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从木瓜蛋白酶消化的抗体片段中进行西妥昔单抗Fab的生化分离,并与铜进行放射性标记,以用于放射免疫治疗诊断。

Biochemical separation of Cetuximab-Fab from papain-digested antibody fragments and radiolabeling with Cu for potential use in radioimmunotheranostics.

作者信息

Chakravarty Rubel, Rohra Nanda, Jadhav Sachin, Sarma Haladhar Dev, Jain Ratnesh, Chakraborty Sudipta

机构信息

Radiopharmaceuticals Division, Bhabha Atomic Research Centre, Trombay, Mumbai, 400085, India; Homi Bhabha National Institute, Anushaktinagar, Mumbai, 400094, India.

Department of Chemical Engineering, Institute of Chemical Technology, Matunga, Mumbai, 400019, India.

出版信息

Appl Radiat Isot. 2023 Jun;196:110795. doi: 10.1016/j.apradiso.2023.110795. Epub 2023 Mar 28.

Abstract

Engineered Fab fragments of monoclonal antibodies (mAbs) after radiolabeling with suitable radiometals have the potential to play a key role in personalized radioimmunotheranostics of cancer patients. In this study, we have generated Fab fragment of Cetuximab, a mAb targeting epidermal growth factor receptor (EGFR) expression and purified from the Fc and other fragments by ultrafiltration and affinity chromatography. The Cetuximab-Fab was conjugated with a suitable bifunctional chelator and radiolabeled with no-carrier-added (NCA) Cu produced via Zn (n, p) Cu reaction in a nuclear reactor. The radioimmunoconjugate obtained after size exclusion chromatographic separation possessed >95% radiochemical purity and it retained its integrity over at least three half-lives of the radiometal. Biodistribution studies was performed in fibrosarcoma tumor bearing Swiss mice, which demonstrated the explicit need for purification of the Cetuximab-Fab from Fc fragments. Enhanced and rapid tumor uptake with decent tumor-to-background ratio with prolonged retention was observed when radiolabeled purified Cetuximab-Fab was intravenously administered in animal models. Overall, this preclinical study established the pivotal role of separation science and technology to obtain the radioimmunoconjugate with requisite purity in order to demonstrate optimal pharmacokinetics and maximized treatment efficacy.

摘要

用合适的放射性金属进行放射性标记后的单克隆抗体(mAb)工程化Fab片段,有潜力在癌症患者的个性化放射免疫诊疗中发挥关键作用。在本研究中,我们制备了西妥昔单抗的Fab片段,西妥昔单抗是一种靶向表皮生长因子受体(EGFR)表达的单克隆抗体,并通过超滤和亲和色谱从Fc片段及其他片段中纯化得到。西妥昔单抗-Fab与合适的双功能螯合剂偶联,并在核反应堆中通过Zn(n,p)Cu反应产生的无载体添加(NCA)Cu进行放射性标记。经尺寸排阻色谱分离后得到的放射免疫缀合物的放射化学纯度>95%,并且在放射性金属的至少三个半衰期内保持其完整性。在荷纤维肉瘤肿瘤的瑞士小鼠中进行了生物分布研究,结果表明从Fc片段中纯化西妥昔单抗-Fab非常必要。当在动物模型中静脉注射放射性标记的纯化西妥昔单抗-Fab时,观察到肿瘤摄取增强且迅速,肿瘤与背景比值良好,且滞留时间延长。总体而言,这项临床前研究确立了分离科学技术在获得具有所需纯度的放射免疫缀合物以证明最佳药代动力学和最大化治疗效果方面的关键作用。

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