Chondrocytes Are Released As Viable Cells During Cartilage Resorption Associated with the Formation of Intrachondral Canals in the Rat Tibial Epiphysis

Overview

Journal Cell Tissue Res

Specialties Anatomy & Histology
Cell Biology

Date 2005 Apr 23

PMID 15846519

Citations 14

Authors

Jesus Alvarez

Lorena Costales

Alfonso Lopez-Muniz

Jose M Lopez

Affiliations

Soon will be listed here.

Abstract

The development of cartilage canals is the first event of the ossification of the epiphyses in mammals. Canal formation differs from vascular invasion during primary ossification, since the former involves resorption of resting cartilage and is uncoupled from bone deposition. To learn more about the fate of resorbed chondrocytes during this process, we have carried out structural, cell proliferation, and in situ hybridization studies during the first stages of ossification of the rat tibial proximal epiphysis. Results concerning the formation of the cartilage canals implied the release of resting chondrocytes from the cartilage matrix to the canal cavity. Released chondrocytes had a well-preserved structure, expressed type-II collagen, and maintained the capacity to divide. All these data suggested that chondrocytes released into the canals remained viable for a specific time. Analysis of the proliferative activity at different regions of the cartilage canals showed that the percentage of proliferative chondrocytes at areas of active cartilage resorption was significantly higher than that in zones of low resorption. These results are consistent with the hypothesis that resting chondrocytes surrounding canals have a role in supplying cells for the development of the secondary ossification center. Since released chondrocytes are at an early stage of differentiation greatly preceding their entry into the apoptotic pathway and are exposed to a specific matrix, cellular, and humoral microenvironment, they might differentiate to other cell types and contribute to the ossification of the epiphysis.

Citing Articles

The Formation of the Epiphyseal Bone Plate Occurs via Combined Endochondral and Intramembranous-Like Ossification.

Fernandez-Iglesias A, Fuente R, Gil-Pena H, Alonso-Duran L, Santos F, Lopez J Int J Mol Sci. 2021; 22(2).

PMID: 33477458 PMC: 7830543. DOI: 10.3390/ijms22020900.

Prolyl Hydroxylase Domain-Containing Protein 2 (Phd2) Regulates Chondrocyte Differentiation and Secondary Ossification in Mice.

Cheng S, Aghajanian P, Pourteymoor S, Alarcon C, Mohan S Sci Rep. 2016; 6:35748.

PMID: 27775044 PMC: 5075779. DOI: 10.1038/srep35748.

Cartilage canals in newborn dogs: histochemical and immunohistochemical findings.

Di Giancamillo A, Andreis M, Taini P, Veronesi M, Di Giancamillo M, Modina S Eur J Histochem. 2016; 60(3):2701.

PMID: 27734993 PMC: 5062639. DOI: 10.4081/ejh.2016.2701.

Regulation of Long Bone Growth in Vertebrates; It Is Time to Catch Up.

Rosello-Diez A, Joyner A Endocr Rev. 2015; 36(6):646-80.

PMID: 26485225 PMC: 4702496. DOI: 10.1210/er.2015-1048.

IGF-I Signaling in Osterix-Expressing Cells Regulates Secondary Ossification Center Formation, Growth Plate Maturation, and Metaphyseal Formation During Postnatal Bone Development.

Wang Y, Menendez A, Fong C, ElAlieh H, Kubota T, Long R J Bone Miner Res. 2015; 30(12):2239-48.

PMID: 26011431 PMC: 9042009. DOI: 10.1002/jbmr.2563.