Clinical effects of balofloxacin on dental and oral surgical infectious diseases
The clinical effects of a new oral quinolone, balofloxacin (BLFX), on infectious diseases in the fields of dentistry and oral surgery were investigated. The subjects were 156 patients (75 males and 81 females) consisting of 63 with periodontitis, 41 with pericoronitis and 52 with osteitis of jaw. Wi...
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Published in | Japanese Journal of Chemotherapy Vol. 43; no. Supplement5; pp. 479 - 489 |
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Main Authors | , , , , , , , , , , , , , |
Format | Journal Article |
Language | Japanese |
Published |
Japanese Society of Chemotherapy
1995
公益社団法人 日本化学療法学会 |
Subjects | |
Online Access | Get full text |
ISSN | 1340-7007 1884-5886 |
DOI | 10.11250/chemotherapy1995.43.Supplement5_479 |
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Abstract | The clinical effects of a new oral quinolone, balofloxacin (BLFX), on infectious diseases in the fields of dentistry and oral surgery were investigated. The subjects were 156 patients (75 males and 81 females) consisting of 63 with periodontitis, 41 with pericoronitis and 52 with osteitis of jaw. With the exception of 10 severe cases, the infectious diseases were mild (75 patients) or moderate (71 patients). The patients were given the drug at a daily dose of 200 mg (in 2 divisions or at one time) or 400 mg (in 2 divisions) for 3-12 days. According to the Drug Efficacy Criteria, the efficacy rate was 82.5%(52/63) for periodonitis, and 87.8%(36/41) for pericoronitis and 94.2%(49/52) for osteitis of jaw, for an overall efficacy rate of 87.8%. The efficacy rate was not influenced by the severity of infectious symptoms, the presence or absence of surgical treatment, or daily dose. The pyogenic bacteria isolated from 67 patients with closure abscess included 109 strains, consisting of 52 strains of aerobic grampositive bacteria, 8 strains of aerobic gram-negative bacteria and 49 strains of anaerobic bacteria. 100 (91.7%) of the 109 isolates were eradicated by BLFX treatment. Mild gastrointestinal symptoms, headache and drug eruption appeared as adverse events in 7 patients (4.4%), but all improved rapidly after the discontinuation of administration. Slight eosinophilia was observed in five patients and elevated LDH in one, as abnormal changes in clinical laboratory test values, but none were especially problematic in terms of safety. |
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AbstractList | The clinical effects of a new oral quinolone, balofloxacin (BLFX), on infectious diseases in the fields of dentistry and oral surgery were investigated. The subjects were 156 patients (75 males and 81 females) consisting of 63 with periodontitis, 41 with pericoronitis and 52 with osteitis of jaw. With the exception of 10 severe cases, the infectious diseases were mild (75 patients) or moderate (71 patients).The patients were given the drug at a daily dose of 200 mg (in 2 divisions or at one time) or 400 mg (in 2 divisions) for 3-12 days. According to the Drug Efficacy Criteria, the efficacy rate was 82.5%(52/63) for periodonitis, and 87.8%(36/41) for pericoronitis and 94.2%(49/52) for osteitis of jaw, for an overall efficacy rate of 87.8%. The efficacy rate was not influenced by the severity of infectious symptoms, the presence or absence of surgical treatment, or daily dose. The pyogenic bacteria isolated from 67 patients with closure abscess included 109 strains, consisting of 52 strains of aerobic grampositive bacteria, 8 strains of aerobic gram-negative bacteria and 49 strains of anaerobic bacteria. 100 (91.7%) of the 109 isolates were eradicated by BLFX treatment.Mild gastrointestinal symptoms, headache and drug eruption appeared as adverse events in 7 patients (4.4%), but all improved rapidly after the discontinuation of administration. Slight eosinophilia was observed in five patients and elevated LDH in one, as abnormal changes in clinical laboratory test values, but none were especially problematic in terms of safety.
