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角质形成细胞生长因子可促进胎鼠肺Ⅱ型细胞的成熟。

Keratinocyte growth factor enhances maturation of fetal rat lung type II cells.

作者信息

Chelly N, Mouhieddine-Gueddiche O B, Barlier-Mur A M, Chailley-Heu B, Bourbon J R

机构信息

INSERM, U319, Developpement Normal et Pathologique des Fonctions Epithéliales, Université Paris 7-Denis Diderot, Paris, France.

出版信息

Am J Respir Cell Mol Biol. 1999 Mar;20(3):423-32. doi: 10.1165/ajrcmb.20.3.3201.

Abstract

Keratinocyte growth factor (KGF) or fibroblast growth factor (FGF)-7, a peptide produced by stromal cells and in particular by lung mesenchyme, has recently been shown to influence early lung morphogenesis and to be a mitogen for fetal and adult alveolar type II cells. Although contradictory findings have been reported regarding its effects on surfactant protein expression, its effects on surfactant phospholipids have not been studied. We investigated the effects of KGF on the synthesis of surfactant components by cultured fetal rat type II cells isolated during the late gestational period, when surfactant accumulates in preparation for extrauterine life. We show that KGF is a potent stimulus of surfactant phospholipid synthesis, particularly for the major component of surfactant, disaturated phosphatidylcholine (DSPC). KGF increased choline incorporation into DSPC in a dose-dependent manner up to 25 ng/ml (1.3 x 10(-9) M), and this effect was greater for surfactant than for nonsurfactant DSPC. KGF was several times more potent in this respect than acidic FGF at the same molar concentration. KGF, similar to epidermal growth factor, also stimulated acetate incorporation and increased the surfactant phospholipid and DSPC content of cultured cells twofold. These effects correlated with increased choline phosphate cytidylyltransferase activity and increased fatty acid synthase activity and gene expression. KGF also induced a dose-dependent stimulation of surfactant protein-A, -B, and -C gene expression, leading to a 2- to 3-fold increase in their messenger RNAs. KGF therefore stimulates the synthesis of all surfactant components in developing type II cells at the time of surfactant accumulation. Its secretion by lung fibroblasts may thus be an important factor in promoting the maturation of fetal lung epithelium and the synthesis of sufficient surfactant. The results suggest that KGF could provide a new therapeutic agent for the management of the immature or injured lung.

摘要

角质形成细胞生长因子(KGF)即成纤维细胞生长因子(FGF)-7,是一种由基质细胞尤其是肺间充质产生的肽,最近已被证明可影响早期肺形态发生,并且是胎儿和成年肺泡II型细胞的有丝分裂原。尽管关于其对表面活性蛋白表达的影响已有相互矛盾的报道,但其对表面活性磷脂的影响尚未得到研究。我们研究了KGF对培养的孕晚期分离的胎鼠II型细胞表面活性成分合成的影响,此时表面活性物质开始积累以准备宫外生活。我们发现KGF是表面活性磷脂合成的有效刺激物,特别是对于表面活性物质的主要成分二饱和磷脂酰胆碱(DSPC)。KGF以剂量依赖的方式增加胆碱掺入DSPC,最高可达25 ng/ml(1.3×10⁻⁹ M),并且这种作用对表面活性物质比非表面活性物质的DSPC更大。在相同摩尔浓度下,KGF在这方面比酸性FGF的效力高几倍。与表皮生长因子类似,KGF还刺激乙酸掺入,并使培养细胞的表面活性磷脂和DSPC含量增加两倍。这些作用与胆碱磷酸胞苷转移酶活性增加、脂肪酸合酶活性增加以及基因表达增加相关。KGF还诱导表面活性蛋白-A、-B和-C基因表达的剂量依赖性刺激,导致其信使RNA增加2至3倍。因此,在表面活性物质积累时,KGF刺激发育中的II型细胞中所有表面活性成分的合成。肺成纤维细胞分泌KGF可能是促进胎儿肺上皮成熟和合成足够表面活性物质的重要因素。结果表明,KGF可为未成熟或受损肺的治疗提供一种新的治疗剂。

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