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Dynamics of Airway Blood Vessels and Lymphatics: Lessons from Development and Inflammation

Overview
Journal Proc Am Thorac Soc
Specialty Pulmonary Medicine
Date 2011 Nov 5
PMID 22052927
Citations 11
Authors
Donald M McDonald
Li-Chin Yao
Peter Baluk
Affiliations
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Abstract

Blood vessels and lymphatic vessels in the respiratory tract play key roles in inflammation. By undergoing adaptive remodeling and growth, blood vessels undergo changes that enable the extravasation of plasma and leukocytes into inflamed tissues, and lymphatic vessels adjust to the increased fluid clearance and cell traffic involved in immune responses. Blood vessels and lymphatics in adult airways are strikingly different from those of late-stage embryos. Before birth, blood vessels in mouse airways make up a primitive plexus similar to that of the yolk sac. This plexus undergoes rapid and extensive remodeling at birth. In the early neonatal period, parts of the plexus regress. Capillaries then rapidly regrow, and with arterioles and venules form the characteristic adult vascular pattern. Lymphatic vessels of the airways also undergo rapid changes around birth, when lymphatic endothelial cells develop button-like intercellular junctions specialized for efficient fluid uptake. Among the mechanisms that underlie the onset of rapid vascular remodeling at birth, changes in tissue oxygen tension and mechanical forces associated with breathing are likely to be involved, along with growth factors that promote the growth and maturation of blood vessels and lymphatics. Whatever the mechanisms, the dynamic nature of airway blood vessels and lymphatics during perinatal development foretells the extraordinary vascular plasticity found in many diseases.

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References
1.
Metzger R, Klein O, Martin G, Krasnow M . The branching programme of mouse lung development. Nature. 2008; 453(7196):745-50. PMC: 2892995. DOI: 10.1038/nature07005. View
2.
El-Chemaly S, Levine S, Moss J . Lymphatics in lung disease. Ann N Y Acad Sci. 2008; 1131:195-202. PMC: 2946892. DOI: 10.1196/annals.1413.017. View
3.
Baluk P, Tammela T, Ator E, Lyubynska N, Achen M, Hicklin D . Pathogenesis of persistent lymphatic vessel hyperplasia in chronic airway inflammation. J Clin Invest. 2005; 115(2):247-57. PMC: 544601. DOI: 10.1172/JCI22037. View
4.
Metzger R, Krasnow M . Genetic control of branching morphogenesis. Science. 1999; 284(5420):1635-9. DOI: 10.1126/science.284.5420.1635. View
5.
Dunnill M . The pathology of asthma, with special reference to changes in the bronchial mucosa. J Clin Pathol. 1960; 13:27-33. PMC: 479992. DOI: 10.1136/jcp.13.1.27. View