To study ischemic acute renal failure in an experimental model, the renal artery of the rat can be occluded for 15 to 60 min. Venkatachalam et al.³ observed that after 25 min of renal artery occlusion, S1 and S2 segment cells underwent reversible changes, whereas S3 segment cells underwent progressive cell injury and death.³ Within 5 min of blood reflow, brush border microvilli in all three segments of the proximal tubule underwent coalescence and interiorization. A small number of microvilli were fragmented and shed into the lumen of the proximal tubule. By 30 min of reflow, microvillous changes began to reverse so that by 4 h of reflow the S1 and S2 segment cells appeared normal. In contrast, the damaged S3 cells developed progressive necrosis and were exfoliated into the lumen. The surviving tubular epithelial cells underwent mitosis to repopulate the tubule 24 to 48 h following the ischemic insult.³ When kidneys were subjected to 1 h of ischemia, Reimer et al.¹ observed more extensive cellular necrosis and more debris in the urinary space. Brush border microvilli were also found to develop extensive blebs that were capable of obstructing the lumen of the proximal tubule.

An objection to using animal models to study acute renal failure is that differences in the extent of histologic injury have been found when comparing animals with man. The extent of blood flow limitation is also different. In experimental animals renal blood flow is totally abolished or severely depressed for up to 1 h, whereas patients who develop acute renal failure more often have less profound hypoperfusion of the kidneys, but of longer duration. Some studies of renal biopsy material from patients with acute renal failure have found minimal differences compared with normal kidneys.⁶ In other studies, tubular necrosis is usually more focal and tubular obstruction is less common in patients than in experimental animals with acute renal failure.⁷ On the other hand, in human biopsy material microvilli changes in the proximal tubule are frequent. Other changes such as flattening of tubular cells and mitosis are also common, suggesting that regeneration is occurring following a prior episode of necrosis even if necrotic cells are no longer present. In addition, Racusen et al.⁸ have recently demonstrated extensive shedding of viable tubular epithelial cells into the urine of patients with ischemic acute renal failure.⁸ This latter finding suggests that epithelial cells may be lost from the tubule even without developing necrosis. This would help to explain the paucity of necrotic cells in renal biopsies from some patients with acute renal failure, yet account for the extensive changes in renal function, which will be discussed below.