Clinical study of long-term treatment using erythromycin in chronic lower respiratory tract infection
In order to establish useful therapeutic methods in chronic lower respiratory tract infection, we carried out long-term tratment (12-41 months) of erythrymycin (EM) using dosages of 600-1, 200 mg/day. Thirteen cases with diffuse panbronchiolitis (DPB) were the subjects of this study. All patients co...
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| Published in | Japanese Journal of Chemotherapy Vol. 46; no. 7; pp. 239 - 247 |
|---|---|
| Main Authors | , , , , |
| Format | Journal Article |
| Language | Japanese |
| Published |
Japanese Society of Chemotherapy
1998
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/chemotherapy1995.46.239 |
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| Abstract | In order to establish useful therapeutic methods in chronic lower respiratory tract infection, we carried out long-term tratment (12-41 months) of erythrymycin (EM) using dosages of 600-1, 200 mg/day. Thirteen cases with diffuse panbronchiolitis (DPB) were the subjects of this study. All patients complained of large amounts of purulent sputum and DOE, and had decreasing of PO2 levels. Major infections of Haemophilus influenzae and Pseudomonas aeruginosa bacteria were detected by TTA before EM therapy. The clinical responses to treatment were markedly effective (1 case) effective (10 cases) and mildly effective (2 cases). Two cases infected by P. aeruginosa had effective responses to treatment. Improvement of QOL was noted in all cases, and no significant side effects were noted during the long-term treatment. Early intervention with EM treatment was required because the clinical responses were considered less efffective in cases with elevated PCO2. The causative bacteria of acute exacerbation during EM treatment were mainly H. influenzae or Streptococcus pneumoniae, which easily developed after viral infections of P. aeruginosa or in cases which bacteria can not be detected significant amounts from sputum. In erythromycin- ineffective patients, long-term clarithromycin treatment was found effective. EM therapy for DPB may be discontinued, when the clinical manifestations of disease (especially purulent sputum) disappear, and the diffuse, nodular opacities in chest roentgenogram almost completely resolve. We consider these results indicate that this therapy is a new and useful treatment for chronic lower respiratory tract infections. |
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| AbstractList | In order to establish useful therapeutic methods in chronic lower respiratory tract infection, we carried out long-term tratment (12-41 months) of erythrymycin (EM) using dosages of 600-1, 200 mg/day. Thirteen cases with diffuse panbronchiolitis (DPB) were the subjects of this study. All patients complained of large amounts of purulent sputum and DOE, and had decreasing of PO2 levels. Major infections of Haemophilus influenzae and Pseudomonas aeruginosa bacteria were detected by TTA before EM therapy. The clinical responses to treatment were markedly effective (1 case) effective (10 cases) and mildly effective (2 cases). Two cases infected by P. aeruginosa had effective responses to treatment. Improvement of QOL was noted in all cases, and no significant side effects were noted during the long-term treatment. Early intervention with EM treatment was required because the clinical responses were considered less efffective