The Role of DMP1 in CKD-MBD.
Aline MartinDominik KentrupPublished in: Current osteoporosis reports (2021)
Patients and mice with CKD show perturbations of DMP1 expression in bone, associated with impaired osteocyte maturation, mineralization, and increased fibroblast growth factor 23 (FGF23) production. In humans with CKD, low circulating DMP1 levels are independently associated with increased cardiovascular events. We recently showed that DMP1 supplementation lowers circulating FGF23 levels and improves bone mineralization and cardiac outcomes in mice with CKD. Mortality rates are extremely high among patients with CKD and have only marginally improved over decades. Bone disease and FGF23 excess contribute to mortality in CKD by increasing the risk of bone fractures and cardiovascular disease, respectively. Previous studies focused on DMP1 loss-of-function mutations have established its role in the regulation of FGF23 and bone mineralization. Recent studies show that DMP1 supplementation may fill a crucial therapeutic gap by improving bone and cardiac health in CKD.
Keyphrases
- chronic kidney disease
- end stage renal disease
- cardiovascular events
- bone mineral density
- cardiovascular disease
- soft tissue
- bone loss
- bone regeneration
- coronary artery disease
- public health
- left ventricular
- type diabetes
- risk factors
- ejection fraction
- adipose tissue
- skeletal muscle
- high fat diet induced
- insulin resistance
- atrial fibrillation
- wild type
- patient reported