Biophysical properties of normal and diseased renal glomeruli

Author:

Wyss Hans M.1,Henderson Joel M.2,Byfield Fitzroy J.3,Bruggeman Leslie A.4,Ding Yaxian5,Huang Chunfa5,Suh Jung Hee6,Franke Thomas1,Mele Elisa1,Pollak Martin R.7,Miner Jeffrey H.6,Janmey Paul A.3,Weitz David A.1,Miller R. Tyler458

Affiliation:

1. Physics, Harvard University, Cambridge, Massachusetts;

2. Department of Pathology, Boston University, Boston, Massachusetts;

3. Center for Medicine and Engineering, University of Pennsylvania, Philadelphia, Pennsylvania;

4. Rammelkamp Center for Research and Education, MetroHealth Medical Center, Case-Western Reserve University, Cleveland, Ohio;

5. Department of Medicine, Louis Stokes Veterans Affairs Medical Center, Cleveland, Ohio;

6. Renal Division, Department of Medicine, Washington University School of Medicine, St. Louis, Missouri;

7. Beth Israel-Deaconess Hospital, Harvard University, Boston, Massachusetts; and

8. Department of Physiology and Biophysics, Case-Western Reserve University, Cleveland, Ohio

Abstract

The mechanical properties of tissues and cells including renal glomeruli are important determinants of their differentiated state, function, and responses to injury but are not well characterized or understood. Understanding glomerular mechanics is important for understanding renal diseases attributable to abnormal expression or assembly of structural proteins and abnormal hemodynamics. We use atomic force microscopy (AFM) and a new technique, capillary micromechanics, to measure the elastic properties of rat glomeruli. The Young's modulus of glomeruli was 2,500 Pa, and it was reduced to 1,100 Pa by cytochalasin and latunculin, and to 1,400 Pa by blebbistatin. Cytochalasin or latrunculin reduced the F/G actin ratios of glomeruli but did not disrupt their architecture. To assess glomerular biomechanics in disease, we measured the Young's moduli of glomeruli from two mouse models of primary glomerular disease, Col4a3−/−mice (Alport model) and Tg26HIV/nlmice (HIV-associated nephropathy model), at stages where glomerular injury was minimal by histopathology. Col4a3−/−mice express abnormal glomerular basement membrane proteins, and Tg26HIV/nlmouse podocytes have multiple abnormalities in morphology, adhesion, and cytoskeletal structure. In both models, the Young's modulus of the glomeruli was reduced by 30%. We find that glomeruli have specific and quantifiable biomechanical properties that are dependent on the state of the actin cytoskeleton and nonmuscle myosins. These properties may be altered early in disease and represent an important early component of disease. This increased deformability of glomeruli could directly contribute to disease by permitting increased distension with hemodynamic force or represent a mechanically inhospitable environment for glomerular cells.

Publisher

American Physiological Society

Subject

Cell Biology,Physiology

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