Zyxin regulates embryonic stem cell fate by modulating mechanical and biochemical signaling interface

Songjing Zhang; Lor Huai Chong; Jessie Yong Xing Woon; Theng Xuan Chua; Elsie Cheruba; Ai Kia Yip; Hoi Yeung Li; Keng Hwee Chiam; Cheng Gee Koh

doi:10.1038/s42003-023-04421-0

Zyxin regulates embryonic stem cell fate by modulating mechanical and biochemical signaling interface

Songjing Zhang
, Lor Huai Chong
, Jessie Yong Xing Woon
, Theng Xuan Chua
, Elsie Cheruba
, Ai Kia Yip
, Hoi Yeung Li
, Keng Hwee Chiam
, Cheng Gee Koh

Malaysia Sch of Pharmacy

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

11 Citations (Scopus)

Abstract

Biochemical signaling and mechano-transduction are both critical in regulating stem cell fate. How crosstalk between mechanical and biochemical cues influences embryonic development, however, is not extensively investigated. Using a comparative study of focal adhesion constituents between mouse embryonic stem cell (mESC) and their differentiated counterparts, we find while zyxin is lowly expressed in mESCs, its levels increase dramatically during early differentiation. Interestingly, overexpression of zyxin in mESCs suppresses Oct4 and Nanog. Using an integrative biochemical and biophysical approach, we demonstrate involvement of zyxin in regulating pluripotency through actin stress fibres and focal adhesions which are known to modulate cellular traction stress and facilitate substrate rigidity-sensing. YAP signaling is identified as an important biochemical effector of zyxin-induced mechanotransduction. These results provide insights into the role of zyxin in the integration of mechanical and biochemical cues for the regulation of embryonic stem cell fate.

Original language	English
Article number	62
Number of pages	15
Journal	Communications Biology
Volume	6
Issue number	1
DOIs	https://doi.org/10.1038/s42003-023-04421-0
Publication status	Published - 18 Jan 2023

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title = "Zyxin regulates embryonic stem cell fate by modulating mechanical and biochemical signaling interface",

abstract = "Biochemical signaling and mechano-transduction are both critical in regulating stem cell fate. How crosstalk between mechanical and biochemical cues influences embryonic development, however, is not extensively investigated. Using a comparative study of focal adhesion constituents between mouse embryonic stem cell (mESC) and their differentiated counterparts, we find while zyxin is lowly expressed in mESCs, its levels increase dramatically during early differentiation. Interestingly, overexpression of zyxin in mESCs suppresses Oct4 and Nanog. Using an integrative biochemical and biophysical approach, we demonstrate involvement of zyxin in regulating pluripotency through actin stress fibres and focal adhesions which are known to modulate cellular traction stress and facilitate substrate rigidity-sensing. YAP signaling is identified as an important biochemical effector of zyxin-induced mechanotransduction. These results provide insights into the role of zyxin in the integration of mechanical and biochemical cues for the regulation of embryonic stem cell fate.",

author = "Songjing Zhang and Chong, \{Lor Huai\} and Woon, \{Jessie Yong Xing\} and Chua, \{Theng Xuan\} and Elsie Cheruba and Yip, \{Ai Kia\} and Li, \{Hoi Yeung\} and Chiam, \{Keng Hwee\} and Koh, \{Cheng Gee\}",

note = "Funding Information: We thank Singapore Ministry of Education MOE Tier 2 grant (MOE2018-T2-1-058), MOE Tier 1 grant (RG106/20) and Nanyang Technological University, Singapore SUG grant to C.G.K. for funding support. We also thank Jonathan Loh Yuin-Han (Institute of Molecular and Cell Biology, ASTAR) for the gift of H1, hiPSC and BJ-5ta cell lines and Pakorn Kanchanawong (Mechanobiology Institute, Singapore) for sharing the mCherry-Zyxin cDNA construct. Publisher Copyright: {\textcopyright} 2023, The Author(s).",

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doi = "10.1038/s42003-023-04421-0",

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T1 - Zyxin regulates embryonic stem cell fate by modulating mechanical and biochemical signaling interface

AU - Zhang, Songjing

AU - Chong, Lor Huai

AU - Woon, Jessie Yong Xing

AU - Chua, Theng Xuan

AU - Cheruba, Elsie

AU - Yip, Ai Kia

AU - Li, Hoi Yeung

AU - Chiam, Keng Hwee

AU - Koh, Cheng Gee

N1 - Funding Information: We thank Singapore Ministry of Education MOE Tier 2 grant (MOE2018-T2-1-058), MOE Tier 1 grant (RG106/20) and Nanyang Technological University, Singapore SUG grant to C.G.K. for funding support. We also thank Jonathan Loh Yuin-Han (Institute of Molecular and Cell Biology, ASTAR) for the gift of H1, hiPSC and BJ-5ta cell lines and Pakorn Kanchanawong (Mechanobiology Institute, Singapore) for sharing the mCherry-Zyxin cDNA construct. Publisher Copyright: © 2023, The Author(s).

PY - 2023/1/18

Y1 - 2023/1/18

N2 - Biochemical signaling and mechano-transduction are both critical in regulating stem cell fate. How crosstalk between mechanical and biochemical cues influences embryonic development, however, is not extensively investigated. Using a comparative study of focal adhesion constituents between mouse embryonic stem cell (mESC) and their differentiated counterparts, we find while zyxin is lowly expressed in mESCs, its levels increase dramatically during early differentiation. Interestingly, overexpression of zyxin in mESCs suppresses Oct4 and Nanog. Using an integrative biochemical and biophysical approach, we demonstrate involvement of zyxin in regulating pluripotency through actin stress fibres and focal adhesions which are known to modulate cellular traction stress and facilitate substrate rigidity-sensing. YAP signaling is identified as an important biochemical effector of zyxin-induced mechanotransduction. These results provide insights into the role of zyxin in the integration of mechanical and biochemical cues for the regulation of embryonic stem cell fate.

AB - Biochemical signaling and mechano-transduction are both critical in regulating stem cell fate. How crosstalk between mechanical and biochemical cues influences embryonic development, however, is not extensively investigated. Using a comparative study of focal adhesion constituents between mouse embryonic stem cell (mESC) and their differentiated counterparts, we find while zyxin is lowly expressed in mESCs, its levels increase dramatically during early differentiation. Interestingly, overexpression of zyxin in mESCs suppresses Oct4 and Nanog. Using an integrative biochemical and biophysical approach, we demonstrate involvement of zyxin in regulating pluripotency through actin stress fibres and focal adhesions which are known to modulate cellular traction stress and facilitate substrate rigidity-sensing. YAP signaling is identified as an important biochemical effector of zyxin-induced mechanotransduction. These results provide insights into the role of zyxin in the integration of mechanical and biochemical cues for the regulation of embryonic stem cell fate.

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SN - 2399-3642

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Zyxin regulates embryonic stem cell fate by modulating mechanical and biochemical signaling interface

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