Embryonic ablation of osteoblast <i>Smad4</i> interrupts matrix synthesis in response to canonical wnt signaling and causes an osteogenesis imperfecta-like phenotype

Salazar, Valerie S.; Zarkadis, Nicholas; Huang, Lisa; Norris, Jin; Grimston, Susan K.; Mbalaviele, Gabriel; Civitelli, Roberto

doi:10.1242/jcs.131953

Cited by 39 publications

(32 citation statements)

References 44 publications

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“…These data indicate that deletion of p38α in osteochondroprogenitors leads to a strong decrease in bone mass of both intramembranous and endochondral origins. They also corroborate previous reports showing that the bone phenotype in young Osx1-GFP::Cre mice was overcome by 12 weeks of age, with no differences observed between Osx1-GFP::Cre and control mice [20], [21]. There was no change in the number of osteocytes per area but, since the cortical area in p38α-deficient tibiae was lower, the total number of osteocytes was also lower in cortical samples from knockout mice (Fig.…”

Section: Resultssupporting

confidence: 92%

The p38α MAPK Function in Osteoprecursors Is Required for Bone Formation and Bone Homeostasis in Adult Mice

et al. 2014

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Backgroundp38 MAPK activity plays an important role in several steps of the osteoblast lineage progression through activation of osteoblast-specific transcription factors and it is also essential for the acquisition of the osteoblast phenotype in early development. Although reports indicate p38 signalling plays a role in early skeletal development, its specific contributions to adult bone remodelling are still to be clarified.Methodology/Principal FindingsWe evaluated osteoblast-specific deletion of p38α to determine its significance in early skeletogenesis, as well as for bone homeostasis in adult skeleton. Early p38α deletion resulted in defective intramembranous and endochondral ossification in both calvaria and long bones. Mutant mice showed reduction of trabecular bone volume in distal femurs, associated with low trabecular thickness. In addition, knockout mice also displayed decreased femoral cortical bone volume and thickness. Deletion of p38α did not affect osteoclast function. Yet it impaired osteoblastogenesis and osteoblast maturation and activity through decreased expression of osteoblast-specific transcription factors and their targets. Furthermore, the inducible Cre system allowed us to control the onset of p38α disruption after birth by removal of doxycycline. Deletion of p38α at three or eight weeks postnatally led to significantly lower trabecular and cortical bone volume after 6 or 12 months.ConclusionsOur data demonstrates that, in addition to early skeletogenesis, p38α is essential for osteoblasts to maintain their function in mineralized adult bone, as bone anabolism should be sustained throughout life. Moreover, our data also emphasizes that clinical development of p38 inhibitors should take into account their potential bone effects.

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Section: Resultssupporting

confidence: 92%

The p38α MAPK Function in Osteoprecursors Is Required for Bone Formation and Bone Homeostasis in Adult Mice

et al. 2014

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“…The finding that Wnt/b-catenin signaling affects matrix processing is consistent with reports that link b-catenin signaling with the transforming growth factor-b pathway, fibroblast proliferation, and collagen synthesis (41)(42)(43)(44)(45). Among the top upregulated genes was lysyl oxidase, a collagen cross-linking enzyme that has been linked to disrupted matrix synthesis in a transforming growth factor-b-dependent manner (23,(46)(47)(48), although inhibition of another family member, LOXL2, protects from fibrosis (49) and is currently in phase 2 clinical trials for the treatment of idiopathic pulmonary fibrosis (50). Mmp-13, a macrophage-associated metalloproteinase, also known as collagenase-3, is also highly increased in Lrp5-null lungs after bleomycin injury, and has been shown to limit the development of fibrosis (25,26).…”

Section: Discussionsupporting

confidence: 86%

Lrp5/β-Catenin Signaling Controls Lung Macrophage Differentiation and Inhibits Resolution of Fibrosis

Sennello

Misharin

Flozak

et al. 2017

Am J Respir Cell Mol Biol

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Previous studies established that attenuating Wnt/b-catenin signaling limits lung fibrosis in the bleomycin mouse model of this disease, but the contribution of this pathway to distinct lung cell phenotypes relevant to tissue repair and fibrosis remains incompletely understood. Using microarray analysis, we found that bleomycin-injured lungs from mice that lack the Wnt coreceptor low density lipoprotein receptor-related protein 5 (Lrp5) and exhibit reduced fibrosis showed enrichment for pathways related to extracellular matrix processing, immunity, and lymphocyte proliferation, suggesting the contribution of an immunematrix remodeling axis relevant to fibrosis. Activation of b-catenin signaling was seen in lung macrophages using the b-catenin reporter mouse, Axin2

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“…Fractured and nonfractured contralateral controls femurs were collected 5 days post fracture and 6 mm of mid diaphysis bone were dissected, cleaned of bone marrow, snap frozen in liquid nitrogen, and processed for total RNA extraction according using Trizol and RNeasy Plus kit, as previously described (Salazar et al, 2013).…”

Section: Standardized Fracturesmentioning

confidence: 99%

“…Where indicated, cells were seeded to confluence and pretreated with cycloheximide (Sigma Aldrich, diluted to 25-100 mg/ml in growth medium) for 1 h prior to 4 h stimulation with Wnt3a+cyclohexamide. BMSCs were prepared from bone marrow from 4-to 6-month-old mice (male and female) collected as previously described (Salazar et al, 2013) and plated in BMSC medium [ascorbic acid-free α-MEM (Invitrogen) containing 20% FBS, 40 mM L-glutamine, 100 U/ml penicillin-G and 100 mg/ml streptomycin]. After 3 days, non-adherent cells were removed by vigorous washing.…”

Section: Cell Culturementioning

confidence: 99%

Specification of osteoblast cell fate by canonical Wnt signaling requires Bmp2

et al. 2016

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Enhanced BMP or canonical Wnt (cWnt) signaling are therapeutic strategies employed to enhance bone formation and fracture repair, but the mechanisms each pathway utilizes to specify cell fate of bone-forming osteoblasts remain poorly understood. Among all BMPs expressed in bone, we find that singular deficiency of Bmp2 blocks the ability of cWnt signaling to specify osteoblasts from limb bud or bone marrow progenitors. When exposed to cWnts, Bmp2-deficient cells fail to progress through the Runx2/ Osx1 checkpoint and thus do not upregulate multiple genes controlling mineral metabolism in osteoblasts. Cells lacking Bmp2 after induction of Osx1 differentiate normally in response to cWnts, suggesting that pre-Osx1+ osteoprogenitors are an essential source and a target of BMP2. Our analysis furthermore reveals Grainyhead-like 3 (Grhl3) as a transcription factor in the osteoblast gene regulatory network induced during bone development and bone repair, which acts upstream of Osx1 in a BMP2-dependent manner. The Runx2/Osx1 transition therefore receives crucial regulatory inputs from BMP2 that are not compensated for by cWnt signaling, and this is mediated at least in part by induction and activation of Grhl3.

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Embryonic ablation of osteoblast Smad4 interrupts matrix synthesis in response to canonical wnt signaling and causes an osteogenesis imperfecta-like phenotype

Cited by 39 publications

References 44 publications

The p38α MAPK Function in Osteoprecursors Is Required for Bone Formation and Bone Homeostasis in Adult Mice

The p38α MAPK Function in Osteoprecursors Is Required for Bone Formation and Bone Homeostasis in Adult Mice

Lrp5/β-Catenin Signaling Controls Lung Macrophage Differentiation and Inhibits Resolution of Fibrosis

Specification of osteoblast cell fate by canonical Wnt signaling requires Bmp2

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