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Histochemical assessment of osteoclast-like giant cells in Rankl mice. | LitMetric

AI Article Synopsis

  • The study investigates mice lacking the Rankl gene to determine if they have progenitor cells that can develop into osteoclasts, despite the absence of RANK/RANKL signaling.
  • Researchers used immunohistochemistry and transmission electron microscopy to analyze the tibiae and femora of these mice, observing osteoclast-like giant cells that engage with the mineralized extracellular matrix.
  • Results indicate that while these giant cells exhibit some characteristics of osteoclasts, such as interaction with osteoblasts, they do not possess all classical markers of mature osteoclasts, suggesting a partial acquisition of osteoclastic traits.

Article Abstract

Objectives: We examined mice with gene deletion of Receptor activator of nuclear factor-κB (Rank) ligand (Rankl) to histologically clarify whether they contained progenitor cells committed to osteoclastic differentiation up to the stage requiring RANK/RANKL signaling.

Methods: The tibiae and femora of ten-week-old male wild-type, c-fos, and Rankl mice were used for immunohistochemistry and transmission electron microscopy (TEM).

Results: In Rankl mice, we observed osteoclast-like giant cells, albeit in low numbers, with single or two nuclei, engulfing the mineralized extracellular matrix. TEM revealed that these giant cells contained large numbers of mitochondria, vesicles/vacuoles, and clear zone-like structures but no ruffled borders. They often engulfed fragmented bony/cartilaginous components of the extracellular matrix that had been degraded. Additionally, osteoclast-like giant cells exhibited immunoreactivity for vacuolar H-ATPase, galectin-3, and siglec-15 but not for tartrate-resistant acid phosphatase, cathepsin K, or MMP-9, all of which are classical hallmarks of osteoclasts. Furthermore, osteoclast-like giant cells were ephrinB2-positive as they were near EphB4-positive osteoblasts that are also positive for alkaline phosphatase and Runx2 in Rankl mice. Unlike Rankl mice, c-fos mice lacking osteoclast progenitors and mature osteoclasts had no ephrinB2-positive osteoclast-like cells or alkaline phosphatase-positive/Runx2-reactive osteoblasts. This suggests that similar to authentic osteoclasts, osteoclast-like giant cells might have the potential to activate osteoblasts in Rankl mice.

Conclusions: It seems plausible that osteoclast-like giant cells may have acquired some osteoclastic traits and the ability to resorb mineralized matrices even when the absence of RANK/RANKL signaling halted the osteoclastic differentiation cascade.

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Source
http://dx.doi.org/10.1016/j.job.2023.04.003DOI Listing

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