Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation
Alveolar bone is not spontaneously regenerated following trauma or periodontitis. We previously proposed an animal model for new alveolar bone regeneration therapy based on the non-viral BMP-2/7 gene expression vector and in vivo electroporation, which induced the formation of new alveolar bone ove...
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doaj-8f6321440fba48b99cbe0c5b4ea924672020-11-25T03:48:42ZengPAGEPress PublicationsEuropean Journal of Histochemistry 1121-760X2038-83062018-08-0162310.4081/ejh.2018.2947Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporationMariko Kawai0Yohei Kataoka1Junya Sonobe2Hiromitsu Yamamoto3Hiroki Maruyama4Toshio Yamamoto5Kazuhisa Bessho6Kiyoshi Ohura7Osaka Dental University, Department of PharmacologyOkayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, Department of Oral MorphologyDepartment of Oral and Maxillofacial Surgery, Kyoto UniversityDepartment of Oral and Maxillofacial Surgery, Kyoto UniversityNiigata University Graduate School of Medicine and Dental Sciences, Department of Clinical NephroscienceDepartment of Oral Morphology, Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical SciencesDepartment of Oral and Maxillofacial Surgery, Kyoto UniversityDepartment of Pharmacology, Osaka Dental University Alveolar bone is not spontaneously regenerated following trauma or periodontitis. We previously proposed an animal model for new alveolar bone regeneration therapy based on the non-viral BMP-2/7 gene expression vector and in vivo electroporation, which induced the formation of new alveolar bone over the course of a week. Here, we analysed alveolar bone during a period of three weeks following gene transfer to periodontal tissue. Non-viral plasmid vector pCAGGS-BMP-2/7 or pCAGGS control was injected into palatal periodontal tissue of the first molar of the rat maxilla and immediately electroporated with 32 pulses of 50 V for 50 msec. Over the following three weeks, rats were double bone-stained by calcein and tetracycline every three days and mineral apposition rates (MAR) were measured. Double bone-staining revealed that MAR of alveolar bone was as similar level three days before BMP-2/7 gene transfer as three days after gene transfer. However, from 3 to 6 days, 6 to 9 days, 9 to 12 days, 12 to 15 days, 15 to 18 days, and 18 to 20 days after, MARs were significantly higher than prior to gene transfer. Our proposed gene therapy for alveolar bone regeneration combining non-viral BMP-2/7 gene expression vector and in vivo electroporation could increase alveolar bone regeneration potential in the targeted area for up to three weeks. https://ejh.it/index.php/ejh/article/view/2947BMPgene transferin vivo electroporationalveolar bonehistomorphometry |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Mariko Kawai Yohei Kataoka Junya Sonobe Hiromitsu Yamamoto Hiroki Maruyama Toshio Yamamoto Kazuhisa Bessho Kiyoshi Ohura |
spellingShingle |
Mariko Kawai Yohei Kataoka Junya Sonobe Hiromitsu Yamamoto Hiroki Maruyama Toshio Yamamoto Kazuhisa Bessho Kiyoshi Ohura Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation European Journal of Histochemistry BMP gene transfer in vivo electroporation alveolar bone histomorphometry |
author_facet |
Mariko Kawai Yohei Kataoka Junya Sonobe Hiromitsu Yamamoto Hiroki Maruyama Toshio Yamamoto Kazuhisa Bessho Kiyoshi Ohura |
author_sort |
Mariko Kawai |
title |
Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation |
title_short |
Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation |
title_full |
Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation |
title_fullStr |
Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation |
title_full_unstemmed |
Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation |
title_sort |
analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of bmp-2/7 gene via in vivo electroporation |
publisher |
PAGEPress Publications |
series |
European Journal of Histochemistry |
issn |
1121-760X 2038-8306 |
publishDate |
2018-08-01 |
description |
Alveolar bone is not spontaneously regenerated following trauma or periodontitis. We previously proposed an animal model for new alveolar bone regeneration therapy based on the non-viral BMP-2/7 gene expression vector and in vivo electroporation, which induced the formation of new alveolar bone over the course of a week. Here, we analysed alveolar bone during a period of three weeks following gene transfer to periodontal tissue. Non-viral plasmid vector pCAGGS-BMP-2/7 or pCAGGS control was injected into palatal periodontal tissue of the first molar of the rat maxilla and immediately electroporated with 32 pulses of 50 V for 50 msec. Over the following three weeks, rats were double bone-stained by calcein and tetracycline every three days and mineral apposition rates (MAR) were measured. Double bone-staining revealed that MAR of alveolar bone was as similar level three days before BMP-2/7 gene transfer as three days after gene transfer. However, from 3 to 6 days, 6 to 9 days, 9 to 12 days, 12 to 15 days, 15 to 18 days, and 18 to 20 days after, MARs were significantly higher than prior to gene transfer. Our proposed gene therapy for alveolar bone regeneration combining non-viral BMP-2/7 gene expression vector and in vivo electroporation could increase alveolar bone regeneration potential in the targeted area for up to three weeks.
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topic |
BMP gene transfer in vivo electroporation alveolar bone histomorphometry |
url |
https://ejh.it/index.php/ejh/article/view/2947 |
work_keys_str_mv |
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