首页> 外文期刊>European journal of pharmaceutics and biopharmaceutics: official journal of Arbeitsgemeinschaft fuer Pharmazeutische Verfahrenstechnik e.V >A comparison of three Peyer’s patch “M-like” cell culture models: particle uptake, bacterial interaction, and epithelial histology
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A comparison of three Peyer’s patch “M-like” cell culture models: particle uptake, bacterial interaction, and epithelial histology

机译:三个Peyer贴剂“M样”细胞培养模型的比较:粒子摄取,细菌相互作用和上皮组织学

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Graphical abstract Comparison of structure of three human Peyer’s patch M-like cell Caco-2/Raji B co-culture models. Caco-2: grey cells attached to filter; Raji B: black non-adherent cells. Ap, apical side. Display Omitted Abstract Intestinal Peyer’s patch (PP) microfold (M) cells transport microbes and particulates across the follicle-associated epithelium (FAE) as part of the mucosal immune surveillance system. In vitro human M-like cell co-culture models are used as screens to investigate uptake of antigens-in-nanoparticles, but the models are labour-intensive and there is inter-laboratory variability. We compared the three most established filter-grown Caco-2/Raji B cell co-culture systems. These were Model A (Kernéis et al., 1997), Model B (Gullberg et al., 2000), and Model C (Des Rieux et al. 2007). The criteria used were transepithelial resistance (TEER), the apparent permeability coefficient (P app ) of [ 14 C]-mannitol, M cell-like histology, as well as latex particle and Salmonella typhimurium translocation. Each co-culture model displayed substantial increases in particle translocation. Truncated microvilli compared to mono-cultures was their most consistent feature. The inverted model developed by des Rieux et al. (2007) displayed reductions in TEER and an increased (P app ), accompanied by the largest increase in particle translocation compared to the other two models. The normally-oriented model developed by Gullberg et al. (2000) was the only one to consistently display an increased translocation of Salmonella typhimurium . By applying a double Matrigel? coating on filters, altering the medium feeding regime for Raji B cells, and restricting the passage number of B cells, improvements to the Gullberg model B were achieved, as reflected by increased particle translocation and improved histology. In conclusion, this is the first time all three designs have been compared in one study and each displays phenotypic features of M-like cells. While Model C was the most robust co-culture, the Model B protocol could be improved by optimizing several variables and is less complicated to establish than the two inverted models. ]]>
机译:三种人Peyer贴片M样细胞Caco-2 / Raji B合培养模型结构的图形摘要比较。 Caco-2:附着灰色细胞过滤; Raji B:黑色非粘附细胞。 ap,apick侧。显示省略的抽象肠道Peyer的贴剂(PP)微塑料(M)细胞在卵泡相关上皮(Fae)上的微生物和颗粒作为粘膜免疫监测系统的一部分。体外人体m样细胞共培养模型用作筛网,以研究抗原纳米颗粒的摄取,但模型是劳动密集型的,并且存在实验室间变异性。我们比较了三种最成熟的过滤性Caco-2 / Raji B细胞共同培养系统。这些是模型A(Kernéis等,1997),模型B(Gullberg等,2000)和Model C(des Rieux等人2007)。使用的标准是Transepithelial抵抗(Teer),[14 c] - 甲醇,m个细胞样组织学的表观渗透系数(P app),以及胶乳颗粒和沙门氏菌酪蛋白易位。每个共培养模型显示粒子易位的显着增加。与单培养物相比,截短的微流动是它们最一致的特征。 Des Rieux等人开发的倒模。 (2007)展示了TEER和增加(P APP)的减少,伴随着与其他两个模型相比的粒子易位的最大增加。由Gullberg等人开发的正常型模型。 (2000)是唯一一个持续显示增加的沙门氏菌伤寒骨盆易位的人。通过应用双层matrigel?在过滤器上涂覆,改变Raji B细胞的介质进料制度,并限制B细胞的通过数量,通过增加的粒子易位和改进的组织学反映来实现对Gullberg模型B的改进。总之,这是第一次在一项研究中比较了所有三种设计,每个设计都显示了M样细胞的表型特征。虽然模型C是最强大的共同培养,但通过优化多个变量,可以提高模型B协议,而不是建立比两个反相模型更复杂。 ]]>

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