歯科・口腔外科領域感染症を対象に新規経口用キノロン薬balofloxacin (BLFX) の臨床効果について検討した。患者は歯周組織炎63例, 歯冠周囲炎41例および顎炎52例の計156例 (男性75例, 女性81例) で, 重症10例以外は軽症 (75例) または中等症 (71例) の感染であった。患者は1日200mg (分2または分1) または400mg (分2) を3~12日間服用した。その結果, 効果判定基準による有効率は歯周組織炎82.5%(52/63例), 歯冠周囲炎87.8%(36/41例), 顎炎94.2%(49/52例) で, 全体では87.8%であった。この有効率は感染症状の重症度や外科的処置の有無, あるいは1日用量によってほとんど影響されなかった。閉鎖膿瘍を有する67症例より分離された起炎菌は好気性グラム陽性菌52株, 好気性グラム陰性菌8株および嫌気性菌49株の計109株で, そのうち100株 (91.7%) が消失した。副作用は軽い消化器症状や頭痛, 薬疹が7例 (4.4%) に発現したが.いずれも投薬中止または終了で速やかに回復した。臨床検査値異常変動も軽度の好酸球増多5例とLDH上昇1例のみで, 安全性上, 特に問題は認めなかった。 The clinical effects of a new oral quinolone, balofloxacin (BLFX), on infectious diseases in the fields of dentistry and oral surgery were investigated. The subjects were 156 patients (75 males and 81 females) consisting of 63 with periodontitis, 41 with pericoronitis and 52 with osteitis of jaw. With the exception of 10 severe cases, the infectious diseases were mild (75 patients) or moderate (71 patients). The patients were given the drug at a daily dose of 200 mg (in 2 divisions or at one time) or 400 mg (in 2 divisions) for 3-12 days. According to the Drug Efficacy Criteria, the efficacy rate was 82.5%(52/63) for periodonitis, and 87.8%(36/41) for pericoronitis and 94.2%(49/52) for osteitis of jaw, for an overall efficacy rate of 87.8%. The efficacy rate was not influenced by the severity of infectious symptoms, the presence or absence of surgical treatment, or daily dose. The pyogenic bacteria isolated from 67 patients with closure abscess included 109 strains, consisting of 52 strains of aerobic grampositive bacteria, 8 strains of aerobic gram-negative bacteria and 49 strains of anaerobic bacteria. 100 (91.7%) of the 109 isolates were eradicated by BLFX treatment. Mild gastrointestinal symptoms, headache and drug eruption appeared as adverse events in 7 patients (4.4%), but all improved rapidly after the discontinuation of administration. Slight eosinophilia was observed in five patients and elevated LDH in one, as abnormal changes in clinical laboratory test values, but none were especially problematic in terms of safety. |
Author | Ohta, Yoshihide Kato, Hisashi Busujima, Yasunobu Yamamoto, Tadashi Tomita, Fumisada Kaneko, Akihiro Karakida, Kazunari Naitoh, Hiroyuki Yamane, Nobuo Kanno, Kazuyuki Morihana, Takefumi Shiiki, Kazuo Takakura, Atsushi Sasaki, Jiro |
Author_FL | 佐々木 次郎 唐木田 一成 太田 嘉英 毒島 保信 金子 明寛 加藤 久視 椎木 一雄 菅野 和幸 森鼻 健史 山本 忠 高倉 淳 内藤 博之 富田 文貞 山根 伸夫 |
Author_FL_xml | – sequence: 1 fullname: 佐々木 次郎 – sequence: 2 fullname: 唐木田 一成 – sequence: 3 fullname: 山根 伸夫 – sequence: 4 fullname: 太田 嘉英 – sequence: 5 fullname: 毒島 保信 – sequence: 6 fullname: 高倉 淳 – sequence: 7 fullname: 椎木 一雄 – sequence: 8 fullname: 菅野 和幸 – sequence: 9 fullname: 内藤 博之 – sequence: 10 fullname: 金子 明寛 – sequence: 11 fullname: 富田 文貞 – sequence: 12 fullname: 加藤 久視 – sequence: 13 fullname: 森鼻 健史 – sequence: 14 fullname: 山本 忠 |
Author_xml | – sequence: 1 fullname: Yamane, Nobuo organization: Department of Oral Surgery, School of Medicine, Tokai University – sequence: 1 fullname: Naitoh, Hiroyuki organization: Department of Dentistry and Oral Surgery, Iwaki Kyoritsu General Hospital – sequence: 1 fullname: Morihana, Takefumi organization: Department of Dentistry and Oral Surgery, Hitachi Totsuka General Hospital – sequence: 1 fullname: Kato, Hisashi organization: Department of Dentistry and Oral Surgery, Ashikaga Red Cross Hospital – sequence: 1 fullname: Yamamoto, Tadashi organization: Department of Dentistry and Oral Surgery, Toyohashi municipal Hospital – sequence: 1 fullname: Kanno, Kazuyuki organization: Department of Dentistry and Oral Surgery, Iwaki Kyoritsu General Hospital – sequence: 1 fullname: Tomita, Fumisada organization: Department of Dentistry and Oral Surgery, Ashikaga Red Cross Hospital – sequence: 