Estradiol and RSPO3 regulate vertebral trabecular bone mass independent of each other

Karin H Nilsson; Jianyao Wu; Karin L Gustafsson; Maha El Shahawy; Antti Koskela; Juha Tuukkanen; Jan Tuckermann; Petra Henning; Ulf H Lerner; Claes Ohlsson; Sofia Movérare-Skrtic

doi:10.1152/ajpendo.00383.2021

Estradiol and RSPO3 regulate vertebral trabecular bone mass independent of each other

Am J Physiol Endocrinol Metab. 2022 Mar 1;322(3):E211-E218. doi: 10.1152/ajpendo.00383.2021. Epub 2022 Jan 24.

Authors

Affiliations

¹ Sahlgrenska Osteoporosis Centre, Centre for Bone and Arthritis Research, Institute of Medicine, Sahlgrenska Academy at University of Gothenburg, Gothenburg, Sweden.
² Department of Anatomy and Cell Biology, Faculty of Medicine, Institute of Cancer Research and Translational Medicine, University of Oulu, Oulu, Finland.
³ Institute of Comparative Molecular Endocrinology (CME), University of Ulm, Ulm, Germany.
⁴ Region Västra Götaland, Department of Drug Treatment, Sahlgrenska University Hospital, Gothenburg, Sweden.

Abstract

Osteoporosis is an age-dependent serious skeletal disease that leads to great suffering for the patient and high social costs, especially as the global population reaches higher age. Decreasing estrogen levels after menopause result in a substantial bone loss and increased fracture risk, whereas estrogen treatment improves bone mass in women. RSPO3, a secreted protein that modulates WNT signaling, increases trabecular bone mass and strength in the vertebrae of mice, and is associated with trabecular density and risk of distal forearm fractures in humans. The aim of the present study was to determine if RSPO3 is involved in the bone-sparing effect of estrogens. We first observed that estradiol (E2) treatment increases RSPO3 expression in bone of ovariectomized (OVX) mice, supporting a possible role of RSPO3 in the bone-sparing effect of estrogens. As RSPO3 is mainly expressed by osteoblasts in the bone, we used a mouse model devoid of osteoblast-derived RSPO3 (Runx2-creRspo3^flox/flox mice) to determine if RSPO3 is required for the bone-sparing effect of E2 in OVX mice. We confirmed that osteoblast-specific RSPO3 inactivation results in a substantial reduction in trabecular bone mass and strength in the vertebrae. However, E2 increased vertebral trabecular bone mass and strength similarly in mice devoid of osteoblast-derived RSPO3 and control mice. Unexpectedly, osteoblast-derived RSPO3 was needed for the full estrogenic response on cortical bone thickness. In conclusion, although osteoblast-derived RSPO3 is a crucial regulator of vertebral trabecular bone, it is required for a full estrogenic effect on cortical, but not trabecular, bone in OVX mice. Thus, estradiol and RSPO3 regulate vertebral trabecular bone mass independent of each other.NEW & NOTEWORTHY Osteoblast-derived RSPO3 is known to be a crucial regulator of vertebral trabecular bone. Our new findings show that RSPO3 and estrogen regulate trabecular bone independent of each other, but that RSPO3 is necessary for a complete estrogenic effect on cortical bone.

Keywords: RSPO3; estrogen; trabecular bone.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Bone Density
Cancellous Bone / metabolism
Estradiol / pharmacology
Estrogens / pharmacology
Female
Fractures, Bone*
Humans
Mice
Osteoporosis* / genetics
Osteoporosis* / metabolism
Ovariectomy
Thrombospondins / genetics
Thrombospondins / pharmacology

Substances

Estrogens
RSPO3 protein, human
Thrombospondins
Estradiol

Associated data

figshare/10.6084/m9.figshare.17212013.v1