EXPERIMENTAL AND CLINICAL STUDIES ON CEFODIZIME IN PEDIATRICS

EXPERIMENTAL AND CLINICAL STUDIES ON CEFODIZIME IN PEDIATRICS

Cefodizime (CDZM), a newly developed injectable cephem antibiotic, was given via bolus intravenous injection at each of 3 dose levels of 10, 20 and 40 mg/kg to each 3 children, and serum and urinary levels and urinary recovery rates were followed. A total of 57 patients received CDZM in the followin...

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Veröffentlicht in:Japanese journal of antibiotics 1990/04/25, Vol.43(4), pp.603-622
Hauptverfasser: MOTOHIRO, TAKASHI, ODA, KEIKO, ARAMAKI, MASAFUMI, KAWAKAMI, AKIRA, TANAKA, KOICHI, KOGA, TATSUHIKO, SAKATA, YASUTAKA, YAMASHITA, FUMIO, TAKAJO, NOBUHIKO, OKABAYASHI, SAYURI, SHIMIZU, TAKASHI, YAMADA, TAKASHI, MURAKAMI, TAIYU, OHBU, KEIZO, IMAI, SHOICHI, ARAKI, HISAAKI, TAKAHASHI, KOICHI, HARADA, HIROKO, KANEKO, SHINYA, YAMAMURA, JUNICHI, ISHIKAWA, YUTAKA, MATSUMOTO, KOJI, NAGAYAMA, KIYOTAKA, YASUOKA, CHIKAI, HAYASHI, MASAO, SHIMADA, YASUSHI, SHINDO, SHIZUO, NINOMIYA, MASAYUKI, YOSHINAGA, YOICHIRO, MIHARA, SEIKO, AMAMOTO, MASANO, YAMAKAWA, RYOICHI, HASHIMOTO, NOBUO, TANAKA, NOBUO, KATO, EIJI, HARADA, YUTAKA, ISHIMOTO, KOJI, TAKAGI, JUNICHI, MORITA, JUN, NISHIYAMA, TOHRU, AIDA, KATSUMARO, SASAKI, HIROKAZU, OKI, SHINICHIRO, FUJISAWA, TAKUJI, TOMINAGA, KAORU, TOMITA, SHOBUN, KOGA, TATSUO, KUBOTA, KAORU, KUDA, NAOKI
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Age Factors
Bacterial Infections - drug therapy
Cefotaxime - adverse effects
Cefotaxime - analogs & derivatives
Cefotaxime - pharmacokinetics
Cefotaxime - therapeutic use
Child
Drug Evaluation
Female
Humans
Injections, Intravenous
Male
Multicenter Studies as Topic
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container_issue 4
container_start_page 603
container_title Japanese journal of antibiotics
container_volume 43
creator MOTOHIRO, TAKASHI
ODA, KEIKO
ARAMAKI, MASAFUMI
KAWAKAMI, AKIRA
TANAKA, KOICHI
KOGA, TATSUHIKO
SAKATA, YASUTAKA
YAMASHITA, FUMIO
TAKAJO, NOBUHIKO
OKABAYASHI, SAYURI
SHIMIZU, TAKASHI
YAMADA, TAKASHI
MURAKAMI, TAIYU
OHBU, KEIZO
IMAI, SHOICHI
ARAKI, HISAAKI
TAKAHASHI, KOICHI
HARADA, HIROKO
KANEKO, SHINYA
YAMAMURA, JUNICHI
ISHIKAWA, YUTAKA
MATSUMOTO, KOJI
NAGAYAMA, KIYOTAKA
YASUOKA, CHIKAI
HAYASHI, MASAO
SHIMADA, YASUSHI
SHINDO, SHIZUO
NINOMIYA, MASAYUKI
YOSHINAGA, YOICHIRO
MIHARA, SEIKO
AMAMOTO, MASANO
YAMAKAWA, RYOICHI
HASHIMOTO, NOBUO
TANAKA, NOBUO
KATO, EIJI
HARADA, YUTAKA
ISHIMOTO, KOJI
TAKAGI, JUNICHI
MORITA, JUN
NISHIYAMA, TOHRU
AIDA, KATSUMARO
SASAKI, HIROKAZU
OKI, SHINICHIRO
FUJISAWA, TAKUJI
TOMINAGA, KAORU
TOMITA, SHOBUN
KOGA, TATSUO
KUBOTA, KAORU
KUDA, NAOKI
description Cefodizime (CDZM), a newly developed injectable cephem antibiotic, was given via bolus intravenous injection at each of 3 dose levels of 10, 20 and 40 mg/kg to each 3 children, and serum and urinary levels and urinary recovery rates were followed. A total of 57 patients received CDZM in the following regimen via bolus intravenous injection, and clinical efficacies, and microbial responses were evaluated. Mean dosage per application: 20.9 mg/kg, number of application per day: between 2 and 4 (2 times for 3 patients, 3 for 26 patients and 4 for 28 patients), mean duration of the therapy: 1 week. Patients consisted of 1 case of peritonsillar abscess, 2 acute bronchitis, 38 pneumonia, 8 urinary tract infection, 1 staphylococcal scalded skin syndrome, 2 cellulitis, 4 purulent lymphadenitis and 1 typhoid fever.In addition to the patients mentioned above 6 patients who dropped out were involved in the evaluation of adverse reactions and influence of the drug on laboratory test data, and the following results were obtained. 