Literature DB >> 28645539

Gli1-labeled adult mesenchymal stem/progenitor cells and hedgehog signaling contribute to endochondral heterotopic ossification.

Chen Kan1, Lijun Chen1, Yangyang Hu1, Na Ding1, Yuyun Li2, Tammy L McGuire3, Haimei Lu1, John A Kessler3, Lixin Kan4.   

Abstract

Heterotopic ossification (HO), acquired or hereditary, endochondral or intramembranous, is the formation of true bone outside the normal skeleton. Since perivascular Gli1+ progenitors contribute to injury induced organ fibrosis, and CD133 is expressed by a variety of populations of adult stem cells, this study utilized Cre-lox based genetic lineage tracing to test the contribution to endochondral HO of adult stem/progenitor cells that expressed either Gli1 or CD133. We found that both lineages contributed broadly to different normal tissues with distinct patterns, but that only Gli1-creERT labeled stem/progenitor cells contributed to all stages of endochondral HO in a BMP dependent, injury induced, transgenic mouse model. Hedgehog (Hh) signaling was abnormal at endochondral HO lesion sites with increased signaling surrounding the lesion but diminished signaling within it. Thus, local dysregulation of Hh signaling participates in the pathophysiology of endochondral HO. However, unlike a previous report of intramembranous HO, systemic inhibition of Hh signaling was insufficient to prevent the initiation of the endochondral HO process or to treat the existing endochondral HO, suggesting that Hh participates in, but is not essential for endochondral HO in this model. This could potentially reflect the underlying difference between intramembranous and endochondral HO. Nevertheless, identification of this novel stem/precursor cell population as a HO-contributing cell population provides a potential drugable target.
Copyright © 2017. Published by Elsevier Inc.

Entities:  

Keywords:  Adult mesenchymal stem/progenitor cells (MSC); CD133; Gli1; Hedgehog (Hh) signaling; Heterotopic ossification (HO); Lineage tracing

Mesh:

Substances:

Year:  2017        PMID: 28645539      PMCID: PMC5801258          DOI: 10.1016/j.bone.2017.06.014

Source DB:  PubMed          Journal:  Bone        ISSN: 1873-2763            Impact factor:   4.398


  25 in total

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Authors:  Lixin Kan; John A Kessler
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Authors:  Lixin Kan; Chian-Yu Peng; Tammy L McGuire; John A Kessler
Journal:  Bone       Date:  2012-12-20       Impact factor: 4.398

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5.  [Temporal and spatial distribution of Gli1+ cells and their function during periodontal development].

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Review 6.  Cellular Plasticity in Musculoskeletal Development, Regeneration, and Disease.

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7.  Tendon-derived cathepsin K-expressing progenitor cells activate Hedgehog signaling to drive heterotopic ossification.

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9.  Targeting local lymphatics to ameliorate heterotopic ossification via FGFR3-BMPR1a pathway.

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Review 10.  The Survey of Cells Responsible for Heterotopic Ossification Development in Skeletal Muscles-Human and Mouse Models.

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