A Human iPSC Double-Reporter System Enables Purification of Cardiac Lineage Subpopulations with Distinct Function and Drug Response Profiles

Joe Z. Zhang; Vittavat Termglinchan; Ning Yi Shao; Ilanit Itzhaki; Chun Liu; Ning Ma; Lei Tian; Vicky Y. Wang; Alex C.Y. Chang; Hongchao Guo; Tomoya Kitani; Haodi Wu; Chi Keung Lam; Kazuki Kodo; Nazish Sayed; Helen M. Blau; Joseph C. Wu

doi:10.1016/j.stem.2019.02.015

A Human iPSC Double-Reporter System Enables Purification of Cardiac Lineage Subpopulations with Distinct Function and Drug Response Profiles

Joe Z. Zhang, Vittavat Termglinchan, Ning Yi Shao, Ilanit Itzhaki, Chun Liu, Ning Ma, Lei Tian, Vicky Y. Wang, Alex C.Y. Chang, Hongchao Guo, Tomoya Kitani, Haodi Wu, Chi Keung Lam, Kazuki Kodo, Nazish Sayed, Helen M. Blau, Joseph C. Wu

Department of Pediatrics

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

86 Citations (Scopus)

Abstract

Wu and colleagues create a double-knockin human TBX5^Clover2 and NKX2-5^TagRFP reporter to delineate cardiac lineages during differentiation. Molecular and functional analyses uncover that differential expression of TBX5 and NKX2-5 specifies different cardiac fate. This reporter is applicable for studying cardiac lineage determination in vitro and isolating cardiac subpopulations.

Original language	English
Pages (from-to)	802-811.e5
Journal	Cell stem cell
Volume	24
Issue number	5
DOIs	https://doi.org/10.1016/j.stem.2019.02.015
Publication status	Published - 2019 May 2

Keywords

CORIN
NKX2-5
TBX5
cardiomyocyte subtypes
endothelial cell lineage
epicardial lineage
hiPSC double reporter
human first and second heart field
precise drug testing
purification

ASJC Scopus subject areas

Molecular Medicine
Genetics
Cell Biology

UN SDGs

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

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10.1016/j.stem.2019.02.015

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Zhang, J. Z., Termglinchan, V., Shao, N. Y., Itzhaki, I., Liu, C., Ma, N., Tian, L., Wang, V. Y., Chang, A. C. Y., Guo, H., Kitani, T., Wu, H., Lam, C. K., Kodo, K., Sayed, N., Blau, H. M., & Wu, J. C. (2019). A Human iPSC Double-Reporter System Enables Purification of Cardiac Lineage Subpopulations with Distinct Function and Drug Response Profiles. Cell stem cell, 24(5), 802-811.e5. https://doi.org/10.1016/j.stem.2019.02.015

Zhang, JZ, Termglinchan, V, Shao, NY, Itzhaki, I, Liu, C, Ma, N, Tian, L, Wang, VY, Chang, ACY, Guo, H, Kitani, T, Wu, H, Lam, CK, Kodo, K, Sayed, N, Blau, HM & Wu, JC 2019, 'A Human iPSC Double-Reporter System Enables Purification of Cardiac Lineage Subpopulations with Distinct Function and Drug Response Profiles', Cell stem cell, vol. 24, no. 5, pp. 802-811.e5. https://doi.org/10.1016/j.stem.2019.02.015

@article{17819b171d68466abbef486e93917862,

title = "A Human iPSC Double-Reporter System Enables Purification of Cardiac Lineage Subpopulations with Distinct Function and Drug Response Profiles",

abstract = "Wu and colleagues create a double-knockin human TBX5Clover2 and NKX2-5TagRFP reporter to delineate cardiac lineages during differentiation. Molecular and functional analyses uncover that differential expression of TBX5 and NKX2-5 specifies different cardiac fate. This reporter is applicable for studying cardiac lineage determination in vitro and isolating cardiac subpopulations.",

keywords = "CORIN, NKX2-5, TBX5, cardiomyocyte subtypes, endothelial cell lineage, epicardial lineage, hiPSC double reporter, human first and second heart field, precise drug testing, purification",

author = "Zhang, {Joe Z.} and Vittavat Termglinchan and Shao, {Ning Yi} and Ilanit Itzhaki and Chun Liu and Ning Ma and Lei Tian and Wang, {Vicky Y.} and Chang, {Alex C.Y.} and Hongchao Guo and Tomoya Kitani and Haodi Wu and Lam, {Chi Keung} and Kazuki Kodo and Nazish Sayed and Blau, {Helen M.} and Wu, {Joseph C.}",

note = "Funding Information: We thank Professor Michael Z. Lin (Department of Bioengineering, Stanford University) for providing the ASAP2 lentiviral vector. This work was supported by the American Heart Association Merit Award; Leducq Foundation 18CVD05; Burroughs Wellcome Fund 1015009 ; NIH grants R01 HL130020 , R01 HL133272 , R01 HL126527 , and R01 HL128170 (J.C.W.); R01 NS089533 (H.M.B.); K01 HL135455 (N.S.); and K99 HL133473 (H.W.); American Heart Association Postdoctoral Fellowship 16POST31150011 (H.W.); and TRDRP Fellowship 26FT-0029 (J.Z.Z). Funding Information: We thank Professor Michael Z. Lin (Department of Bioengineering, Stanford University)for providing the ASAP2 lentiviral vector. This work was supported by the American Heart Association Merit Award; Leducq Foundation 18CVD05; Burroughs Wellcome Fund 1015009; NIH grants R01 HL130020, R01 HL133272, R01 HL126527, and R01 HL128170 (J.C.W.); R01 NS089533 (H.M.B.); K01 HL135455 (N.S.); and K99 HL133473 (H.W.); American Heart Association Postdoctoral Fellowship 16POST31150011 (H.W.); and TRDRP Fellowship 26FT-0029 (J.Z.Z). J.Z.Z. conducted experiments and wrote the manuscript. V.T. K.K. T.K. and N.M. generated the reporter. I.I. performed patch-clamp experiments. N.-Y.S. and L.T. analyzed RNA-Seq data. A.C.Y.C. performed Seahorse experiments. C.L. and N.S. performed EC experiments. V.Y.W. developed MATLAB codes. H.G. H.W. C.K.L. and H.M.B. edited the manuscript. J.C.W. designed the study, wrote the manuscript, and provided funding support. J.C.W. is a co-founder of Khloris Biosciences but has no competing interests, as the work presented was performed independently. H.M.B. is a co-founder of Myoforte Therapeutics but has no competing interests, as the work presented was performed independently. Publisher Copyright: {\textcopyright} 2019 Elsevier Inc.",