in cases with elevated PCO2. The causative bacteria of acute exacerbation during EM treatment were mainly H. influenzae or Streptococcus pneumoniae, which easily developed after viral infections of P. aeruginosa or in cases which bacteria can not be detected significant amounts from sputum. In erythromycin- ineffective patients, long-term clarithromycin treatment was found effective. EM therapy for DPB may be discontinued, when the clinical manifestations of disease (especially purulent sputum) disappear, and the diffuse, nodular opacities in chest roentgenogram almost completely resolve. We consider these results indicate that this therapy is a new and useful treatment for chronic lower respiratory tract infections. In order to establish useful therapeutic methods in chronic lower respiratory tract infection, we carried out long-term tratment (12-41 months) of erythrymycin (EM) using dosages of 600-1, 200 mg/day. Thirteen cases with diffuse panbronchiolitis (DPB) were the subjects of this study. All patients complained of large amounts of purulent sputum and DOE, and had decreasing of PO2 levels. Major infections of Haemophilus influenzae and Pseudomonas aeruginosa bacteria were detected by TTA before EM therapy. The clinical responses to treatment were markedly effective (1 case) effective (10 cases) and mildly effective (2 cases). Two cases infected by P. aeruginosa had effective responses to treatment. Improvement of QOL was noted in all cases, and no significant side effects were noted during the long-term treatment. Early intervention with EM treatment was required because the clinical responses were considered less efffective in cases with elevated PCO2. The causative bacteria of acute exacerbation during EM treatment were mainly H. influenzae or Streptococcus pneumoniae, which easily developed after viral infections of P. aeruginosa or in cases which bacteria can not be detected significant amounts from sputum. In erythromycin- ineffective patients, long-term clarithromycin treatment was found effective. EM therapy for DPB may be discontinued, when the clinical manifestations of disease (especially purulent sputum) disappear, and the diffuse, nodular opacities in chest roentgenogram almost completely resolve. We consider these results indicate that this therapy is a new and useful treatment for chronic lower respiratory tract infections. 難治性慢性下気道感染症に対する有用な治療法を確立するためにerythromycin (EM) 長期治療の臨床的検討を行った。対象はびまん性汎細気管支炎13例。全例多量の膿性痰と労作時呼吸困難, PaO2の低下を伴い, TTA検出菌はHaemophilus influenzaeとPseudomonas aeruginosaであった。EMの投与量は600~1,200mg/日, 投与期間は12~41か月であった。臨床効果は著効1例, 有効10例, やや有効2例で緑膿菌感染例2例も有効であった。QOLは全例に改善した。しかし治療前PaCO2の上昇していた症例では臨床効果は低く, EM長期治療の早期の開始が望まれた。長期投与による副作用はなかった。EM長期治療中の急性増悪はウイルス性上気道炎を契機におこり, 主な急性増悪菌はH. influenzaeかStreptococcus pneumoniaeであった。EM長期治療が無効症例にはclarithromycin長期投与が有効であった。EM長期治療の終了時期については。臨床症状 (特に膿性痰) が消失し, 胸部X線上びまん性粒状影が消失した時期にEM長期治療の終了を考慮してもよいと考えられる。以上から慢性下気道感染症に対するEM長期治療は有用な治療法である。 |
| Author | Konishi, Mitsuru Narita, Nobuhiro Maeda, Koichi Sawaki, Masayoshi Mikasa, Keiichi |
| Author_FL | 前田 光一 三笠 桂一 澤木 政好 成田 亘啓 古西 満 |
