Associations between vascular calcification, arterial stiffness and bone mineral density in chronic kidney disease

doi:10.1093/ndt/gfm660

NDT Advance Access originally published online on October 12, 2007
Nephrology Dialysis Transplantation 2008 23(2):586-593; doi:10.1093/ndt/gfm660

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Associations between vascular calcification, arterial stiffness and bone mineral density in chronic kidney disease

Nigel D. Toussaint¹^,2, Kenneth K. Lau³, Boyd J. Strauss²^,4, Kevan R. Polkinghorne¹^,2 and Peter G. Kerr¹^,2

¹Department of Nephrology, Monash Medical Centre, Clayton, Victoria, Australia, ²Department of Medicine, Monash University, Clayton, Victoria, Australia, ³Department of Radiology and ⁴Clinical Nutrition and Metabolism Unit, Monash Medical Centre, Clayton, Victoria, Australia

Correspondence and offprint requests to: Dr Nigel Toussaint, Department of Nephrology, Monash Medical Centre, 246 Clayton Road, Clayton, Victoria 3168, Australia. Tel: +61-03-9594-3072 (w), +61-0418-560-198 (m); E-mail: Nigel.Toussaint{at}med.monash.edu.au

Abstract

Background. Vascular calcification (VC) and arterial stiffnessare major contributors to cardiovascular (CV) disease in chronickidney disease (CKD). Both are independent predictors of CVmortality and are inversely correlated with bone mineral density(BMD). Few studies have addressed the extent of VC in the pre-dialysisCKD population, with associated measurements of BMD and arterialcompliance.

Methods. We report cross-sectional data on 48 patients withCKD (GFR 17–55 ml/min) assessing the prevalence of VCand its associations. All patients had computed tomography (CT)scans through abdominal aorta and superficial femoral arteries(SFAs) to determine VC, pulse wave velocity (PWV) using SphygmoCordevice (AtCor PWV Inc., Westmead, Australia) measuring arterialstiffness, and dual-energy X-ray absorptiometry (DEXA) scansto determine BMD, as well as serum markers of renal functionand mineral metabolism.

Results. Patients, 71% male, 54% diabetic, had a median age64.5 years. Mean estimated GFR was 35.1 ± 10 ml/min.Mean PWV was 10.0 ± 4.5 m/s and mean aortic VC scorewas 421.5 ± 244 Hounsfield units, with 90% of subjectshaving some aortic VC present. In univariate linear regressionanalysis, aortic VC correlated positively with age (r 0.50,P < 0.001), triglycerides (r 0.47, P = 0.002) and PWV (r0.33, P = 0.03). There was also greater VC with declining renalfunction (r –0.28, P = 0.05). There was no significantassociation between VC and serum markers of mineral metabolism,however phosphate and Ca x P correlated positively with PWV(r 0.35, P = 0.02, r 0.36, P = 0.02, respectively). There wasalso a positive association between PWV and triglycerides (P= 0.008), and a trend towards greater PWV with increasing age(P = 0.09). In multivariate regression analysis only increasingage and triglyceride levels were significantly associated withaortic VC and PWV. Mean spine and femoral T-scores on DEXA were0.48 and –1.31 respectively, with 13% of subjects havingfemoral T-score <–2.5 (osteoporotic range). SFA VCinversely correlated with femoral T-scores (r –0.43, P= 0.004); however, there was a positive (likely false) associationbetween spine T-scores and aortic VC (r 0.37, P = 0.01), relatedto the limitation of vertebral DEXA in CKD.

Conclusion. There is a high prevalence of VC in pre-dialysisCKD patients, worse with increasing age, triglycerides and reducingrenal function. Correlation exists between VC and PWV and determinationof one or both may be useful for CKD patient CV risk assessment.Femoral BMD is inversely associated with SFA VC, but measurementof vertebral BMD by DEXA is unreliable in CKD patients withaortic VC.

Keywords: arterial stiffness; bone mineral density; cardiovascular disease; chronic kidney disease; mineral metabolism; vascular calcification

Received for publication: 29. 7.07
Accepted in revised form: 27. 8.07

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