单克隆抗体AR-3在胰腺癌患者中的生物分布和药代动力学筛选

G Mariani, N Molen, D Bacciardi, U Boggi, C Bonino, A Costa, P Viacava, M Castagna, L Bodei, L Tarditi
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摘要

本药物动力学研究是为了评估小鼠单克隆抗体(MoAb) AR-3-IgG1作为胰腺癌免疫显像剂的潜在用途。该MoAb定义了一种黏液样抗原(CAR-3),在大部分胰腺癌中表达,实际上在人类肿瘤异种移植的实验动物模型中显示出有利的体内定位特性。对5例疑似胰腺癌患者静脉注射131I-AR-3-IgG1。用计算机化的伽马照相机记录全身图和腹部区域的局部视图,并在肝脏和脾脏上绘制感兴趣的特定区域,帮助确定这些器官的活动动力学。注射后0.1-144小时的血液样本和相同时间间隔内的每日尿液收集用于确定血浆分布和从体内去除活性的动力学。我们测试了不同的多室模型,以拟合实验数据,并假设在肝脏、脾脏和骨髓中存在显著的非特异性示踪剂积累,正如在大多数注射到人类体内的放射性碘化小鼠MoAbs中已经观察到的那样。手术证实5例患者中3例为胰腺癌(慢性胰腺炎和壶腹周围癌各1例);在所有这3例患者中,MoAb AR-3免疫染色显示存在CAR-3抗原(具有细胞质和腔内/分泌分布模式)。肝脏、脾脏和骨髓中的非特异性放射性积累极低,主要与这些器官循环活动的血池效应有关。(摘要删节250字)
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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Biodistribution and pharmacokinetic screening in humans of monoclonal antibody AR-3 as a possible immunoscintigraphy agent in patients with pancreatic cancer.

This pharmacokinetic study was performed in order to assess the potential usefulness of the murine monoclonal antibody (MoAb) AR-3-IgG1 as an immunoscintigraphy agent for pancreatic cancer. This MoAb, which defines a mucin-like antigen (CAR-3) expressed by a large fraction of pancreatic cancers, shows in fact favourable in vivo localizing properties in the experimental animal model of human tumor xenograft. 131I-AR-3-IgG1 was injected i.v. into 5 patients with suspected pancreatic cancer. Whole-body maps and spot views of the abdominal area were recorded with a computerized gamma-camera, and specific regions of interest drawn over the liver and spleen helped to define the kinetics of activity in these organs. Blood samples taken from 0.1-144 hours post-injection and daily urine collections over the same interval served to define the kinetics of plama distribution and removal of activity from the body. Different multicompartmental models were tested to fit the experimental data, assuming as the starting hypothesis that there was to be significant nonspecific tracer accumulation in the liver, spleen and bone marrow, as already observed for the majority of radioiodinated murine MoAbs injected into humans. Surgery confirmed pancreatic cancer in 3 out of the 5 patients (chronic pancreatitis and periampullary cancer in one each); in all these 3 patients immunostaining with the MoAb AR-3 demonstrated the presence of the CAR-3 antigen (with a cytoplasmic and endoluminal/secretory pattern of distribution). Nonspecific radioactivity accumulation in the liver, spleen and bone marrow was extremely low, linked essentially to the blood pool effect of circulating activity in these organs.(ABSTRACT TRUNCATED AT 250 WORDS)

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