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Oct 26, 2019 (publication date) through Oct 26, 2025
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Publication Name
World Journal of Cardiology
ISSN
1949-8462
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Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

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Copyright ©The Author(s) 2019.
World J Cardiol. Oct 26, 2019; 11(10): 221-235
Published online Oct 26, 2019. doi: 10.4330/wjc.v11.i10.221
Table 1 Comparison between animal and cell models
PropertiesAnimalCellular
Maintain genetic backgroundNoYes
Cost of maintenanceExpensiveLess Expensive
Ease of maintenanceSimpleDifficult
Time required++++
Drug effectsPotentially not translatableTranslatable
Study of paracrine effectsYesNo
Study of circulatory effectsYesNo
Full Size Table
Table 2 Methods of delivery for reprogramming factors
MethodAdvantagesDisadvantages
Retroviral transductionEfficient, validated for multiple cell types, easyTransgene integration
Lentiviral deliveryVery efficientTransgene integration
Adenoviral transductionDoes not integrateLow efficiency, only validated for fibroblasts
Plasmid DNA transfer (episomal)Good efficiency, does not integrate, able to replicate autonomously, validated for multiple cell typesLow efficiency in fibroblast reprogramming
Lox p lentivirus deliveryHigh efficiency, excision of the integrated sequence, gene expression profile closer to hES cellsGenomic instability and genome rearrangements and loxP site remains integrated
Sendai virusEfficient, does not integrate, validated for multiple cell typesCost if purchased commercially or challenging if generated by a laboratory
PiggyBAC transposonEfficient, precise and efficient self-excision, does not remain integratedPublished work only in fibroblasts, licensing patent issues, pBt gene may remain active post-transposition
Polyarginine tagged polypeptideDoes not integrateLow efficiency, time-consuming, technically challenging and work only on fibroblasts
RNA modified synthetic mRNAVery efficient, does not integrate, factor available commerciallyCost if purchased commercially or challenging if generated by a laboratory and work only on fibroblasts
Full Size Table
Table 3 Advantages and disadvantages of different cell types for modeling disease in vitro
PropertiesFibroblastsiPSCs
Proliferation capacity+++
Self-renewalNoYes
LongevityLimitedUnlimited
DifferentiationNoYes
MetabolismQuiescentEnergetic
AcquisitionEasyDifficult
Cost++++
Ease of maintenanceSimpleDifficult
Necessary expertiseLowHigh
Disease modeling+++
StructureSingle elongated cellsRound colonies/beating CM sheets
MaturationNot applicableRequired for CM
iPSCs: Induced pluripotent stem cells; CM: Cardiomyopathy.
Full Size Table
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