Reduction of Cold-Induced Hypertension by Antisense Oligodeoxynucleotides to Angiotensinogen mRNA and AT
            <sub>1</sub>
            -Receptor mRNA in Brain and Blood

Peng, J; Kimura, Birgitta; Fregly, Melvin J.; Phillips, M. Ian

doi:10.1161/01.hyp.31.6.1317

Cited by 57 publications

(52 citation statements)

References 26 publications

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“…15,16 The utility of this strategy has been demonstrated successfully by in vivo administration of AS-ODNs against neural and inducible isoforms of nitric oxide synthase, the angiotensin subtype 1 receptor, the Na ϩ -P i cotransporter, intercellular adhesion molecule-1, and transforming growth factor-␤1 in the kidney. [25][26][27][28][29][30][31] In the present study, effective renal cellular uptake of AS-ODN was confirmed by distribution of Texas red-labeled ODN in renal tubular epithelium and vasculature 24 hours after renal interstitial injection.…”

Section: Discussionsupporting

confidence: 72%

Selective Inhibition of the Renal Dopamine Subtype D _1A Receptor Induces Antinatriuresis in Conscious Rats

1999

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Abstract-BothAntisense oligodeoxynucleotide (AS-ODN) provides a novel strategy to inhibit the synthesis of a specific gene product. 13,14 Because renal tubule epithelial cells, especially proximal tubule cells, can take up large quantities of oligodeoxynucleotide (ODN), the kidney appears to be an excellent target organ for a site-directed AS-ODN approach. 15,16 In the present study, AS-ODN directed toward dopamine D 1A receptor subtype mRNA was delivered directly into the renal interstitium to inhibit selectively the synthesis of the renal D 1A receptor subtype, and the role of the renal D 1A receptor subtype in the control of sodium excretion and blood pressure was evaluated in conscious uninephrectomized rats. MethodsSprague-Dawley female rats (body weight, 200 to 240 g, Harlan Sprague Dawley Inc, Harlan Teklad, Madison, WI) were used. The rats were provided with free access to regular rat chow (0.28% NaCl, Bioserve) and tap water unless described otherwise. All experimental procedures on animals were approved by the

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Section: Discussionsupporting

confidence: 72%

Selective Inhibition of the Renal Dopamine Subtype D _1A Receptor Induces Antinatriuresis in Conscious Rats

1999

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“…Most of the uptake is in the kidney and liver. A reduction in AT 1 -R after treatment with the AT 1 -AS-ODN reveals reductions in the protein in kidney, aorta and liver (8).…”

Section: Antisense Oligonucleotidesmentioning

confidence: 96%

Somatic gene therapy for hypertension

2000

Braz J Med Biol Res

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Gene therapy for hypertension is needed for the next generation of antihypertensive drugs. Current drugs, although effective, have poor compliance, are expensive and short-lasting (hours or one day). Gene therapy offers a way to produce long-lasting antihypertensive effects (weeks, months or years). We are currently using two strategies: a) antisense oligodeoxynucleotides (AS-ODN) and b) antisense DNA delivered in viral vectors to inhibit genes associated with vasoconstrictive properties. It is not necessary to know all the genes involved in hypertension, since many years of experience with drugs show which genes need to be controlled. AS-ODN are short, single-stranded DNA that can be injected in naked form or in liposomes. AS-ODN, targeted to angiotensin type 1 receptors (AT 1 -R), angiotensinogen (AGT), angiotensin converting enzyme, and ß1-adrenergic receptors effectively reduce hypertension in rat models (SHR, 2K-1C) and coldinduced hypertension. A single dose is effective up to one month when delivered with liposomes. No side effects or toxic effects have been detected, and repeated injections can be given. For the vector, adenoassociated virus (AAV) is used with a construct to include a CMV promoter, antisense DNA to AGT or AT 1 -R and a reporter gene. Results in SHR demonstrate reduction and slowing of development of hypertension, with a single dose administration. Left ventricular hypertrophy is also reduced by AAV-AGT-AS treatment. Double transgenic mice (human renin plus human AGT) with high angiotensin II causing high blood pressure, treated with AAV-AT 1 -R-AS, show a normalization of blood pressure for over six months with a single injection of vector. We conclude that ODNs will probably be developed first because they can be treated like drugs for the treatment of hypertension with long-term effects. Viral vector delivery needs more engineering to be certain of its safety, but one day may be used for a very prolonged control of blood pressure.

