Hematopoietic stem cells (HSCs) are regulated by signals from the bone marrow (BM) niche that tune hematopoiesis at steady state and in hematologic disorders. To understand HSC-niche interactions in altered nonmalignant homeostasis, we selected b-thalassemia, a hemoglobin disorder, as a paradigm. In this severe congenital anemia, alterations secondary to the primary hemoglobin defect have a potential impact on HSC-niche cross talk. We report that HSCs in thalassemic mice (th3) have an impaired function, caused by the interaction with an altered BM niche. The HSC self-renewal defect is rescued after cell transplantation into a normal microenvironment, thus proving the active role of the BM stroma. Consistent with the common finding of osteoporosis in patients, we found reduced bone deposition with decreased levels of parathyroid hormone (PTH), which is a key regulator of bone metabolism but also of HSC activity. In vivo activation of PTH signaling through the reestablished Jagged1 and osteopontin levels correlated with the rescue of the functional pool of th3 HSCs by correcting HSC-niche cross talk. Reduced HSC quiescence was confirmed in thalassemic patients, along with altered features of the BM stromal niche. Our findings reveal a defect in HSCs in b-thalassemia induced by an altered BM microenvironment and provide novel and relevant insight for improving transplantation and gene therapy approaches.

Aprile, A., Gulino, A., Storto, M., Villa, I., Beretta, S., Merelli, I., et al. (2020). Hematopoietic stem cell function in b-thalassemia is impaired and is rescued by targeting the bone marrow niche. BLOOD, 136(5 (30 July 2020)), 610-622 [10.1182/blood.2019002721].

Hematopoietic stem cell function in b-thalassemia is impaired and is rescued by targeting the bone marrow niche

Beretta S.;Merelli I.;
2020

Abstract

Hematopoietic stem cells (HSCs) are regulated by signals from the bone marrow (BM) niche that tune hematopoiesis at steady state and in hematologic disorders. To understand HSC-niche interactions in altered nonmalignant homeostasis, we selected b-thalassemia, a hemoglobin disorder, as a paradigm. In this severe congenital anemia, alterations secondary to the primary hemoglobin defect have a potential impact on HSC-niche cross talk. We report that HSCs in thalassemic mice (th3) have an impaired function, caused by the interaction with an altered BM niche. The HSC self-renewal defect is rescued after cell transplantation into a normal microenvironment, thus proving the active role of the BM stroma. Consistent with the common finding of osteoporosis in patients, we found reduced bone deposition with decreased levels of parathyroid hormone (PTH), which is a key regulator of bone metabolism but also of HSC activity. In vivo activation of PTH signaling through the reestablished Jagged1 and osteopontin levels correlated with the rescue of the functional pool of th3 HSCs by correcting HSC-niche cross talk. Reduced HSC quiescence was confirmed in thalassemic patients, along with altered features of the BM stromal niche. Our findings reveal a defect in HSCs in b-thalassemia induced by an altered BM microenvironment and provide novel and relevant insight for improving transplantation and gene therapy approaches.
Articolo in rivista - Articolo scientifico
bone marrow, mice, thalassemia, hematopoietic stem cells, transplantation, parathyroid hormones;
English
28-apr-2020
2020
136
5 (30 July 2020)
610
622
none
Aprile, A., Gulino, A., Storto, M., Villa, I., Beretta, S., Merelli, I., et al. (2020). Hematopoietic stem cell function in b-thalassemia is impaired and is rescued by targeting the bone marrow niche. BLOOD, 136(5 (30 July 2020)), 610-622 [10.1182/blood.2019002721].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/311004
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