Lanza R P, Borland K M, Staruk J E, Appel M C, Solomon B A, Chick W L
BioHybrid Technologies, Inc., Shrewsbury, Massachusetts 01545.
Endocrinology. 1992 Aug;131(2):637-42. doi: 10.1210/endo.131.2.1353441.
Extended survival of canine islet xenografts implanted in spontaneously diabetic BB/Wor rats has been achieved by islet encapsulation inside cylindrical chambers fabricated from permselective acrylic membranes. Intraperitoneal implantation of the encapsulated islets reversed the diabetic state of the 10 recipients within 24 h. Plasma glucose levels declined from a preimplantation level of 459 +/- 30 to 102 +/- 14 mg/dl during the first 10 days. All of the animals sustained these levels for at least 1 month, and 2 animals for at least 2 and 8 months, respectively. To confirm that glucose homeostasis resulted from the encapsulated islet grafts, the implants were removed from 2 rats 1 month postimplantation, whereas a third was removed at 2 months. Hyperglycemia was observed immediately in all 3 animals, with glucose levels rising from 100 +/- 3 to 510 +/- 43 mg/dl within 1 day. In contrast, diabetic control rats (n = 4) receiving nonencapsulated islets became hyperglycemic in less than 1 week. The iv glucose tolerance test K value (decline in glucose levels, percent per min) at 10 days was 2.3 +/- 0.4 compared with 0.6 +/- 0.1 (P less than 0.005) and 3.1 +/- 0.1 (P less than 0.02) for untreated diabetic (n = 4) and normal control (n = 4) groups. Histological analyses and electron microscopy of long term functioning grafts revealed well preserved islets, with hormone-producing alpha-, beta-, and delta-cells; the membranes were generally free of fibrosis and host cell adherence. These results demonstrate that permselective artificial membranes can protect discordant islet xenografts from both graft rejection and autoimmune destruction for more than 1 month in an animal model that is similar in several respects to human type I diabetes.
将犬胰岛异种移植物植入自发性糖尿病BB/Wor大鼠体内,通过将胰岛封装在由选择性渗透丙烯酸膜制成的圆柱形腔室内,实现了移植物的长期存活。腹腔内植入封装的胰岛在24小时内逆转了10只受体的糖尿病状态。在最初的10天内,血浆葡萄糖水平从植入前的459±30降至102±14mg/dl。所有动物维持这些水平至少1个月,2只动物分别维持至少2个月和8个月。为了证实葡萄糖稳态是由封装的胰岛移植物导致的,在植入后1个月从2只大鼠体内取出移植物,而第3只在2个月时取出。所有3只动物立即出现高血糖,葡萄糖水平在1天内从100±3升至510±43mg/dl。相比之下,接受未封装胰岛的糖尿病对照大鼠(n = 4)在不到1周内就出现了高血糖。植入后10天的静脉葡萄糖耐量试验K值(葡萄糖水平下降,每分钟百分比)为2.3±0.4,而未治疗的糖尿病组(n = 4)和正常对照组(n = 4)分别为0.6±0.1(P<0.005)和3.1±0.1(P<0.02)。对长期功能良好的移植物进行组织学分析和电子显微镜检查发现,胰岛保存良好,有产生激素的α、β和δ细胞;膜通常没有纤维化和宿主细胞黏附。这些结果表明,在一个在几个方面与人类I型糖尿病相似的动物模型中,选择性渗透人工膜可以保护不匹配的胰岛异种移植物免受移植排斥和自身免疫破坏超过1个月。