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| References | 11) 三笠桂一, 澤木政好, 古西満, 他慢性下気道感染症におけるエリスロマイシン治療のNatural Killer細胞活性に与える影響1こついて. 感染症誌63: 811-815, 1989 8) 善本英一郎, 澤木政好, 三笠桂一, 他: びまん性汎細気管支炎に対するErythromycin (EM) 長期治療申に発症したEM耐性肺炎球菌による急性増悪の症例に対する臨床的細菌学的検討. 感染症誌66: 737-742, 1992 7) 三笠桂一, 澤木政好, 喜多英二, 他: 慢性下気道感染症に対するErythromycin長期化学痰法の検討- 第5報7年以上の経過を観察しえた症例について-. 感染症誌66: 1390-1395, 1992 4) 稲富恵子: びまん性細気管支炎全国症例調査報告, 8予後. 厚生省特定疾患間質性肺疾患調査研究班, 昭和57年度研究報告書p.38-41 10) 三笠桂一, 喜多英, 澤木政好, 他: 細菌の細胞障害毒素産生と接着因子に及ぼすErythromycinの作用について. 感染症誌67: 648-653, 1993 9) Kita E, Sawaki M, Oku D, et al.: Suppression of virulence factors of Pseudomonas aeruginosa by Erythromycin. J. Antimicrob. Chemother. 27: 273-284, 1991 13) 前田光一, 澤木政好, 喜多上, 他: 慢性下気道感染症におけるマクロライド薬投与によるサイトカインの変動. 日化療会誌43: 825-829, 1995 14) Mikasa K, Kita E, Sawaki M, et al.: The antiinflammatory effect of erythromycin in zymosan-induced peritonitis of mice. J Antimicrob Chemother 30: 339-348, 1992 15) Mikasa K, Sawaki M, Kita E, et al.: Significant survival benefit to patients with advanced non-smallcell lung cancer from treatment with clan thromycin. Chemotherapy 43: 288-296, 1997 6) 三笠桂一, 澤木政好, 古西満, 他: 慢性下気道感染症に対するErythromycin長期化学療法の検討- 第3報投与期問3年以上の症例を中心に-. 感染症誌66: 561-567, 1992 2) 澤木政好, 三上理一郎, 国松幹和, 他: 慢性下気道感染症における細菌感染の実態一経時的経気管吸引法 (TTA) 施行例の検討から-. 感染症誌59: 389-395, 1985 12) Kita E, Sawaki M, Nishikawa F, et al.: Enhanced interleukin production after long term administration of Erythromycin stearate. Pharmacology 41: 177-183, 1990 3) 澤木政好, 三上理一郎, 三笠桂一, 他: 慢性下気道感染症におけるErythromycin長期化学療法の検討- 第一報: Amoxicillinとの対比-. 感染症誌60: 37-44, 1986 5) 本間行彦: びまん性細気管支炎全国症例調査報告. 5呼吸機能. 厚生省特定疾患問質性肺疾患調査報告班, 昭和57年度研究報告書P.14-23 1) 澤木政好, 三上理一郎, 三笠桂一, 他: 慢性下気道感染症における複数菌感染の実態に関する経気管吸引法による研究. 感染症誌58: 469-476, 1984 |
| References_xml | – reference: 4) 稲富恵子: びまん性細気管支炎全国症例調査報告, 8予後. 厚生省特定疾患間質性肺疾患調査研究班, 昭和57年度研究報告書p.38-41 – reference: 2) 澤木政好, 三上理一郎, 国松幹和, 他: 慢性下気道感染症における細菌感染の実態一経時的経気管吸引法 (TTA) 施行例の検討から-. 感染症誌59: 389-395, 1985 – reference: 8) 善本英一郎, 澤木政好, 三笠桂一, 他: びまん性汎細気管支炎に対するErythromycin (EM) 長期治療申に発症したEM耐性肺炎球菌による急性増悪の症例に対する臨床的細菌学的検討. 感染症誌66: 737-742, 1992 – reference: 12) Kita E, Sawaki M, Nishikawa F, et al.: Enhanced interleukin production after long term administration of Erythromycin stearate. Pharmacology 41: 177-183, 1990 – reference: 13) 前田光一, 澤木政好, 喜多上, 他: 慢性下気道感染症におけるマクロライド薬投与によるサイトカインの変動. 日化療会誌43: 825-829, 1995 – reference: 1) 澤木政好, 三上理一郎, 三笠桂一, 他: 慢性下気道感染症における複数菌感染の実態に関する経気管吸引法による研究. 感染症誌58: 469-476, 1984 – reference: 5) 本間行彦: びまん性細気管支炎全国症例調査報告. 5呼吸機能. 厚生省特定疾患問質性肺疾患調査報告班, 昭和57年度研究報告書P.14-23 – reference: 15) Mikasa K, Sawaki M, Kita E, et al.: Significant survival benefit to patients with advanced non-smallcell lung cancer from treatment with clan thromycin. Chemotherapy 43: 288-296, 1997 – reference: 11) 三笠桂一, 澤木政好, 古西満, 他慢性下気道感染症におけるエリスロマイシン治療のNatural Killer細胞活性に与える影響1こついて. 感染症誌63: 811-815, 1989 – reference: 10) 三笠桂一, 喜多英, 澤木政好, 他: 細菌の細胞障害毒素産生と接着因子に及ぼすErythromycinの作用について. 感染症誌67: 648-653, 1993 – reference: 3) 澤木政好, 三上理一郎, 三笠桂一, 他: 慢性下気道感染症におけるErythromycin長期化学療法の検討- 第一報: Amoxicillinとの対比-. 感染症誌60: 37-44, 1986 – reference: 9) Kita E, Sawaki M, Oku D, et al.: Suppression of virulence factors of Pseudomonas aeruginosa by Erythromycin. J. Antimicrob. Chemother. 27: 273-284, 1991 – reference: 7) 三笠桂一, 澤木政好, 喜多英二, 他: 慢性下気道感染症に対するErythromycin長期化学痰法の検討- 第5報7年以上の経過を観察しえた症例について-. 感染症誌66: 1390-1395, 1992 – reference: 6) 三笠桂一, 澤木政好, 古西満, 他: 慢性下気道感染症に対するErythromycin長期化学療法の検討- 第3報投与期問3年以上の症例を中心に-. 感染症誌66: 561-567, 1992 – reference: 14) Mikasa K, Kita E, Sawaki M, et al.: The antiinflammatory effect of erythromycin in zymosan-induced peritonitis of mice. J Antimicrob Chemother 30: 339-348, 1992 |
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| Title | Clinical study of long-term treatment using erythromycin in chronic lower respiratory tract infection |
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