Absence of Proteoglycan 4 (<i>Prg4</i>) Leads to Increased Subchondral Bone Porosity Which Can Be Mitigated Through Intra‐Articular Injection of PRG4

Abubacker, Saleem; Premnath, Priyatha; Shonak, Anchita; Léonard, Catherine; Shah, Sophia; Zhu, Ying; Jay, Gregory D.; Schmidt, Tannin A.; Boyd, Steven K.; Krawetz, Roman

doi:10.1002/jor.24378

Cited by 19 publications

(25 citation statements)

References 48 publications

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“…4 a). Moreover, the expression levels of the chondrogenic markers Col2a1, Acan, Sox9, Prg4 and Cnmd, which were reported previously [ 37 , 38 ], were upregulated in chondrogenic or fibrochondrogenic medium but not in fibrogenic medium ( Fig. 4 b).…”

Section: Resultssupporting

confidence: 80%

Decoding the annulus fibrosus cell atlas by scRNA-seq to develop an inducible composite hydrogel: A novel strategy for disc reconstruction

Han

Wang

Luo

et al. 2022

Bioactive Materials

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Section: Resultssupporting

confidence: 80%

Decoding the annulus fibrosus cell atlas by scRNA-seq to develop an inducible composite hydrogel: A novel strategy for disc reconstruction

Han

Wang

Luo

et al. 2022

Bioactive Materials

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“…While PRG4 is known to be essential for cartilage homeostasis 19 , 30 , 33 and that osteochondral progenitor cells in the joint environment express Prg4 34 , 35 , little is known regarding the role of Prg4 in chondrogenesis. Therefore, we isolated presumptive MPCs (Sca1 + CD140a + ) from the ear and (bone) marrow and induced these cells to undergo chondrogenic differentiation in the presence of rhPRG4 (Fig.…”

Section: Resultsmentioning

confidence: 99%

Proteoglycan 4 (PRG4) treatment enhances wound closure and tissue regeneration

et al. 2022

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The wound healing response is one of most primitive and conserved physiological responses in the animal kingdom, as restoring tissue integrity/homeostasis can be the difference between life and death. Wound healing in mammals is mediated by immune cells and inflammatory signaling molecules that regulate tissue resident cells, including local progenitor cells, to mediate closure of the wound through formation of a scar. Proteoglycan 4 (PRG4), a protein found throughout the animal kingdom from fish to elephants, is best known as a glycoprotein that reduces friction between articulating surfaces (e.g. cartilage). Previously, PRG4 was also shown to regulate the inflammatory and fibrotic response. Based on this, we asked whether PRG4 plays a role in the wound healing response. Using an ear wound model, topical application of exogenous recombinant human (rh)PRG4 hastened wound closure and enhanced tissue regeneration. Our results also suggest that rhPRG4 may impact the fibrotic response, angiogenesis/blood flow to the injury site, macrophage inflammatory dynamics, recruitment of immune and increased proliferation of adult mesenchymal progenitor cells (MPCs) and promoting chondrogenic differentiation of MPCs to form the auricular cartilage scaffold of the injured ear. These results suggest that PRG4 has the potential to suppress scar formation while enhancing connective tissue regeneration post-injury by modulating aspects of each wound healing stage (blood clotting, inflammation, tissue generation and tissue remodeling). Therefore, we propose that rhPRG4 may represent a potential therapy to mitigate scar and improve wound healing.

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“…Ten mice were euthanized at 16-weeks of age, and hind limbs (n = 10 right) were harvested for biomechanical testing and 3D Xray microscopy (XRM) imaging. Age-matched PRG4 knockout mice (Prg4 -/-, n = 6) were generated and maintained on a C57BL/6 genetic background, as previously described 57 . Limbs were disarticulated at the hip, followed by transection of the ligaments and careful isolation of distal femurs from tibiae and menisci with the help of a dissection microscope (Leica).…”

Section: Animalsmentioning

confidence: 99%

High spatial resolution analysis using indentation mapping differentiates biomechanical properties of normal vs. degenerated mouse articular cartilage

Masson

Besler

Edwards

et al. 2021

Preprint

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Characterizing the biomechanical properties of articular cartilage is crucial to understanding processes of tissue homeostasis vs. degeneration. In mouse models, however, limitations are imposed by their small joint size and thin cartilage surfaces. Here we present a 3D automated surface mapping system and methodology that allows for mechanical characterization of mouse cartilage with high spatial resolution. We performed repeated indentation mappings, followed by cartilage thickness measurement via needle probing, at 31 predefined positions distributed over the medial and lateral femoral condyles of healthy mice. High-resolution 3D x-ray microscopy (XRM) imaging was used to validate tissue thickness measurements. The automated indentation mapping was reproducible, and needle probing yielded cartilage thicknesses comparable to XRM imaging. When comparing healthy vs. degenerated cartilage, topographical variations in biomechanics were identified, with altered thickness and stiffness (instantaneous modulus) across condyles and within anteroposterior sub-regions. This quantitative technique comprehensively characterized cartilage function in mice femoral condyle cartilage. Hence, it has the potential to improve our understanding of tissue structure-function interplay in mouse models of repair and disease.

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Absence of Proteoglycan 4 (Prg4) Leads to Increased Subchondral Bone Porosity Which Can Be Mitigated Through Intra‐Articular Injection of PRG4

Cited by 19 publications

References 48 publications

Decoding the annulus fibrosus cell atlas by scRNA-seq to develop an inducible composite hydrogel: A novel strategy for disc reconstruction

Decoding the annulus fibrosus cell atlas by scRNA-seq to develop an inducible composite hydrogel: A novel strategy for disc reconstruction

Proteoglycan 4 (PRG4) treatment enhances wound closure and tissue regeneration

High spatial resolution analysis using indentation mapping differentiates biomechanical properties of normal vs. degenerated mouse articular cartilage

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