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Publication : Minimal amounts of kindlin-3 suffice for basal platelet and leukocyte functions in mice.

First Author  Klapproth S Year  2015
Journal  Blood Volume  126
Issue  24 Pages  2592-600
PubMed ID  26438512 Mgi Jnum  J:229952
Mgi Id  MGI:5754930 Doi  10.1182/blood-2015-04-639310
Citation  Klapproth S, et al. (2015) Minimal amounts of kindlin-3 suffice for basal platelet and leukocyte functions in mice. Blood 126(24):2592-600
abstractText  Hematopoietic cells depend on integrin-mediated adhesion and signaling, which is induced by kindlin-3 and talin-1. To determine whether platelet and polymorphonuclear neutrophil (PMN) functions require specific thresholds of kindlin-3, we generated mouse strains expressing 50%, 10%, or 5% of normal kindlin-3 levels. We report that in contrast to kindlin-3-null mice, which die perinatally of severe bleeding and leukocyte adhesion deficiency, mice expressing as little as 5% of kindlin-3 were viable and protected from spontaneous bleeding and infections. However, platelet adhesion and aggregation were reduced in vitro and bleeding times extended. Similarly, leukocyte adhesion, extravasation, and bacterial clearance were diminished. Quantification of protein copy numbers revealed stoichiometric quantities of kindlin-3 and talin-1 in platelets and neutrophils, indicating that reduction of kindlin-3 in our mouse strains progressively impairs the cooperation with talin-1. Our findings show that very low levels of kindlin-3 enable basal platelet and neutrophil functions, whereas in stress situations such as injury and infection, platelets and neutrophils require a maximum of functional integrins that is achieved with high and stoichiometric quantities of kindlin-3 and talin-1.
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