Literature DB >> 16980845

Differential gene expression between juvenile and adult dura mater: a window into what genes play a role in the regeneration of membranous bone.

Derrick C Wan1, Oliver O Aalami, Zhen Wang, Randall P Nacamuli, Florence Lorget, Rik Derynck, Michael T Longaker.   

Abstract

BACKGROUND: Although reossification of large calvarial defects is possible in children, adults lack this tissue engineering capacity. In this study, the authors compared the differences in gene expression between juvenile and adult dura mater using a mouse cDNA microarray with 42,000 unique elements.
METHODS: Non-suture-associated parietal bone was harvested from 6-day-old and 60-day-old mice. The dura mater was carefully dissected from the calvarial disk and snap-frozen. RNA was extracted from pooled dura mater for microarray analysis. The 25 most differentially expressed genes were listed, as were selected bone-related genes. In addition, quantitative real-time reverse-transcriptase polymerase chain reaction confirmation of selected genes-BMP-2, BMP-4, and BMP-7; and osteopontin (OP), osteocalcin (OC), and FGFR-1-was performed.
RESULTS: Juvenile dura mater expressed significantly greater amounts of BMP-2 and OP. Minimal difference in OC expression was observed between juvenile and adult dura mater. Extracellular matrix proteins (Col3a1, 5a1, 6a1, and fibronectin 1), osteoblast differentiation markers (Runx2/Cbfa1, Itm2a, and FGFR-1), and the growth factor Ptn were among other genes with greater expression in juvenile dura mater. Markers of osteoclasts (Acp5, MMP9, Ctsk) and the multiple candidate gene Ntrk2 were also expressed at higher levels in the juvenile dura mater.
CONCLUSIONS: These findings suggest a more differentiated osteoprogenitor population to exist along with a greater presence of osteoclasts in the juvenile dura mater relative to adults. In addition to establishing a baseline difference in gene expression between juvenile and adult dura mater, new genes potentially critical to the regenerative potential of juvenile calvaria were identified.

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Year:  2006        PMID: 16980845     DOI: 10.1097/01.prs.0000232366.23897.2b

Source DB:  PubMed          Journal:  Plast Reconstr Surg        ISSN: 0032-1052            Impact factor:   4.730


  8 in total

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2.  Molecular analysis of coronal perisutural tissues in a craniosynostotic rabbit model using polymerase chain reaction suppression subtractive hybridization.

Authors:  James J Cray; Phillip H Gallo; Emily L Durham; Joseph E Losee; Mark P Mooney; Sandeep Kathju; Gregory M Cooper
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3.  Transforming growth factor beta 1 augments calvarial defect healing and promotes suture regeneration.

Authors:  Sameer Shakir; Zoe M MacIsaac; Sanjay Naran; Darren M Smith; Michael R Bykowski; James J Cray; Timothy K Craft; Dan Wang; Lee Weiss; Phil G Campbell; Mark P Mooney; Joseph E Losee; Gregory M Cooper
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4.  Increased megakaryocytic proliferation, pro-platelet deposition and expression of fibrosis-associated factors in children with chronic myeloid leukaemia with bone marrow fibrosis.

Authors:  K Hussein; A Stucki-Koch; G Göhring; H Kreipe; M Suttorp
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Review 6.  Bone morphogenetic proteins in craniofacial surgery: current techniques, clinical experiences, and the future of personalized stem cell therapy.

Authors:  Kristofer E Chenard; Chad M Teven; Tong-Chuan He; Russell R Reid
Journal:  J Biomed Biotechnol       Date:  2012-11-20

7.  Vertical osteoconductivity of sputtered hydroxyapatite-coated mini titanium implants after dura mater elevation: Rabbit calvarial model.

Authors:  Xin Wang; Osama Zakaria; Marwa Madi; Shohei Kasugai
Journal:  J Tissue Eng       Date:  2015-06-30       Impact factor: 7.813

8.  BMP-IHH-mediated interplay between mesenchymal stem cells and osteoclasts supports calvarial bone homeostasis and repair.

Authors:  Yuxing Guo; Yuan Yuan; Ling Wu; Thach-Vu Ho; Junjun Jing; Hideki Sugii; Jingyuan Li; Xia Han; Jifan Feng; Chuanbin Guo; Yang Chai
Journal:  Bone Res       Date:  2018-10-17       Impact factor: 13.567

  8 in total

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