Your search keyword '"Julian Leberzammer"' showing total 3 results

1. Chemokines, molecular drivers of thromboinflammation and immunothrombosis

Author

Julian Leberzammer and Philipp von Hundelshausen

Subjects

platelet, atherothrombosis, inflammation, leukocyte, red blood cell, endothelial cell, Immunologic diseases. Allergy, RC581-607

Abstract

Blood clotting is a finely regulated process that is essential for hemostasis. However, when dysregulated or spontaneous, it promotes thrombotic disorders. The fact that these are triggered, accompanied and amplified by inflammation is reflected in the term thromboinflammation that includes chemokines. The role of chemokines in thrombosis is therefore illuminated from a cellular perspective, where endothelial cells, platelets, red blood cells, and leukocytes may be both the source and target of chemokines. Chemokine-dependent prothrombotic processes may thereby occur independently of chemokine receptors or be mediated by chemokine receptors, although the binding and activation of classical G protein-coupled receptors and their signaling pathways differ from those of atypical chemokine receptors, which do not function via cell activation and recruitment. Regardless of binding to their receptors, chemokines can induce thrombosis by forming platelet-activating immune complexes with heparin or other polyanions that are pathognomonic for HIT and VITT. In addition, chemokines can bind to NETs and alter their structure. They also change the electrical charge of the cell surface of platelets and interact with coagulation factors, thereby modulating the balance of fibrinolysis and coagulation. Moreover, CXCL12 activates CXCR4 on platelets independently of classical migratory chemokine activity and causes aggregation and thrombosis via the PI3Kβ and Btk signaling pathways. In contrast, typical chemokine-chemokine receptor interactions are involved in the processes that contribute to the adhesiveness of the endothelium in the initial phase of venous thrombosis, where neutrophils and monocytes subsequently accumulate in massive numbers. Later, the reorganization and resolution of a thrombus require coordinated cell migration and invasion of the thrombus, and, as such, indeed, chemokines recruit leukocytes to existing thrombi. Therefore, chemokines contribute in many independent ways to thrombosis.

Published

2023

2. Targeting platelet-derived CXCL12 impedes arterial thrombosis

Author

Julian Leberzammer, Stijn M. Agten, Xavier Blanchet, Rundan Duan, Hans Ippel, Remco T. A. Megens, Christian Schulz, Maria Aslani, Johan Duchene, Yvonne Döring, Natalie J. Jooss, Pengyu Zhang, Richard Brandl, Konstantin Stark, Wolfgang Siess, Kerstin Jurk, Johan W. M. Heemskerk, Tilman M. Hackeng, Kevin H. Mayo, Christian Weber, Philipp von Hundelshausen, Biochemie, RS: Carim - B01 Blood proteins & engineering, Biomedische Technologie, and RS: Carim - B03 Cell biochemistry of thrombosis and haemostasis

Subjects

Blood Platelets, EXPRESSION, Platelet Aggregation, FACTOR-I, Immunology, 610 Medicine & health, Platelet Glycoprotein GPIIb-IIIa Complex, Biochemistry, ACTIVATION, Mice, GPVI, Agammaglobulinaemia Tyrosine Kinase, Animals, CXCR4, P-SELECTIN, Thrombosis, Cell Biology, Hematology, Platelet Activation, Chemokine CXCL12, biological factors, ATHEROSCLEROSIS, CHEMOKINES, BTK, embryonic structures, Collagen, biological phenomena, cell phenomena, and immunity, SDF-1-ALPHA