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“…Animals did not appear stressed during BP measurement. The tail-cuff method is a common method used by Sun et al, [27][28][29] Wang et al, 31,32 Peng et al 33 and Zhu et al 34 to delineate CIH. It has been confirmed by the intraarterial cannulation that the non-invasive tail-cuff method is effective and reliable in monitoring systolic BP in rats exposed to cold.…”

Section: Animal Study Protocolsmentioning

confidence: 99%

AAV delivery of mineralocorticoid receptor shRNA prevents progression of cold-induced hypertension and attenuates renal damage

et al. 2006

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The aim of this study was to determine the effect of RNA interference inhibition of mineralocorticoid receptor (MR) on cold-induced hypertension (CIH) and renal damage. Recombinant adeno-associated virus (AAV) carrying short hairpin small interference (si)RNA for MR (AAV.MR-shRNA) was constructed and tested for the ability to inhibit renal MR and to control CIH. Three groups of rats with CIH received AAV.MR-shRNA (1.25 Â 10 9 particles/rat, intravenous), AAV carrying scrambled shRNA (AAV.Control-shRNA) (1.25 Â 10 9 particles/rat, intravenous) and phosphate buffer solution (PBS), respectively. All rats were kept in a cold chamber (6.71C) throughout the experiment. Adeno-associated virus delivery of MR-shRNA prevented progression of CIH. Blood pressure (BP) of the AAV.MR-shRNA-treated group did not increase and remained at 14573 mm Hg, whereas BP of the AAV.Control-shRNA-treated and PBStreated group increased to 16774 and 16173 mm Hg, respectively, at 3 weeks after gene delivery. Thus, the antihypertensive effect of a single injection of AAV.MRshRNA lasted for at least 3 weeks (length of the study). Adeno-associated virus carrying short hairpin siRNA for MR significantly increased urinary sodium excretion and decreased proteinuria. It also decreased serum creatinine and blood urea nitrogen, suggesting enhanced renal function. Both Western blot and immunohistochemical analysis showed that MR expression was decreased significantly in the kidney in the AAV.MR-shRNA-treated rats, confirming that renal MR is effectively inhibited by AAV.MR-shRNA. Adeno-associated virus carrying short hairpin siRNA for MR also significantly attenuated renal hypertrophy. In addition, AAV delivery of MR-shRNA prevented atrophy and dilation of renal tubules and abolished tubular deposition of proteinaceous material seen in CIH rats. Conclusions: (1) AAV delivery of MR-shRNA effectively silenced MR in vivo. (2) RNA interference inhibition of MR may open a new avenue for the long-term control of hypertension and renal damage.

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Reduction of Cold-Induced Hypertension by Antisense Oligodeoxynucleotides to Angiotensinogen mRNA and AT ₁ -Receptor mRNA in Brain and Blood

Cited by 57 publications

References 26 publications

Selective Inhibition of the Renal Dopamine Subtype D _1A Receptor Induces Antinatriuresis in Conscious Rats

Selective Inhibition of the Renal Dopamine Subtype D _1A Receptor Induces Antinatriuresis in Conscious Rats

Somatic gene therapy for hypertension

AAV delivery of mineralocorticoid receptor shRNA prevents progression of cold-induced hypertension and attenuates renal damage

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Reduction of Cold-Induced Hypertension by Antisense Oligodeoxynucleotides to Angiotensinogen mRNA and AT 1 -Receptor mRNA in Brain and Blood

Cited by 57 publications

References 26 publications

Selective Inhibition of the Renal Dopamine Subtype D 1A Receptor Induces Antinatriuresis in Conscious Rats

Selective Inhibition of the Renal Dopamine Subtype D 1A Receptor Induces Antinatriuresis in Conscious Rats

Somatic gene therapy for hypertension

AAV delivery of mineralocorticoid receptor shRNA prevents progression of cold-induced hypertension and attenuates renal damage

Contact Info

Product

Resources

About

Reduction of Cold-Induced Hypertension by Antisense Oligodeoxynucleotides to Angiotensinogen mRNA and AT ₁ -Receptor mRNA in Brain and Blood

Selective Inhibition of the Renal Dopamine Subtype D _1A Receptor Induces Antinatriuresis in Conscious Rats

Selective Inhibition of the Renal Dopamine Subtype D _1A Receptor Induces Antinatriuresis in Conscious Rats