Adenoviral Vector-Mediated Transfer of Human Heme Oxygenase in Rats Decreases Renal Heme-Dependent Arachidonic Acid Epoxygenase Activity

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Vol. 293, Issue 2, 494-500, May 2000

Adenoviral Vector-Mediated Transfer of Human Heme Oxygenase in Rats Decreases Renal Heme-Dependent Arachidonic Acid Epoxygenase Activity¹

Nader G. Abraham, Shanlong Jiang, Liming Yang, Barbara A. Zand, Michal Laniado-Schwartzman, Jackleen Marji, George S. Drummond and Attallah Kappas

The Rockefeller University, New York, New York (N.G.A., S.J., G.S.D., A.K.); and Department of Pharmacology, New York Medical College, Valhalla, New York (L.Y., B.A.Z., M.L.-S., J.M.)

Intravenous administration of an adenovirus human heme oxygenase (HO)-1 gene construct to rats resulted in functional expressionof human HO-1 in brain, heart, lung, liver, and kidney. Becauseaccurate assessment of human HO-1 mRNA in various tissues by Northernanalysis is not sufficiently sensitive, we developed a methodfor quantifying human HO-1 mRNA copies with quantitative reversetranscription- polymerase chain reaction techniques; this allowedus to use the same primers for both the sample and internal standard.Administration of the adenovirus human HO-1 gene resulted in thedetection of human HO-1 mRNA in various tissues with the highestlevels seen in the kidney followed, in order, by lung > liver> brain > heart. Human HO-1 was detectable for up to 4 weeks inall tissues studied. Administration of adenovirus human HO-1 resultedin maximal increase of HO activity after 1 to 2 weeks in rats.The increase in HO activity due to gene transfer also was associatedwith a parallel decrease (~25%) in cytochrome P-450 (CYP) contentand in CYP-dependant arachidonic acid metabolism. In addition,we investigated the possibility that the human HO-1 gene alteredthe expression of the endogenous rat enzyme after administrationof cobalt chloride s.c.. Cobalt chloride administration resultedin increased HO activity in all tissues examined in rats transducedwith the human HO-1 gene to the same degree as in nontransducedrats. The metal was a more potent inducer of renal HO activitythan was the adenoviral-mediated human HO-1 vector. The increasein HO activity after adenoviral-mediated human HO-1 transfer wasassociated with a decrease in microsomal heme-CYP and CYP activity.The increase in HO-1 activity after adenovirus-mediated humanHO-1 gene transfer may prove useful as a means of selectivelyincreasing enzyme activity in a specific organ and regulatinghomeostasis by modulation of vasoactive molecules such as carbonmonoxide and bilirubin and, in addition, providing a means ofdelivering the human HO-1 gene for experimentalpurposes.

¹ This study was supported in part by Grants RO1 HL54138 and EY06531 from the National Institutes ofHealth.

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				S. Quan, L. Yang, N. G. Abraham, and A. Kappas Regulation of human heme oxygenase in endothelial cells by using sense and antisense retroviral constructs PNAS, October 9, 2001; 98(21): 12203 - 12208. [Abstract] [Full Text] [PDF]

Adenoviral Vector-Mediated Transfer of Human Heme Oxygenase in Rats Decreases Renal Heme-Dependent Arachidonic Acid Epoxygenase Activity1

Adenoviral Vector-Mediated Transfer of Human Heme Oxygenase in Rats Decreases Renal Heme-Dependent Arachidonic Acid Epoxygenase Activity¹