Deficiency in Perlecan/HSPG2 During Bone Development Enhances Osteogenesis and Decreases Quality of Adult Bone in Mice

Lowe, Dylan A; Lepori-Bui, Nadia; Fomin, Peter V.; Sloofman, Laura; Farach-Carson, Mary C.; Wang, Liyun; Kirn‐Safran, Catherine B.

doi:10.1007/s00223-014-9859-2

Cited by 30 publications

(31 citation statements)

References 36 publications

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“…1). Homozygous animals showed low levels of perlecan that appeared to be restricted to the intracellular compartment, which is consistent with a previous report that showed that perlecan in (Neo/Neo) mice is sequestered in the endoplasmic reticulum and is likely degraded (Lowe et al, 2014). In heterozygous and wild-type E16.5 embryos, perlecan was found throughout the distal humerus, (Fig.…”

Section: Resultssupporting

confidence: 92%

Knockdown of the pericellular matrix molecule perlecan lowers in situ cell and matrix stiffness in developing cartilage

Leng

et al. 2016

Developmental Biology

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The pericellular matrix (PCM) is a component of the extracellular matrix that is found immediately surrounding individual chondrocytes in developing and adult cartilage, and is rich in the proteoglycan perlecan. Mutations in perlecan are the basis of several developmental disorders, which are thought to arise from disruptions in the mechanical stability of the PCM. We tested the hypothesis that defects in PCM organization will reduce the stiffness of chondrocytes in developing cartilage by combining a murine model of Schwartz-Jampel syndrome, in which perlecan is knocked down, with our novel atomic force microscopy technique that can measure the stiffness of living cells and surrounding matrix in embryonic and postnatal tissues in situ. Perlecan knockdown altered matrix organization and significantly decreased the stiffness of both chondrocytes and interstitial matrix as a function of age and genotype. Our results demonstrate that the knockdown of a spatially restricted matrix molecule can have a profound influence on cell and tissue stiffness, implicating a role for outside-in mechanical signals from the PCM in regulating the intracellular mechanisms required for the overall development of cartilage.

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Section: Resultssupporting

confidence: 92%

Knockdown of the pericellular matrix molecule perlecan lowers in situ cell and matrix stiffness in developing cartilage

Leng

et al. 2016

Developmental Biology

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“…A report concluded that there are 15 members in the HSPGs. Among these members, Sdc2 and HSPG2 have been suggested to be involved in skeleton formation (41,42).…”

Section: Discussionmentioning

confidence: 99%

“…Sdc2 is abundant in putative precursor cells of hard and connective tissue, and its expression is high in prechondrogenic cells, decreases in differentiating chondrocytes, and persists in the perichondrium and periosteum at the onset of osteogenesis (42). HSPG2 is abundant in the extracellular matrix of cartilage and the lacunocanalicular space of adult bones, and deficiency in HSPG2 during bone development enhances osteogenesis and decreases quality of adult bone in mice (41).…”

Section: Discussionmentioning

confidence: 99%

“…Given HSPGs are receptors for apoE, Sdc2 and HSPG2 have been suggested to be involved in skeleton formation (41,42), and thus we analyzed the regulation of Sdc2 and HSPG2 by E2 during osteoblast differentiation as well. Our results showed that either in the saline group or in E2 treated group, both Sdc2 and HSPG2 genes were induced at day 5 and 25 of differentiation ( Figures 6A and 6D, p < 0.05, p < 0.01, p < 0.001).…”

Section: Regulation Of Syndecan 2 (Sdc2) and Hspg2 By E2 During Osteomentioning

confidence: 99%

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Multifarious effects of 17-β-estradiol on apolipoprotein E receptors gene expression during osteoblast differentiation <i>in vitro </i>

Gui

Duan

Tang

et al. 2016

BST

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“…In addition to the disorganization of the growth plate and chondro-osseous junction of bones caused by the absence of perlecan, there are other distortions in the growth of joints including the temporo-mandibular joint, myotonia and electrical disturbances of muscle and modifications to the structures of facial bones (30). Moreover, perlecan deficiency in hypomorphic mutant mice influences bone formation by enhancing osteogenesis and concurrently affects mineralization, leading to increased brittleness at older ages (31). …”

Section: Perlecan Geneticsmentioning

confidence: 99%

The role of perlecan and endorepellin in the control of tumor angiogenesis and endothelial cell autophagy

Douglass¹,

Goyal²,

Iozzo³

2015

Connective Tissue Research

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During tumor growth and angiogenesis there is a dynamic remodelling of tissue architecture often accompanied by the release of extracellular matrix constituents full of biological activity. One of the key constituents of the tumor microenvironment is the large heparan sulfate proteoglycan perlecan. This proteoglycan, strategically located at cell surfaces and within basement membranes, is a well-defined pro-angiogenic molecule when intact. However, when partially processed by proteases released during cancer remodelling and invasion, the C-terminal fragment of perlecan, known as endorepellin, has opposite effects than its parent molecule. Endorepellin is a potent inhibitor of angiogenesis by exerting a dual receptor antagonism by simultaneously engaging VEGFR2 and α2β1 integrin. Signaling through the α2β1 integrin leads to actin disassembly and block of endothelial cell migration, necessary for capillary morphogenesis. Signaling through the VEGFR2 induces dephosphorylation of the receptor via activation of SHP-1 and suppression of downstream proangiogenic effectors, especially attenuating VEGFA expression. A novel and emerging role of endorepellin is its ability to evoke autophagy by activating Peg3 and various canonical autophagic markers. This effect is specific for endothelial cells as these are the primary cells expressing both VEGFR2 and α2β1 integrin. Thus, an endogenous fragment of a ubiquitous proteoglycan can regulate both angiogenesis and autophagy through a dual receptor antagonism. The biological properties of this natural endogenous protein place endorepellin as a potential therapeutic agent against cancer or diseases where angiogenesis is prominent.

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Deficiency in Perlecan/HSPG2 During Bone Development Enhances Osteogenesis and Decreases Quality of Adult Bone in Mice

Cited by 30 publications

References 36 publications

Knockdown of the pericellular matrix molecule perlecan lowers in situ cell and matrix stiffness in developing cartilage

Knockdown of the pericellular matrix molecule perlecan lowers in situ cell and matrix stiffness in developing cartilage

Multifarious effects of 17-β-estradiol on apolipoprotein E receptors gene expression during osteoblast differentiation <i>in vitro </i>

The role of perlecan and endorepellin in the control of tumor angiogenesis and endothelial cell autophagy

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