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dc.contributor.author久次米, 雄馬ja
dc.contributor.author佐藤, 元孝ja
dc.contributor.author前川, 高熙ja
dc.contributor.author梅田, 駿ja
dc.contributor.author松下, 慎ja
dc.contributor.author鄭, 則秀ja
dc.contributor.author三宅, 修ja
dc.contributor.alternativeKujime, Yumaen
dc.contributor.alternativeSato, Mototakaen
dc.contributor.alternativeMaekawa, Takahiroen
dc.contributor.alternativeUmeda, Shunen
dc.contributor.alternativeMatsushita, Makotoen
dc.contributor.alternativeTei, Norihideen
dc.contributor.alternativeMiyake, Osamuen
dc.date.accessioned2024-07-08T01:30:16Z-
dc.date.available2024-07-08T01:30:16Z-
dc.date.issued2024-06-30-
dc.identifier.urihttp://hdl.handle.net/2433/287993-
dc.description.abstractThe administration of cabazitaxel for patients with castration-resistant prostate cancer (CRPC) requires prior docetaxel therapy. Sequential chemotherapy may have to be discontinued due to docetaxelassociated side effects. This study investigated the relationship between treatment outcome of docetaxel and cabazitaxel and their associated side effects. We retrospectively analyzed 69 patients with CRPC who had been administered docetaxel withand without subsequent cabazitaxel at Toyonaka Municipal Hospital from October 2014 to June 2022. Twenty-eight patients (41%) discontinued docetaxel because of side effects, and the median number of docetaxel cycles at discontinuation was 2 (range : 1-11). Fourteen of these patients received no treatment following docetaxel. A comparison of the 28 patients who had discontinued docetaxel due to side effects with 41 patients who had not revealed a significant difference in the total numbers of chemotherapy cycles (2.5 vs 9 ; P<0.001) and time to treatment failure (56 days vs 301 days ; P= 0.001), with a trend toward shorter overall survival from the start of docetaxel treatment (259 days vs 512 days ; P=0.06). Multivariate analysis identified discontinuation of docetaxel due to side effects (OR=0.07 ; P<0.001) and lower hemoglobin (OR=0.01 ; P=0.001) as significant factors inhibiting the introduction of cabazitaxel. Reducing the side effects of docetaxel, including early drug switching, may allow more CRPC patients to be reached with cabazitaxel. Consequently, the resulting taxane-based chemotherapy may contribute to an additional survival advantage.en
dc.language.isojpn-
dc.publisher泌尿器科学術研究会ja
dc.rights許諾条件により本文は2025-07-01に公開ja
dc.subjectCastration-resistant prostate canceren
dc.subjectChemotherapyen
dc.subject.ndc494.9-
dc.titleドセタキセルの有害事象がカバジタキセルの導入に与える影響に関する臨床的検討ja
dc.title.alternativeThe Association of Docetaxel Side Effects and Introduction of Subsequent Cabazitaxel for Castration-Resistant Prostate Cancer : A Clinical Studyen
dc.typedepartmental bulletin paper-
dc.type.niitypeDepartmental Bulletin Paper-
dc.identifier.ncidAN00208315-
dc.identifier.jtitle泌尿器科紀要ja
dc.identifier.volume70-
dc.identifier.issue6-
dc.identifier.spage141-
dc.identifier.epage147-
dc.textversionpublisher-
dc.sortkey01-
dc.address市立豊中病院泌尿器科ja
dc.address市立豊中病院泌尿器科ja
dc.address市立豊中病院泌尿器科ja
dc.address市立豊中病院泌尿器科ja
dc.address市立豊中病院泌尿器科ja
dc.address市立豊中病院泌尿器科ja
dc.address市立豊中病院泌尿器科ja
dc.address.alternativeThe Department of Urology, Toyonaka Municipal Hospitalen
dc.address.alternativeThe Department of Urology, Toyonaka Municipal Hospitalen
dc.address.alternativeThe Department of Urology, Toyonaka Municipal Hospitalen
dc.address.alternativeThe Department of Urology, Toyonaka Municipal Hospitalen
dc.address.alternativeThe Department of Urology, Toyonaka Municipal Hospitalen
dc.address.alternativeThe Department of Urology, Toyonaka Municipal Hospitalen
dc.address.alternativeThe Department of Urology, Toyonaka Municipal Hospitalen
dc.identifier.pmid38967025-
dc.identifier.selfDOI10.14989/ActaUrolJap_70_6_141-
dcterms.accessRightsembargoed access-
datacite.date.available2025-07-01-
dc.identifier.pissn0018-1994-
dc.identifier.jtitle-alternativeActa urologica Japonicala
dc.identifier.jtitle-alternativeHinyokika Kiyoen
出現コレクション:Vol.70 No.6

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