1. CD36-triggered cell invasion and persistent tissue colonization by tumor microvesicles during metastasis
- Author
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Urjita Joshi, Georg J. Arnold, Remco T. A. Megens, Susanne Pfeiler, Christiane Bruns, Christian Weber, Verena Samara, Geraldine Müller-Stoy, Steffen Massberg, Raffaele Coletti, Petra Grünauer, S Wörmann, Andreas Klingl, Hana Algül, Manovriti Thakur, Konstantin Stark, Hellen Ishikawa-Ankerhold, Thomas Fröhlich, Bernd Engelmann, RS: Carim - B01 Blood proteins & engineering, RS: CARIM - R3.07 - Structure-function analysis of the chemokine interactome for therapeutic targeting and imaging in atherosclerosis, Biochemie, and Biomedische Technologie
- Subjects
CD36 Antigens ,0301 basic medicine ,THP-1 Cells ,Cell ,BIOLOGY ,MELANOMA ,COMMUNICATION ,Biology ,Biochemistry ,Metastasis ,Blood cell ,03 medical and health sciences ,0302 clinical medicine ,Immune system ,Cell-Derived Microparticles ,super-resolution microscopy ,Genetics ,medicine ,Humans ,Neoplasm Invasiveness ,Neoplasm Metastasis ,MACROPHAGES ,Molecular Biology ,Ly6C(-)macrophages ,Microvesicle ,MICROPARTICLES ,EXTRACELLULAR VESICLES ,microvesicle extravasation ,medicine.disease ,CANCER ,Microvesicles ,Extravasation ,Pancreatic Neoplasms ,030104 developmental biology ,medicine.anatomical_structure ,Cancer research ,Lysosomes ,Infiltration (medical) ,030217 neurology & neurosurgery ,Biotechnology - Abstract
Tumor microvesicles are a peculiar type of extracellular vesicles that circulate in the blood of patients with metastatic cancer. The itineraries and immune cell interactions of tumor microvesicles during the intravascular and extravascular stages of metastasis are largely unknown. We found that the lipid receptor CD36 is a major mediator of the engulfment of pancreatic tumor microvesicles by myeloid immune cells in vitro and critically samples circulating tumor microvesicles by resident liver macrophages in mice in vivo. Direct nanoscopic imaging of individual tumor microvesicles shows that the microvesicles rapidly decay during engulfment whereby their cargo is targeted concomitantly to the plasma membrane and the cytoplasm excluding lysosomal compartments. CD36 also promotes internalization of blood cell (nontumor) microvesicles, which involves endolysosomal pathways. A portion of tumor microvesicles circulating in the liver microcirculation traverses the vessel wall in a CD36-dependent way. Extravasated microvesicles colonize distinct perivascular Ly6C(-) macrophages for at least 2 wk. Thus, the microvesicles are increasingly integrated into CD36-induced premetastatic cell clusters and enhance development of liver metastasis. Hence, promotion of metastasis by pancreatic tumor microvesicles is associated with CD36-regulated immune cell invasion and extravasation of microvesicles and persistent infiltration of specific tissue macrophages by microvesicle cargo.Pfeiler, S., Thakur, M., Grunauer, P., Megens, R. T. A., Joshi, U., Coletti, R., Samara, V., Muller-Stoy, G., Ishikawa-Ankerhold, H., Stark, K., Klingl, A., Frohlich, T., Arnold, G. J., Wormann, S., Bruns, C. J., Algul, H., Weber, C., Massberg, S., Engelmann, B. CD36-triggered cell invasion and persistent tissue colonization by tumor microvesicles during metastasis.
- Published
- 2019