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放射性标记的嵌合抗-G(D3)神经节苷脂单克隆抗体KM871在SK-MEL-28黑色素瘤异种移植瘤中的特异性定位、γ相机成像及细胞内运输

Specific localization, gamma camera imaging, and intracellular trafficking of radiolabelled chimeric anti-G(D3) ganglioside monoclonal antibody KM871 in SK-MEL-28 melanoma xenografts.

作者信息

Lee F T, Rigopoulos A, Hall C, Clarke K, Cody S H, Smyth F E, Liu Z, Brechbiel M W, Hanai N, Nice E C, Catimel B, Burgess A W, Welt S, Ritter G, Old L J, Scott A M

机构信息

Ludwig Institute For Cancer Research, Melbourne Branch, Austin and Repatriation Medical Centre, Studley Road, Heidelberg, Victoria 3084, Australia.

出版信息

Cancer Res. 2001 Jun 1;61(11):4474-82.

Abstract

The chimeric monoclonal antibody KM871, directed against the G(D3) antigen, is under evaluation for its potential to target melanoma. To facilitate the in vivo evaluation of biodistribution properties and measurement of pharmacokinetics, KM871 was radiolabeled with (125)I via tyrosine residues and with (111)In via the bifunctional metal ion chelator C-functionalized trans-cyclohexyl diethylenetriaminepentaacetic acid (CHX-A"-DTPA) to lysine residues. Using antigen-positive SK-MEL-28 melanoma cells, immunoreactivities of 42 and 40% cell binding were obtained, respectively, for the two radioconjugates. Binding was enhanced in the presence of added unlabeled antibody. A humanized A33 antibody was similarly labeled with the two isotopes and used as a control. To determine and compare in vivo biodistribution characteristics of KM871 radiolabeled with (111)In or (125)I, mixtures of the radioconjugates were injected i.v. into BALB/c nude mice bearing G(D3)-positive-SK-MEL-28 melanoma xenografts. Gamma camera images were acquired; groups of five mice were sacrificed at various time intervals, and tumors, blood, and tissues were analyzed. (111)In-labeled CHX-A"-DTPA-KM871 showed a maximum tumor uptake of 41.9 +/- 7.0% injected dose/g at 72 h with prolonged retention over a 15-day period. The tumor:blood ratio was 3:1 by 72 h, and higher ratios were observed at later time points. No abnormal accumulation of (111)In-labeled conjugate was found in normal tissues. In contrast, there was little accumulation of (125)I-labeled KM871 in the same tumors. The specificity of antibody localization was confirmed by the low tumor uptake values for radiolabeled control antibody. Gamma camera imaging demonstrated excellent uptake of (111)In-labeled CHX-A"-DTPA-KM871 in the xenografts. Chromatographic analyses of xenograft cytosolic extracts demonstrated tumor internalization and catabolism of radiolabeled KM871 with the formation of small molecular weight metabolites. Laser scanning confocal microscopy demonstrated that the majority of intracellular KM871 is localized to lysosomes. Despite the catabolism of the radioconjugate, a dose-dependent increase in KM871 tumor localization was shown through immunohistochemical examination of xenograft biopsies. This study demonstrates for the first time the in vivo localization of a radiolabeled anti-G(D3) monoclonal antibody to G(D3)-expressing xenografts using gamma camera scanning techniques and tumor cell internalization of KM871 tagged with a green fluorescent dye, Alexa Fluor 488, through confocal microscopy. KM871 has potential for targeting tumors in patients with melanoma.

摘要

针对G(D3)抗原的嵌合单克隆抗体KM871,正因其靶向黑色素瘤的潜力而接受评估。为便于在体内评估其生物分布特性和测量药代动力学,KM871通过酪氨酸残基用(125)I进行放射性标记,并通过双功能金属离子螯合剂C-功能化反式环己基二乙烯三胺五乙酸(CHX-A”-DTPA)与赖氨酸残基结合用(111)In进行放射性标记。使用抗原阳性的SK-MEL-28黑色素瘤细胞,两种放射性缀合物分别获得了42%和40%的细胞结合免疫反应性。在添加未标记抗体的情况下,结合增强。一种人源化A33抗体同样用这两种同位素进行标记并用作对照。为确定和比较用(111)In或(125)I放射性标记的KM871的体内生物分布特征,将放射性缀合物混合物静脉注射到携带G(D3)阳性SK-MEL-28黑色素瘤异种移植物的BALB/c裸鼠体内。采集γ相机图像;在不同时间间隔处死每组五只小鼠,并分析肿瘤、血液和组织。(111)In标记的CHX-A”-DTPA-KM871在72小时时显示最大肿瘤摄取量为41.9±7.0%注射剂量/克,在15天内保持时间延长。到72小时时肿瘤与血液的比率为3:1,在随后的时间点观察到更高的比率。在正常组织中未发现(111)In标记的缀合物异常蓄积。相比之下,(125)I标记的KM871在相同肿瘤中的蓄积很少。放射性标记对照抗体的低肿瘤摄取值证实了抗体定位的特异性。γ相机成像显示(111)In标记的CHX-A”-DTPA-KM871在异种移植物中摄取良好。异种移植物胞质提取物的色谱分析表明放射性标记的KM871在肿瘤内化并分解代谢,形成小分子代谢物。激光扫描共聚焦显微镜显示细胞内的大多数KM871定位于溶酶体。尽管放射性缀合物发生了分解代谢,但通过异种移植物活检的免疫组织化学检查显示KM871在肿瘤中的定位呈剂量依赖性增加。本研究首次使用γ相机扫描技术证明了放射性标记的抗G(D3)单克隆抗体在体内定位于表达G(D3)的异种移植物,以及通过共聚焦显微镜观察到用绿色荧光染料Alexa Fluor 488标记的KM871在肿瘤细胞内化。KM871有潜力靶向黑色素瘤患者的肿瘤。

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