目的:为提高非诺贝特溶解度,将非诺贝特包载于PEG_(2000)-DSPE胶束中,研究其在SD大鼠体内的口服药动学情况。方法:对非诺贝特PEG_(2000)-DSPE胶束进行表征,大鼠单剂量灌胃给予非诺贝特PEG_(2000)-DSPE胶束和非诺贝特混悬液,眼底静脉丛取...目的:为提高非诺贝特溶解度,将非诺贝特包载于PEG_(2000)-DSPE胶束中,研究其在SD大鼠体内的口服药动学情况。方法:对非诺贝特PEG_(2000)-DSPE胶束进行表征,大鼠单剂量灌胃给予非诺贝特PEG_(2000)-DSPE胶束和非诺贝特混悬液,眼底静脉丛取血,HPLC法测定血浆中非诺贝特酸含量,并用药物与统计(Drug and Statistics,DAS)软件分析处理药动学数据。结果:成功制备了非诺贝特PEG_(2000)-DSPE胶束,平均粒径为(23.40±3.62)nm,包封率和载药量分别为(97.65±3.32)%和(1.33±0.32)%。大鼠体内口服药动学结果表明非诺贝特PEG_(2000)-DSPE胶束和非诺贝特混悬液的药动学行为均符合二室模型,非诺贝特PEG20 00-DSPE胶束和非诺贝特混悬液的AUC_((0-24))分别为(61.41±5.71)μg·h·ml^(-1)和(8.49±0.66)μg·h·ml^(-1),C_(max)分别为(9.67±1.65)μg·ml^(-1)和(0.71±0.09)μg·ml^(-1)。非诺贝特PEG_(2000)-DSPE胶束的AUC_((0-24))和C_(max)相比于非诺贝特混悬液组分别提高了7倍和14倍。非诺贝特PEG_(2000)-DSPE胶束相对于原料药生物利用度为723.3%。结论:非诺贝特PEG_(2000)-DSPE胶束显著提高了非诺贝特在大鼠体内的口服吸收速度和生物利用度。PEG_(2000)-DSPE胶束作为口服药物载体具有优良的应用前景。展开更多
目的建立EMR-Lipid dSPE结合气相色谱-串联质谱法(gas chromatography-tandem mass spectrometry,GC-MS/MS)同时测定玉米油中218种农药残留的分析方法。方法样品采用乙腈提取并经冷冻离心初次除油后用EMR-Lipid dSPE分散固相萃取净化,...目的建立EMR-Lipid dSPE结合气相色谱-串联质谱法(gas chromatography-tandem mass spectrometry,GC-MS/MS)同时测定玉米油中218种农药残留的分析方法。方法样品采用乙腈提取并经冷冻离心初次除油后用EMR-Lipid dSPE分散固相萃取净化,气相色谱-质谱联用仪多反应监测(multiple reaction monitoring,MRM)模式检测,采用基质匹配标准溶液内标法定量。结果218种农药在5~200 ng/mL范围内线性关系良好,相关系数均大于0.995,在0.05、0.10、0.50 mg/kg 3个添加水平的回收率为63.3%~119.9%,相对标准偏差(relative standard deviations,RSDs)为0.78%~18.10%,定量限(limits of the quantitation,LOQs)为10~20μg/kg。结论该方法前处理简单、高效,灵敏度、准确度和精密度高,能满足玉米油中218种农药多残留的分析要求。展开更多
为建立以HPLC-ELSD法测定顺铂脂质体中DSPE-PEG2000含量的方法,以Waters Sun Fire prep Silica(250 mm×4.6 mm,5μm)为分离柱(柱温25℃),甲醇-冰醋酸-三乙胺(500∶8∶2,V/V/V)为流动相(流速1 m L/min),蒸发光散射检测器检测(雾化温...为建立以HPLC-ELSD法测定顺铂脂质体中DSPE-PEG2000含量的方法,以Waters Sun Fire prep Silica(250 mm×4.6 mm,5μm)为分离柱(柱温25℃),甲醇-冰醋酸-三乙胺(500∶8∶2,V/V/V)为流动相(流速1 m L/min),蒸发光散射检测器检测(雾化温度50℃,蒸发温度100℃,气体流速1.6 m L/min).结果表明,DSPE-PEG2000在21.08421.6μg/m L浓度范围内线性关系良好(r=0.999 3),加样回收率为99.03%101.23%(RSD=1.08%,n=9).该法能简便、快速、准确地测定顺铂脂质体中DSPE-PEG2000含量,重复性良好.展开更多
Endotoxin detection is an important step in drug characterization. Herein we found that a chemotherapeutic drug nanoformulation composed of irinotecan hydrochloride(CPT-11) and an amphiphilic molecule DSPE-mPEG_(2000)...Endotoxin detection is an important step in drug characterization. Herein we found that a chemotherapeutic drug nanoformulation composed of irinotecan hydrochloride(CPT-11) and an amphiphilic molecule DSPE-mPEG_(2000) can interfere with the limulus amebocyte lysate assay(LAL). Furthermore, the rabbit pyrogen test(RPT) results indicated that at a relatively high dosage, the drug irinotecan hydrochloride can induce a hypothermia effect which may render the RPT results ambiguous in determination of the safety of the drug formulation.Our findings demonstrate limitations of endotoxin detection in micellar drugs,and call for the necessity of developing reliable endotoxin detection methods that can overcome the interference of nanomaterials in order to better ensure the drug safety of patients in future pharmaceutical drug development.展开更多
