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Effects of phosphatidylcholine and sodium deoxycholate on human primary adipocytes and fresh human adipose tissue

机译:磷脂酰胆碱和脱氧胆酸钠对人原代脂肪细胞和新鲜人脂肪组织的影响

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Recent studies introduced the novel concept of chemical lipolysis where phosphatidylcholine (PC), an active component of commercial preparations, plays a pivotal role. Other studies suggested that sodium deoxycholate (DOC), an excipient contained in medical preparations, could be the real active component performing an adipocytolytic action. We investigated the effects of PC and DOC on human primary adipocyte cultures and on human fresh adipose tissue. Human adipocytes isolated by Rodbell's method, were cultured onto type I collagen-coated glass coverslips, placed into 24-well tissue culture plates. Cells were incubated with or without DOC (5-7-9%), PC (5%) or DOC/PC mixture and observed under phase contrast microscope. After incubation, cells were stained with Oil Red-O and with acridine orange/ethidium bromide to observe necrotic cells with phase contrast microscope and fluorescent microscope, respectively. Histological specimens from adipose tissue biopsies were observed with phase contrast microscopy and with scanning electron microscopy. To investigate the lipid pattern variability in the different experimental conditions, culture medium obtained from the different treatments was subjected to lipid extraction and subsequently to thin layer chromatography (TLC). Microscopic observation of adipocytes showed that DOC treatment led to a detrimental morphological effect in a dose-dependent manner. PC treatment did not significantly affect adipocyte viability. On the contrary, results from experiments aimed to analyze the effects of PC/DOC combined treatment suggested a PC protective role against the DOC harmful effects on adipocytes. Results indicated that clinical effects, observed in local treatment with pharmaceutical preparation, could be due only to DOC, a detergent inducing nonspecific lysis of cell membranes following adipocyte necrosis. On the other hand, PC could likely be incorporated in the lipid bilayer, thus strongly reducing the disruptive DOC effects.
机译:最近的研究介绍了化学脂肪分解的新概念,其中磷脂酰胆碱(PC)是商业制剂的活性成分,起着关键作用。其他研究表明,药物制剂中所含的赋形剂脱氧胆酸钠(DOC)可能是执行脂肪分解细胞作用的真正活性成分。我们调查了PC和DOC对人原代脂肪细胞培养以及对人新鲜脂肪组织的影响。将通过Rodbell方法分离的人脂肪细胞培养到I型胶原蛋白包被的玻璃盖玻片上,并置于24孔组织培养板中。将细胞在有或没有DOC(5-7-9%),PC(5%)或DOC / PC混合物的情况下孵育,并在相差显微镜下观察。孵育后,将细胞用油红-O和a啶橙/溴化乙锭染色,分别用相差显微镜和荧光显微镜观察坏死细胞。用相差显微镜和扫描电子显微镜观察来自脂肪组织活检的组织学标本。为了研究在不同实验条件下脂质模式的可变性,将从不同处理获得的培养基进行脂质提取,然后进行薄层色谱法(TLC)。脂肪细胞的显微镜观察表明,DOC处理以剂量依赖的方式导致有害的形态学作用。 PC处理并未显着影响脂肪细胞的生存能力。相反,旨在分析PC / DOC联合治疗效果的实验结果表明,PC对DOC对脂肪细胞的有害作用具有保护作用。结果表明,在用药物制剂进行局部治疗时观察到的临床效果可能仅归因于DOC,DOC是一种去污剂,可引起脂肪细胞坏死后细胞膜的非特异性裂解。另一方面,PC可能会掺入脂质双层中,从而大大降低破坏性DOC的影响。

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