中国临床药理学杂志
中國臨床藥理學雜誌
중국림상약이학잡지
THE CHINESE JOURNAL OF CLINICAL PHARMACOLOGY
2010年
3期
205-208
,共4页
李苏%廖海%詹靖%管忠震
李囌%廖海%詹靖%管忠震
리소%료해%첨정%관충진
伊沙匹隆%液相色谱-串联质谱%血药浓度%药代动力学
伊沙匹隆%液相色譜-串聯質譜%血藥濃度%藥代動力學
이사필륭%액상색보-천련질보%혈약농도%약대동역학
ixabepilone%LC-MS/MS%plasma concentration%pharmaco-kinetics
目的 建立液相色谱-串联质谱联用方法测定人血浆中伊沙匹隆(抗肿瘤药)浓度,并研究其在乳腺癌患者中的药代动力学.方法 用BDS Hypersil C_(18)色谱柱(100 mm ×2.1 mm,3μm),流动相为0.01 mol·L~(-1)乙酸胺-乙腈=40:60,样本经质谱ESI源正离子化后,用多反应离子监测方式对伊沙匹隆进行测定.结果 血浆中伊沙匹隆在2~500 ng·mL~(-1)线性良好;提取回收率为61.85%~65.85%,批内、批间精密度良好(RSD<5%).11例乳腺癌患者的主要药代动力学参数:C_(max)为(295.34±140.74)ng·mL~(-1),t_(1/2)为(41.77±19.05)h,AUC_(0-∞)为(2.80±1.66)μg·h·mL~(-1),V_(ss)为(1267.20±419.96)L,CL为(36.72±33.00)L·h~(-1).结论 本方法准确、快速、简单,适用于血浆中伊沙匹隆浓度测定.伊沙匹隆在中国乳腺癌患者中的药代动力学行为与国外患者相似.
目的 建立液相色譜-串聯質譜聯用方法測定人血漿中伊沙匹隆(抗腫瘤藥)濃度,併研究其在乳腺癌患者中的藥代動力學.方法 用BDS Hypersil C_(18)色譜柱(100 mm ×2.1 mm,3μm),流動相為0.01 mol·L~(-1)乙痠胺-乙腈=40:60,樣本經質譜ESI源正離子化後,用多反應離子鑑測方式對伊沙匹隆進行測定.結果 血漿中伊沙匹隆在2~500 ng·mL~(-1)線性良好;提取迴收率為61.85%~65.85%,批內、批間精密度良好(RSD<5%).11例乳腺癌患者的主要藥代動力學參數:C_(max)為(295.34±140.74)ng·mL~(-1),t_(1/2)為(41.77±19.05)h,AUC_(0-∞)為(2.80±1.66)μg·h·mL~(-1),V_(ss)為(1267.20±419.96)L,CL為(36.72±33.00)L·h~(-1).結論 本方法準確、快速、簡單,適用于血漿中伊沙匹隆濃度測定.伊沙匹隆在中國乳腺癌患者中的藥代動力學行為與國外患者相似.
목적 건립액상색보-천련질보련용방법측정인혈장중이사필륭(항종류약)농도,병연구기재유선암환자중적약대동역학.방법 용BDS Hypersil C_(18)색보주(100 mm ×2.1 mm,3μm),류동상위0.01 mol·L~(-1)을산알-을정=40:60,양본경질보ESI원정리자화후,용다반응리자감측방식대이사필륭진행측정.결과 혈장중이사필륭재2~500 ng·mL~(-1)선성량호;제취회수솔위61.85%~65.85%,비내、비간정밀도량호(RSD<5%).11례유선암환자적주요약대동역학삼수:C_(max)위(295.34±140.74)ng·mL~(-1),t_(1/2)위(41.77±19.05)h,AUC_(0-∞)위(2.80±1.66)μg·h·mL~(-1),V_(ss)위(1267.20±419.96)L,CL위(36.72±33.00)L·h~(-1).결론 본방법준학、쾌속、간단,괄용우혈장중이사필륭농도측정.이사필륭재중국유선암환자중적약대동역학행위여국외환자상사.
Objective To establish LC-MS/MS method for the deter-mination of ixabepilone in breast cancer patients and evaluate its pharma-cokinetics profile. Methods A BDS Hypersil C_(18) (100 mm ×2. 1 mm,3 μm) column was used with the mobile phase of 0. 01 mol ·L~(-1) ammoni-um acetate-acetonitrile = 40: 60. The concentration was detected by ESI -MS. Results A good linear relationship was obtained in the concen-tration from 2 to 500 ng·mL~(-1). The average recovery of this method was 61.85%-65.85%. Inter-batch RSD and intra-batch RSD were both less than 5 %. The pharmacokinetic parameters of ixabepilone were as follows:C_(max) was (295.34±140.74) ng· mL~(-1),t_(1/2) was (41.77 ± 19. 05) h, AUC_(0-∞) was (2.80 ± 1.66) μg· h· mL~(-1), V_(ss) was (1267.20 ±419.96) L and CL was (36.72 ±33.00) L· h~(-1) ,respec-tively, Condusion The method is simple, rapid and accurate. The method was suitable for the quantitatve determination of ixabepilone. The datas of pharmaeokinetic parameters in Chinese breast cancer patiens is similar to other studies in USA.
