGE Eye (15,358), CHARGE IMT (31,181), ICBP (69,395), and NeuroCHARGE (12,385) consortia. Tests for kidney outcomes were conducted in up to 67,093 participants from the CKDGen consortium. We used 19 kidney SNPs and 64 vascular SNPs. Vascular outcomes tested were blood pressure, coronary artery disease, carotid intima-media thickness, pulse wave velocity, retinal venular caliber, and brain white matter lesions. Kidney outcomes were estimated glomerular filtration rate and albuminuria. In general, we found that kidney disease variants were not associated with vascular phenotypes (127 of 133 tests were nonsignificant). The one exception was rs653178 near SH2B3 (SH2B adaptor protein 3), which showed direction-consistent association with systolic (P = 9.3 ×10(-10)) and diastolic (P = 1.6 ×10(-14)) blood pressure and coronary artery disease (P = 2.2 ×10(-6)), all previously reported. Similarly, the 64 SNPs associated with vascular phenotypes were not associated with kidney phenotypes (187 of 192 tests were nonsignificant), with the exception of 2 high-correlated SNPs at the SH2B3 locus (P = 1.06 ×10(-07) and P = 7.05 ×10(-08)). The combined effect size of the SNPs for kidney and vascular outcomes may be too low to detect shared genetic associations. Overall, although we confirmed one locus (SH2B3) as associated with both kidney and cardiovascular disease, our primary findings suggest that there is little overlap between kidney and cardiovascular disease risk variants in the overall population. The reciprocal risks of kidney and cardiovascular disease may not be genetically mediated, but rather a function of the disease milieu itself.
AbstractList	Chronic kidney disease is associated with cardiovascular disease. We tested for evidence of a shared genetic basis to these traits.BACKGROUNDChronic kidney disease is associated with cardiovascular disease. We tested for evidence of a shared genetic basis to these traits.We conducted 2 targeted analyses. First, we examined whether known single-nucleotide polymorphisms (SNPs) underpinning kidney traits were associated with a series of vascular phenotypes. Additionally, we tested whether vascular SNPs were associated with markers of kidney damage. Significance was set to 1.5×10(-4) (0.05/325 tests).STUDY DESIGNWe conducted 2 targeted analyses. First, we examined whether known single-nucleotide polymorphisms (SNPs) underpinning kidney traits were associated with a series of vascular phenotypes. Additionally, we tested whether vascular SNPs were associated with markers of kidney damage. Significance was set to 1.5×10(-4) (0.05/325 tests).Vascular outcomes were analyzed in participants from the AortaGen (20,634), CARDIoGRAM (86,995), CHARGE Eye (15,358), CHARGE IMT (31,181), ICBP (69,395), and NeuroCHARGE (12,385) consortia. Tests for kidney outcomes were conducted in up to 67,093 participants from the CKDGen consortium.SETTING & PARTICIPANTSVascular outcomes were analyzed in participants from the AortaGen (20,634), CARDIoGRAM (86,995), CHARGE Eye (15,358), CHARGE IMT (31,181), ICBP (69,395), and NeuroCHARGE (12,385) consortia. Tests for kidney outcomes were conducted in up to 67,093 participants from the CKDGen consortium.We used 19 kidney SNPs and 64 vascular SNPs.PREDICTORWe used 19 kidney SNPs and 64 vascular SNPs.Vascular outcomes tested were blood pressure, coronary artery disease, carotid intima-media thickness, pulse wave velocity, retinal venular caliber, and brain white matter lesions. Kidney outcomes were estimated glomerular filtration rate and albuminuria.OUTCOMES & MEASUREMENTSVascular outcomes tested were blood pressure, coronary artery disease, carotid intima-media thickness, pulse wave velocity, retinal venular caliber, and brain white matter lesions. Kidney outcomes were estimated glomerular filtration rate and albuminuria.In general, we found that kidney disease variants were not associated with vascular phenotypes (127 of 133 tests were nonsignificant). The one exception was rs653178 near SH2B3 (SH2B adaptor protein 3), which showed direction-consistent association with systolic (P = 9.3 ×10(-10)) and diastolic (P = 1.6 ×10(-14)) blood pressure and coronary artery disease (P = 2.2 ×10(-6)), all previously reported. Similarly, the 64 SNPs associated with vascular phenotypes were not associated with kidney phenotypes (187 of 192 tests were nonsignificant), with the exception of 2 high-correlated SNPs at the SH2B3 locus (P = 1.06 ×10(-07) and P = 7.05 ×10(-08)).RESULTSIn general, we found that kidney disease variants were not associated with vascular phenotypes (127 of 133 tests were nonsignificant). The one exception was rs653178 near SH2B3 (SH2B adaptor protein 3), which showed direction-consistent association with systolic (P = 9.3 ×10(-10)) and diastolic (P = 1.6 ×10(-14)) blood pressure and coronary artery disease (P = 2.2 ×10(-6)), all previously reported. Similarly, the 64 SNPs associated with vascular phenotypes were not associated with kidney phenotypes (187 of 192 tests