Complementation of Ah receptor deficiency in hepatoma cells: Negative feedback regulation and cell cycle control by the Ah receptor

Carsten Weiß; Siva Kumar Kolluri; Franz Kiefer; Martin Göttlicher

doi:10.1006/excr.1996.0214

Complementation of Ah receptor deficiency in hepatoma cells: Negative feedback regulation and cell cycle control by the Ah receptor

Carsten Weiß, Siva Kumar Kolluri, Franz Kiefer, Martin Göttlicher

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

153 Scopus citations

Abstract

The Ah receptor (AhR) is a ligand-dependent transcription factor subunit that heterodimerizes with the AhR nuclear translocator (Arnt) and mediates the predominant biological effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD). TCDD activates target genes in xenobiotica metabolism in many cell lines and, more specifically, delays G1-S progression of 5L hepatoma cells. Here we describe transient and stable AhR-expression analysis in AhR- deficient subclones of the TCDD-sensitive 5L cells. We tested the integrity of the AhR-signaling system beyond the lack of the receptor in the variant subclone and analyzed the role of AhR in cell cycle regulation. Transiently expressed AhR has a high basal activity on promoters containing AhR-binding sites, so-called XREs, when transfected into receptor-deficient variant cells compared to wild-type cells. Single- and double-hybrid analysis dissociates AhR ligand responsiveness, transactivation, and heterodimerization with Arnt from receptor binding to an XRE. Hybrid receptors also show the high basal activity in the absence of exogenous TCDD in AhR-deficient variant cells, indicating that the endogenous AhR-activating signal acts directly on the receptor rather than XRE-dependent promoters or DNA binding of the receptor. Stable expression of AhR in variant cell clones by retroviral infection fully reconstitutes TCDD responsiveness, including target-gene induction and delay of cell cycle progression. These AhR-reconstituted cells, like AhR-containing wild-type cells, show low basal activity of the transiently expressed AhR hybrid. Thus, the increased basal activity in AhR-deficient cells suggests a negative feedback control of AhR activity. In vitro ligand-binding assays are compatible with the idea that the increased basal activity is due to the accumulation of an AhR-binding endogenous ligand. In conclusion, AhR is causally responsible for TCDD-dependent cell cycle regulation and feedback control of AhR activity.

Original language	English
Pages (from-to)	154-163
Number of pages	10
Journal	Experimental Cell Research
Volume	226
Issue number	1
DOIs	https://doi.org/10.1006/excr.1996.0214
State	Published - 10 Jul 1996
Externally published	Yes

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@article{c4e963d0e423440dbb040644198a3967,

title = "Complementation of Ah receptor deficiency in hepatoma cells: Negative feedback regulation and cell cycle control by the Ah receptor",

abstract = "The Ah receptor (AhR) is a ligand-dependent transcription factor subunit that heterodimerizes with the AhR nuclear translocator (Arnt) and mediates the predominant biological effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD). TCDD activates target genes in xenobiotica metabolism in many cell lines and, more specifically, delays G1-S progression of 5L hepatoma cells. Here we describe transient and stable AhR-expression analysis in AhR- deficient subclones of the TCDD-sensitive 5L cells. We tested the integrity of the AhR-signaling system beyond the lack of the receptor in the variant subclone and analyzed the role of AhR in cell cycle regulation. Transiently expressed AhR has a high basal activity on promoters containing AhR-binding sites, so-called XREs, when transfected into receptor-deficient variant cells compared to wild-type cells. Single- and double-hybrid analysis dissociates AhR ligand responsiveness, transactivation, and heterodimerization with Arnt from receptor binding to an XRE. Hybrid receptors also show the high basal activity in the absence of exogenous TCDD in AhR-deficient variant cells, indicating that the endogenous AhR-activating signal acts directly on the receptor rather than XRE-dependent promoters or DNA binding of the receptor. Stable expression of AhR in variant cell clones by retroviral infection fully reconstitutes TCDD responsiveness, including target-gene induction and delay of cell cycle progression. These AhR-reconstituted cells, like AhR-containing wild-type cells, show low basal activity of the transiently expressed AhR hybrid. Thus, the increased basal activity in AhR-deficient cells suggests a negative feedback control of AhR activity. In vitro ligand-binding assays are compatible with the idea that the increased basal activity is due to the accumulation of an AhR-binding endogenous ligand. In conclusion, AhR is causally responsible for TCDD-dependent cell cycle regulation and feedback control of AhR activity.",

author = "Carsten Wei{\ss} and Kolluri, \{Siva Kumar\} and Franz Kiefer and Martin G{\"o}ttlicher",

note = "Funding Information: Dr. Christopher A. Brad{\textregistered}eld, Dr. Oliver Hankinson, Dr. Lorenz Poellinger, and Dr. Murray Whitelaw are gratefully acknowledged for providing cDNAs for AhR, Arnt, and derived constructs. H. Land provided the vector and VE cell line for generation of retroviral vectors, and Dr. F. J. Wiebel provided the 5L hepatoma cells and their subclones. Dr. Ju{\`E} rgen Moll contributed valuable help with the ¯ow cytometry analysis. The authors thank Dr. Peter Herrlich, Dr. Andrew Cato, Dr. Lorenz Poellinger, Dr. Erik Wade, and Dr. Mihail Iordanov for critical support and Karin Braun for technical help. The work was supported by grants of the Deutsche Forschungsgemein-schaft (M.G., DFG-GO473/2).",

