Bisphosphonate‐induced reactive oxygen species inhibit proliferation and migration of oral fibroblasts: A pathogenesis of bisphosphonate‐related osteonecrosis of the jaw - 九大コレクション | 九州大学附属図書館

＜学術雑誌論文＞
Bisphosphonate‐induced reactive oxygen species inhibit proliferation and migration of oral fibroblasts: A pathogenesis of bisphosphonate‐related osteonecrosis of the jaw

作成者	作成者名 Taniguchi, Naomi タニグチ, ナオミ所属機関所属機関名 Division of Pathological Biochemistry, Tottori University Faculty of Medicine 鳥取大学医学部所属機関所属機関名 Division of Oral and Maxillofacial Biopathological Surgery, Tottori University Faculty of Medicine 鳥取大学医学部
	著者識別子 40325006 作成者名 Osaki, Mitsuhiko 尾崎, 充彦オサキ, ミツヒロ所属機関所属機関名 Division of Pathological Biochemistry, Tottori University Faculty of Medicine 鳥取大学医学部所属機関所属機関名 Chromosomal Engineering Research Center, Tottori University 鳥取大学染色体工学研究センター
	作成者名 Onuma, Kunishige オヌマ, クニシゲ所属機関所属機関名 Division of Pathological Biochemistry, Tottori University Faculty of Medicine
	著者識別子 K008593 作成者名 Ishikawa, Mizuho 石川, 瑞穂イシカワ, ミズホ所属機関所属機関名 Division of Pathological Biochemistry, Tottori University Faculty of Medicine 鳥取大学医学部
	著者識別子 20093635 作成者名 Ryoke, Kazuo 領家, 和男リョウケ, カズオ所属機関所属機関名 Division of Oral and Maxillofacial Biopathological Surgery, Tottori University Faculty of Medicine 鳥取大学医学部
	作成者名 Kodani, Isamu 小谷, 勇コダニ, イサム所属機関所属機関名 Division of Oral and Maxillofacial Biopathological Surgery, Tottori University Faculty of Medicine 鳥取大学医学部
	著者識別子 00250423 0000-0003-4733-1037 作成者名 Okada, Futoshi 岡田, 太オカダ, フトシ所属機関所属機関名 Division of Pathological Biochemistry, Tottori University Faculty of Medicine 鳥取大学医学部所属機関所属機関名 Chromosomal Engineering Research Center, Tottori University 鳥取大学染色体工学研究センター
本文言語	英語
出版者	Wiley
発行日	2020-01-16
収録物名	Journal of Periodontology
巻	91
号	7
開始ページ	947
終了ページ	955
アクセス権	metadata only access
関連DOI	https://doi.org/10.1002/JPER.19-0385
関連URI
概要	Background The onset mechanism for bisphosphonate-related osteonecrosis of the jaw (BRONJ) has been reported, with a focus on bone remodeling, biofilm formation, and epithelial cell proliferation and m...igration. However, the involvement of stromal cells, especially fibroblasts, in the oral cavity is unclear. Therefore, this study was focused on how bisphosphonates (BPs) affect orthotopic periodontal ligament fibroblasts from the viewpoint of oxidative stress compared with ectopically obtained fibroblasts. Methods Normal human periodontal ligament fibroblasts (HPdLFs) and normal human dermal fibroblasts (NHDFs) were used to gain insight into the functional differences in sensitivity and reactions to BPs. Cell growth assay, measurement of reactive oxygen species (ROS) and nitric oxide (NO) production, and wound-healing assay in vitro were performed. Maxillary first molars were extracted in C57BL/6 mice and either BP, N-acetyl-cysteine (NAC), and BP or saline were administered. Results BP-induced IC_<50> values were significantly lower in HPdLFs (30.6 µM) than in NHDFs (109.7 µM). BP resulted in an increase in ROS, but not NO generation in HPdLFs. BPs also inhibited proliferation and migration of HPdLFs but not NHDFs, while the addition of a ROS inhibitor, NAC, reversed those inhibitions. A BRONJ mouse model in which BP was administered and then the tooth was extracted, impaired wound healing of the socket was observed. When NAC was administered before tooth extraction, wound healing was significantly improved. Conclusion These results suggest that BP causes fibroblasts obtained from the oral cavity but not from skin to generate ROS and that the subsequent ROS-mediated inhibition of fibroblast growth and migration definitely delays wound healing, thereby contributing to BRONJ pathogenesis.続きを見る

詳細

PISSN	0022-3492
EISSN	1943-3670
NCID	AA00704406
レコードID	7178695
主題	antioxidants
	bisphosphonates
	etiology, fibroblasts
	periodontal diseases
	reactive oxygen species
タイプ	ORIGINAL ARTICLE
助成情報	助成機関名 Ministry of Education, Culture, Sports, Science and Techonology-Japan 文部科学省研究課題番号 26462837 研究課題名 A study on mechanism of bisphosphonate-related infection of the jaw . ビスフォスフォネート(BP)の顎骨の感染メカニズムの解明
登録日	2024.05.22
更新日	2024.05.22