1. Five minutes after bolus intravenous injection in doses of 10, 20 and 40 mg/kg, serum levels determined by the bioassay method were at their maxima, i.e. 114.0,264.6 and 461.6 μg/ml, respectively. Serum levels of drugs were dose-dependent throughout all the dosage levels tested. Mean serum half-lives of the drug were 1.757, 1.552 and 1.668 hours, respectively, for the 3 dose levels. Serum levels of the drug determined by the HPLC method were similar to those by the bioassay method: The maximum serum levels occurred at 5 minutes after administration, mean maximum concentrations were 105.5,264.0 and 461.7 μg/ml for the 3 dose levels, and a dose response was noted for the 3 dose levels. The half-lives were 1.755, 1.598 and 1.668 hours, respectively. 2. Mean maximum concentrations in urine determined by bioassay for 2 of 3 cases received 10 mg/kg and 3 cases each given 20 and 40 mg/kg of CDZM were 884.3, 3,061 and 7,352 μg/ml, respectively, in the first 2 hours after administration. These levels were also dose-dependent. Mean recovery rates were 74.4, 78.4 and 71.5%, respectively, in the first 8 hours after administration. Mean maximum concentrations in urine measured by HPLC were similar to those determined by bioassay, i.e. 962.3, 3,404 and 7,899 μg/ml in the first 2 hours. They were, also, dose-dependent. Mean recovery rates were 82.1, 86.0 and 76.5%, respectively, in the first 8 hours after administration. The HPLC determinations gave slight
doi_str_mv 10.11553/antibiotics1968b.43.603
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A total of 57 patients received CDZM in the following regimen via bolus intravenous injection, and clinical efficacies, and microbial responses were evaluated. Mean dosage per application: 20.9 mg/kg, number of application per day: between 2 and 4 (2 times for 3 patients, 3 for 26 patients and 4 for 28 patients), mean duration of the therapy: 1 week. Patients consisted of 1 case of peritonsillar abscess, 2 acute bronchitis, 38 pneumonia, 8 urinary tract infection, 1 staphylococcal scalded skin syndrome, 2 cellulitis, 4 purulent lymphadenitis and 1 typhoid fever.In addition to the patients mentioned above 6 patients who dropped out were involved in the evaluation of adverse reactions and influence of the drug on laboratory test data, and the following results were obtained. 1. Five minutes after bolus intravenous injection in doses of 10, 20 and 40 mg/kg, serum levels determined by the bioassay method were at their maxima, i.e. 114.0,264.6 and 461.6 μg/ml, respectively. Serum levels of drugs were dose-dependent throughout all the dosage levels tested. Mean serum half-lives of the drug were 1.757, 1.552 and 1.668 hours, respectively, for the 3 dose levels. Serum levels of the drug determined by the HPLC method were similar to those by the bioassay method: The maximum serum levels occurred at 5 minutes after administration, mean maximum concentrations were 105.5,264.0 and 461.7 μg/ml for the 3 dose levels, and a dose response was noted for the 3 dose levels. The half-lives were 1.755, 1.598 and 1.668 hours, respectively. 