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Publication : Accelerated Bone Loss in Transgenic Mice Expressing Constitutively Active TGF-β Receptor Type I.

First Author  Toejing P Year  2023
Journal  Int J Mol Sci Volume  24
Issue  13 PubMed ID  37445982
Mgi Jnum  J:337955 Mgi Id  MGI:7508299
Doi  10.3390/ijms241310797 Citation  Toejing P, et al. (2023) Accelerated Bone Loss in Transgenic Mice Expressing Constitutively Active TGF-beta Receptor Type I. Int J Mol Sci 24(13)
abstractText  Transforming growth factor beta (TGF-beta) is a key factor mediating the intercellular crosstalk between the hematopoietic stem cells and their microenvironment. Here, we investigated the skeletal phenotype of transgenic mice expressing constitutively active TGF-beta receptor type I under the control of Mx1-Cre (Mx1;TbetaRI(CA) mice). muCT analysis showed decreased cortical thickness, and cancellous bone volume in both femurs and mandibles. Histomorphometric analysis confirmed a decrease in cancellous bone volume due to increased osteoclast number and decreased osteoblast number. Primary osteoblasts showed decreased ALP and mineralization. Constitutive TbetaRI activation increased osteoclast differentiation. qPCR analysis showed that Tnfsf11/Tnfrsf11b ratio, Ctsk, Sufu, and Csf1 were increased whereas Runx2, Ptch1, and Ptch2 were decreased in Mx1;TbetaRI(CA) femurs. Interestingly, Gli1, Wnt3a, Sp7, Alpl, Ptch1, Ptch2, and Shh mRNA expression were reduced whereas Tnfsf11/Tnfrsf11b ratio was increased in Mx1;TbetaRI(CA) mandibles. Similarly, osteoclast-related genes were increased in Mx1;TbetaRI(CA) osteoclasts whereas osteoblast-related genes were reduced in Mx1;TbetaRI(CA) osteoblasts. Western blot analysis indicated that SMAD2 and SMAD3 phosphorylation was increased in Mx1;TbetaRI(CA) osteoblasts, and SMAD3 phosphorylation was increased in Mx1;TbetaRI(CA) osteoclasts. CTSK was increased while RUNX2 and PTCH1 was decreased in Mx1;TbetaRI(CA) mice. Microindentation analysis indicated decreased hardness in Mx1;TbetaRI(CA) mice. Our study indicated that Mx1;TbetaRI(CA) mice were osteopenic by increasing osteoclast number and decreasing osteoblast number, possibly by suppressing Hedgehog signaling pathways.
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