A network of trans-cortical capillaries as mainstay for blood circulation in long bones

Closed circulatory systems (CCS) underlie the function of vertebrate organs, but in long bones their structure is unclear, although they constitute the exit route for bone marrow (BM) leukocytes. To understand neutrophil emigration from BM, we studied the vascular system of murine long bones. Here w...

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Published inNature metabolism Vol. 1; no. 2; p. 236
Main Authors Grüneboom, Anika, Hawwari, Ibrahim, Weidner, Daniela, Culemann, Stephan, Müller, Sylvia, Henneberg, Sophie, Brenzel, Alexandra, Merz, Simon, Bornemann, Lea, Zec, Kristina, Wuelling, Manuela, Kling, Lasse, Hasenberg, Mike, Voortmann, Sylvia, Lang, Stefanie, Baum, Wolfgang, Ohs, Alexandra, Kraff, Oliver, Quick, Harald H, Jäger, Marcus, Landgraeber, Stefan, Dudda, Marcel, Danuser, Renzo, Stein, Jens V, Rohde, Manfred, Gelse, Kolja, Garbe, Annette I, Adamczyk, Alexandra, Westendorf, Astrid M, Hoffmann, Daniel, Christiansen, Silke, Engel, Daniel Robert, Vortkamp, Andrea, Krönke, Gerhard, Herrmann, Martin, Kamradt, Thomas, Schett, Georg, Hasenberg, Anja, Gunzer, Matthias
Format Journal Article
LanguageEnglish
Published Germany 01.02.2019
Subjects
Animals
Bone and Bones - blood supply
Bone Marrow - blood supply
Capillaries - physiology
Humans
Mice
Mice, Inbred DBA
Microcirculation
Regional Blood Flow
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Summary:Closed circulatory systems (CCS) underlie the function of vertebrate organs, but in long bones their structure is unclear, although they constitute the exit route for bone marrow (BM) leukocytes. To understand neutrophil emigration from BM, we studied the vascular system of murine long bones. Here we show that hundreds of capillaries originate in BM, cross murine cortical bone perpendicularly along the shaft and connect to the periosteal circulation. Structures similar to these trans-cortical-vessels (TCVs) also exist in human limb bones. TCVs express arterial or venous markers and transport neutrophils. Furthermore, over 80% arterial and 59% venous blood passes through TCVs. Genetic and drug-mediated modulation of osteoclast count and activity leads to substantial changes in TCV numbers. In a murine model of chronic arthritic bone inflammation, new TCVs develop within weeks. Our data indicate that TCVs are a central component of the CCS in long bones and may represent an important route for immune cell export from the BM.
ISSN:2522-5812
DOI:10.1038/s42255-018-0016-5