2. Mean maximum concentrations in urine determined by bioassay for 2 of 3 cases received 10 mg/kg and 3 cases each given 20 and 40 mg/kg of CDZM were 884.3, 3,061 and 7,352 μg/ml, respectively, in the first 2 hours after administration. These levels were also dose-dependent. Mean recovery rates were 74.4, 78.4 and 71.5%, respectively, in the first 8 hours after administration. Mean maximum concentrations in urine measured by HPLC were similar to those determined by bioassay, i.e. 962.3, 3,404 and 7,899 μg/ml in the first 2 hours. They were, also, dose-dependent. Mean recovery rates were 82.1, 86.0 and 76.5%, respectively, in the first 8 hours after administration. The HPLC determinations gave slightly higher levels than the bioassay. 3. Clinical efficacies were excellent or good in 93.0% (53 patients), thus the efficacy was generally good. 4. Bacteriologically, 16 strains were followed and 15 of them (93.8%) were found to have been eliminated, giving a very high elimination rate. 5. In the 63 cases including 6 dropped-out cases, 2 cases with adverse reactions, both diarrhea, were found. 6. 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J. Antibiotics</addtitle><description>Cefodizime (CDZM), a newly developed injectable cephem antibiotic, was given via bolus intravenous injection at each of 3 dose levels of 10, 20 and 40 mg/kg to each 3 children, and serum and urinary levels and urinary recovery rates were followed. A total of 57 patients received CDZM in the following regimen via bolus intravenous injection, and clinical efficacies, and microbial responses were evaluated. Mean dosage per application: 20.9 mg/kg, number of application per day: between 2 and 4 (2 times for 3 patients, 3 for 26 patients and 4 for 28 patients), mean duration of the therapy: 1 week. Patients consisted of 1 case of peritonsillar abscess, 2 acute bronchitis, 38 pneumonia, 8 urinary tract infection, 1 staphylococcal scalded skin syndrome, 2 cellulitis, 4 purulent lymphadenitis and 1 typhoid fever.In addition to the patients mentioned above 6 patients who dropped out were involved in the evaluation of adverse reactions and influence of the drug on laboratory test data, and the following results were obtained. 1. Five minutes after bolus intravenous injection in doses of 10, 20 and 40 mg/kg, serum levels determined by the bioassay method were at their maxima, i.e. 114.0,264.6 and 461.6 μg/ml, respectively. Serum levels of drugs were dose-dependent throughout all the dosage levels tested. Mean serum half-lives of the drug were 1.757, 1.552 and 1.668 hours, respectively, for the 3 dose levels. Serum levels of the drug determined by the HPLC method were similar to those by the bioassay method: The maximum serum levels occurred at 5 minutes after administration, mean maximum concentrations were 105.5,264.0 and 461.7 μg/ml for the 3 dose levels, and a dose response was noted for the 3 dose levels. The half-lives were 1.755, 1.598 and 1.668 hours, respectively. 2. Mean maximum concentrations in urine determined by bioassay for 2 of 3 cases received 10 mg/kg and 3 cases each given 20 and 40 mg/kg of CDZM were 884.3, 3,061 and 7,352 μg/ml, respectively, in the first 2 hours after administration. These levels were also dose-dependent. Mean recovery rates were 74.4, 78.4 and 71.5%, respectively, in the first 8 hours after administration. Mean maximum concentrations in urine measured by HPLC were similar to those determined by bioassay, i.e. 962.3, 3,404 and 7,899 μg/ml in the first 2 hours. They were, also, dose-dependent. Mean recovery rates were 82.1, 86.0 and 76.5%, respectively, in the first 8 hours after administration. The HPLC determinations gave slightly higher levels than the bioassay. 