Abstract
Cytoskeletal polarization is crucial for many aspects of immune function, ranging from neutrophil migration to the sampling of gut flora by intestinal dendritic cells. It also plays a key role during lymphocyte cell–cell interactions, the most conspicuous of which is perhaps the immunological synapse (IS) formed between a T cell and an antigen-presenting cell (APC). IS formation is associated with the reorientation of the T cell’s microtubule-organizing center (MTOC) to a position just beneath the cell–cell interface. This cytoskeletal remodeling event aligns secretory organelles inside the T cell with the IS, enabling the directional release of cytokines and cytolytic factors toward the APC. MTOC polarization is therefore crucial for maintaining the specificity of a T cell’s secretory and cytotoxic responses. It has been known for some time that T cell receptor (TCR) stimulation activates the MTOC polarization response. It has been difficult, however, to identify the machinery that couples early TCR signaling to cytoskeletal remodeling. Over the past few years, considerable progress has been made in this area. This review will present an overview of recent advances, touching on both the mechanisms that drive MTOC polarization and the effector responses that require it. Particular attention will be paid to both novel and atypical members of the protein kinase C family, which are now known to play important roles in both the establishment and the maintenance of the polarized state.
Highlights
Cytoskeletal polarization is crucial for many aspects of immune function, ranging from neutrophil migration to the sampling of gut flora by intestinal dendritic cells
The immunological synapse (IS) was first observed in conjugates between T cells and antigenpresenting cells (APCs), it is clear that natural killer (NK) cells and B cells use similar structures to engage target cells and cells coated with surface-bound antigen, respectively (Dustin and Long, 2010; Harwood and Batista, 2010)
In addition to highlighting the importance of T cell receptor (TCR) signaling, these results provided perhaps the first indication that the molecular pathways involved in integrinmediated adhesion were separate from those that guided microtubule-organizing center (MTOC) polarization
Summary
Cytoskeletal polarization is crucial for many aspects of immune function, ranging from neutrophil migration to the sampling of gut flora by intestinal dendritic cells. This enables the directional secretion of proteins and other cargo toward the APC, which is thought to be crucial for maintaining the specificity of T cell responses (Huse et al, 2008). Because contact with the glass surface is established prior to TCR stimulation (typically using an antibody against a class I MHC protein expressed by the T cells) it is likely that we have isolated the pathways guiding MTOC polarity, which we can study independently of mechanisms controlling adhesion.
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