Fukumori Y, Ichikawa H, Tokumitsu H, Miyamoto M, Jono K, Kanamori R, Akine Y, Tokita N
Faculty of Pharmaceutical Sciences, Kobe-Gakuin University, Japan.
Chem Pharm Bull (Tokyo). 1993 Jun;41(6):1144-8. doi: 10.1248/cpb.41.1144.
Microcapsules of hygroscopic, highly water-soluble gadopentetate dimeglumine (Gd-DTPA-DM) for use in preliminary in vivo experiments for neutron-capture therapy were designed. They were prepared with such properties as a particle size small enough to be suspended and injected through a syringe, a negligible release of Gd-DTPA-DM, and a high drug content by means of the Wurster process, a spray coating method using a spouted bed with a draft tube. They were composed of lactose cores of 53-63 microm, an undercoat of ethyl cellulose (EC) and polyvinylpyrrolidone (PVP), a drug-layer of Gd-DTPA-DM, EC and PVP, a waterproof coat and a release-sustaining overcoat of EC and cholesterol (1:1), and a surface treated with hydrogenated egg lecithin. By curing at 110 degrees C for 30 min after mixing with 20% pulverized mannitol powder, the 20% overcoating suppressed the release of Gd-DTPA-DM from 75-106 microm microcapsules to less than 10% for the first 20 min, which was the period required to prepare a suspension, inject it and irradiate the neutron. The microcapsules could be used to confirm that the intracellular presence of Gd is not critical in gadolinium neutron-capture therapy.
设计了用于中子俘获治疗初步体内实验的吸湿性、高水溶性钆喷酸葡甲胺(Gd-DTPA-DM)微胶囊。采用Wurster法(一种使用带导流管的喷动床的喷雾包衣方法)制备微胶囊,使其具有足够小的粒径以便通过注射器悬浮和注射、Gd-DTPA-DM释放可忽略不计以及药物含量高的特性。它们由53 - 63微米的乳糖核、乙基纤维素(EC)和聚乙烯吡咯烷酮(PVP)的底涂层、Gd-DTPA-DM、EC和PVP的药物层、防水涂层以及EC和胆固醇(1:1)的缓释外涂层组成,并经氢化卵磷脂处理表面。与20%的甘露醇粉末混合后在110℃固化30分钟,20%的外涂层将75 - 106微米微胶囊中Gd-DTPA-DM在最初20分钟内的释放抑制到小于10%,这是制备悬浮液、注射并照射中子所需的时间。这些微胶囊可用于确认在钆中子俘获治疗中钆在细胞内的存在并非关键因素。
