Rimm D L, Koslov E R, Kebriaei P, Cianci C D, Morrow J S
Department of Pathology, Yale University School of Medicine, New Haven, CT 06510, USA.
Proc Natl Acad Sci U S A. 1995 Sep 12;92(19):8813-7. doi: 10.1073/pnas.92.19.8813.
Calcium-dependent homotypic cell-cell adhesion, mediated by molecules such as E-cadherin, guides the establishment of classical epithelial cell polarity and contributes to the control of migration, growth, and differentiation. These actions involve additional proteins, including alpha- and beta-catenin (or plakoglobin) and p120, as well as linkage to the cortical actin cytoskeleton. The molecular basis for these interactions and their hierarchy of interaction remain controversial. We demonstrate a direct interaction between F-actin and alpha (E)-catenin, an activity not shared by either the cytoplasmic domain of E-cadherin or beta-catenin. Sedimentation assays and direct visualization by transmission electron microscopy reveal that alpha 1(E)-catenin binds and bundles F-actin in vitro with micromolar affinity at a catenin/G-actin monomer ratio of approximately 1:7 (mol/mol). Recombinant human beta-catenin can simultaneously bind to the alpha-catenin/actin complex but does not bind actin directly. Recombinant fragments encompassing the amino-terminal 228 residues of alpha 1(E)-catenin or the carboxyl-terminal 447 residues individually bind actin in cosedimentation assays with reduced affinity compared with the full-length protein, and neither fragment bundles actin. Except for similarities to vinculin, neither region contains sequences homologous to established actin-binding proteins. Collectively these data indicate that alpha 1 (E)-catenin is a novel actin-binding and -bundling protein and support a model in which alpha 1(E)-catenin is responsible for organizing and tethering actin filaments at the zones of E-cadherin-mediated cell-cell contact.
由E-钙黏蛋白等分子介导的钙依赖性同型细胞间黏附,引导经典上皮细胞极性的建立,并有助于控制细胞迁移、生长和分化。这些作用涉及其他蛋白质,包括α-连环蛋白和β-连环蛋白(或桥粒斑珠蛋白)以及p120,还涉及与皮质肌动蛋白细胞骨架的连接。这些相互作用的分子基础及其相互作用层次仍存在争议。我们证明了F-肌动蛋白与α(E)-连环蛋白之间存在直接相互作用,E-钙黏蛋白的细胞质结构域或β-连环蛋白均不具有这种活性。沉降分析和透射电子显微镜直接观察表明,α1(E)-连环蛋白在体外以微摩尔亲和力结合并束状化F-肌动蛋白,连环蛋白与G-肌动蛋白单体的比例约为1:7(摩尔/摩尔)。重组人β-连环蛋白可同时结合α-连环蛋白/肌动蛋白复合物,但不直接结合肌动蛋白。在沉降分析中,包含α1(E)-连环蛋白氨基末端228个残基或羧基末端447个残基的重组片段与全长蛋白相比,以降低的亲和力单独结合肌动蛋白,且两个片段均不束状化肌动蛋白。除了与纽蛋白相似外,这两个区域均不包含与已确定的肌动蛋白结合蛋白同源的序列。这些数据共同表明,α1(E)-连环蛋白是一种新型的肌动蛋白结合和束状化蛋白,并支持一种模型,即α1(E)-连环蛋白负责在E-钙黏蛋白介导的细胞间接触区域组织和拴系肌动蛋白丝。
