scholarly journals Comparative studies of the desert rodent Dipodomys merriami and Munich‐Wistar rat urine concentrating mechanisms

2012 ◽  
Vol 26 (S1) ◽  
Author(s):  
Arati C Babaria ◽  
William H Dantzler ◽  
Thomas L Pannabecker
2012 ◽  
Vol 303 (7) ◽  
pp. R748-R756 ◽  
Author(s):  
Tadeh Issaian ◽  
Vinoo B. Urity ◽  
William H. Dantzler ◽  
Thomas L. Pannabecker

We hypothesize that the inner medulla of the kangaroo rat Dipodomys merriami, a desert rodent that concentrates its urine to over 6,000 mosmol/kg H2O, provides unique examples of architectural features necessary for production of highly concentrated urine. To investigate this architecture, inner medullary vascular segments in the outer inner medulla were assessed with immunofluorescence and digital reconstructions from tissue sections. Descending vasa recta (DVR) expressing the urea transporter UT-B and the water channel aquaporin 1 lie at the periphery of groups of collecting ducts (CDs) that coalesce in their descent through the inner medulla. Ascending vasa recta (AVR) lie inside and outside groups of CDs. DVR peel away from vascular bundles at a uniform rate as they descend the inner medulla, and feed into networks of AVR that are associated with organized clusters of CDs. These AVR form interstitial nodal spaces, with each space composed of a single CD, two AVR, and one or more ascending thin limbs or prebend segments, an architecture that may lead to solute compartmentation and fluid fluxes essential to the urine concentrating mechanism. Although we have identified several apparent differences, the tubulovascular architecture of the kangaroo rat inner medulla is remarkably similar to that of the Munich Wistar rat at the level of our analyses. More detailed studies are required for identifying interspecies functional differences.


Ecology ◽  
2001 ◽  
Vol 82 (4) ◽  
pp. 1130 ◽  
Author(s):  
Randall L. Tracy ◽  
Glenn E. Walsberg

2012 ◽  
Vol 302 (6) ◽  
pp. R720-R726 ◽  
Author(s):  
Vinoo B. Urity ◽  
Tadeh Issaian ◽  
Eldon J. Braun ◽  
William H. Dantzler ◽  
Thomas L. Pannabecker

We hypothesize that the inner medulla of the kangaroo rat Dipodomys merriami , a desert rodent that concentrates its urine to more than 6,000 mosmol/kgH2O water, provides unique examples of architectural features necessary for production of highly concentrated urine. To investigate this architecture, inner medullary nephron segments in the initial 3,000 μm below the outer medulla were assessed with digital reconstructions from physical tissue sections. Descending thin limbs of Henle (DTLs), ascending thin limbs of Henle (ATLs), and collecting ducts (CDs) were identified by immunofluorescence using antibodies that label segment-specific proteins associated with transepithelial water flux (aquaporin 1 and 2, AQP1 and AQP2) and chloride flux (the chloride channel ClC-K1); all tubules and vessels were labeled with wheat germ agglutinin. In the outer 3,000 μm of the inner medulla, AQP1-positive DTLs lie at the periphery of groups of CDs. ATLs lie inside and outside the groups of CDs. Immunohistochemistry and reconstructions of loops that form their bends in the outer 3,000 μm of the inner medulla show that, relative to loop length, the AQP1-positive segment of the kangaroo rat is significantly longer than that of the Munich-Wistar rat. The length of ClC-K1 expression in the prebend region at the terminal end of the descending side of the loop in kangaroo rat is about 50% shorter than that of the Munich-Wistar rat. Tubular fluid of the kangaroo rat DTL may approach osmotic equilibrium with interstitial fluid by water reabsorption along a relatively longer tubule length, compared with Munich-Wistar rat. A relatively shorter-length prebend segment may promote a steeper reabsorptive driving force at the loop bend. These structural features predict functionality that is potentially significant in the production of a high urine osmolality in the kangaroo rat.


2011 ◽  
Vol 25 (S1) ◽  
Author(s):  
Tadeh Issaian ◽  
Vinoo B Urity ◽  
Eldon J Braun ◽  
William H Dantzler ◽  
Thomas L Pannabecker

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