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Am J Physiol Renal Physiol 290: F1355-F1366, 2006. First published December 27, 2005; doi:10.1152/ajprenal.00481.2005
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Three-dimensional architecture of inner medullary vasa recta

Thomas L. Pannabecker and William H. Dantzler

Department of Physiology, College of Medicine, University of Arizona, Tucson, Arizona

Submitted 2 December 2005 ; accepted in final form 16 December 2005

The manner in which vasa recta function and contribute to the concentrating mechanism depends on their three-dimensional relationships to each other and to tubular elements. We have examined the three-dimensional architecture of vasculature relative to tubular structures in the central region of rat kidney inner medulla from the base through the first 3 mm by combining immunohistochemistry and semiautomated image acquisition techniques with graphical modeling software. Segments of descending vasa recta (DVR), ascending vasa recta (AVR), descending thin limb (DTL), ascending thin limb (ATL), and collecting duct (CD) were identified with antibodies against segment-specific proteins associated with solute and water transport (urea channel B, PV-1, aquaporin-1, ClC-K1, aquaporin-2, respectively) by immunofluorescence. Results indicate: 1) DVR, like DTLs, are excluded from CD clusters that we have previously shown to be the organizing element for the inner medulla; 2) AVR, like ATLs, are nearly uniformly distributed transversely across the entire inner medulla outside of and within CD clusters; 3) DVR and AVR outside CD clusters appear to be sufficiently juxtaposed to permit good countercurrent exchange; 4) within CD clusters, about four AVR closely abut each CD, surrounding it in a highly symmetrical fashion; and 5) AVR abutting each CD and ATLs within CD clusters form repeating nodal interstitial spaces bordered by a CD on one side, one or more ATLs on the opposite side, and one AVR on each of the other two sides. These relationships may be highly significant for both establishing and maintaining the inner medullary osmotic gradient.

three-dimensional reconstruction; PV-1; urea channel B; aquaporin; ClC-K; {alpha}B-crystallin; countercurrent multiplier; concentrating mechanism; vasa recta



Address for reprint requests and other correspondence: T. L. Pannabecker, Dept. of Physiology, College of Medicine, Univ. of Arizona, Tucson, AZ 85724-5051 (e-mail: pannabec{at}u.arizona.edu)




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