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Literature DB >> 31607375

Primary human chondrocytes respond to compression with phosphoproteomic signatures that include microtubule activation.

Donald L Zignego¹, Jonathan K Hilmer², Brian Bothner², William J Schell¹, Ronald K June³.

Abstract

Chondrocytes are responsible for maintaining the cartilage that helps joints bear load and move smoothly. These cells typically respond to physiological compression with pathways consistent with matrix synthesis, and chondrocyte mechanotransduction is essential for homeostasis. In osteoarthritis (OA), chondrocyte mechanotransduction appears to be dysregulated, yet the mechanisms remain poorly understood. The objective of this study is to document the phosphoproteomic responses of primary osteoarthritic chondrocytes to physiological sinusoidal compression. We show that OA chondrocytes respond to physiological compression by first activating proteins consistent with cytoskeletal remodeling and decreased transcription, and then later activating proteins for transcription. These results show that several microtubule-related proteins respond to compression. Our results demonstrate that compression is a relevant physiological stimulus for osteoarthritic chondrocytes. Future analyses may build on these results to find differences in compression-induced phosphoproteins between normal and OA cells that lead to druggable targets to restore homeostasis to diseased joints.

Entities: CellLine Chemical Disease Gene Species

Keywords: Cartilage biomechanics; Cartilage repair; Chondrocyte biology; Mechanobiology; Mechanotransduction; Osteoarthritis

Year: 2019 PMID： 31607375 PMCID： PMC7021325 DOI： 10.1016/j.jbiomech.2019.109367

Source DB: PubMed Journal: J Biomech ISSN： 0021-9290 Impact factor: 2.712

66 in total

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Authors: S Hayashi; T Nishiyama; Y Miura; T Fujishiro; N Kanzaki; S Hashimoto; T Matsumoto; M Kurosaka; R Kuroda
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Journal: Nat Protoc Date: 2009 Impact factor: 13.491

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Authors: Aaron A Jutila; Donald L Zignego; William J Schell; Ronald K June
Journal: Ann Biomed Eng Date: 2014-11-14 Impact factor: 3.934

5. Hyper-osmotic stress induces volume change and calcium transients in chondrocytes by transmembrane, phospholipid, and G-protein pathways.

Authors: G R Erickson; L G Alexopoulos; F Guilak
Journal: J Biomech Date: 2001-12 Impact factor: 2.712

6. Candidate mediators of chondrocyte mechanotransduction via targeted and untargeted metabolomic measurements.

Authors: Aaron A Jutila; Donald L Zignego; Bradley K Hwang; Jonathan K Hilmer; Timothy Hamerly; Cody A Minor; Seth T Walk; Ronald K June
Journal: Arch Biochem Biophys Date: 2014-01-16 Impact factor: 4.013

7. Investigating conversion of mechanical force into biochemical signaling in three-dimensional chondrocyte cultures.

Authors: Carole Bougault; Anne Paumier; Elisabeth Aubert-Foucher; Frédéric Mallein-Gerin
Journal: Nat Protoc Date: 2009-05-28 Impact factor: 13.491

8. The structurally disordered KRAB repression domain is incorporated into a protease resistant core upon binding to KAP-1-RBCC domain.

Authors: Hongzhuang Peng; Lisa C Gibson; Allan D Capili; Katherine L B Borden; Michael J Osborne; Sandra L Harper; David W Speicher; Kehao Zhao; Ronen Marmorstein; Thomas A Rock; Frank J Rauscher
Journal: J Mol Biol Date: 2007-03-24 Impact factor: 5.469

Primary human chondrocytes respond to compression with phosphoproteomic signatures that include microtubule activation.

1. DcR3 induces cell proliferation through MAPK signaling in chondrocytes of osteoarthritis.

2. Mechanical power and efficiency of level walking with different stride rates.

3. Systematic and integrative analysis of large gene lists using DAVID bioinformatics resources.

4. Encapsulation of chondrocytes in high-stiffness agarose microenvironments for in vitro modeling of osteoarthritis mechanotransduction.

5. Hyper-osmotic stress induces volume change and calcium transients in chondrocytes by transmembrane, phospholipid, and G-protein pathways.

6. Candidate mediators of chondrocyte mechanotransduction via targeted and untargeted metabolomic measurements.

7. Investigating conversion of mechanical force into biochemical signaling in three-dimensional chondrocyte cultures.

8. The structurally disordered KRAB repression domain is incorporated into a protease resistant core upon binding to KAP-1-RBCC domain.

9. Mechanical compression modulates matrix biosynthesis in chondrocyte/agarose culture.

10. iTRAQ-based proteomics reveals novel biomarkers of osteoarthritis.

1. MicroRNA‑186‑5p downregulation inhibits osteoarthritis development by targeting MAPK1.

Review 2. An overview of substrate stiffness guided cellular response and its applications in tissue regeneration.

3. Metabolomic Profiling and Mechanotransduction of Single Chondrocytes Encapsulated in Alginate Microgels.