Literature DB >> 28351866

Shh promotes direct interactions between epidermal cells and osteoblast progenitors to shape regenerated zebrafish bone.

Benjamin E Armstrong1,2, Astra Henner1, Scott Stewart3, Kryn Stankunas3,4.   

Abstract

Zebrafish innately regenerate amputated fins by mechanisms that expand and precisely position injury-induced progenitor cells to re-form tissue of the original size and pattern. For example, cell signaling networks direct osteoblast progenitors (pObs) to rebuild thin cylindrical bony rays with a stereotypical branched morphology. Hedgehog/Smoothened (Hh/Smo) signaling has been variably proposed to stimulate overall fin regenerative outgrowth or promote ray branching. Using a photoconvertible patched2 reporter, we resolve active Hh/Smo output to a narrow distal regenerate zone comprising pObs and adjacent motile basal epidermal cells. This Hh/Smo activity is driven by epidermal Sonic hedgehog a (Shha) rather than Ob-derived Indian hedgehog a (Ihha), which nevertheless functions atypically to support bone maturation. Using BMS-833923, a uniquely effective Smo inhibitor, and high-resolution imaging, we show that Shha/Smo is functionally dedicated to ray branching during fin regeneration. Hh/Smo activation enables transiently divided clusters of Shha-expressing epidermis to escort pObs into similarly split groups. This co-movement likely depends on epidermal cellular protrusions that directly contact pObs only where an otherwise occluding basement membrane remains incompletely assembled. Progressively separated pObs pools then continue regenerating independently to collectively re-form a now branched skeletal structure.
© 2017. Published by The Company of Biologists Ltd.

Entities:  

Keywords:  BMS-833923; Basal epidermis; Basement membrane; Bone patterning; Calcification; Caudal fins; Cyclopamine; Hedgehog signaling; Indian hedgehog; Osteoblasts; Ray branching; Regeneration; Smoothened inhibitor; Sonic hedgehog; Zebrafish

Mesh:

Substances:

Year:  2017        PMID: 28351866      PMCID: PMC5399624          DOI: 10.1242/dev.143792

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  59 in total

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