Overexpression of HIF Prolyl‐Hydoxylase‐2 transgene in the renal medulla induced a salt sensitive hypertension

Renal medullary hypoxia‐inducible factor ( HIF )‐1α and its target genes, such as haem oxygenase and nitric oxide synthase, have been indicated to play an important role in the regulation of sodium excretion and blood pressure. HIF prolyl hydroxylase domain‐containing proteins ( PHD s) are major enzymes to promote the degradation of HIF ‐1α. We recently reported that high salt intake suppressed the renal medullary PHD 2 expression and thereby activated HIF ‐1α‐mediated gene regulation in the renal medulla in response to high salt. To further define the functional role of renal medullary PHD 2 in the regulation of renal adaptation to high salt intake and the longer term control of blood pressure, we transfected PHD 2 expression plasmids into the renal medulla in uninephrectomized rats and determined its effects on pressure natriuresis, sodium excretion after salt overloading and the long‐term control of arterial pressure after high salt challenge. It was shown that overexpression of PHD 2 transgene increased PHD 2 levels and decreased HIF ‐1α levels in the renal medulla, which blunted pressure natriuresis, attenuated sodium excretion, promoted sodium retention and produced salt sensitive hypertension after high salt challenge compared with rats treated with control plasmids. There was no blood pressure change in PHD 2‐treated rats that were maintained in low salt diet. These results suggested that renal medullary PHD 2 is an important regulator in renal adaptation to high salt intake and a deficiency in PHD 2‐mediated molecular adaptation in response to high salt intake in the renal medulla may represent a pathogenic mechanism producing salt sensitive hypertension.