Profiling of Stem/Progenitor Cell Regulatory Genes of the Synovial Joint by Genome-Wide RNA-Seq Analysis

Yue Zhou, Mo Chen, Christopher L. Ricupero, Ling He, Jiaqian Wu, Kenian Chen, Richard A. Friedman, Paolo Guarnieri, Zuolin Wang, Xuedong Zhou, Jeremy J. Mao

Résultat de rechercheexamen par les pairs

9 Citations (Scopus)

Résumé

Synovial joints suffer from arthritis and trauma that may be severely debilitative. Despite robust investigations in the roles of individual genes in synovial joint development and arthritis, little is known about global profiles of genes that regulate stem/progenitor cells of a synovial joint. The temporomandibular joint is a poorly understood synovial arthrosis with few clinical treatment options. Here, we isolated the articular and mature zones of the mandibular condyle by laser capture microdissection, performed genome-wide profiling, and analyzed molecular signaling pathways relevant to stem/progenitor cell functions. A total of 804 genes were differentially expressed between the articular and mature zones. Pathway analyses revealed 29 enriched signaling pathways, including the PI3K-Akt, Wnt, and Toll-like receptor signaling pathways that may regulate stem/progenitor cell homeostasis and differentiation into the chondrocyte lineage. Upstream regulator analyses further predicted potential upstream key regulators such as Xbp1, Nupr1, and Hif1a, and associated underlying mechanism networks were described. Among the multiple candidates of growth and transcriptional factors that may regulate stem/progenitor cells, we immunolocalized Sox9, Ihh, Frzb, Dkk1, Lgr5, and TGFβ3 in the articular and mature zones. These findings provide a comprehensive genetic mapping of growth and transcriptional genes in the articular and mature zones of a synovial joint condyle. Differentially expressed genes may play crucial roles in the regulation of stem/progenitor cells in development, homeostasis, and tissue regeneration.

Langue d'origineEnglish
Numéro d'article9327487
JournalBioMed Research International
Volume2018
DOI
Statut de publicationPublished - 2018

Financement

The authors thank Y. W. Tse and P. Ralph-Birkett for their administrative assistance. The work is supported by NIH Grants R01DE023112 and R01AR065023 to Jeremy J. Mao, NIH/K12DE023583 to Mo Chen, the National Natural Science Foundation of China Grants 81271110 to Zuolin Wang and 81371136 to Xuedong Zhou.

Bailleurs de fondsNuméro du bailleur de fonds
National Institutes of HealthR01AR065023, K12DE023583, R01DE023112
National Natural Science Foundation of China81371136, 81271110

    ASJC Scopus Subject Areas

    • General Biochemistry,Genetics and Molecular Biology
    • General Immunology and Microbiology

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