首页> 外文期刊>Journal of drug targeting >Trapping effect on a small molecular drug with vascular-disrupting agent CA4P in rodent H22 hepatic tumor model: in vivo magnetic resonance imaging and postmortem inductively coupled plasma atomic emission spectroscopy
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Trapping effect on a small molecular drug with vascular-disrupting agent CA4P in rodent H22 hepatic tumor model: in vivo magnetic resonance imaging and postmortem inductively coupled plasma atomic emission spectroscopy

机译:在啮齿类动物H22肝肿瘤模型中用血管破坏剂CA4P捕获小分子药物的效果:体内磁共振成像和事后电感耦合等离子体原子发射光谱法

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The aim of the present study is to verify the trapping effect of combretastatin A-4-phosphate (CA4P) on small molecular drugs in rodent tumors. Mice with H22 hepatocarcinoma were randomized into groups A and B. Magnetic resonance imaging (MRI) of T1WI, T2WI, and DWI was performed as baseline. Mice in group A were injected with Gd-DTPA and PBS. Mice in group B were injected with Gd-DTPA and CA4P. All mice undergo CE-T1WI at 0 h, 3 h, 6 h, 12 h, and 24 h. Enhancing efficacy of the two groups on CE-T1WI was compared with the signal-to-noise ratio (SNR) calculated. Concentrations of gadolinium measured by ICP-AES in the tumor were compared between groups. On the early CE-T1WI, tumors were equally enhanced in both groups. On the delayed CE-T1WI, the enhancing effect of group A was weaker than that of group B. The SNR and the concentration of gadolinium within the tumor of group A were lower than that of group B at 6 h, 12 h, and 24 h after administration. This study indicates that CA4P could improve the retention of Gd-DTPA in the tumor and MRI allowed dynamically monitoring trapping effects of CA4P on local retention of Gd-DTPA as a small molecular drug.
机译:本研究的目的是验证康普他汀A-4-磷酸(CA4P)对啮齿动物肿瘤中小分子药物的捕获作用。将H22肝癌小鼠随机分为A组和B组。以T1WI,T2WI和DWI的磁共振成像(MRI)作为基线。 A组小鼠注射Gd-DTPA和PBS。 B组小鼠注射Gd-DTPA和CA4P。所有小鼠在0 h,3 h,6 h,12 h和24 h接受CE-T1WI。将两组在CE-T1WI上的增强功效与计算的信噪比(SNR)进行了比较。在各组之间比较通过ICP-AES测量的肿瘤中cent的浓度。在早期CE-T1WI上,两组肿瘤均得到同样的增强。在延迟的CE-T1WI上,A组的增强作用弱于B组。在6 h,12 h和24 h,A组肿瘤内的SNR和and浓度低于B组。给药后h。这项研究表明,CA4P可以改善肿瘤中Gd-DTPA的保留,而MRI可以动态监测CA4P作为小分子药物对Gd-DTPA的局部保留的捕获作用。

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