Multipotent progenitors resident in the skeletal muscle interstitium exhibit robust BMP‐dependent osteogenic activity and mediate heterotopic ossification

MN Wosczyna, AA Biswas, CA Cogswell… - Journal of Bone and …, 2012 - academic.oup.com
MN Wosczyna, AA Biswas, CA Cogswell, DJ Goldhamer
Journal of Bone and Mineral Research, 2012academic.oup.com
Heterotopic ossification is a debilitating condition that can result from traumatic injury,
surgery, or genetic disease. We investigated the cellular origins of heterotopic
skeletogenesis in the mouse using lineage tracing and bioassays of heterotopic ossification
based on intramuscular transplantation. We identified, characterized, and purified a tissue‐
resident stem/progenitor cell population that exhibits robust osteogenic potential and
represents a major cell‐of‐origin for heterotopic ossification. These progenitors reside in the …
Abstract
Heterotopic ossification is a debilitating condition that can result from traumatic injury, surgery, or genetic disease. We investigated the cellular origins of heterotopic skeletogenesis in the mouse using lineage tracing and bioassays of heterotopic ossification based on intramuscular transplantation. We identified, characterized, and purified a tissue‐resident stem/progenitor cell population that exhibits robust osteogenic potential and represents a major cell‐of‐origin for heterotopic ossification. These progenitors reside in the interstitium of skeletal muscle and other tissues, and are distinct from the endothelium, which does not exhibit osteogenic activity in response to bone morphogenetic protein 2 (BMP2) stimulation. Intramuscular transplantation, together with clonal analysis in culture, revealed that these progenitors are multipotent, exhibiting the capacity for both BMP‐dependent skeletogenic differentiation and spontaneous adipogenic differentiation. Identifying the cells‐of‐origin responsible for heterotopic ossification provides a potential therapeutic target to treat, mitigate, or prevent this disabling condition. © 2012 American Society for Bone and Mineral Research.
Oxford University Press