Heat shock-induced protection and enhancement of Na+-glucose cotransport by LLC-PK1 monolayers.

Monolayers of the porcine-derived renal epithelial cell line, LLC-PK1, were used to characterize the effects of heat stress on Na+-glucose cotransport. Transepithelial current dependent on 5 mM glucose ( I Glc), phloridzin-sensitive current ( I phz), and total transepithelial current ( I total) were measured as indicators of Na+-glucose cotransport. Severe heat shock (SHS; 45°C for 1 h, then 37°C for measurements) decreased transepithelial electrical resistance (TER), I Glc, I phz, and I total50-70%. Mild heat shock (MHS; 42°C for 3 h, then 37°C for 12 h) induced accumulation of 72-kDa heat shock protein (HSP-72), decreased damage to TER from SHS, and prevented damage to I Glc, I phz, and I total. Kinetic analysis showed that SHS damaged and MHS protected total Na+-glucose transport capacity ( V max of I Glc). MHS alone increased TER (50%), I Glc (20%), I total (20%), and V max of I Glc (25%). On enhancement of the Na+ gradient by depletion of intracellular Na+, MHS increased I Glc 50% and had no effect on transepithelial Na+-dependent sulfate reabsorptive flux measured concurrently or in Na+-replete tissues. These effects of MHS were not reflected in effects on cell survival or luminal membrane surface area as indicated by lactate dehydrogenase or alkaline phosphatase release. In conclusion, HSP-72-inducing heat treatment both protected and enhanced Na+-glucose cotransport independently of the luminal membrane Na+ gradient and selectively with respect to effects on TER, reabsorptive sulfate transport, cell survival, and luminal membrane surface area.