Abstract

Chronic kidney disease (CKD) is a growing pandemic associated with very high mortality rates due to cardiovascular disease. Standard cardiovascular risk factors do not account for the increased risk associated with CKD. Novel risk factors discovered in the study of CKD: phosphorus, vascular calcification, and fibroblast growth factor 23 (FGF23) are all incorporated in the new chronic kidney disease - mineral bone disorder (CKD-MBD) syndrome. The cause of the CKD-MBD was unknown until recent progress stemming from the previous funding period of this application, and there was no therapy addressing cardiovascular risk. In its inception, the CKD-MBD is characterized by a developing osteodystrophy, stimulation of vascular calcification and stimulation of osteocytic protein levels in the circulation. We have found that the CKD-MBD is caused by increased renal production of circulating Wnt inhibitors and changes in c-klotho function. In a model of early CKD in the background of atherosclerosis and diabetes stimulated vascular calcification, we demonstrated increased production of Dkk-1 in the remnant kidney and increased circulating Dkk-1, sclerostin and c-klotho. Neutralization of Dkk-1 by a monoclonal antibody stimulated bone formation rates, corrected the osteodystrophy, prevented CKD stimulated vascular calcification (VC), and increased the expression of membrane c-klotho in the aorta and kidney. In addition, the osteoblastic transcription factor, RUNX2 was inhibited in the aorta, and vascular smooth muscle contractile protein expression was increased. Increased plasma c-klotho and FGF23 levels were not affected by Dkk-1 neutralization, but FGF23 levels were reduced to normal by phosphate binder therapy. Phosphate binder therapy had no effect on vascular calcification, but combined with the Dkk-1 antibody the CKD-MBD as characterized in the CKD-2 mice was completely treated.
The aims of the current application ask whether the treatment of the CKD-MBD in early CKD, improves cardiovascular outcomes.
In aim one, the effects of neutralization of the Wnt inhibitor, Dkk-1, on vascular stiffness will be studied using our vascular calcification model and murine model of Alport's syndrome.
In aim two, the effects of neutralization of the Wnt inhibitor, Dkk-1, on survival and cardiac function in CKD will be studied.
In aim three, the question of whether, early control of phosphate homeostasis and FGF23 add to the effects of treating the CKD-MBD with neutralization of the Wnt inhibitor, Dkk-1, will be analyzed. The successful completion of the proposed studies will provide preclinical proof of concept that treatment and prevention of the CKD-MBD improves cardiovascular outcomes in CKD, a major innovation, paving the pathway to clinical trials.

Public Health Relevance

The studies proposed in this application utilize the recent discovery of what causes the blood vessel and bone disease in kidney failure. The next step is proposed in the application that is to try and treat the heart disease and decrease the death rate that accompanies kidney disease by eliminating the causes of the blood vessel and bone disease. Successful studies in animals as proposed in the application will lead to human trials as the step that follows the studies in the application.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
2R01DK070790-09A1
Application #
8818891
Study Section
Skeletal Biology Development and Disease Study Section (SBDD)
Program Officer
Kimmel, Paul
Project Start
2005-04-01
Project End
2019-06-30
Budget Start
2014-09-01
Budget End
2015-06-30
Support Year
9
Fiscal Year
2014
Total Cost
$343,125
Indirect Cost
$118,125

  Institution

Name
Washington University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Hruska, Keith A; Lanske, Beate; Moe, Orson W (2017) Crosstalk between kidney and bone - Bench to bedside. Bone 100:1-3
Sugatani, Toshifumi; Agapova, Olga A; Fang, Yifu et al. (2017) Ligand trap of the activin receptor type IIA inhibits osteoclast stimulation of bone remodeling in diabetic mice with chronic kidney disease. Kidney Int 91:86-95
Hruska, Keith A; Sugatani, Toshifumi; Agapova, Olga et al. (2017) The chronic kidney disease - Mineral bone disorder (CKD-MBD): Advances in pathophysiology. Bone 100:80-86
Agapova, Olga A; Fang, Yifu; Sugatani, Toshifumi et al. (2016) Ligand trap for the activin type IIA receptor protects against vascular disease and renal fibrosis in mice with chronic kidney disease. Kidney Int 89:1231-43
Seifert, Michael E; Ashoor, Isa F; Chiang, Myra L et al. (2016) Fibroblast growth factor-23 and chronic allograft injury in pediatric renal transplant recipients: a Midwest Pediatric Nephrology Consortium study. Pediatr Transplant 20:378-87
Seifert, Michael E; Hruska, Keith A (2016) The Kidney-Vascular-Bone Axis in the Chronic Kidney Disease-Mineral Bone Disorder. Transplantation 100:497-505
Sugatani, Toshifumi; Agapova, Olga; Malluche, Hartmut H et al. (2015) SIRT6 deficiency culminates in low-turnover osteopenia. Bone 81:168-177
Freedman, Barry I; Divers, Jasmin; Russell, Gregory B et al. (2015) Plasma FGF23 and Calcified Atherosclerotic Plaque in African Americans with Type 2 Diabetes Mellitus. Am J Nephrol 42:391-401
Hruska, Keith A; Seifert, Michael; Sugatani, Toshifumi (2015) Pathophysiology of the chronic kidney disease-mineral bone disorder. Curr Opin Nephrol Hypertens 24:303-9
Anyaegbu, Elizabeth I; Shaw, Andrey S; Hruska, Keith A et al. (2015) Clinical phenotype of APOL1 nephropathy in young relatives of patients with end-stage renal disease. Pediatr Nephrol 30:983-9

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