3. Clinical efficacies were excellent or good in 93.0% (53 patients), thus the efficacy was generally good. 4. Bacteriologically, 16 strains were followed and 15 of them (93.8%) were found to have been eliminated, giving a very high elimination rate. 5. In the 63 cases including 6 dropped-out cases, 2 cases with adverse reactions, both diarrhea, were found. 6. Abnormal findings in laboratory examinations were noted; 2 cases of thrombocytosis, 5 eosinophilia, 1 each of slight elevation of GOT or GPT, and 4 cases with simultaneously abnormal GOT and GPT.</description><subject>Age Factors</subject><subject>Bacterial Infections - drug therapy</subject><subject>Cefotaxime - adverse effects</subject><subject>Cefotaxime - analogs &amp; derivatives</subject><subject>Cefotaxime - pharmacokinetics</subject><subject>Cefotaxime - therapeutic use</subject><subject>Child</subject><subject>Drug Evaluation</subject><subject>Female</subject><subject>Humans</subject><subject>Injections, Intravenous</subject><subject>Male</subject><subject>Multicenter Studies as Topic</subject><issn>0368-2781</issn><issn>2186-5477</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>1990</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNpdkFFrwjAUhcPYcOL8CYP8gbrcpE3Shz1IG12Gq6IVxl5KGtOtok7a7mH_fhHFh73cy-U798A5CGEgI4AoYk_m0NVl_d3VtoWYy3IUshEn7Ab1KUgeRKEQt6hPGJcBFRLu0bBt65IwEJJ6hx7qUYj9o-yjZ_W-UEv9prJ8PMPjLMXJTGc68ccqX6darfA8w4mazFP94WVYZ3ihUj3OlzpZPaC7yuxaN7zsAVpPVJ68BLP59OQRbIESGVjLmXOE2lBIQStDuGMETEmFiGgMznBC2YZIYQ1IEnFbRVUYV0wCEZVxlg3Q49n3-FPu3aY4NvXeNL_FJYbnr2e-bTvz6a7cNL6jnSv-F1aErAhPw7d2Fdkv0xTuwP4AUeZipw</recordid><startdate>199004</startdate><enddate>199004</enddate><creator>MOTOHIRO, TAKASHI</creator><creator>ODA, KEIKO</creator><creator>ARAMAKI, MASAFUMI</creator><creator>KAWAKAMI, AKIRA</creator><creator>TANAKA, KOICHI</creator><creator>KOGA, TATSUHIKO</creator><creator>SAKATA, YASUTAKA</creator><creator>YAMASHITA, FUMIO</creator><creator>TAKAJO, NOBUHIKO</creator><creator>OKABAYASHI, SAYURI</creator><creator>SHIMIZU, TAKASHI</creator><creator>YAMADA, TAKASHI</creator><creator>MURAKAMI, TAIYU</creator><creator>OHBU, KEIZO</creator><creator>IMAI, SHOICHI</creator><creator>ARAKI, HISAAKI</creator><creator>TAKAHASHI, KOICHI</creator><creator>HARADA, HIROKO</creator><creator>KANEKO, SHINYA</creator><creator>YAMAMURA, JUNICHI</creator><creator>ISHIKAWA, YUTAKA</creator><creator>MATSUMOTO, KOJI</creator><creator>NAGAYAMA, KIYOTAKA</creator><creator>YASUOKA, CHIKAI</creator><creator>HAYASHI, MASAO</creator><creator>SHIMADA, YASUSHI</creator><creator>SHINDO, SHIZUO</creator><creator>NINOMIYA, MASAYUKI</creator><creator>YOSHINAGA, YOICHIRO</creator><creator>MIHARA, SEIKO</creator><creator>AMAMOTO, MASANO</creator><creator>YAMAKAWA, RYOICHI</creator><creator>HASHIMOTO, NOBUO</creator><creator>TANAKA, NOBUO</creator><creator>KATO, EIJI</creator><creator>HARADA, YUTAKA</creator><creator>ISHIMOTO, KOJI</creator><creator>TAKAGI, JUNICHI</creator><creator>MORITA, JUN</creator><creator>NISHIYAMA, TOHRU</creator><creator>AIDA, KATSUMARO</creator><creator>SASAKI, HIROKAZU</creator><creator>OKI, SHINICHIRO</creator><creator>FUJISAWA, TAKUJI</creator><creator>TOMINAGA, KAORU</creator><creator>TOMITA, SHOBUN</creator><creator>KOGA, TATSUO</creator><creator>KUBOTA, KAORU</creator><creator>KUDA, NAOKI</creator><general>Japan