To test the hypothesis that neutralization of polyanions of the glomerular filter in vivo will lead to loss of charge-dependent glomerular permselectivity, we have infused i.v. the polycation hexadimethrine (HDM) into rats. Heavy proteinuria resulted after a lag period of 30 to 50 min, and it resolved when the infusion was stopped. Concurrent administration of heparin prevented the proteinuria. Urinary proteins were examined by immunoelectrophoresis, isoelectric focusing with immunofixation, and sodium dodecylsulfate polyacrylamide electrophoresis. The major protein was rat albumin, but there were also large quantities of intact rat IgG. HDM was bound at known sites of glomerular polyanion in the laminae rarae of the basement membrane and on the epithelial cell glycocalyx. Associated with this binding were reversible abnormalities of the epithelial cells similar to those seen during in vitro neutralization of glomerular polyanion. Aside from proteinaceous tubular casts, no other histologic abnormality was noted. These studies provide direct evidence that neutralization of glomerular polyanions in vivo results in heavy proteinuria. The appearance of substantial quantities of rat IgG in the urine implies that abnormalities of size as well as charge-dependent permselectivity occur, suggesting that the polyanions of the glomerular filter may be important in maintaining its structure as well as its function.