Cell-cell contacts via N-cadherin induce a regulatory renin secretory phenotype in As4.1 cells

Jai Won Chang; Soohyun Kim; Eun Young Lee; Chae Hun Leem; Suhn Hee Kim; Chun Sik Park

doi:10.4196/kjpp.2022.26.6.479

Cell-cell contacts via N-cadherin induce a regulatory renin secretory phenotype in As4.1 cells

Jai Won Chang, Soohyun Kim, Eun Young Lee, Chae Hun Leem, Suhn Hee Kim, Chun Sik Park

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

1 Scopus citations

Abstract

The lack of a clonal renin-secreting cell line has greatly hindered the investigation of the regulatory mechanisms of renin secretion at the cellular, biochemical, and molecular levels. In the present study, we investigated whether it was possible to induce phenotypic switching of the renin-expressing clonal cell line As4.1 from constitutive inactive renin secretion to regulated active renin secretion. When grown to postconfluence for at least two days in media containing fetal bovine serum or insulin-like growth factor-1, the formation of cell-cell contacts via N-cadherin triggered downstream cellular signaling cascades and activated smooth muscle-specific genes, culminating in phenotypic switching to a regulated active renin secretion phenotype, including responding to the key stimuli of active renin secretion. With the use of phenotype-switched As4.1 cells, we provide the first evidence that active renin secretion via exocytosis is regulated by phosphorylation/dephosphorylation of the 20 kDa myosin light chain. The molecular mechanism of phenotypic switching in As4.1 cells described here could serve as a working model for full phenotypic modulation of other secretory cell lines with incomplete phenotypes.

Original language	English
Pages (from-to)	479-499
Number of pages	21
Journal	Korean Journal of Physiology and Pharmacology
Volume	26
Issue number	6
DOIs	https://doi.org/10.4196/kjpp.2022.26.6.479
State	Published - Nov 2022

Bibliographical note

Funding Information:
This study was supported by grants from the Korea Research

Funding Information:
This study was supported by grants from the Korea Research Foundation (No. 1997-001-F00035), the Korea Science and Engineering Foundation (No. 98-0403-09-01-5), and the Asan Institute for Life Sciences, Seoul, Republic of Korea, awarded to CS Park (No. 2001-035).

Publisher Copyright:
Copyright © 2022 Korean J Physiol Pharmacol.

Keywords

MRTF-A
Myosin light chain
Myosin light chain phosohatase-1
Myosin light-chain kinase
N-cadherin
Phenotype switching

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10.4196/kjpp.2022.26.6.479

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title = "Cell-cell contacts via N-cadherin induce a regulatory renin secretory phenotype in As4.1 cells",

abstract = "The lack of a clonal renin-secreting cell line has greatly hindered the investigation of the regulatory mechanisms of renin secretion at the cellular, biochemical, and molecular levels. In the present study, we investigated whether it was possible to induce phenotypic switching of the renin-expressing clonal cell line As4.1 from constitutive inactive renin secretion to regulated active renin secretion. When grown to postconfluence for at least two days in media containing fetal bovine serum or insulin-like growth factor-1, the formation of cell-cell contacts via N-cadherin triggered downstream cellular signaling cascades and activated smooth muscle-specific genes, culminating in phenotypic switching to a regulated active renin secretion phenotype, including responding to the key stimuli of active renin secretion. With the use of phenotype-switched As4.1 cells, we provide the first evidence that active renin secretion via exocytosis is regulated by phosphorylation/dephosphorylation of the 20 kDa myosin light chain. The molecular mechanism of phenotypic switching in As4.1 cells described here could serve as a working model for full phenotypic modulation of other secretory cell lines with incomplete phenotypes.",

keywords = "MRTF-A, Myosin light chain, Myosin light chain phosohatase-1, Myosin light-chain kinase, N-cadherin, Phenotype switching",

author = "Chang, {Jai Won} and Soohyun Kim and Lee, {Eun Young} and Leem, {Chae Hun} and Kim, {Suhn Hee} and Park, {Chun Sik}",

note = "Funding Information: This study was supported by grants from the Korea Research Funding Information: This study was supported by grants from the Korea Research Foundation (No. 1997-001-F00035), the Korea Science and Engineering Foundation (No. 98-0403-09-01-5), and the Asan Institute for Life Sciences, Seoul, Republic of Korea, awarded to CS Park (No. 2001-035). Publisher Copyright: Copyright {\textcopyright} 2022 Korean J Physiol Pharmacol.",

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AU - Leem, Chae Hun

AU - Kim, Suhn Hee

AU - Park, Chun Sik

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N2 - The lack of a clonal renin-secreting cell line has greatly hindered the investigation of the regulatory mechanisms of renin secretion at the cellular, biochemical, and molecular levels. In the present study, we investigated whether it was possible to induce phenotypic switching of the renin-expressing clonal cell line As4.1 from constitutive inactive renin secretion to regulated active renin secretion. When grown to postconfluence for at least two days in media containing fetal bovine serum or insulin-like growth factor-1, the formation of cell-cell contacts via N-cadherin triggered downstream cellular signaling cascades and activated smooth muscle-specific genes, culminating in phenotypic switching to a regulated active renin secretion phenotype, including responding to the key stimuli of active renin secretion. With the use of phenotype-switched As4.1 cells, we provide the first evidence that active renin secretion via exocytosis is regulated by phosphorylation/dephosphorylation of the 20 kDa myosin light chain. The molecular mechanism of phenotypic switching in As4.1 cells described here could serve as a working model for full phenotypic modulation of other secretory cell lines with incomplete phenotypes.

AB - The lack of a clonal renin-secreting cell line has greatly hindered the investigation of the regulatory mechanisms of renin secretion at the cellular, biochemical, and molecular levels. In the present study, we investigated whether it was possible to induce phenotypic switching of the renin-expressing clonal cell line As4.1 from constitutive inactive renin secretion to regulated active renin secretion. When grown to postconfluence for at least two days in media containing fetal bovine serum or insulin-like growth factor-1, the formation of cell-cell contacts via N-cadherin triggered downstream cellular signaling cascades and activated smooth muscle-specific genes, culminating in phenotypic switching to a regulated active renin secretion phenotype, including responding to the key stimuli of active renin secretion. With the use of phenotype-switched As4.1 cells, we provide the first evidence that active renin secretion via exocytosis is regulated by phosphorylation/dephosphorylation of the 20 kDa myosin light chain. The molecular mechanism of phenotypic switching in As4.1 cells described here could serve as a working model for full phenotypic modulation of other secretory cell lines with incomplete phenotypes.

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KW - Myosin light-chain kinase

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Cell-cell contacts via N-cadherin induce a regulatory renin secretory phenotype in As4.1 cells

Abstract

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Keywords

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