Antibiotics Research Association</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope></search><sort><creationdate>199004</creationdate><title>EXPERIMENTAL AND CLINICAL STUDIES ON CEFODIZIME IN PEDIATRICS</title><author>MOTOHIRO, TAKASHI ; ODA, KEIKO ; ARAMAKI, MASAFUMI ; KAWAKAMI, AKIRA ; TANAKA, KOICHI ; KOGA, TATSUHIKO ; SAKATA, YASUTAKA ; YAMASHITA, FUMIO ; TAKAJO, NOBUHIKO ; OKABAYASHI, SAYURI ; SHIMIZU, TAKASHI ; YAMADA, TAKASHI ; MURAKAMI, TAIYU ; OHBU, KEIZO ; IMAI, SHOICHI ; ARAKI, HISAAKI ; TAKAHASHI, KOICHI ; HARADA, HIROKO ; KANEKO, SHINYA ; YAMAMURA, JUNICHI ; ISHIKAWA, YUTAKA ; MATSUMOTO, KOJI ; NAGAYAMA, KIYOTAKA ; YASUOKA, CHIKAI ; HAYASHI, MASAO ; SHIMADA, YASUSHI ; SHINDO, SHIZUO ; NINOMIYA, MASAYUKI ; YOSHINAGA, YOICHIRO ; MIHARA, SEIKO ; AMAMOTO, MASANO ; YAMAKAWA, RYOICHI ; HASHIMOTO, NOBUO ; TANAKA, NOBUO ; KATO, EIJI ; HARADA, YUTAKA ; ISHIMOTO, KOJI ; TAKAGI, JUNICHI ; MORITA, JUN ; NISHIYAMA, TOHRU ; AIDA, KATSUMARO ; SASAKI, HIROKAZU ; OKI, SHINICHIRO ; FUJISAWA, TAKUJI ; TOMINAGA, KAORU ; TOMITA, SHOBUN ; KOGA, TATSUO ; KUBOTA, KAORU ; KUDA, NAOKI</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-j1208-cc63ee02c47872fa06e301ab2775291ea6023d087ca18056cf5f49f38107faec3</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>jpn</language><creationdate>1990</creationdate><topic>Age Factors</topic><topic>Bacterial Infections - drug therapy</topic><topic>Cefotaxime - adverse effects</topic><topic>Cefotaxime - analogs &amp; derivatives</topic><topic>Cefotaxime - pharmacokinetics</topic><topic>Cefotaxime - therapeutic use</topic><topic>Child</topic><topic>Drug Evaluation</topic><topic>Female</topic><topic>Humans</topic><topic>Injections, Intravenous</topic><topic>Male</topic><topic>Multicenter Studies as Topic</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>MOTOHIRO, TAKASHI</creatorcontrib><creatorcontrib>ODA, KEIKO</creatorcontrib><creatorcontrib>ARAMAKI, MASAFUMI</creatorcontrib><creatorcontrib>KAWAKAMI, AKIRA</creatorcontrib><creatorcontrib>TANAKA, KOICHI</creatorcontrib><creatorcontrib>KOGA, TATSUHIKO</creatorcontrib><creatorcontrib>SAKATA, YASUTAKA</creatorcontrib><creatorcontrib>YAMASHITA, FUMIO</creatorcontrib><creatorcontrib>TAKAJO, NOBUHIKO</creatorcontrib><creatorcontrib>OKABAYASHI, SAYURI</creatorcontrib><creatorcontrib>SHIMIZU, TAKASHI</creatorcontrib><creatorcontrib>YAMADA, TAKASHI</creatorcontrib><creatorcontrib>MURAKAMI, TAIYU</creatorcontrib><creatorcontrib>OHBU, KEIZO</creatorcontrib><creatorcontrib>IMAI, SHOICHI</creatorcontrib><creatorcontrib>ARAKI, HISAAKI</creatorcontrib><creatorcontrib>TAKAHASHI, KOICHI</creatorcontrib><creatorcontrib>HARADA, HIROKO</creatorcontrib><creatorcontrib>KANEKO, SHINYA</creatorcontrib><creatorcontrib>YAMAMURA, JUNICHI</creatorcontrib><creatorcontrib>ISHIKAWA, YUTAKA</creatorcontrib><creatorcontrib>MATSUMOTO, KOJI</creatorcontrib><creatorcontrib>NAGAYAMA, KIYOTAKA</creatorcontrib><creatorcontrib>YASUOKA, CHIKAI</creatorcontrib><creatorcontrib>HAYASHI, MASAO</creatorcontrib><creatorcontrib>SHIMADA, YASUSHI</creatorcontrib><creatorcontrib>SHINDO, SHIZUO</creatorcontrib><creatorcontrib>NINOMIYA, MASAYUKI</creatorcontrib><creatorcontrib>YOSHINAGA, YOICHIRO</creatorcontrib><creatorcontrib>MIHARA, SEIKO</creatorcontrib><creatorcontrib>AMAMOTO, MASANO</creatorcontrib><creatorcontrib>YAMAKAWA, RYOICHI</creatorcontrib><creatorcontrib>HASHIMOTO, NOBUO</creatorcontrib><creatorcontrib>TANAKA, NOBUO</creatorcontrib><creatorcontrib>KATO, EIJI</creatorcontrib><creatorcontrib>HARADA, YUTAKA</creatorcontrib><creatorcontrib>ISHIMOTO, KOJI</creatorcontrib><creatorcontrib>TAKAGI, JUNICHI</creatorcontrib><creatorcontrib>MORITA, JUN</creatorcontrib><creatorcontrib>NISHIYAMA, TOHRU</creatorcontrib><creatorcontrib>AIDA, KATSUMARO</creatorcontrib><creatorcontrib>SASAKI, HIROKAZU</creatorcontrib><creatorcontrib>OKI, SHINICHIRO</creatorcontrib><creatorcontrib>FUJISAWA, TAKUJI</creatorcontrib><creatorcontrib>TOMINAGA, KAORU</creatorcontrib><creatorcontrib>TOMITA, SHOBUN</creatorcontrib><creatorcontrib>KOGA, TATSUO</creatorcontrib><creatorcontrib>KUBOTA, KAORU</creatorcontrib><creatorcontrib>KUDA, NAOKI</creatorcontrib><collection>Medline</collection><collection>MEDLINE</collection><collection>MEDLINE (Ovid)</collection><collection>MEDLINE</collection><collection>MEDLINE</collection><collection>PubMed</collection><jtitle>Japanese journal of antibiotics</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>MOTOHIRO, TAKASHI</au><au>ODA, KEIKO</au><au>ARAMAKI, MASAFUMI</au><au>KAWAKAMI, AKIRA</au><au>TANAKA, KOICHI</au><au>KOGA, TATSUHIKO</au><au>SAKATA, YASUTAKA</au><au>YAMASHITA, FUMIO</au><au>TAKAJO, NOBUHIKO</au><au>OKABAYASHI, SAYURI</au><au>SHIMIZU, TAKASHI</au><au>YAMADA, TAKASHI</au><au>MURAKAMI, TAIYU</au><au>OHBU, KEIZO</au><au>IMAI, SHOICHI</au><au>ARAKI, HISAAKI</au><au>TAKAHASHI, KOICHI</au><au>HARADA, HIROKO</au><au>KANEKO, SHINYA</au><au>YAMAMURA, JUNICHI</au><au>ISHIKAWA, YUTAKA</au><au>MATSUMOTO, KOJI</au><au>NAGAYAMA, KIYOTAKA</au><au>YASUOKA, CHIKAI</au><au>HAYASHI, MASAO</au><au>SHIMADA, YASUSHI</au><au>SHINDO, SHIZUO</au><au>NINOMIYA, MASAYUKI</au><au>YOSHINAGA, YOICHIRO</au><au>MIHARA, SEIKO</au><au>AMAMOTO, MASANO</au><au>YAMAKAWA, RYOICHI</au><au>HASHIMOTO, NOBUO</au><au>TANAKA, NOBUO</au><au>KATO, EIJI</au><au>HARADA, YUTAKA</au><au>ISHIMOTO, KOJI</au><au>TAKAGI, JUNICHI</au><au>MORITA, JUN</au><au>NISHIYAMA, TOHRU</au><au>AIDA, KATSUMARO</au><au>SASAKI, HIROKAZU</au><au>OKI, SHINICHIRO</au><au>FUJISAWA, TAKUJI</au><au>TOMINAGA, KAORU</au><au>TOMITA, SHOBUN</au><au>KOGA, TATSUO</au><au>KUBOTA, KAORU</au><au>KUDA, NAOKI</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>EXPERIMENTAL AND CLINICAL STUDIES ON CEFODIZIME IN PEDIATRICS</atitle><jtitle>Japanese journal of antibiotics</jtitle><addtitle>Jpn. J. Antibiotics</addtitle><date>1990-04</date><risdate>1990</risdate><volume>43</volume><issue>4</issue><spage>603</spage><epage>622</epage><pages>603-622</pages><issn>0368-2781</issn><eissn>2186-5477</eissn><abstract>Cefodizime (CDZM), a newly developed injectable cephem antibiotic, was given via bolus intravenous injection at each of 3 dose levels of 10, 20 and 40 mg/kg to each 3 children, and serum and urinary levels and urinary recovery rates were followed. A total of 57 patients received CDZM in the following regimen via bolus intravenous injection, and clinical efficacies, and microbial responses were evaluated. Mean dosage per application: 20.9 mg/kg, number of application per day: between 2 and 4 (2 times for 3 patients, 3 for 26 patients and 4 for 28 patients), mean duration of the therapy: 1 week. Patients consisted of 1 case of peritonsillar abscess, 2 acute bronchitis, 38 pneumonia, 8 urinary tract infection, 1 staphylococcal scalded skin syndrome, 2 cellulitis, 4 purulent lymphadenitis and 1 typhoid fever.In addition to the patients mentioned above 6 patients who dropped out were involved in the evaluation of adverse reactions and influence of the drug on laboratory test data, and the following results were obtained. 