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Epigenetic mechanisms silence a disintegrin and metalloprotease 33 expression in bronchial epithelial cells

Epigenetic mechanisms silence a disintegrin and metalloprotease 33 expression in bronchial epithelial cells
Epigenetic mechanisms silence a disintegrin and metalloprotease 33 expression in bronchial epithelial cells
Background: A disintegrin and metalloprotease 33 (ADAM33) polymorphism is strongly associated with asthma and bronchial hyperresponsiveness.
Although considered to be a mesenchymal cell–specific gene, recent reports have suggested epithelial expression of ADAM33 in patients with severe asthma.

Objectives: Because dysregulated expression of ADAM33 can contribute to disease pathogenesis, we characterized the mechanism or mechanisms that control its transcription and investigated ADAM33 expression in bronchial biopsy specimens and brushings from healthy and asthmatic subjects.

Methods: The ADAM33 promoter and CpG island methylation were analyzed by using bioinformatics, luciferase reporters, and bisulfite sequencing of genomic DNA. Epithelial-mesenchymal transition was induced by using TGF-b1. ADAM33 mRNA was scrutinized in bronchial biopsy specimens and brushings by using reverse transcriptase–quantitative polymerase chain reaction, melt-curve analysis, and direct sequencing.

Results: The predicted ADAM33 promoter (2550 to 187) had promoter transcriptional activity. Bisulfite sequencing showed that the predicted promoter CpG island (2362 to 180) was hypermethylated in epithelial cells but hypomethylated in ADAM33-expressing fibroblasts.

Treatment of epithelial cells with 5-aza-deoxycytidine caused demethylation of the CpG island and induced ADAM33 expression. In contrast, phenotypic transformation of epithelial cells through a TGF-b–induced epithelial mesenchymal transition was insufficient to induce ADAM33 expression. ADAM33 mRNA was confirmed in bronchial biopsy specimens, but no validated signal was detected in bronchial brushings from healthy or asthmatic subjects.

Conclusion: The ADAM33 gene contains a regulatory CpG island within its promoter, the methylation status of which tightly controls its expression in a cell type–specific manner. ADAM33 repression is a stable feature of airway epithelial cells, irrespective of disease. (J Allergy Clin Immunol 2008;121:1393-9.)
promoter, cpg island, methylation, expression, adam33, epithelial-mesenchymal transition
0091-6749
1393-1399
Yang, Youwen
88415c3b-4613-4730-be20-8423ccae345a
Haitchi, Hans Michael
68dadb29-305d-4236-884f-e9c93f4d78fe
Cakebread, Julie
51e36732-a222-4cc3-ab7f-b89e60a78fb5
Sammut, David
0c7ac14b-6c2e-4d45-85a0-327703d1afd0
Harvey, Anna
0fbcf100-4a45-4a0a-8672-9924c60818f7
Powell, Robert M.
884d6594-3f50-4be5-9516-d64b29dad63d
Holloway, John W.
4bbd77e6-c095-445d-a36b-a50a72f6fe1a
Howarth, Peter
ff19c8c4-86b0-4a88-8f76-b3d87f142a21
Holgate, Stephen T.
2e7c17a9-6796-436e-8772-1fe6d2ac5edc
Davies, Donna E.
7de8fdc7-3640-4e3a-aa91-d0e03f990c38
Yang, Youwen
88415c3b-4613-4730-be20-8423ccae345a
Haitchi, Hans Michael
68dadb29-305d-4236-884f-e9c93f4d78fe
Cakebread, Julie
51e36732-a222-4cc3-ab7f-b89e60a78fb5
Sammut, David
0c7ac14b-6c2e-4d45-85a0-327703d1afd0
Harvey, Anna
0fbcf100-4a45-4a0a-8672-9924c60818f7
Powell, Robert M.
884d6594-3f50-4be5-9516-d64b29dad63d
Holloway, John W.
4bbd77e6-c095-445d-a36b-a50a72f6fe1a
Howarth, Peter
ff19c8c4-86b0-4a88-8f76-b3d87f142a21
Holgate, Stephen T.
2e7c17a9-6796-436e-8772-1fe6d2ac5edc
Davies, Donna E.
7de8fdc7-3640-4e3a-aa91-d0e03f990c38

