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用放射性标记抗体和免疫片段对实体瘤进行诊断与治疗。

Diagnosis of and therapy for solid tumors with radiolabeled antibodies and immune fragments.

作者信息

Carrasquillo J A, Krohn K A, Beaumier P, McGuffin R W, Brown J P, Hellström K E, Hellström I, Larson S M

出版信息

Cancer Treat Rep. 1984 Jan;68(1):317-28.

PMID:6607111
Abstract

Antibodies which are directed against human tumor-associated antigens can potentially be used as carriers of radioactivity for in vivo diagnosis (radioimmunodetection) or treatment (radioimmunotherapy) of solid tumors, including colon, hepatoma, cholangiocarcinoma, and melanoma. Murine monoclonal antibodies (MOAB), produced by the hybridoma technique of Kohler and Milstein, are replacing conventional heterosera as sources of antibodies, because MOAB can be produced in large quantities as reproducible reagents with homogeneous binding properties. We have studied human melanoma using MOAB IgG and Fab fragments that recognize the human melanoma-associated antigens p97 and "high-molecular-weight antigen." Both antigens are found in the membrane of melanomas at much larger concentrations than in normal adult tissues. We have performed radioimmunodetection studies with whole immunoglobulin and have detected 88% of lesions greater than 1.5 cm. We have used Fab fragments for radioimmunotherapy and have found that large doses of radiolabeled antibodies (up to 342 mCi) can be repetitively given to patients without excessive end-organ toxicity. Two of three patients treated with high-dose radiolabeled antimelanoma Fab showed an effect from the treatment. Although both technical and biologic problems remain, the use of radiolabeled antibodies that are directed against tumor-associated antigens holds future promise as a new therapeutic approach to solid tumors that are resistant to conventional therapy.

摘要

针对人类肿瘤相关抗原的抗体有可能用作放射性载体,用于实体瘤(包括结肠癌、肝癌、胆管癌和黑色素瘤)的体内诊断(放射免疫检测)或治疗(放射免疫疗法)。由科勒和米尔斯坦的杂交瘤技术产生的鼠单克隆抗体(MOAB)正在取代传统的异种血清作为抗体来源,因为MOAB可以大量生产,作为具有均匀结合特性的可重复试剂。我们使用识别人类黑色素瘤相关抗原p97和“高分子量抗原”的MOAB IgG和Fab片段研究了人类黑色素瘤。这两种抗原在黑色素瘤细胞膜中的浓度比正常成人组织中高得多。我们用全免疫球蛋白进行了放射免疫检测研究,检测到88%直径大于1.5厘米的病变。我们使用Fab片段进行放射免疫治疗,发现可以向患者重复给予大剂量的放射性标记抗体(高达342毫居里)而不会产生过度的终末器官毒性。三名接受高剂量放射性标记抗黑色素瘤Fab治疗的患者中有两名显示出治疗效果。尽管技术和生物学问题仍然存在,但使用针对肿瘤相关抗原的放射性标记抗体作为对传统治疗耐药的实体瘤的一种新治疗方法具有未来前景。

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