Angiotensinogen gene expression is stimulated by the cAMP-responsive element binding protein in opossum kidney cells. | Zendy

Jing Qian | Zendy; Teng Wang | Zendy; X. Wu | Zendy; Jie Wu | Zendy; Chunxi Ge | Zendy; S Lachance | Zendy; S Carrière | Zendy; John S.D. Chan | Zendy

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Angiotensinogen gene expression is stimulated by the cAMP-responsive element binding protein in opossum kidney cells.

Author(s) -

Jing Qian,

Teng Wang,

X. Wu,

Jie Wu,

Chunxi Ge,

S Lachance,

S Carrière,

John S.D. Chan

Publication year - 1997

Publication title -

journal of the american society of nephrology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 4.451

H-Index - 279

eISSN - 1533-3450

pISSN - 1046-6673

DOI - 10.1681/asn.v871072

Subject(s) - creb , microbiology and biotechnology , transfection , forskolin , biology , gene expression , protein kinase a , enhancer , fusion gene , cell culture , creb1 , angiotensin ii , expression vector , gene , endocrinology , kinase , transcription factor , recombinant dna , biochemistry , genetics , blood pressure

It has been reported previously that the addition of isoproterenol or forskolin stimulates the expression of the angiotensinogen (ANG) gene in opossum kidney (OK) 27 cells, an OK cell line with a fusion gene containing the 5'-flanking regulatory sequence of the rat ANG gene fused with a human growth hormone (hGH) gene as a reporter, pOGH (ANG N-1498/+18), permanently integrated into their genomes. To investigate whether the effect of isoproterenol or forskolin on the expression of the ANG gene is mediated via the nuclear 43-kD cAMP-responsive element binding protein (CREB), OK 27 cells were transiently transfected with an expression plasmid containing the cDNA for the 43-kD CREB (pRSV/CREB). The level of expression of the pOGH (ANG N-1498/+18) in OK 27 cells was estimated by the amount of immunoreactive hGH secreted into the culture medium. Transfection of pRSV/CREB alone stimulated the expression of pOGH (ANG N-1498/+18). The addition of isoproterenol or forskolin further enhanced the stimulatory effect of pRSV/ CREB on the expression of pOGH (ANG N-1498/+18). The enhancing effect of isoproterenol was inhibited by the presence of propranolol (an inhibitor of beta-adrenoceptors) and (R)-p-adenosine 3'5'-cyclic monophospho-orthioate (Rp)-cAMP (an inhibitor of cAMP-dependent protein kinase A I and II). Transfection of pRSV/CREB had no effect on the expression of thymidine kinase growth hormone in OK 13 cells, an OK cell line with a fusion gene containing the promoter/enhancer DNA sequence of the viral thymidine-kinase gene fused with an hGH gene as a reporter, thymidine kinase growth hormone, permanently integrated into their genomes. These studies demonstrate that isoproterenol stimulates the expression of ANG gene via the cAMP-dependent protein kinase A and probably via the interaction of the 43-kD CREB with the 5'-flanking region of the ANG gene. Our data indicate that the nuclear 43-kD CREB may have a modulatory role on the expression of the ANG gene in OK cells.

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