Inhibition of Fibroblast Growth Factor-23 (FGF-23) Rescues Bone and Hematopoietic Stem Cell Niche Defects in Beta-Thalassemia, Uncovering the Missing Link between Hematopoiesis and Bone

Abstract: The bone marrow (BM) niche regulation and interactions with hematopoietic stem cells (HSC) have been extensively studied in steady state conditions and malignancies, but are still underexplored in hematological inherited disorders. We provided the first demonstration of impaired HSC function caused by an altered BM niche in a non-malignant disease, beta-thalassemia (BT) (Aprile et al., Blood 2020). BT is a globally widespread congenital hemoglobin disorder, resulting in severe anemia, ineffective erythropoiesi… Show more

“…Data on BThal mice indicate that multi-factorial alterations in the BM niche can impair HSC self-renewal and repopulating capacity. During the analysis of stromal components and soluble factors of the BM microenvironment, high systemic and BM local levels of FGF23 were detected [ 137 ]. FGF23 is a negative regulator of bone metabolism and PTH secretion [ 138 ], mainly produced by bone and erythroid cells in response to the anemia-related factor EPO [ 139 ].…”

“…FGF23 is a negative regulator of bone metabolism and PTH secretion [ 138 ], mainly produced by bone and erythroid cells in response to the anemia-related factor EPO [ 139 ]. The enhanced activation of FGF23 signaling has been proposed as the mechanism underlying bone disease and low PTH levels in th3 mice, negatively impacting the functional crosstalk between HSCs and the stromal niche [ 137 ].…”

“…Thus, more tunable molecules targeting the BThal stromal niche alterations should be explored and, in this view, investigation of mechanisms acting upstream the bone and PTH defects could be a promising option. Encouraging results highlighted the efficacy of the FGF23 inhibition strategy to correct bone mineralization and deposition and rescue the impaired HSC–niche crosstalk in BThal [ 137 ].…”

Targeting the Hematopoietic Stem Cell Niche in β-Thalassemia and Sickle Cell Disease

“…Data on BThal mice indicate that multi-factorial alterations in the BM niche can impair HSC self-renewal and repopulating capacity. During the analysis of stromal components and soluble factors of the BM microenvironment, high systemic and BM local levels of FGF23 were detected [ 137 ]. FGF23 is a negative regulator of bone metabolism and PTH secretion [ 138 ], mainly produced by bone and erythroid cells in response to the anemia-related factor EPO [ 139 ].…”

“…FGF23 is a negative regulator of bone metabolism and PTH secretion [ 138 ], mainly produced by bone and erythroid cells in response to the anemia-related factor EPO [ 139 ]. The enhanced activation of FGF23 signaling has been proposed as the mechanism underlying bone disease and low PTH levels in th3 mice, negatively impacting the functional crosstalk between HSCs and the stromal niche [ 137 ].…”

“…Thus, more tunable molecules targeting the BThal stromal niche alterations should be explored and, in this view, investigation of mechanisms acting upstream the bone and PTH defects could be a promising option. Encouraging results highlighted the efficacy of the FGF23 inhibition strategy to correct bone mineralization and deposition and rescue the impaired HSC–niche crosstalk in BThal [ 137 ].…”

Targeting the Hematopoietic Stem Cell Niche in β-Thalassemia and Sickle Cell Disease