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用于在猴脑中有或无放射治疗情况下进行化疗药物控释的可生物降解聚合物。

Biodegradable polymers for controlled delivery of chemotherapy with and without radiation therapy in the monkey brain.

作者信息

Brem H, Tamargo R J, Olivi A, Pinn M, Weingart J D, Wharam M, Epstein J I

机构信息

Department of Neurosurgery, Johns Hopkins University School of Medicine, Baltimore, Maryland.

出版信息

J Neurosurg. 1994 Feb;80(2):283-90. doi: 10.3171/jns.1994.80.2.0283.

Abstract

Sustained drug delivery by biodegradable polymer devices can increase the therapeutic efficacy of drugs by producing high local tissue concentrations over extended periods of time. It has been shown previously that implantation of controlled-release polymers impregnated with the nitrosourea carmustine (BCNU) extended the period of survival in rats bearing the 9L glioma compared with similar rats treated with systemically administered BCNU. This study evaluated the effect on the monkey brain of interstitial delivery of BCNU by the biodegradable polyanhydride copolymer poly[bis(p-carboxyphenoxy)propane]anhydride (PCPP) and sebacic acid (SA) in a 20:80 formulation (PCPP:SA). The effect of combining interstitial BCNU with radiation therapy was also evaluated. Eighteen male cynomolgus monkeys were randomly assigned to one of four groups: a control group; a group with implantation of empty polymer; a group with implantation of BCNU-loaded polymer; and a group with implantation of empty polymer in the right hemisphere and BCNU-loaded polymer in the left hemisphere, followed by irradiation. The effects were evaluated radiologically and histologically at specified times. A local reaction by the brain to the polymer was found, which was greater when the polymer contained BCNU. Local cerebral edema was observed radiographically on postoperative Day 14 and had resolved by Day 72. Histologically, a subacute cellular inflammatory response was seen on postoperative Day 16, which had changed to a chronic inflammatory response by Day 72. In the group with radiation therapy administered to the hemisphere bearing BCNU-loaded polymer, only localized pathological changes were detected. In all animals, brain distant from the polymer implantation site was normal. No neurological or general deleterious effects were seen in any of the animals. It is concluded that the interstitial delivery of BCNU by the polyanhydride polymer PCPP:SA is safe in the primate brain and that concomitant radiation therapy did not lead to any adverse effects. These experimental findings are important to an understanding of the clinical effects of PCPP:SA implants in treating brain diseases.

摘要

可生物降解聚合物装置实现的持续药物递送能够通过在较长时间内产生高局部组织浓度来提高药物的治疗效果。先前的研究表明,与全身给药的卡莫司汀(BCNU)治疗的类似大鼠相比,植入浸渍有亚硝基脲卡莫司汀(BCNU)的控释聚合物可延长携带9L胶质瘤大鼠的生存期。本研究评估了以20:80配方(PCPP:SA)的可生物降解聚酸酐共聚物聚[双(对羧基苯氧基)丙烷]酸酐(PCPP)和癸二酸(SA)对BCNU进行间质递送对猴脑的影响。还评估了间质BCNU与放射治疗联合使用的效果。18只雄性食蟹猴被随机分配到四组中的一组:对照组;植入空聚合物的组;植入载有BCNU聚合物的组;以及右半球植入空聚合物、左半球植入载有BCNU聚合物并随后进行照射的组。在特定时间通过放射学和组织学评估效果。发现大脑对聚合物有局部反应,当聚合物含有BCNU时反应更大。术后第14天通过影像学观察到局部脑水肿,第72天时消退。组织学上,术后第16天可见亚急性细胞炎症反应,到第72天时已转变为慢性炎症反应。在对载有BCNU聚合物的半球进行放射治疗的组中,仅检测到局部病理变化。在所有动物中,远离聚合物植入部位的脑均正常。在任何动物中均未观察到神经或全身有害影响。得出的结论是,聚酸酐聚合物PCPP:SA对BCNU的间质递送在灵长类动物脑中是安全的,并且联合放射治疗未导致任何不良反应。这些实验结果对于理解PCPP:SA植入物治疗脑部疾病的临床效果很重要。

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