TY - JOUR AB - Blood platelets are critical for hemostasis and thrombosis, but also play diverse roles during immune responses. We have recently reported that platelets migrate at sites of infection in vitro and in vivo. Importantly, platelets use their ability to migrate to collect and bundle fibrin (ogen)-bound bacteria accomplishing efficient intravascular bacterial trapping. Here, we describe a method that allows analyzing platelet migration in vitro, focusing on their ability to collect bacteria and trap bacteria under flow. AU - Fan, Shuxia AU - Lorenz, Michael AU - Massberg, Steffen AU - Gärtner, Florian R ID - 6354 IS - 18 JF - Bio-Protocol KW - Platelets KW - Cell migration KW - Bacteria KW - Shear flow KW - Fibrinogen KW - E. coli SN - 2331-8325 TI - Platelet migration and bacterial trapping assay under flow VL - 8 ER - TY - JOUR AB - The insect’s fat body combines metabolic and immunological functions. In this issue of Developmental Cell, Franz et al. (2018) show that in Drosophila, cells of the fat body are not static, but can actively “swim” toward sites of epithelial injury, where they physically clog the wound and locally secrete antimicrobial peptides. AU - Casano, Alessandra M AU - Sixt, Michael K ID - 318 IS - 4 JF - Developmental Cell TI - A fat lot of good for wound healing VL - 44 ER - TY - JOUR AB - Migrating cells penetrate tissue barriers during development, inflammatory responses, and tumor metastasis. We study if migration in vivo in such three-dimensionally confined environments requires changes in the mechanical properties of the surrounding cells using embryonic Drosophila melanogaster hemocytes, also called macrophages, as a model. We find that macrophage invasion into the germband through transient separation of the apposing ectoderm and mesoderm requires cell deformations and reductions in apical tension in the ectoderm. Interestingly, the genetic pathway governing these mechanical shifts acts downstream of the only known tumor necrosis factor superfamily member in Drosophila, Eiger, and its receptor, Grindelwald. Eiger-Grindelwald signaling reduces levels of active Myosin in the germband ectodermal cortex through the localization of a Crumbs complex component, Patj (Pals-1-associated tight junction protein). We therefore elucidate a distinct molecular pathway that controls tissue tension and demonstrate the importance of such regulation for invasive migration in vivo. AU - Ratheesh, Aparna AU - Biebl, Julia AU - Smutny, Michael AU - Veselá, Jana AU - Papusheva, Ekaterina AU - Krens, Gabriel AU - Kaufmann, Walter AU - György, Attila AU - Casano, Alessandra M AU - Siekhaus, Daria E ID - 308 IS - 3 JF - Developmental Cell TI - Drosophila TNF modulates tissue tension in the embryo to facilitate macrophage invasive migration VL - 45 ER - TY - JOUR AB - Dendritic cells (DCs) are sentinels of the adaptive immune system that reside in peripheral organs of mammals. Upon pathogen encounter, they undergo maturation and up-regulate the chemokine receptor CCR7 that guides them along gradients of its chemokine ligands CCL19 and 21 to the next draining lymph node. There, DCs present peripherally acquired antigen to naïve T cells, thereby triggering adaptive immunity. AU - Leithner, Alexander F AU - Renkawitz, Jörg AU - De Vries, Ingrid AU - Hauschild, Robert AU - Haecker, Hans AU - Sixt, Michael K ID - 437 IS - 6 JF - European Journal of Immunology TI - Fast and efficient genetic engineering of hematopoietic precursor cells for the study of dendritic cell migration VL - 48 ER - TY - JOUR AB - The release of IgM is the first line of an antibody response and precedes the generation of high affinity IgG in germinal centers. Once secreted by freshly activated plasmablasts, IgM is released into the efferent lymph of reactive lymph nodes as early as 3 d after immunization. As pentameric IgM has an enormous size of 1,000 kD, its diffusibility is low, and one might wonder how it can pass through the densely lymphocyte-packed environment of a lymph node parenchyma in order to reach its exit. In this issue of JEM, Thierry et al. show that, in order to reach the blood stream, IgM molecules take a specific micro-anatomical route via lymph node conduits. AU - Reversat, Anne AU - Sixt, Michael K ID - 5672 IS - 12 JF - Journal of Experimental Medicine SN - 00221007 TI - IgM's exit route VL - 215 ER -