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通过肼基烟酰胺衍生物放射性标记的锝-99m-人多克隆免疫球蛋白用于大鼠感染病灶的成像。

Technetium-99m-human polyclonal IgG radiolabeled via the hydrazino nicotinamide derivative for imaging focal sites of infection in rats.

作者信息

Abrams M J, Juweid M, tenKate C I, Schwartz D A, Hauser M M, Gaul F E, Fuccello A J, Rubin R H, Strauss H W, Fischman A J

机构信息

Department of Radiology, Massachusetts General Hospital, Boston 02114.

出版信息

J Nucl Med. 1990 Dec;31(12):2022-8.

PMID:2266401
Abstract

The biologic behavior of human polyclonal immunoglobulin (IgG) radiolabeled with technetium-99m (99mTc) by a novel method, via a nicotinyl hydrazine derivative, was evaluated in rats. Technetium-99m- and indium-111-IgG were co-administered to normal rats and biodistribution was determined at 2, 6, and 16 hr. The inflammation imaging properties of the two reagents were compared in rats with deep-thigh infection due to Escherichia coli. Blood clearance of both antibody preparations was well described by a bi-exponential function: (99mTc-IgG: t1/2 = 3.82 +/- 0.89 and 57.52 +/- 1.70 hr. 111In-IgG: 3.93 +/- 0.117 and 40.71 +/- 1.26 hr). Biodistributions in the solid organs were similar, however, small but statistically significant differences were detected: 99mTc-IgG greater than 111In-IgG in lung, liver, and spleen; 99mTc-IgG less than 111In-IgG in kidney and skeletal muscle (p less than 0.01). At all three imaging times, target-to-background ratio and percent residual activity for the two compounds were remarkably similar. These studies establish that human polyclonal IgG labeled with 99mTc via a nicotinyl hydrazine modified intermediate is equivalent to 111In-IgG for imaging focal sites of infection in experimental animals.

摘要

通过一种新型方法,经烟酰肼衍生物用锝-99m(99mTc)对人多克隆免疫球蛋白(IgG)进行放射性标记,并在大鼠体内评估其生物学行为。将99mTc-IgG和铟-111-IgG共同给予正常大鼠,并在2小时、6小时和16小时测定其生物分布。在患有大肠杆菌引起的大腿深部感染的大鼠中比较了这两种试剂的炎症成像特性。两种抗体制剂的血液清除情况均可用双指数函数很好地描述:(99mTc-IgG:t1/2 = 3.82±0.89和57.52±1.70小时。111In-IgG:3.93±0.117和40.71±1.26小时)。在实体器官中的生物分布相似,然而,检测到了虽小但具有统计学意义的差异:肺、肝和脾中99mTc-IgG大于111In-IgG;肾和骨骼肌中99mTc-IgG小于111In-IgG(p<0.01)。在所有三个成像时间点,两种化合物的靶本底比和残留活性百分比非常相似。这些研究表明,通过烟酰肼修饰中间体用99mTc标记的人多克隆IgG在实验动物中成像感染灶时与111In-IgG相当。

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