二烯油基磷脂酰胆碱可阻止大鼠肝星状细胞中转化生长因子- β 1介导的胶原积累。

Q. Cao, K. Mak, C. Lieber
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引用次数: 49

摘要

聚乙烯磷脂酰胆碱(PPC)是一种多不饱和磷脂酰胆碱的混合物,分别对狒狒和大鼠的酒精性和非酒精性肝纤维化有保护作用。在本研究中,我们评估了PPC的主要磷脂酰胆碱dilinoleylphosphatidyolcholine (DLPC)对大鼠培养的肝星状细胞(hsc)中转化生长因子- β 1介导的α 1(I)前胶原表达、金属前蛋白酶-1组织抑制剂(TIMP-1)和基质金属蛋白酶-13 (MMP-13)的抗纤维化作用。在原代培养激活的hsc中,tgf - β 1上调α 1(I)前胶原mRNA水平,同时增加培养基中I型胶原的积累。tgf - β也增加了培养基中TIMP-1 mRNA的表达和TIMP-1的积累,但培养基中MMP-13 mRNA的表达和浓度没有改变。DLPC完全阻断tgf - β 1诱导的α 1(I)前胶原mRNA表达的增加和培养基中胶原积累的减少。DLPC降低了培养基中TIMP-1 mRNA的表达水平和TIMP-1的积累,但没有改变培养基中MMP-13 mRNA的表达和浓度。棕榈酰亚油酰磷脂酰胆碱(PLPC)是PPC中第二丰富的成分,对HSC培养中胶原、TIMP-1和MMP-13的浓度没有影响。我们得出结论,DLPC通过下调α 1(I)前胶原和TIMP-1 mRNA的表达来阻止tgf - β 1介导的HSC纤维化。后一种效应导致TIMP-1的积累减少,在MMP-13 mRNA表达和MMP-13浓度不变的情况下,导致培养基中MMP-13/TIMP-1浓度的比例增大,有利于胶原降解和较少的胶原积累。DLPC的这种作用至少可以部分解释PPC对酒精性和其他肝脏纤维化疾病的抗纤维化作用。
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Dilinoleoylphosphatidylcholine prevents transforming growth factor-beta1-mediated collagen accumulation in cultured rat hepatic stellate cells.
Polyenylphosphatidylcholine (PPC), a mixture of polyunsaturated phosphatidylcholines, protects against alcoholic and nonalcoholic liver fibrosis in baboons and rats, respectively. In this study, we assessed the antifibrogenic action of dilinoleoylphosphatidylcholine (DLPC), the main phosphatidylcholine species of PPC, against transforming growth factor-beta1-mediated expression of alpha1(I) procollagen, tissue inhibitor of metallopreoteinase-1 (TIMP-1) and matrix metalloproteinase-13 (MMP-13) in cultured rat hepatic stellate cells (HSCs). In primary culture-activated HSCs, TGF-beta1 up-regulated the alpha1(I) procollagen mRNA level with a concomitant increase in type I collagen accumulation in culture media. Whereas TIMP-1 mRNA levels and TIMP-1 accumulation in media were also increased by TGF-beta1, MMP-13 mRNA expression and MMP-13 concentration in media were not altered. DLPC fully blocked TGF-beta1-induced increase in alpha1(I) procollagen mRNA expression and decreased collagen accumulation in media. Whereas TIMP-1 mRNA level and TIMP-1 accumulation in media were decreased by DLPC, MMP-13 mRNA expression and MMP-13 concentration in media were not changed by this treatment. Palmitoyl-linoleoylphosphatidylcholine (PLPC), the second most abundant component of PPC, had no effect on the concentrations of collagen, TIMP-1, and MMP-13 in HSC culture. We conclude that DLPC prevents TGF-beta1-mediated HSC fibrogenesis through down-regulation of alpha1(I) procollagen and TIMP-1 mRNA expression. The latter effect leads to a decreased accumulation of TIMP-1 that, in the presence of unchanged MMP-13 mRNA expression and MMP-13 concentration, results in a larger ratio of MMP-13/TIMP-1 concentrations in the culture media, favoring collagen degradation and lesser collagen accumulation. This effect of DLPC may explain, at least in part, the antifibrogenic action of PPC against alcoholic and other fibrotic disorders of the liver.
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