文摘目的:为提高非诺贝特溶解度,将非诺贝特包载于PEG_(2000)-DSPE胶束中,研究其在SD大鼠体内的口服药动学情况。方法:对非诺贝特PEG_(2000)-DSPE胶束进行表征,大鼠单剂量灌胃给予非诺贝特PEG_(2000)-DSPE胶束和非诺贝特混悬液,眼底静脉丛取血,HPLC法测定血浆中非诺贝特酸含量,并用药物与统计(Drug and Statistics,DAS)软件分析处理药动学数据。结果:成功制备了非诺贝特PEG_(2000)-DSPE胶束,平均粒径为(23.40±3.62)nm,包封率和载药量分别为(97.65±3.32)%和(1.33±0.32)%。大鼠体内口服药动学结果表明非诺贝特PEG_(2000)-DSPE胶束和非诺贝特混悬液的药动学行为均符合二室模型,非诺贝特PEG20 00-DSPE胶束和非诺贝特混悬液的AUC_((0-24))分别为(61.41±5.71)μg·h·ml^(-1)和(8.49±0.66)μg·h·ml^(-1),C_(max)分别为(9.67±1.65)μg·ml^(-1)和(0.71±0.09)μg·ml^(-1)。非诺贝特PEG_(2000)-DSPE胶束的AUC_((0-24))和C_(max)相比于非诺贝特混悬液组分别提高了7倍和14倍。非诺贝特PEG_(2000)-DSPE胶束相对于原料药生物利用度为723.3%。结论:非诺贝特PEG_(2000)-DSPE胶束显著提高了非诺贝特在大鼠体内的口服吸收速度和生物利用度。PEG_(2000)-DSPE胶束作为口服药物载体具有优良的应用前景。
文摘目的建立EMR-Lipid dSPE结合气相色谱-串联质谱法(gas chromatography-tandem mass spectrometry,GC-MS/MS)同时测定玉米油中218种农药残留的分析方法。方法样品采用乙腈提取并经冷冻离心初次除油后用EMR-Lipid dSPE分散固相萃取净化,气相色谱-质谱联用仪多反应监测(multiple reaction monitoring,MRM)模式检测,采用基质匹配标准溶液内标法定量。结果218种农药在5~200 ng/mL范围内线性关系良好,相关系数均大于0.995,在0.05、0.10、0.50 mg/kg 3个添加水平的回收率为63.3%~119.9%,相对标准偏差(relative standard deviations,RSDs)为0.78%~18.10%,定量限(limits of the quantitation,LOQs)为10~20μg/kg。结论该方法前处理简单、高效,灵敏度、准确度和精密度高,能满足玉米油中218种农药多残留的分析要求。
文摘为建立以HPLC-ELSD法测定顺铂脂质体中DSPE-PEG2000含量的方法,以Waters Sun Fire prep Silica(250 mm×4.6 mm,5μm)为分离柱(柱温25℃),甲醇-冰醋酸-三乙胺(500∶8∶2,V/V/V)为流动相(流速1 m L/min),蒸发光散射检测器检测(雾化温度50℃,蒸发温度100℃,气体流速1.6 m L/min).结果表明,DSPE-PEG2000在21.08421.6μg/m L浓度范围内线性关系良好(r=0.999 3),加样回收率为99.03%101.23%(RSD=1.08%,n=9).该法能简便、快速、准确地测定顺铂脂质体中DSPE-PEG2000含量,重复性良好.
基金supported by the National Natural Science Foundation of China [Grant No. 31600812]Strategic Priority Research Program of the Chinese Academy of Sciences [Grant No. XDA09030301]+1 种基金Natural Science Foundation Key Project [Grant No. 31630027, 31430031]the National Distinguished Young Scholars Grant [Grant No. 31225009]
文摘Endotoxin detection is an important step in drug characterization. Herein we found that a chemotherapeutic drug nanoformulation composed of irinotecan hydrochloride(CPT-11) and an amphiphilic molecule DSPE-mPEG_(2000) can interfere with the limulus amebocyte lysate assay(LAL). Furthermore, the rabbit pyrogen test(RPT) results indicated that at a relatively high dosage, the drug irinotecan hydrochloride can induce a hypothermia effect which may render the RPT results ambiguous in determination of the safety of the drug formulation.Our findings demonstrate limitations of endotoxin detection in micellar drugs,and call for the necessity of developing reliable endotoxin detection methods that can overcome the interference of nanomaterials in order to better ensure the drug safety of patients in future pharmaceutical drug development.
基金National Natural Science Foundation of China(Grant No.81273454 and 81473156)Beijing National Science Foundation(Grant No.7132113)+1 种基金National Key Basic Research Program(Grant No.2013CB932501)Doctoral Foundation of the Ministry of Education(Grant No.20130001110055)