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甲胺减少肺泡II型细胞板层小体中新合成的磷脂酰胆碱的转运和包装。

Methylamine decreases trafficking and packaging of newly synthesized phosphatidylcholine in lamellar bodies in alveolar type II cells.

作者信息

Chander A, Sen N, Wu A M, Higgins S, Wadsworth S, Spitzer A R

机构信息

Department of Pediatrics, Jefferson Medical College, Thomas Jefferson University, Philadelphia, PA 19107, USA.

出版信息

Biochem J. 1996 Aug 15;318 ( Pt 1)(Pt 1):271-8. doi: 10.1042/bj3180271.

Abstract

Lung lamellar bodies, the storage organelles for lung surfactant phosphatidylcholine (PC), maintain an acidic pH that can be increased with weak bases. This study investigates the effect of a weak base, methylamine, on the pH in lamellar bodies and on the trafficking and packaging of newly synthesized PC in lamellar bodies. Methylamine increased the pH of isolated lung lamellar bodies and of lamellar bodies in intact cells. Metabolic labelling of isolated type II cells with [methyl-3H]choline showed that although methylamine (2.5-10 mM) did not alter the labelling of cellular or microsomal PC and disaturated PC, it decreased the labelling of the PC and disaturated PC in lamellar bodies. The packaging of PC in lamellar bodies (the specific activities ratio between the PC in lamellar bodies and the microsomal PC) also decreased in a time- and concentration-dependent manner. The cellular synthesis of PC or its packaging into lamellar bodies was unaltered by brefeldin A, suggesting that the Golgi was not involved in PC packaging. Although methylamine also increased surfactant secretion, the inhibition of PC packaging in lamellar bodies seems unrelated to the secretagogue effect, (1) on the basis of metabolic consequences of increased secretion and (2) because ATP, another secretagogue, did not inhibit PC packaging. Methylamine seems to inhibit PC packaging by inhibiting trafficking of PC to lipid-rich light subcellular fractions. Together our results suggest that the trafficking of surfactant PC into lamellar bodies might be sensitive to changes in the pH of lamellar bodies.

摘要

肺板层小体是肺表面活性物质磷脂酰胆碱(PC)的储存细胞器,维持着可被弱碱升高的酸性pH值。本研究调查了弱碱甲胺对板层小体pH值以及新合成的PC在板层小体中的运输和包装的影响。甲胺升高了分离的肺板层小体以及完整细胞中板层小体的pH值。用[甲基 - 3H]胆碱对分离的II型细胞进行代谢标记显示,尽管甲胺(2.5 - 10 mM)不会改变细胞或微粒体PC以及二饱和PC的标记,但它降低了板层小体中PC和二饱和PC的标记。板层小体中PC的包装(板层小体中PC与微粒体PC之间的比活性)也以时间和浓度依赖性方式降低。布雷菲德菌素A未改变PC的细胞合成或其在板层小体中的包装,这表明高尔基体不参与PC包装。尽管甲胺也增加了表面活性物质的分泌,但板层小体中PC包装的抑制似乎与促分泌作用无关,(1)基于分泌增加的代谢后果,(2)因为另一种促分泌剂ATP并未抑制PC包装。甲胺似乎通过抑制PC向富含脂质的轻亚细胞组分的运输来抑制PC包装。我们的结果共同表明,表面活性物质PC向板层小体的运输可能对板层小体pH值的变化敏感。

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