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Development of a drug targeting approach for cancer therapy: drug carrier-protein conjugate

机译:癌症治疗药物靶向方法的发展:药物载体 - 蛋白缀合物

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Targeted delivery of anticancer drugs is one of the most actively pursued goals in anticancer chemotherapy. A major disadvantage of anticancer drugs is their lack of selectivity for tumor tissue, which causes severe side effects and results in low cure rates. Any strategy by which a cytotoxic drug is targeted to the tumor, thus increasing the therapeutic index of the drug, is a way of improving cancer chemotherapy and minimizing systematic toxicity. This study covers the preparation of the gelatin microsphere (GM)- albumin (BSA) conjugate for the development of a "drug targeting" approach in cancer therapy. Gelatin microspheres of 5% (w/v) gelatin content were prepared by crosslinking with glutaraldehyde (GTA) at 0.5% (v/v) concentration. The particle size and morphology of microspheres were analyzed by Particle Size Analyzer and Scanning Electron Microscopy (SEM). Gelatin micospheres were chemically conjugated to bovine serum albumin in PBS (0.01M, pH 7.4) at 40C. The solution was then filtered and the GM-BSA conjugates were vacuum dried. The activity of BSA conjugated to GM was tested by using Immunodiffusion Techniques. The percent antigen-antibody binding between BSA and anti-BSA was evaluated by measuring the band widths of precipitates formed in the agar medium.
机译:有针对性的抗癌药物的交付是抗癌化疗最受积极的追求目标之一。抗癌药物的主要缺点是它们对肿瘤组织的选择性缺乏选择性,这导致严重的副作用并导致低固化率。任何细胞毒性药物靶向肿瘤的策略,从而增加药物的治疗指数,是改善癌症化疗和最小化系统毒性的一种方式。该研究涵盖了明胶微球(GM) - 白蛋白(BSA)缀合物的制备,用于癌症治疗中的“药物靶向”方法的开发。通过用0.5%(v / v)浓度的戊二醛(GTA)交联制备5%(w / v)明胶含量的明胶微球。通过粒度分析仪和扫描电子显微镜(SEM)分析微球的粒度和形态。将明胶酰亚胺酰亚胺在40℃下在PBS(0.01M,pH7.4)中的牛血清白蛋白进行化学缀合。然后过滤溶液,将GM-BSA缀合物真空干燥。通过使用免疫分离技术测试与GM缀合的BSA的活性。通过测量在琼脂培养基中形成的沉淀物的带宽来评价BSA和抗BSA之间的抗原抗体百分比百分比。

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