Localized Lipid Packing of Transmembrane Domains Impedes Integrin Clustering

Integrin clustering plays a pivotal role in a host of cell functions. Hetero-dimeric integrin adhesion receptors regulate cell migration, survival, and differentiation by communicating signals bidirectionally across the plasma membrane. Thus far, crystallographic structures of integrin components are solved only separately, and for some integrin types. Also, the sequence of interactions that leads to signal transduction remains ambiguous. Particularly, it remains controversial whether the homo-dimerization of integrin transmembrane domains occurs following the integrin activation (i.e. when integrin ectodomain is stretched out) or if it regulates integrin clustering. This study employs molecular dynamics modeling approaches to address these questions in molecular details and sheds light on the crucial effect of the plasma membrane. Conducting a normal mode analysis of the intact αllbβ3 integrin, it is demonstrated that the ectodomain and transmembrane-cytoplasmic domains are connected via a membrane-proximal hinge region, thus merely transmembrane-cytoplasmic domains are modeled. By measuring the free energy change and force required to form integrin homo-oligomers, this study suggests that the β-subunit homo-oligomerization potentially regulates integrin clustering, as opposed to α-subunit, which appears to be a poor regulator for the clustering process. If α-subunits are to regulate the clustering they should overcome a high-energy barrier formed by a stable lipid pack around them. Finally, an outside-in activation-clustering scenario is speculated, explaining how further loading the already-active integrin affects its homo-oligomerization so that focal adhesions grow in size.

Focal adhesions are complex, dynamic structures of multiple proteins that act as the cell's mechanical anchorage to its surrounding. Integrins are proteins linking the cell inner and outer environments, which act as a bridge that crosses the cell membrane. Integrins respond to mechanical loads exerted to them by changing their conformations. Several diseases, such as atherosclerosis and different types of cancer, are caused by altered function of integrins. Essential to the formation of focal adhesions is the process of integrin clustering. Bidirectional integrin signaling involves conformational changes in this protein, clustering, and finally the assembly of a large intracellular adhesion complex. Integrin clustering is defined as the interaction of integrins to form lateral assemblies that eventually lead to focal adhesion formation. The effect of the plasma membrane on formation of integrin clusters has been largely neglected in current literature; subsequently some apparently contradictory data has been reported by a number of researchers in the field. Using a molecular dynamics modeling approach, a computational method that simulates systems in a full-atomic scale, we probe the role of the plasma membrane in integrin clustering and hypothesize a clustering scenario that explains the relationship between integrin activation and focal adhesion growth.