1. Five minutes after bolus intravenous injection in doses of 10, 20 and 40 mg/kg, serum levels determined by the bioassay method were at their maxima, i.e. 114.0,264.6 and 461.6 μg/ml, respectively. Serum levels of drugs were dose-dependent throughout all the dosage levels tested. Mean serum half-lives of the drug were 1.757, 1.552 and 1.668 hours, respectively, for the 3 dose levels. Serum levels of the drug determined by the HPLC method were similar to those by the bioassay method: The maximum serum levels occurred at 5 minutes after administration, mean maximum concentrations were 105.5,264.0 and 461.7 μg/ml for the 3 dose levels, and a dose response was noted for the 3 dose levels. The half-lives were 1.755, 1.598 and 1.668 hours, respectively. 2. Mean maximum concentrations in urine determined by bioassay for 2 of 3 cases received 10 mg/kg and 3 cases each given 20 and 40 mg/kg of CDZM were 884.3, 3,061 and 7,352 μg/ml, respectively, in the first 2 hours after administration. These levels were also dose-dependent. Mean recovery rates were 74.4, 78.4 and 71.5%, respectively, in the first 8 hours after administration. Mean maximum concentrations in urine measured by HPLC were similar to those determined by bioassay, i.e. 962.3, 3,404 and 7,899 μg/ml in the first 2 hours. They were, also, dose-dependent. Mean recovery rates were 82.1, 86.0 and 76.5%, respectively, in the first 8 hours after administration. The HPLC determinations gave slightly higher levels than the bioassay. 3. Clinical efficacies were excellent or good in 93.0% (53 patients), thus the efficacy was generally good. 4. Bacteriologically, 16 strains were followed and 15 of them (93.8%) were found to have been eliminated, giving a very high elimination rate. 5. In the 63 cases including 6 dropped-out cases, 2 cases with adverse reactions, both diarrhea, were found. 6. Abnormal findings in laboratory examinations were noted; 2 cases of thrombocytosis, 5 eosinophilia, 1 each of slight elevation of GOT or GPT, and 4 cases with simultaneously abnormal GOT and GPT.</abstract><cop>Japan</cop><pub>Japan Antibiotics Research Association</pub><pmid>2199688</pmid><doi>10.11553/antibiotics1968b.43.603</doi><tpages>20</tpages><oa>free_for_read</oa></addata></record>
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identifier ISSN: 0368-2781
ispartof The Japanese Journal of Antibiotics, 1990/04/25, Vol.43(4), pp.603-622
issn 0368-2781
2186-5477
language jpn
recordid cdi_pubmed_primary_2199688
source MEDLINE; EZB Electronic Journals Library
subjects Age Factors
Bacterial Infections - drug therapy
Cefotaxime - adverse effects
Cefotaxime - analogs & derivatives
Cefotaxime - pharmacokinetics
Cefotaxime - therapeutic use
Child
Drug Evaluation
Female
Humans
Injections, Intravenous
Male
Multicenter Studies as Topic
title EXPERIMENTAL AND CLINICAL STUDIES ON CEFODIZIME IN PEDIATRICS
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