Yang, Youwen, Haitchi, Hans Michael, Cakebread, Julie, Sammut, David, Harvey, Anna, Powell, Robert M., Holloway, John W., Howarth, Peter, Holgate, Stephen T. and Davies, Donna E. (2008) Epigenetic mechanisms silence a disintegrin and metalloprotease 33 expression in bronchial epithelial cells. Journal of Allergy and Clinical Immunology, 121 (6), 1393-1399. (doi:10.1016/j.jaci.2008.02.031).

Record type: Article

Abstract

Background: A disintegrin and metalloprotease 33 (ADAM33) polymorphism is strongly associated with asthma and bronchial hyperresponsiveness.
Although considered to be a mesenchymal cell–specific gene, recent reports have suggested epithelial expression of ADAM33 in patients with severe asthma.

Objectives: Because dysregulated expression of ADAM33 can contribute to disease pathogenesis, we characterized the mechanism or mechanisms that control its transcription and investigated ADAM33 expression in bronchial biopsy specimens and brushings from healthy and asthmatic subjects.

Methods: The ADAM33 promoter and CpG island methylation were analyzed by using bioinformatics, luciferase reporters, and bisulfite sequencing of genomic DNA. Epithelial-mesenchymal transition was induced by using TGF-b1. ADAM33 mRNA was scrutinized in bronchial biopsy specimens and brushings by using reverse transcriptase–quantitative polymerase chain reaction, melt-curve analysis, and direct sequencing.

Results: The predicted ADAM33 promoter (2550 to 187) had promoter transcriptional activity. Bisulfite sequencing showed that the predicted promoter CpG island (2362 to 180) was hypermethylated in epithelial cells but hypomethylated in ADAM33-expressing fibroblasts.

Treatment of epithelial cells with 5-aza-deoxycytidine caused demethylation of the CpG island and induced ADAM33 expression. In contrast, phenotypic transformation of epithelial cells through a TGF-b–induced epithelial mesenchymal transition was insufficient to induce ADAM33 expression. ADAM33 mRNA was confirmed in bronchial biopsy specimens, but no validated signal was detected in bronchial brushings from healthy or asthmatic subjects.

Conclusion: The ADAM33 gene contains a regulatory CpG island within its promoter, the methylation status of which tightly controls its expression in a cell type–specific manner. ADAM33 repression is a stable feature of airway epithelial cells, irrespective of disease. (J Allergy Clin Immunol 2008;121:1393-9.)

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More information

Published date: June 2008
Keywords: promoter, cpg island, methylation, expression, adam33, epithelial-mesenchymal transition
Organisations: Infection Inflammation & Immunity

Identifiers

Local EPrints ID: 73670
URI: http://eprints.soton.ac.uk/id/eprint/73670
DOI: doi:10.1016/j.jaci.2008.02.031
ISSN: 0091-6749
PURE UUID: b35ff4b5-bc43-413e-8e53-c62a7da855a0
ORCID for Hans Michael Haitchi: ORCID iD orcid.org/0000-0001-8603-302X
ORCID for John W. Holloway: ORCID iD orcid.org/0000-0001-9998-0464
ORCID for Donna E. Davies: ORCID iD orcid.org/0000-0002-5117-2991

Catalogue record

Date deposited: 10 Mar 2010
Last modified: 14 Mar 2024 02:47

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Contributors

Author: Youwen Yang
Author: Hans Michael Haitchi ORCID iD
Author: Julie Cakebread
Author: David Sammut
Author: Anna Harvey
Author: Robert M. Powell
Author: John W. Holloway ORCID iD
Author: Peter Howarth
Author: Stephen T. Holgate
Author: Donna E. Davies ORCID iD

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