The "long pentraxins" are an emerging family of genes that have conserved in their carboxy-terminal halves a pentraxin domain homologous to the prototypical acute phase protein pentraxins (C-reactive protein and serum amyloid P component) and acquired novel amino-terminal domains. In this report, a genomic fragment of 1371 nucleotides from the human "long pentraxin" gene PTX3 is characterized as a promoter on tumor necrosis factor- (TNF) and interleukin (IL)-1 exposure in transfected 8387 human fibroblasts by chloramphenicol acetyltransferase and RNase protection assays. In the same cells, the PTX3 promoter does not respond to IL-6 stimulation. Furthermore, IL-1 and TNF responsiveness is not seen in the Hep 3B hepatoma cell line. The minimal promoter contains one NF-B element which is shown to be necessary for induction and able to bind p50 homodimers and p65 heterodimers but not c-Rel. Mutants in this site lose the ability to bind NF-B proteins and to respond to TNF and IL-1 in functional assays. Sp1- and AP-1 binding sites lying in proximity to the NF-B site do not seem to play a major role for cytokine responsiveness. Finally, cotransfection experiments with expression vectors validate that the natural promoter contains a functional NF-B site.

Characterization of the promoter for the human long pentraxin PTX3 : role of NF-kappaB in tumor necrosis factor-alfa and interleukin-1beta regulation / A. Basile, A. Sica, E. D'Aniello, F. Breviario, G. Garrido, M. Castellano, A. Mantovani, M. Introna. - In: THE JOURNAL OF BIOLOGICAL CHEMISTRY. - ISSN 0021-9258. - 272:13(1997 Mar 28), pp. 8172-8178. [10.1074/jbc.272.13.8172]

Characterization of the promoter for the human long pentraxin PTX3 : role of NF-kappaB in tumor necrosis factor-alfa and interleukin-1beta regulation

A. Basile
Primo
;
A. Mantovani
Penultimo
;
1997

Abstract

The "long pentraxins" are an emerging family of genes that have conserved in their carboxy-terminal halves a pentraxin domain homologous to the prototypical acute phase protein pentraxins (C-reactive protein and serum amyloid P component) and acquired novel amino-terminal domains. In this report, a genomic fragment of 1371 nucleotides from the human "long pentraxin" gene PTX3 is characterized as a promoter on tumor necrosis factor- (TNF) and interleukin (IL)-1 exposure in transfected 8387 human fibroblasts by chloramphenicol acetyltransferase and RNase protection assays. In the same cells, the PTX3 promoter does not respond to IL-6 stimulation. Furthermore, IL-1 and TNF responsiveness is not seen in the Hep 3B hepatoma cell line. The minimal promoter contains one NF-B element which is shown to be necessary for induction and able to bind p50 homodimers and p65 heterodimers but not c-Rel. Mutants in this site lose the ability to bind NF-B proteins and to respond to TNF and IL-1 in functional assays. Sp1- and AP-1 binding sites lying in proximity to the NF-B site do not seem to play a major role for cytokine responsiveness. Finally, cotransfection experiments with expression vectors validate that the natural promoter contains a functional NF-B site.
Settore MED/46 - Scienze Tecniche di Medicina di Laboratorio
28-mar-1997
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/19829
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