Literature DB >> 18824759

Short hairpin RNA interference therapy for ischemic heart disease.

Mei Huang1, Denise A Chan, Fangjun Jia, Xiaoyan Xie, Zongjin Li, Grant Hoyt, Robert C Robbins, Xiaoyuan Chen, Amato J Giaccia, Joseph C Wu.   

Abstract

BACKGROUND: During hypoxia, upregulation of hypoxia inducible factor-1 alpha transcriptional factor can activate several downstream angiogenic genes. However, hypoxia inducible factor-1 alpha is naturally degraded by prolyl hydroxylase-2 (PHD2) protein. Here we hypothesize that short hairpin RNA (shRNA) interference therapy targeting PHD2 can be used for treatment of myocardial ischemia and this process can be followed noninvasively by molecular imaging. METHODS AND
RESULTS: PHD2 was cloned from mouse embryonic stem cells by comparing the homolog gene in human and rat. The best candidate shRNA sequence for inhibiting PHD2 was inserted into the pSuper vector driven by the H1 promoter followed by a separate hypoxia response element-incorporated promoter driving a firefly luciferase reporter gene. This construct was used to transfect mouse C2C12 myoblast cell line for in vitro confirmation. Compared with the control short hairpin scramble (shScramble) as control, inhibition of PHD2 increased levels of hypoxia inducible factor-1 alpha protein and several downstream angiogenic genes by >30% (P<0.01). Afterward, shRNA targeting PHD2 (shPHD2) plasmid was injected intramyocardially following ligation of left anterior descending artery in mice. Animals were randomized into shPHD2 experimental group (n=25) versus shScramble control group (n=20). Bioluminescence imaging detected plasmid-mediated transgene expression for 4 to 5 weeks. Echocardiography showed the shPHD2 group had improved fractional shortening compared with the shScramble group at Week 4 (33.7%+/-1.9% versus 28.4%+/-2.8%; P<0.05). Postmortem analysis showed increased presence of small capillaries and venules in the infarcted zones by CD31 staining. Finally, Western blot analysis of explanted hearts also confirmed that animals treated with shPHD2 had significantly higher levels of hypoxia inducible factor-1 alpha protein.
CONCLUSIONS: This is the first study to image the biological role of shRNA therapy for improving cardiac function. Inhibition of PHD2 by shRNA led to significant improvement in angiogenesis and contractility by in vitro and in vivo experiments. With further validation, the combination of shRNA therapy and molecular imaging can be used to track novel cardiovascular gene therapy applications in the future.

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Year:  2008        PMID: 18824759      PMCID: PMC3657507          DOI: 10.1161/CIRCULATIONAHA.107.760785

Source DB:  PubMed          Journal:  Circulation        ISSN: 0009-7322            Impact factor:   29.690


  39 in total

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Authors:  Christopher W Pugh; Peter J Ratcliffe
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3.  Gene silencing in alveolar type II cells using cell-specific promoter in vitro and in vivo.

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4.  Activation of the hypoxia-inducible factor-pathway and stimulation of angiogenesis by application of prolyl hydroxylase inhibitors.

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Journal:  FASEB J       Date:  2003-04-22       Impact factor: 5.191

Review 5.  Harnessing the response to tissue hypoxia: HIF-1 alpha and therapeutic angiogenesis.

Authors:  Karen A Vincent; Olivier Feron; Ralph A Kelly
Journal:  Trends Cardiovasc Med       Date:  2002-11       Impact factor: 6.677

Review 6.  HIF-1: the knowns and unknowns of hypoxia sensing.

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8.  Safety and feasibility of catheter-based local intracoronary vascular endothelial growth factor gene transfer in the prevention of postangioplasty and in-stent restenosis and in the treatment of chronic myocardial ischemia: phase II results of the Kuopio Angiogenesis Trial (KAT).

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9.  Role of prolyl hydroxylation in oncogenically stabilized hypoxia-inducible factor-1alpha.

Authors:  Denise A Chan; Patrick D Sutphin; Nicholas C Denko; Amato J Giaccia
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Review 10.  Hypoxia-inducible factor (HIF-1)alpha: its protein stability and biological functions.

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  45 in total

1.  Cardiomyocyte-specific prolyl-4-hydroxylase domain 2 knock out protects from acute myocardial ischemic injury.

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Review 3.  Molecular mechanisms of action and therapeutic uses of pharmacological inhibitors of HIF-prolyl 4-hydroxylases for treatment of ischemic diseases.

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Review 5.  RNA interference and ischemic injury.

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Journal:  Mol Biol Rep       Date:  2011-05-24       Impact factor: 2.316

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7.  In vivo, cardiac-specific knockdown of a target protein, malic enzyme-1, in rat via adenoviral delivery of DNA for non-native miRNA.

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8.  Influence of silencing soluble epoxide hydrolase with RNA interference on cardiomyocytes apoptosis induced by doxorubicin.

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Journal:  J Huazhong Univ Sci Technolog Med Sci       Date:  2011-06-14

9.  Short hairpin RNA gene silencing of prolyl hydroxylase-2 with a minicircle vector improves neovascularization of hindlimb ischemia.

Authors:  Maarten A Lijkwan; Alwine A Hellingman; Ernst J Bos; Koen E A van der Bogt; Mei Huang; Nigel G Kooreman; Margreet R de Vries; Hendrika A B Peters; Robert C Robbins; Jaap F Hamming; Paul H A Quax; Joseph C Wu
Journal:  Hum Gene Ther       Date:  2014-01-07       Impact factor: 5.695

10.  Impaired Ca(2+)-handling in HIF-1alpha(+/-) mice as a consequence of pressure overload.

Authors:  Monique Silter; Harald Kögler; Anke Zieseniss; Jörg Wilting; Katrin Schäfer; Karl Toischer; Adam G Rokita; Gerhard Breves; Lars S Maier; Dörthe M Katschinski
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