Nagata Koh, Yamamoto Akitsugu, Ban Nobuhiro, Tanaka Arowu R, Matsuo Michinori, Kioka Noriyuki, Inagaki Nobuya, Ueda Kazumitsu
Laboratory of Cellular Biochemistry, Division of Applied Life Sciences, Graduate School of Agriculture, Kyoto University, Kyoto 606-8502, Japan.
Biochem Biophys Res Commun. 2004 Nov 5;324(1):262-8. doi: 10.1016/j.bbrc.2004.09.043.
ABCA3 is highly expressed at the membrane of lamellar bodies in alveolar type II cells, in which pulmonary surfactant is stored. ABCA3 gene mutations cause fatal surfactant deficiency in newborns. We established HEK293 cells stably expressing human ABCA3 and analyzed the function. Exogenously expressed ABCA3 is glycosylated and localized at the intracellular vesicle membrane. ABCA3 is efficiently photoaffinity labeled by 8-azido-[alpha(32)P]ATP, but not by 8-azido-[gamma(32)P]ATP, when the membrane fraction is incubated in the presence of orthovanadate. Photoaffinity labeling of ABCA3 shows unique metal ion-dependence and is largely reduced by membrane pretreatment with 5% methyl-beta-cyclodextrin, which depletes cholesterol. Electron micrographs show that HEK293/hABCA3 cells contain multivesicular, lamellar body-like structures, which do not exist in HEK293 host cells. Some fuzzy components such as lipids accumulate in the vesicles. These results suggest that ABCA3 shows ATPase activity, which is induced by lipids, and may be involved in the biogenesis of lamellar body-like structures.
ABCA3在II型肺泡细胞板层小体的膜上高度表达,肺表面活性物质储存在该细胞中。ABCA3基因突变会导致新生儿致命的表面活性物质缺乏。我们建立了稳定表达人ABCA3的HEK293细胞并分析其功能。外源表达的ABCA3被糖基化并定位于细胞内囊泡膜。当膜组分在原钒酸盐存在下孵育时,ABCA3能被8-叠氮基-[α(32)P]ATP有效地进行光亲和标记,但不能被8-叠氮基-[γ(32)P]ATP标记。ABCA3的光亲和标记显示出独特的金属离子依赖性,并且在用5%甲基-β-环糊精进行膜预处理后会大大降低,5%甲基-β-环糊精会消耗胆固醇。电子显微镜照片显示,HEK293/hABCA3细胞含有多囊泡、板层小体样结构,而这些结构在HEK293宿主细胞中不存在。一些模糊的成分如脂质在囊泡中积累。这些结果表明,ABCA3显示出由脂质诱导的ATP酶活性,并且可能参与板层小体样结构的生物发生。