Abstract

The prevention and treatment of arterial thrombosis continue to be clinically challenging, and understanding the relevant molecular mechanisms in detail may facilitate the quest to identify novel targets and therapeutic approaches that improve protection from ischemic and bleeding events. The chemokine CXCL12 augments collagen-induced platelet aggregation by activating its receptor CXCR4. Here we show that inhibition of CXCR4 attenuates platelet aggregation induced by collagen or human plaque homogenate under static and arterial flow conditions by antagonizing the action of platelet-secreted CXCL12. We further show that platelet-specific CXCL12 deficiency in mice limits arterial thrombosis by affecting thrombus growth and stability without increasing tail bleeding time. Accordingly, neointimal lesion formation after carotid artery injury was attenuated in these mice. Mechanistically, CXCL12 activated via CXCR4 a signaling cascade involving Bruton’s tyrosine kinase (Btk) that led to integrin αIIbβ3 activation, platelet aggregation, and granule release. The heterodimeric interaction between CXCL12 and CCL5 can inhibit CXCL12-mediated effects as mimicked by CCL5-derived peptides such as [VREY]4. An improved variant of this peptide, i[VREY]4, binds to CXCL12 in a complex with CXCR4 on the surface of activated platelets, thereby inhibiting Btk activation and preventing platelet CXCL12-dependent arterial thrombosis. In contrast to standard antiplatelet therapies such as aspirin or P2Y12 inhibition, i[VREY]4 reduced CXCL12-induced platelet aggregation and yet did not prolong in vitro bleeding time. We provide evidence that platelet-derived CXCL12 is involved in arterial thrombosis and can be specifically targeted by peptides that harbor potential therapeutic value against atherothrombosis.

Published

2022

3. Chemokines and galectins form heterodimers to modulate inflammation

Author

Christian Weber, Ingrid Dijkgraaf, Rundan Duan, Johan Duchene, Hans-Joachim Gabius, Kiril Bidzhekov, Kevin H. Mayo, Julian Leberzammer, Yvonne Döring, Aurelio J. Dregni, Hans Ippel, Michelle C. Miller, Xavier Blanchet, Oliver Soehnlein, Tilman M. Hackeng, Remco T. A. Megens, Herbert Kaltner, Veit Eckardt, Anna Kristin Ludwig, Philipp von Hundelshausen, Alexander Faussner, Kanin Wichapong, Biochemie, and RS: Carim - B01 Blood proteins & engineering

Subjects

Chemokine, DIMERIZATION, G protein‐coupled receptor, Biochemistry, Interactome, Mice, 0302 clinical medicine, Structural Biology, BINDING, Leukocytes, chemotaxis, Receptor, NEUTROPHILS, 0303 health sciences, biology, Chemistry, Effector, Articles, CXCL12, 3. Good health, Cell biology, RECEPTORS, Galectin-3, Signal Transduction, animal structures, Galectins, Immunology, galectin‐3, Article, 03 medical and health sciences, galectin-3, otorhinolaryngologic diseases, Genetics, Animals, TRAFFICKING, G protein-coupled receptor, MOLECULE, Molecular Biology, 030304 developmental biology, Galectin, Inflammation, Chemotaxis, stomatognathic diseases, ATHEROSCLEROSIS, biology.protein, T-CELLS, PATTERNS, lectin, 030217 neurology & neurosurgery

Abstract

Chemokines and galectins are simultaneously upregulated and mediate leukocyte recruitment during inflammation. Until now, these effector molecules have been considered to function independently. Here, we tested the hypothesis that they form molecular hybrids. By systematically screening chemokines for their ability to bind galectin‐1 and galectin‐3, we identified several interacting pairs, such as CXCL12 and galectin‐3. Based on NMR and MD studies of the CXCL12/galectin‐3 heterodimer, we identified contact sites between CXCL12 β‐strand 1 and Gal‐3 F‐face residues. Mutagenesis of galectin‐3 residues involved in heterodimer formation resulted in reduced binding to CXCL12, enabling testing of functional activity comparatively. Galectin‐3, but not its mutants, inhibited CXCL12‐induced chemotaxis of leukocytes and their recruitment into the mouse peritoneum. Moreover, galectin‐3 attenuated CXCL12‐stimulated signaling via its receptor CXCR4 in a ternary complex with the chemokine and receptor, consistent with our structural model. This first report of heterodimerization between chemokines and galectins reveals a new type of interaction between inflammatory mediators that can underlie a novel immunoregulatory mechanism in inflammation. Thus, further exploration of the chemokine/galectin interactome is warranted., Chemokines and galectins are simultaneously upregulated during inflammation and mediate leukocyte recruitment. A systematic screen now demonstrates their physical interaction as heterodimers, identifying several novel interacting pairs.

Published

2020