TY - JOUR
T1 - Regeneration of the elbow joint in the developing chick embryo recapitulates development
AU - Özpolat, B. Duygu
AU - Zapata, Mariana
AU - Daniel Frugé, John
AU - Coote, Jeffrey
AU - Lee, Jangwoo
AU - Muneoka, Ken
AU - Anderson, Rosalie
N1 - Funding Information:
We thank members of the Muneoka and Anderson Laboratories for critical reading and comments on the manuscript. This work was supported by funding from NIH - P01HD022610 (KM), ARO - W911NF0910305 (KM) and the John L. and Mary Wright Ebaugh Endowment Fund at Tulane University and NIHR 15 HD060012-01 (RA) and 3R15HD060012-01S1 (RA), and the Loyola University Mullahy Biology Endowed Fund for Undergraduate Research .
PY - 2012/12/15
Y1 - 2012/12/15
N2 - Synovial joints are among the most important structures that give us complex motor abilities as humans. Degenerative joint diseases, such as arthritis, cause loss of normal joint functioning and affect over 40 million people in the USA and approximately 350 million people worldwide. Therapies based on regenerative medicine hold the promise of effectively repairing or replacing damaged joints permanently. Here, for the first time, we introduce a model for synovial joint regeneration utilizing the chick embryo. In this model, a block of tissue that contains the prospective elbow is excised, leaving a window with strips of anterior and posterior tissue intact (window excision, WE). In contrast, we also slice out the same area containing the elbow and the distal piece of the limb is pinned back onto the stump (slice excision, SE). Interestingly, when the elbow is removed via WE, regeneration of the joint takes place, whereas the elbow joint does not regenerate following SE. In order to investigate whether the regeneration response recapitulates the developmental program of forming joints, we used GDF-5 and Autotaxin (Atx) as joint tissue specific markers, and Sox-9 and Col-9 as cartilage markers for in situ hybridization on sections at different time points after WE and SE surgeries. Re-expression of GDF-5 and Atx is observed in the WE samples by 60 h after surgery. In contrast, the majority of the samples that underwent SE surgery did not express GDF-5 and Atx. Also, in SE fusion of cartilage elements takes place and the joint interzone does not form. This is indicated by continuous Col-9 expression in SE limbs, whereas Col-9 is downregulated at the joint interzone in the regenerating WE samples. This order and pattern of gene expression observed in regenerates is similar to the development of a joint suggesting that regeneration recapitulates development at the molecular level. This model defines some of the conditions required for inducing joint regeneration in an otherwise nonregenerating environment. This knowledge can be useful for designing new therapeutic approaches for joint loss or for conditions affecting joint integrity in humans.
AB - Synovial joints are among the most important structures that give us complex motor abilities as humans. Degenerative joint diseases, such as arthritis, cause loss of normal joint functioning and affect over 40 million people in the USA and approximately 350 million people worldwide. Therapies based on regenerative medicine hold the promise of effectively repairing or replacing damaged joints permanently. Here, for the first time, we introduce a model for synovial joint regeneration utilizing the chick embryo. In this model, a block of tissue that contains the prospective elbow is excised, leaving a window with strips of anterior and posterior tissue intact (window excision, WE). In contrast, we also slice out the same area containing the elbow and the distal piece of the limb is pinned back onto the stump (slice excision, SE). Interestingly, when the elbow is removed via WE, regeneration of the joint takes place, whereas the elbow joint does not regenerate following SE. In order to investigate whether the regeneration response recapitulates the developmental program of forming joints, we used GDF-5 and Autotaxin (Atx) as joint tissue specific markers, and Sox-9 and Col-9 as cartilage markers for in situ hybridization on sections at different time points after WE and SE surgeries. Re-expression of GDF-5 and Atx is observed in the WE samples by 60 h after surgery. In contrast, the majority of the samples that underwent SE surgery did not express GDF-5 and Atx. Also, in SE fusion of cartilage elements takes place and the joint interzone does not form. This is indicated by continuous Col-9 expression in SE limbs, whereas Col-9 is downregulated at the joint interzone in the regenerating WE samples. This order and pattern of gene expression observed in regenerates is similar to the development of a joint suggesting that regeneration recapitulates development at the molecular level. This model defines some of the conditions required for inducing joint regeneration in an otherwise nonregenerating environment. This knowledge can be useful for designing new therapeutic approaches for joint loss or for conditions affecting joint integrity in humans.
KW - Chick limb regeneration
KW - Elbow development
KW - Elbow regeneration
KW - Joint development
KW - Joint regeneration
KW - Limb regeneration
UR - http://www.scopus.com/inward/record.url?scp=84868303263&partnerID=8YFLogxK
U2 - 10.1016/j.ydbio.2012.09.020
DO - 10.1016/j.ydbio.2012.09.020
M3 - Article
C2 - 23036343
AN - SCOPUS:84868303263
SN - 0012-1606
VL - 372
SP - 229
EP - 238
JO - Developmental Biology
JF - Developmental Biology
IS - 2
ER -