year = "2019",

month = may,

day = "2",

doi = "10.1016/j.stem.2019.02.015",

language = "English",

volume = "24",

pages = "802--811.e5",

journal = "Cell stem cell",

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publisher = "Cell Press",

number = "5",

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TY - JOUR

T1 - A Human iPSC Double-Reporter System Enables Purification of Cardiac Lineage Subpopulations with Distinct Function and Drug Response Profiles

AU - Zhang, Joe Z.

AU - Termglinchan, Vittavat

AU - Shao, Ning Yi

AU - Itzhaki, Ilanit

AU - Liu, Chun

AU - Ma, Ning

AU - Tian, Lei

AU - Wang, Vicky Y.

AU - Chang, Alex C.Y.

AU - Guo, Hongchao

AU - Kitani, Tomoya

AU - Wu, Haodi

AU - Lam, Chi Keung

AU - Kodo, Kazuki

AU - Sayed, Nazish

AU - Blau, Helen M.

AU - Wu, Joseph C.

N1 - Funding Information: We thank Professor Michael Z. Lin (Department of Bioengineering, Stanford University) for providing the ASAP2 lentiviral vector. This work was supported by the American Heart Association Merit Award; Leducq Foundation 18CVD05; Burroughs Wellcome Fund 1015009 ; NIH grants R01 HL130020 , R01 HL133272 , R01 HL126527 , and R01 HL128170 (J.C.W.); R01 NS089533 (H.M.B.); K01 HL135455 (N.S.); and K99 HL133473 (H.W.); American Heart Association Postdoctoral Fellowship 16POST31150011 (H.W.); and TRDRP Fellowship 26FT-0029 (J.Z.Z). Funding Information: We thank Professor Michael Z. Lin (Department of Bioengineering, Stanford University)for providing the ASAP2 lentiviral vector. This work was supported by the American Heart Association Merit Award; Leducq Foundation 18CVD05; Burroughs Wellcome Fund 1015009; NIH grants R01 HL130020, R01 HL133272, R01 HL126527, and R01 HL128170 (J.C.W.); R01 NS089533 (H.M.B.); K01 HL135455 (N.S.); and K99 HL133473 (H.W.); American Heart Association Postdoctoral Fellowship 16POST31150011 (H.W.); and TRDRP Fellowship 26FT-0029 (J.Z.Z). J.Z.Z. conducted experiments and wrote the manuscript. V.T. K.K. T.K. and N.M. generated the reporter. I.I. performed patch-clamp experiments. N.-Y.S. and L.T. analyzed RNA-Seq data. A.C.Y.C. performed Seahorse experiments. C.L. and N.S. performed EC experiments. V.Y.W. developed MATLAB codes. H.G. H.W. C.K.L. and H.M.B. edited the manuscript. J.C.W. designed the study, wrote the manuscript, and provided funding support. J.C.W. is a co-founder of Khloris Biosciences but has no competing interests, as the work presented was performed independently. H.M.B. is a co-founder of Myoforte Therapeutics but has no competing interests, as the work presented was performed independently. Publisher Copyright: © 2019 Elsevier Inc.

PY - 2019/5/2

Y1 - 2019/5/2

N2 - Wu and colleagues create a double-knockin human TBX5Clover2 and NKX2-5TagRFP reporter to delineate cardiac lineages during differentiation. Molecular and functional analyses uncover that differential expression of TBX5 and NKX2-5 specifies different cardiac fate. This reporter is applicable for studying cardiac lineage determination in vitro and isolating cardiac subpopulations.

AB - Wu and colleagues create a double-knockin human TBX5Clover2 and NKX2-5TagRFP reporter to delineate cardiac lineages during differentiation. Molecular and functional analyses uncover that differential expression of TBX5 and NKX2-5 specifies different cardiac fate. This reporter is applicable for studying cardiac lineage determination in vitro and isolating cardiac subpopulations.

KW - CORIN

KW - NKX2-5

KW - TBX5

KW - cardiomyocyte subtypes

KW - endothelial cell lineage

KW - epicardial lineage

KW - hiPSC double reporter

KW - human first and second heart field

KW - precise drug testing

KW - purification

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UR - http://www.scopus.com/inward/citedby.url?scp=85063945893&partnerID=8YFLogxK

U2 - 10.1016/j.stem.2019.02.015

DO - 10.1016/j.stem.2019.02.015

M3 - Article

C2 - 30880024

AN - SCOPUS:85063945893

SN - 1934-5909

VL - 24

SP - 802-811.e5

JO - Cell stem cell

JF - Cell stem cell

IS - 5

ER -

A Human iPSC Double-Reporter System Enables Purification of Cardiac Lineage Subpopulations with Distinct Function and Drug Response Profiles

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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