year = "1996",

month = jul,

day = "10",

doi = "10.1006/excr.1996.0214",

language = "English",

volume = "226",

pages = "154--163",

journal = "Experimental Cell Research",

issn = "0014-4827",

publisher = "Elsevier Inc.",

number = "1",

}

TY - JOUR

T1 - Complementation of Ah receptor deficiency in hepatoma cells

T2 - Negative feedback regulation and cell cycle control by the Ah receptor

AU - Weiß, Carsten

AU - Kolluri, Siva Kumar

AU - Kiefer, Franz

AU - Göttlicher, Martin

N1 - Funding Information: Dr. Christopher A. Brad®eld, Dr. Oliver Hankinson, Dr. Lorenz Poellinger, and Dr. Murray Whitelaw are gratefully acknowledged for providing cDNAs for AhR, Arnt, and derived constructs. H. Land provided the vector and VE cell line for generation of retroviral vectors, and Dr. F. J. Wiebel provided the 5L hepatoma cells and their subclones. Dr. JuÈ rgen Moll contributed valuable help with the ¯ow cytometry analysis. The authors thank Dr. Peter Herrlich, Dr. Andrew Cato, Dr. Lorenz Poellinger, Dr. Erik Wade, and Dr. Mihail Iordanov for critical support and Karin Braun for technical help. The work was supported by grants of the Deutsche Forschungsgemein-schaft (M.G., DFG-GO473/2).

PY - 1996/7/10

Y1 - 1996/7/10

N2 - The Ah receptor (AhR) is a ligand-dependent transcription factor subunit that heterodimerizes with the AhR nuclear translocator (Arnt) and mediates the predominant biological effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD). TCDD activates target genes in xenobiotica metabolism in many cell lines and, more specifically, delays G1-S progression of 5L hepatoma cells. Here we describe transient and stable AhR-expression analysis in AhR- deficient subclones of the TCDD-sensitive 5L cells. We tested the integrity of the AhR-signaling system beyond the lack of the receptor in the variant subclone and analyzed the role of AhR in cell cycle regulation. Transiently expressed AhR has a high basal activity on promoters containing AhR-binding sites, so-called XREs, when transfected into receptor-deficient variant cells compared to wild-type cells. Single- and double-hybrid analysis dissociates AhR ligand responsiveness, transactivation, and heterodimerization with Arnt from receptor binding to an XRE. Hybrid receptors also show the high basal activity in the absence of exogenous TCDD in AhR-deficient variant cells, indicating that the endogenous AhR-activating signal acts directly on the receptor rather than XRE-dependent promoters or DNA binding of the receptor. Stable expression of AhR in variant cell clones by retroviral infection fully reconstitutes TCDD responsiveness, including target-gene induction and delay of cell cycle progression. These AhR-reconstituted cells, like AhR-containing wild-type cells, show low basal activity of the transiently expressed AhR hybrid. Thus, the increased basal activity in AhR-deficient cells suggests a negative feedback control of AhR activity. In vitro ligand-binding assays are compatible with the idea that the increased basal activity is due to the accumulation of an AhR-binding endogenous ligand. In conclusion, AhR is causally responsible for TCDD-dependent cell cycle regulation and feedback control of AhR activity.

AB - The Ah receptor (AhR) is a ligand-dependent transcription factor subunit that heterodimerizes with the AhR nuclear translocator (Arnt) and mediates the predominant biological effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD). TCDD activates target genes in xenobiotica metabolism in many cell lines and, more specifically, delays G1-S progression of 5L hepatoma cells. Here we describe transient and stable AhR-expression analysis in AhR- deficient subclones of the TCDD-sensitive 5L cells. We tested the integrity of the AhR-signaling system beyond the lack of the receptor in the variant subclone and analyzed the role of AhR in cell cycle regulation. Transiently expressed AhR has a high basal activity on promoters containing AhR-binding sites, so-called XREs, when transfected into receptor-deficient variant cells compared to wild-type cells. Single- and double-hybrid analysis dissociates AhR ligand responsiveness, transactivation, and heterodimerization with Arnt from receptor binding to an XRE. Hybrid receptors also show the high basal activity in the absence of exogenous TCDD in AhR-deficient variant cells, indicating that the endogenous AhR-activating signal acts directly on the receptor rather than XRE-dependent promoters or DNA binding of the receptor. Stable expression of AhR in variant cell clones by retroviral infection fully reconstitutes TCDD responsiveness, including target-gene induction and delay of cell cycle progression. These AhR-reconstituted cells, like AhR-containing wild-type cells, show low basal activity of the transiently expressed AhR hybrid. Thus, the increased basal activity in AhR-deficient cells suggests a negative feedback control of AhR activity. In vitro ligand-binding assays are compatible with the idea that the increased basal activity is due to the accumulation of an AhR-binding endogenous ligand. In conclusion, AhR is causally responsible for TCDD-dependent cell cycle regulation and feedback control of AhR activity.

UR - https://www.scopus.com/pages/publications/0001459262

U2 - 10.1006/excr.1996.0214

DO - 10.1006/excr.1996.0214

M3 - Article

C2 - 8660951

AN - SCOPUS:0001459262

SN - 0014-4827

VL - 226

SP - 154

EP - 163

JO - Experimental Cell Research

JF - Experimental Cell Research

IS - 1

ER -

Complementation of Ah receptor deficiency in hepatoma cells: Negative feedback regulation and cell cycle control by the Ah receptor

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