Anemia and Mineral Bone Disorder in Kidney Disease Patients: The Role of FGF-23 and Other Related Factors

Nazareno Carullo, David Sorbo(Ospedale San Bortolo), Teresa Faga(Magna Graecia University), Sara Pugliese(Magna Graecia University), Maria Teresa Zicarelli(Magna Graecia University), Davide Costa(Magna Graecia University), Nicola Ielapi(Magna Graecia University), Yuri Battaglia(University of Verona), Antonio Pisani(Federico II University Hospital), Giuseppe Coppolino(Magna Graecia University), Davide Bolignano(Magna Graecia University), Ashour Michael(Magna Graecia University), Raffaele Serra(Magna Graecia University), Michele Andreucci(Magna Graecia University)
International Journal of Molecular Sciences
November 29, 2024
10.3390/ijms252312838
Cited by 12Open Access
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Abstract

Anemia and mineral and bone disorder (MBD) are significant complications of chronic kidney disease (CKD). The erythropoietin (Epo) pathway plays a key role in both of these processes in CKD. Another molecule that plays an important role in CKD-MBD is fibroblast growth factor (FGF)-23, whose main role is to maintain serum phosphate levels in the normal range, acting via its co-receptor Klotho; however, its activity may also be related to anemia and inflammation. In this review, the regulation of Epo and FGF-23 and the molecular mechanisms of their action are outlined. Furthermore, the complex interaction between EPO and FGF-23 is discussed, as well as their association with other anemia-related factors and processes such as Klotho, vitamin D, and iron deficiency. Together, these may be part of a "kidney-bone marrow-bone axis" that promotes CKD-MBD.

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