AI Article Synopsis

  • Human osteogenic progenitors, often referred to as mesenchymal stem cells (MSCs), are a diverse population not clearly defined, with certain human pericytes able to turn into bone-forming osteoblasts.
  • This study focused on the differentiation capabilities of CD146 human pericytes from different tissues and aimed to identify key cell surface markers indicative of osteoblast potential.
  • Findings showed that periosteal pericytes were much better at forming bone compared to soft tissue pericytes, and the CXCR4 signaling pathway was crucial for this process, suggesting that targeting CXCR4 could enhance strategies in skeletal tissue engineering.

Article Abstract

Human osteogenic progenitors are not precisely defined, being primarily studied as heterogeneous multipotent cell populations and termed mesenchymal stem cells (MSCs). Notably, select human pericytes can develop into bone-forming osteoblasts. Here, we sought to define the differentiation potential of CD146 human pericytes from skeletal and soft tissue sources, with the underlying goal of defining cell surface markers that typify an osteoblastogenic pericyte. CD146CD31CD45 pericytes were derived by fluorescence-activated cell sorting from human periosteum, adipose, or dermal tissue. Periosteal CD146CD31CD45 cells retained canonical features of pericytes/MSC. Periosteal pericytes demonstrated a striking tendency to undergo osteoblastogenesis in vitro and skeletogenesis in vivo, while soft tissue pericytes did not readily. Transcriptome analysis revealed higher CXCR4 signaling among periosteal pericytes in comparison to their soft tissue counterparts, and CXCR4 chemical inhibition abrogated ectopic ossification by periosteal pericytes. Conversely, enrichment of CXCR4 pericytes or stromal cells identified an osteoblastic/non-adipocytic precursor cell. In sum, human skeletal and soft tissue pericytes differ in their basal abilities to form bone. Diversity exists in soft tissue pericytes, however, and CXCR4 pericytes represent an osteoblastogenic, non-adipocytic cell precursor. Indeed, enrichment for CXCR4-expressing stromal cells is a potential new tactic for skeletal tissue engineering.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7244476PMC
http://dx.doi.org/10.1038/s41413-020-0097-0DOI Listing

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