Department of Biochemistry, Albert Einstein College of Medicine, Bronx, New York, USA.
PLoS One. 2010 May 24;5(5):e10796. doi: 10.1371/journal.pone.0010796.
Fat storage-Inducing Transmembrane proteins 1 & 2 (FIT1/FITM1 and FIT2/FITM2) belong to a unique family of evolutionarily conserved proteins localized to the endoplasmic reticulum that are involved in triglyceride lipid droplet formation. FIT proteins have been shown to mediate the partitioning of cellular triglyceride into lipid droplets, but not triglyceride biosynthesis. FIT proteins do not share primary sequence homology with known proteins and no structural information is available to inform on the mechanism by which FIT proteins function. Here, we present the experimentally-solved topological models for FIT1 and FIT2 using N-glycosylation site mapping and indirect immunofluorescence techniques. These methods indicate that both proteins have six-transmembrane-domains with both N- and C-termini localized to the cytosol. Utilizing this model for structure-function analysis, we identified and characterized a gain-of-function mutant of FIT2 (FLL(157-9)AAA) in transmembrane domain 4 that markedly augmented the total number and mean size of lipid droplets. Using limited-trypsin proteolysis we determined that the FLL(157-9)AAA mutant has enhanced trypsin cleavage at K86 relative to wild-type FIT2, indicating a conformational change. Taken together, these studies indicate that FIT2 is a 6 transmembrane domain-containing protein whose conformation likely regulates its activity in mediating lipid droplet formation.
脂肪储存诱导跨膜蛋白 1 和 2(FIT1/FITM1 和 FIT2/FITM2)属于内质网中特有的进化保守蛋白家族,参与甘油三酯脂滴的形成。已经表明 FIT 蛋白介导细胞甘油三酯向脂滴的分配,但不参与甘油三酯的生物合成。FIT 蛋白与已知蛋白没有一级序列同源性,也没有结构信息可以说明 FIT 蛋白的作用机制。在这里,我们使用 N-糖基化位点作图和间接免疫荧光技术,提出了 FIT1 和 FIT2 的实验解决拓扑模型。这些方法表明,这两种蛋白质都有六个跨膜结构域,N 端和 C 端都位于细胞质中。利用该结构-功能分析模型,我们鉴定并表征了跨膜结构域 4 中 FIT2 的一个功能获得性突变体(FLL(157-9)AAA),该突变体显著增加了脂滴的总数和平均大小。通过有限胰蛋白酶水解,我们确定 FLL(157-9)AAA 突变体在 K86 处相对于野生型 FIT2 的胰蛋白酶切割增强,表明构象发生变化。综上所述,这些研究表明 FIT2 是一种含有 6 个跨膜结构域的蛋白质,其构象可能调节其在介导脂滴形成中的活性。
