PIM1-minicircle as a therapeutic treatment for myocardial infarction.

PIM1-minicircle as a therapeutic treatment for myocardial infarction.

PIM1, a pro-survival gene encoding a serine/ threonine kinase, influences cell proliferation and survival. Modification of cardiac progenitor cells (CPCs) or cardiomyocytes with PIM1 using a lentivirus-based delivery method showed long-term improved cardiac function after myocardial infarction (MI)....

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Main Authors: Nan Liu, Bingyan J Wang, Kathleen M Broughton, Roberto Alvarez, Sailay Siddiqi, Rebeca Loaiza, Nicky Nguyen, Pearl Quijada, Natalie Gude, Mark A Sussman
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5360264?pdf=render
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spelling doaj-375ca4ddb5724a1b88f7feee99257ba02020-11-25T01:14:57ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-01123e017396310.1371/journal.pone.0173963PIM1-minicircle as a therapeutic treatment for myocardial infarction.Nan LiuBingyan J WangKathleen M BroughtonRoberto AlvarezSailay SiddiqiRebeca LoaizaNicky NguyenPearl QuijadaNatalie GudeMark A SussmanPIM1, a pro-survival gene encoding a serine/ threonine kinase, influences cell proliferation and survival. Modification of cardiac progenitor cells (CPCs) or cardiomyocytes with PIM1 using a lentivirus-based delivery method showed long-term improved cardiac function after myocardial infarction (MI). However, lentivirus based delivery methods have stringent FDA regulation with respect to clinical trials. To provide an alternative and low risk PIM1 delivery method, this study examined the use of a non-viral modified plasmid-minicircle (MC) as a vehicle to deliver PIM1 into mouse CPCs (mCPCs) in vitro and the myocardium in vivo. MC containing a turbo gfp reporter gene (gfp-MC) was used as a transfection and injection control. PIM1 was subcloned into gfp-MC (PIM1-MC) and then transfected into mCPCs at an efficiency of 29.4±3.7%. PIM1-MC engineered mCPCs (PIM1-mCPCs) exhibit significantly (P<0.05) better survival rate under oxidative treatment. PIM1-mCPCs also exhibit 1.9±0.1 and 2.2±0.2 fold higher cell proliferation at 3 and 5 days post plating, respectively, as compared to gfp-MC transfected mCPCs control. PIM1-MC was injected directly into ten-week old adult FVB female mice hearts in the border zone immediately after MI. Delivery of PIM1 into myocardium was confirmed by GFP+ cardiomyocytes. Mice with PIM1-MC injection showed increased protection compared to gfp-MC injection groups measured by ejection fraction at 3 and 7 days post injury (P = 0.0379 and P = 0.0262 by t-test, respectively). Success of PIM1 delivery and integration into mCPCs in vitro and cardiomyocytes in vivo by MC highlights the possibility of a non-cell based therapeutic approach for treatment of ischemic heart disease and MI.http://europepmc.org/articles/PMC5360264?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Nan Liu
Bingyan J Wang
Kathleen M Broughton
Roberto Alvarez
Sailay Siddiqi
Rebeca Loaiza
Nicky Nguyen
Pearl Quijada
Natalie Gude
Mark A Sussman
spellingShingle Nan Liu
Bingyan J Wang
Kathleen M Broughton
Roberto Alvarez
Sailay Siddiqi
Rebeca Loaiza
Nicky Nguyen
Pearl Quijada
Natalie Gude
Mark A Sussman
PIM1-minicircle as a therapeutic treatment for myocardial infarction.
PLoS ONE
author_facet Nan Liu
Bingyan J Wang
Kathleen M Broughton
Roberto Alvarez
Sailay Siddiqi
Rebeca Loaiza
Nicky Nguyen
Pearl Quijada
Natalie Gude
Mark A Sussman
author_sort Nan Liu
title PIM1-minicircle as a therapeutic treatment for myocardial infarction.
title_short PIM1-minicircle as a therapeutic treatment for myocardial infarction.
title_full PIM1-minicircle as a therapeutic treatment for myocardial infarction.
title_fullStr PIM1-minicircle as a therapeutic treatment for myocardial infarction.
title_full_unstemmed PIM1-minicircle as a therapeutic treatment for myocardial infarction.
title_sort pim1-minicircle as a therapeutic treatment for myocardial infarction.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description PIM1, a pro-survival gene encoding a serine/ threonine kinase, influences cell proliferation and survival. Modification of cardiac progenitor cells (CPCs) or cardiomyocytes with PIM1 using a lentivirus-based delivery method showed long-term improved cardiac function after myocardial infarction (MI). However, lentivirus based delivery methods have stringent FDA regulation with respect to clinical trials. To provide an alternative and low risk PIM1 delivery method, this study examined the use of a non-viral modified plasmid-minicircle (MC) as a vehicle to deliver PIM1 into mouse CPCs (mCPCs) in vitro and the myocardium in vivo. MC containing a turbo gfp reporter gene (gfp-MC) was used as a transfection and injection control. PIM1 was subcloned into gfp-MC (PIM1-MC) and then transfected into mCPCs at an efficiency of 29.4±3.7%. PIM1-MC engineered mCPCs (PIM1-mCPCs) exhibit significantly (P<0.05) better survival rate under oxidative treatment. PIM1-mCPCs also exhibit 1.9±0.1 and 2.2±0.2 fold higher cell proliferation at 3 and 5 days post plating, respectively, as compared to gfp-MC transfected mCPCs control. PIM1-MC was injected directly into ten-week old adult FVB female mice hearts in the border zone immediately after MI. Delivery of PIM1 into myocardium was confirmed by GFP+ cardiomyocytes. Mice with PIM1-MC injection showed increased protection compared to gfp-MC injection groups measured by ejection fraction at 3 and 7 days post injury (P = 0.0379 and P = 0.0262 by t-test, respectively). Success of PIM1 delivery and integration into mCPCs in vitro and cardiomyocytes in vivo by MC highlights the possibility of a non-cell based therapeutic approach for treatment of ischemic heart disease and MI.
url http://europepmc.org/articles/PMC5360264?pdf=render
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