Fattakhova Gul'nar, Masilamani Madhan, Borrego Francisco, Gilfillan Alasdair M, Metcalfe Dean D, Coligan John E
Receptor Cell Biology Section, Laboratory of Allergic Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, MD 20852, USA.
Traffic. 2006 Jun;7(6):673-85. doi: 10.1111/j.1600-0854.2006.00423.x.
Aggregation of the high-affinity immunoglobulin E (IgE) receptor (FcepsilonRI), expressed on mast cells and basophils, initiates the immediate hypersensitivity reaction. Aggregated FcepsilonRI has been reported to rapidly migrate to lipid rafts in RBL-2H3 cells. We confirmed that aggregated FcepsilonRI is found in the lipid raft fractions of cellular lysates. Furthermore, we show that the cross-linked FcepsilonRI remains associated with detergent-resistant structures upon internalization. Previous morphological studies have reported that aggregated FepsiloncRI is endocytosed via clathrin-coated pits, which in general are not lipid raft associated. To address this apparent discrepancy, we employed siRNA to suppress expression of components of the clathrin-mediated internalization machinery, namely, clathrin heavy chain, and the AP-2 (alpha-adaptin or mu2-subunit). Transferrin receptor (TfR) is endocytosed by a clathrin-mediated process and, as expected, each transfected siRNA caused a two to threefold elevation of TfR surface expression and almost completely inhibited its endocytosis. In contrast, there was no effect on surface expression levels of FcepsilonRI nor on the endocytosis of the dinitrophenyl-human serum albumin (DNP-HSA)/IgE/FcepsilonRI complex. On the contrary, internalization of DNP-HSA/IgE/FcepsilonRI was inhibited by overexpression of a dominant-negative dynamin mutant. We conclude that internalization of cross-linked FcRI does not require the AP-2/clathrin complex but is dynamin-dependent and may be lipid raft mediated.
表达于肥大细胞和嗜碱性粒细胞上的高亲和力免疫球蛋白E(IgE)受体(FcepsilonRI)聚集可引发速发型超敏反应。据报道,聚集的FcepsilonRI可迅速迁移至RBL-2H3细胞中的脂筏。我们证实,在细胞裂解物的脂筏组分中可发现聚集的FcepsilonRI。此外,我们还表明,交联的FcepsilonRI在内化后仍与抗去污剂结构相关联。先前的形态学研究报道,聚集的FepsiloncRI通过网格蛋白包被小窝进行内吞,而网格蛋白包被小窝通常与脂筏无关。为了解决这一明显的差异,我们使用小干扰RNA(siRNA)来抑制网格蛋白介导的内吞机制的组分,即网格蛋白重链和AP-2(α-衔接蛋白或μ2亚基)的表达。转铁蛋白受体(TfR)通过网格蛋白介导的过程进行内吞,正如预期的那样,每种转染的siRNA都会使TfR的表面表达升高两到三倍,并几乎完全抑制其内吞作用。相比之下,对FcepsilonRI的表面表达水平或二硝基苯基人血清白蛋白(DNP-HSA)/IgE/FcepsilonRI复合物的内吞作用均无影响。相反,DNP-HSA/IgE/FcepsilonRI的内吞作用受到显性负性发动蛋白突变体过表达的抑制。我们得出结论,交联的FcRI的内化不需要AP-2/网格蛋白复合物,而是依赖于发动蛋白,并且可能是由脂筏介导的。
