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藻酸钙-聚赖氨酸包埋后内脏脂肪中强制脂质分解的成纤维细胞的长期存活。

The prolonged survival of fibroblasts with forced lipid catabolism in visceral fat following encapsulation in alginate-poly-L-lysine.

机构信息

Department of Human Nutrition, The Ohio State University, Columbus, OH 43210, USA.

出版信息

Biomaterials. 2012 Aug;33(22):5638-49. doi: 10.1016/j.biomaterials.2012.04.035. Epub 2012 May 9.

Abstract

Although alginate-poly-L-lysine (AP(L)) encapsulation of cells producing bioactive peptides has been widely tested, it is unknown whether AP(L) supports lasting catabolic functions of encapsulated cells in adipose tissue, which are required for obesity reduction. We tested functions of AP(L)-encapsulated fibroblasts isolated from wild-type (WT) and aldehyde dehydrogenase 1a1 knockout mice (KO), which resist obesity on a high-fat (HF) diet, have a higher metabolic rate, and express increased levels of thermogenic uncoupling protein-1 (Ucp1) in their deleterious visceral fat depots compared to WT mice. To enable in vivo detection and quantification, fibroblasts were stably transfected with green-fluorescent protein. WT- or KO-containing microcapsules were injected into two visceral depots of WT mice fed an HF diet. Eighty days after transplantation, microcapsules were located in vivo using magnetic resonance imaging. KO microcapsules prevented weight gain in obese WT mice compared to a mock- and WT capsule-injected groups on an HF diet. The weight loss in KO-treated mice corresponded to lipid reduction and induction of thermogenesis in the injected visceral fat. The non-treated subcutaneous fat was not altered. Our data suggest that the AP(L) polymer supports long-term catabolic functions of genetically-modified fibroblasts, which can be potentially used for depot-specific obesity treatment.

摘要

尽管藻酸盐-聚-L-赖氨酸(AP(L))已被广泛用于封装产生生物活性肽的细胞,但尚不清楚 AP(L)是否支持封装细胞在脂肪组织中的持续分解代谢功能,而这些功能是减少肥胖所必需的。我们测试了从野生型(WT)和醛脱氢酶 1a1 敲除小鼠(KO)分离的 AP(L)包封成纤维细胞的功能。与 WT 小鼠相比,KO 小鼠在高脂肪(HF)饮食中抵抗肥胖,具有更高的代谢率,并在其有害的内脏脂肪储存中表达更高水平的解偶联蛋白 1(Ucp1)。为了能够进行体内检测和定量,成纤维细胞被稳定转染了绿色荧光蛋白。WT 或 KO 成纤维细胞微囊被注射到喂食 HF 饮食的 WT 小鼠的两个内脏脂肪中。移植 80 天后,使用磁共振成像在体内定位微囊。与 HF 饮食中模拟和 WT 微囊注射组相比,KO 微囊可防止肥胖 WT 小鼠体重增加。KO 处理小鼠的体重减轻与注射的内脏脂肪中的脂质减少和产热诱导相对应。未处理的皮下脂肪未改变。我们的数据表明,AP(L)聚合物支持基因修饰成纤维细胞的长期分解代谢功能,这可能可用于特定部位的肥胖治疗。

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