Gene therapy encoding cell cycle factors to treat chronic ischemic heart failure in rats

Author:

Abouleisa Riham R E1,Tang Xian-Liang1,Ou Qinghui1,Salama Abou-Bakr M12,Woolard Amie1,Hammouri Dana13,Abdelhafez Hania14,Cayton Sarah1,Abdulwali Sameeha K15,Arai Momo15,Sithu Israel D67,Conklin Daniel J6,Bolli Roberto1ORCID,Mohamed Tamer M A13468910ORCID

Affiliation:

1. Department of Medicine, Institute of Molecular Cardiology, University of Louisville , 580 South Preston Street, Louisville, KY 40202 , USA

2. Department of Cardiovascular Medicine, Faculty of Medicine, Zagazig University , 872 Shaibet an Nakareyah, Zagazig, Al-Sharqia Governorate 7120001 , Egypt

3. Department of Pharmacology and Toxicology, University of Louisville , 580 South Preston Street, Louisville, KY 40202 , USA

4. Department of Bioengineering, Speed School of Engineering, University of Louisville , 580 South Preston Street, Louisville, KY 40202 , USA

5. College of Medicine, Alfaisal University , Interconnection of Al Takhassousi،Al Zahrawi Street, Riyadh 11533 , Saudi Arabia

6. Department of Medicine, Center for Cardiometabolic Science, Envirome Institute, University of Louisville , 580 South Preston Street, Louisville, KY 40202 , USA

7. Department of Physiology, School of Medicine, University of Louisville , Louisville, 580 South Preston Street, KY 40202 , USA

8. Department of Biochemistry Faculty of Pharmacy, Zagazig University , 872 Shaibet an Nakareyah, Zagazig, Zagazig, Al-Sharqia Governorate 7120001 , Egypt

9. Institute of Cardiovascular Sciences, University of Manchester , Oxford Road, Manchester M13 9PT , UK

10. Surgery Department, Baylor College of Medicine, 6519 Fannin Street, Houston , TX, 77030 , USA

Abstract

Abstract Aims Gene therapies to induce cardiomyocyte (CM) cell cycle re-entry have shown a potential to treat subacute ischaemic heart failure (IHF) but have not been tested in the more relevant setting of chronic IHF. Our group recently showed that polycistronic non-integrating lentivirus encoding Cdk1/CyclinB1 and Cdk4/CyclinD1 (TNNT2-4Fpolycistronic-NIL) is effective in inducing CM cell cycle re-entry and ameliorating subacute IHF models and preventing the subsequent IHF-induced congestions in the liver, kidneys, and lungs in rats and pigs. Here, we aim to test the long-term efficacy of TNNT2-4Fpolycistronic-NIL in a rat model of chronic IHF, a setting that differs pathophysiologically from subacute IHF and has greater clinical relevance. Methods and results Rats were subjected to a 2-h coronary occlusion followed by reperfusion; 4 weeks later, rats were injected intramyocardially with either TNNT2-4Fpolycistronic-NIL or LacZ-NIL. Four months post-viral injection, TNNT2-4Fpolycistronic-NIL–treated rats showed a significant reduction in scar size and a significant improvement in left ventricular (LV) systolic cardiac function but not in the LV dilatation associated with chronic IHF. A mitosis reporter system developed in our lab showed significant induction of CM mitotic activity in TNNT2-4Fpolycistronic-NIL–treated rats. Conclusion This study demonstrates, for the first time, that TNNT2-4Fpolycistronic-NIL gene therapy induces CM cell cycle re-entry in chronic IHF and improves LV function, and that this salubrious effect is sustained for at least 4 months. Given the high prevalence of chronic IHF, these results have significant clinical implications for developing a novel treatment for this deadly disease.

Funder

National Institutes of Health

American Heart Association

Publisher

Oxford University Press (OUP)

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