Vol. 279, Issue 3, F426-F439, September 2000
Identification of a novel kidney-specific gene downregulated
in acute ischemic renal failure
Erding
Hu1,
Zunxuan
Chen1,
Todd
Fredrickson1,
Miklos
Gellai1,
Malcolm
Jugus1,
Lisa
Contino1,
Nigel
Spurr2,
Matthew
Sims2,
Wendy
Halsey2,
Stephanie
Van
Horn2,
Joyce
Mao2,
Ganesh
Sathe2, and
David
Brooks1
Departments of 1 Renal Pharmacology and 2 Genetic
Technology, SmithKline Beecham Pharmaceuticals, King of Prussia,
Pennsylvania 19403
To gain further insights into the
molecular mechanisms involved in acute renal failure, we have isolated
a new gene from rat and human, named KSP32 (kidney-specific protein
with a molecular mass of 32 kDa). KSP32 encodes a novel gene that shows
little homology to other mammalian proteins. It, however, shares
extensive homology with several proteins found in the nematode
Caenorhabditis elegans and plants. The expression of KSP32
mRNA is highly restricted to kidney. In situ hybidization analysis
revealed that the expression of KSP32 mRNA was prominent in the
boundary of kidney cortex and outer medulla, exhibiting a raylike
formation extending from the medulla into the cortex. Finally, KSP32
mRNA was dramatically downregulated in rat following induction of acute
ischemic renal failure. Rapid loss of KSP32 mRNA expression was
observed beginning at ~5 h following renal injury and mRNA levels
remained depressed for at least 96 h. Both KSP32 mRNA levels as well as
renal function recovered 14 days after injury. Administration of an
endothelin receptor antagonist (SB-209670), known to restore renal
function, significantly increased KSP32 expression.
molecular cloning; medullary rays; proximal tubules; polymerase
chain reaction-select