1 fullname: Kaneko, Akihiro organization: Department of Dentistry and Oral Surgery, Ashikaga Red Cross Hospital – sequence: 1 fullname: Busujima, Yasunobu organization: Department of Oral Surgery, School of Medicine, Tokai University – sequence: 1 fullname: Sasaki, Jiro organization: Department of Oral Surgery, School of Medicine, Tokai University – sequence: 1 fullname: Shiiki, Kazuo organization: Department of Dentistry and Oral Surgery, Iwaki Kyoritsu General Hospital – sequence: 1 fullname: Karakida, Kazunari organization: Department of Oral Surgery, School of Medicine, Tokai University – sequence: 1 fullname: Takakura, Atsushi organization: Department of Oral Surgery, School of Medicine, Tokai University – sequence: 1 fullname: Ohta, Yoshihide organization: Department of Oral Surgery, School of Medicine, Tokai University |
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References | 3) Iwasaki H, Miyazaki S, Tsuji A, Yamaguchi K, Goto S: In vitro and in vivo antibacterial activities of Q-35, a novel fluoroquinolone. Chemotherapy 41: 100-112, 1995 7) 佐々木次郎, 他 (12施設および関連施設): 口腔領域感染症に対するT-3262 (Tosufloxacin tosilate) の臨床的検討. 歯薬療法 8: 5-15, 1989 8) 佐々木次郎, 他 (16施設および関連施設): 口腔外科領域感染症に対するNY-198 (Lomenoxacin) の投与量評価のための比較試験成績. 歯薬療法 7: 92-111, 1988 9) 佐々木次郎, 他 (13施設および関連施設): 口腔外科領域感染症に対するオフロキサシンの臨床的検討. 歯薬療法 5: 78-86, 1986 10) 佐々木次郎, 他 (11施設および関連施設): Levofloxacinの歯科, 口腔外科領域感染症に対する臨床的検討. Chemotherapy 40: 379-391, 1992 5) 高井宏, 久野吉雄, 道健一, 佐々木次郎: 歯性感染症に対する抗生物質の効果判定基準について. 歯薬療法 1: 122-160, 1982 11) 佐々木次郎, 他 (13施設および関連施設): 口腔外科領域感染症からの検出菌および薬剤感受性についての検討. 歯薬療法 5: 87-96, 1986 1) Matsumoto M, Kojima K, Nagano H, Matsubara S, Yokota T: Photostability and biological activity of fluoroquinolones substituted at the 8 position after UV irradiation. Antimicrob Agents Chemother 36: 1715-1719, 1992 4) 佐々木次郎, 唐木田一成, 山根伸夫, 太田嘉英, 毒島保信, 高倉淳, 金子明寛, 富田文貞, 加藤久視: 新規経口用キノロン薬balofloxacinの口腔細菌に対する抗菌力と唾液・抜歯創内移行について. 日化療会誌 43 (S-5): 490-494, 1995 6) 日本化学療法学会: 最小発育阻止濃度 (MIC) 測定法再改訂について. Chemotherapy 29: 76-79, 1981 2) Ito T, Otsuki M, Nishino T: In vitro antibacterial activity of Q-35, a new fluoroquinolone. Antimicrob Agents Chemother 36: 1708-1714, 1992 |
References_xml | – reference: 4) 佐々木次郎, 唐木田一成, 山根伸夫, 太田嘉英, 毒島保信, 高倉淳, 金子明寛, 富田文貞, 加藤久視: 新規経口用キノロン薬balofloxacinの口腔細菌に対する抗菌力と唾液・抜歯創内移行について. 日化療会誌 43 (S-5): 490-494, 1995 – reference: 11) 佐々木次郎, 他 (13施設および関連施設): 口腔外科領域感染症からの検出菌および薬剤感受性についての検討. 歯薬療法 5: 87-96, 1986 – reference: 5) 高井宏, 久野吉雄, 道健一, 佐々木次郎: 歯性感染症に対する抗生物質の効果判定基準について. 歯薬療法 1: 122-160, 1982 – reference: 8) 佐々木次郎, 他 (16施設および関連施設): 口腔外科領域感染症に対するNY-198 (Lomenoxacin) の投与量評価のための比較試験成績. 歯薬療法 7: 92-111, 1988 – reference: 3) Iwasaki H, Miyazaki S, Tsuji A, Yamaguchi K, Goto S: In vitro and in vivo antibacterial activities of Q-35, a novel fluoroquinolone. Chemotherapy 41: 100-112, 1995 – reference: 10) 佐々木次郎, 他 (11施設および関連施設): Levofloxacinの歯科, 口腔外科領域感染症に対する臨床的検討. Chemotherapy 40: 379-391, 1992 – reference: 6) 日本化学療法学会: 最小発育阻止濃度 (MIC) 測定法再改訂について. Chemotherapy 29: 76-79, 1981 – reference: 7) 佐々木次郎, 他 (12施設および関連施設): 口腔領域感染症に対するT-3262 (Tosufloxacin tosilate) の臨床的検討. 歯薬療法 8: 5-15, 1989 – reference: 2) Ito T, Otsuki M, Nishino T: In vitro antibacterial activity of Q-35, a new fluoroquinolone. Antimicrob Agents Chemother 36: 1708-1714, 1992 – reference: 9) 佐々木次郎, 他 (13施設および関連施設): 口腔外科領域感染症に対するオフロキサシンの臨床的検討. 歯薬療法 5: 78-86, 1986 – reference: 1) Matsumoto M, Kojima K, Nagano H, Matsubara S, Yokota T: Photostability and biological activity of fluoroquinolones substituted at the 8 position after UV irradiation. Antimicrob Agents Chemother 36: 1715-1719, 1992 |
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Title | Clinical effects of balofloxacin on dental and oral surgical infectious diseases |
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