were nonsignificant), with the exception of 2 high-correlated SNPs at the SH2B3 locus (P = 1.06 ×10(-07) and P = 7.05 ×10(-08)).The combined effect size of the SNPs for kidney and vascular outcomes may be too low to detect shared genetic associations.LIMITATIONSThe combined effect size of the SNPs for kidney and vascular outcomes may be too low to detect shared genetic associations.Overall, although we confirmed one locus (SH2B3) as associated with both kidney and cardiovascular disease, our primary findings suggest that there is little overlap between kidney and cardiovascular disease risk variants in the overall population. The reciprocal risks of kidney and cardiovascular disease may not be genetically mediated, but rather a function of the disease milieu itself.CONCLUSIONSOverall, although we confirmed one locus (SH2B3) as associated with both kidney and cardiovascular disease, our primary findings suggest that there is little overlap between kidney and cardiovascular disease risk variants in the overall population. The reciprocal risks of kidney and cardiovascular disease may not be genetically mediated, but rather a function of the disease milieu itself. Chronic kidney disease is associated with cardiovascular disease. We tested for evidence of a shared genetic basis to these traits. We conducted 2 targeted analyses. First, we examined whether known single-nucleotide polymorphisms (SNPs) underpinning kidney traits were associated with a series of vascular phenotypes. Additionally, we tested whether vascular SNPs were associated with markers of kidney damage. Significance was set to 1.5×10(-4) (0.05/325 tests). Vascular outcomes were analyzed in participants from the AortaGen (20,634), CARDIoGRAM (86,995), CHARGE Eye (15,358), CHARGE IMT (31,181), ICBP (69,395), and NeuroCHARGE (12,385) consortia. Tests for kidney outcomes were conducted in up to 67,093 participants from the CKDGen consortium. We used 19 kidney SNPs and 64 vascular SNPs. Vascular outcomes tested were blood pressure, coronary artery disease, carotid intima-media thickness, pulse wave velocity, retinal venular caliber, and brain white matter lesions. Kidney outcomes were estimated glomerular filtration rate and albuminuria. In general, we found that kidney disease variants were not associated with vascular phenotypes (127 of 133 tests were nonsignificant). The one exception was rs653178 near SH2B3 (SH2B adaptor protein 3), which showed direction-consistent association with systolic (P = 9.3 ×10(-10)) and diastolic (P = 1.6 ×10(-14)) blood pressure and coronary artery disease (P = 2.2 ×10(-6)), all previously reported. Similarly, the 64 SNPs associated with vascular phenotypes were not associated with kidney phenotypes (187 of 192 tests were nonsignificant), with the exception of 2 high-correlated SNPs at the SH2B3 locus (P = 1.06 ×10(-07) and P = 7.05 ×10(-08)). The combined effect size of the SNPs for kidney and vascular outcomes may be too low to detect shared genetic associations. Overall, although we confirmed one locus (SH2B3) as associated with both kidney and cardiovascular disease, our primary findings suggest that there is little overlap between kidney and cardiovascular disease risk variants in the overall population. The reciprocal risks of kidney and cardiovascular disease may not be genetically mediated, but rather a function of the disease milieu itself.
Author	Kao, W H Linda Coresh, Josef O'Donnell, Christopher J Chen, Ming-Huei Bochud, Murielle Turner, Stephen T Dehghan, Abbas Fornage, Myriam Verwoert, Germaine C Köttgen, Anna Reilly, Muredach P Siscovick, David S Cheng, Ching-Yu O'Seaghdha, Conall M Schunkert, Heribert Launer, Lenore J Schmidt, Reinhold Bis, Joshua C Olden, Matthias Teumer, Alexander Rettig, Rainer Sim, Xueling Vollenweider, Peter Pattaro, Cristian Bastardot, Francois Mitchell, Gary F Fox, Caroline S
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Copyright	Copyright © 2013 National Kidney Foundation, Inc. All rights reserved.
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Snippet	Chronic kidney disease is associated with cardiovascular disease. We tested for evidence of a shared genetic basis to these traits. We conducted 2 targeted... Chronic kidney disease is associated with cardiovascular disease. We tested for evidence of a shared genetic basis to these traits.BACKGROUNDChronic kidney...
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SubjectTerms	Adaptor Proteins, Signal Transducing Adult Aged Blood Pressure - genetics Cardiovascular Diseases - genetics Carotid Intima-Media Thickness Female Genome-Wide Association Study Glomerular Filtration Rate - genetics Humans Intracellular Signaling Peptides and Proteins Male Middle Aged Polymorphism, Single Nucleotide Proteins - genetics Renal Insufficiency, Chronic - genetics
Title	Overlap between common genetic polymorphisms underpinning kidney traits and cardiovascular disease phenotypes: the CKDGen consortium
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