Perspective on the development of a bioengineered patch to treat heart failure: rationale and proposed design of phase I clinical trial

Steven Goldman; Jay H. Traverse; Michael R. Zile; Elizabeth Juneman; Barry Greenberg; Rosemary F. Kelly; Jen Watson Koevary; Jordan J. Lancaster

doi:10.20517/2574-1209.2021.149

Perspective on the development of a bioengineered patch to treat heart failure: rationale and proposed design of phase I clinical trial

Steven Goldman, Jay H. Traverse, Michael R. Zile, Elizabeth Juneman, Barry Greenberg, Rosemary F. Kelly, Jen Watson Koevary, Jordan J. Lancaster

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

This perspective focuses on the development of tissue engineered (TE) cell-based therapies to treat left ventricular (LV) dysfunction and chronic heart failure (CHF). The development of induced pluripotent stem cells enabled investigators to seed or co-culture human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) alone and in combination with other cells onto bioengineered scaffolds applied to the epicardial surface of the damaged left ventricle. Using our work as an example, we show how a xenograft implant of a bioengineered scaffold embedded with human neonatal fibroblasts and seeded with hiPSC-CMs partially reversed maladaptive LV remodeling and improved LV systolic/diastolic function in an immune-competent rat model of CHF. The fibroblasts lay down an extracellular matrix and secrete growth factors that increase myocardial blood flow. This approach provides an improved cell payload that covers a larger area of the damaged left ventricle as opposed to direct cell injections into the heart or down the coronary arteries. These studies combined with ongoing studies in immune-competent Yucatan mini swine treated with the same xenograft led to the preliminary design of a proposed Phase I clinical trial that will be presented to the Federal Drug Administration. For the proposed Phase I clinical, this TE patch will be implanted onto the epicardial surface of non-immunosuppressed patients undergoing elective Coronary Artery Bypass Grafting with Ejection Fractions ≥ 20% and ≤ 45%. The primary endpoints will be adverse events/severe adverse events associated with placing the TE patch on the heart. While Phase I trials are primarily safety trials, this proposed trial is designed to obtain some potential efficacy endpoints to help with the design of future Phase II/III clinical trials. These endpoints include changes in LV remodeling that were seen in the preclinical animal models as well as including endpoints that focus on patient well-being.

Original language	English (US)
Article number	54
Journal	Vessel Plus
Volume	6
DOIs	https://doi.org/10.20517/2574-1209.2021.149
State	Published - 2022

Bibliographical note

Funding Information:
This work was supported by the Arizona Department of Health Services; Arizona Biomedical Research Centre Investigator Grant # ADHS16-162516, the NHLBI PACT Program for Cell Development PCT0009-2, the WARMER Research Foundation, the Sarver Heart Center, and the University of Arizona.

Publisher Copyright:
© The Author(s) 2022.

Keywords

Bioengineered patch
cardiomyocyte
cell-based therapy
fibroblast
heart failure
human induced pluripotent stem cells

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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title = "Perspective on the development of a bioengineered patch to treat heart failure: rationale and proposed design of phase I clinical trial",

abstract = "This perspective focuses on the development of tissue engineered (TE) cell-based therapies to treat left ventricular (LV) dysfunction and chronic heart failure (CHF). The development of induced pluripotent stem cells enabled investigators to seed or co-culture human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) alone and in combination with other cells onto bioengineered scaffolds applied to the epicardial surface of the damaged left ventricle. Using our work as an example, we show how a xenograft implant of a bioengineered scaffold embedded with human neonatal fibroblasts and seeded with hiPSC-CMs partially reversed maladaptive LV remodeling and improved LV systolic/diastolic function in an immune-competent rat model of CHF. The fibroblasts lay down an extracellular matrix and secrete growth factors that increase myocardial blood flow. This approach provides an improved cell payload that covers a larger area of the damaged left ventricle as opposed to direct cell injections into the heart or down the coronary arteries. These studies combined with ongoing studies in immune-competent Yucatan mini swine treated with the same xenograft led to the preliminary design of a proposed Phase I clinical trial that will be presented to the Federal Drug Administration. For the proposed Phase I clinical, this TE patch will be implanted onto the epicardial surface of non-immunosuppressed patients undergoing elective Coronary Artery Bypass Grafting with Ejection Fractions ≥ 20% and ≤ 45%. The primary endpoints will be adverse events/severe adverse events associated with placing the TE patch on the heart. While Phase I trials are primarily safety trials, this proposed trial is designed to obtain some potential efficacy endpoints to help with the design of future Phase II/III clinical trials. These endpoints include changes in LV remodeling that were seen in the preclinical animal models as well as including endpoints that focus on patient well-being.",

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note = "Funding Information: This work was supported by the Arizona Department of Health Services; Arizona Biomedical Research Centre Investigator Grant # ADHS16-162516, the NHLBI PACT Program for Cell Development PCT0009-2, the WARMER Research Foundation, the Sarver Heart Center, and the University of Arizona. Publisher Copyright: {\textcopyright} The Author(s) 2022.",

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AU - Juneman, Elizabeth

AU - Greenberg, Barry

AU - Kelly, Rosemary F.

AU - Koevary, Jen Watson

AU - Lancaster, Jordan J.

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Perspective on the development of a bioengineered patch to treat heart failure: rationale and proposed design of phase I clinical trial

Abstract

Bibliographical note

Keywords

UN SDGs

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