A variant form of the human Deleted in Malignant Brain Tumor 1 (DMBT1) gene shows increased expression in inflammatory bowel diseases and interacts with dimeric trefoil factor 3 (TFF3)
A variant form of the human Deleted in Malignant Brain Tumor 1 (DMBT1) gene shows increased expression in inflammatory bowel diseases and interacts with dimeric trefoil factor 3 (TFF3)
The protein deleted in malignant brain tumors (DMBT1) and the trefoil factor (TFF) proteins have all been proposed to have roles in epithelial cell growth and cell differentiation and shown to be up regulated in inflammatory bowel diseases. A panel of monoclonal antibodies was raised against human DMBT1(gp340). Analysis of lung washings and colon tissue extracts by Western blotting in the unreduced state, two antibodies (Hyb213-1 and Hyb213-6) reacted with a double band of 290 kDa in lung lavage. Hyb213-6, in addition, reacted against a double band of 270 kDa in colon extract while Hyb213-1 showed no reaction. Hyb213-6 showed strong cytoplasmic staining in epithelial cells of both the small and large intestine whereas no staining was seen with Hyb213-1. The number of DMBT1(gp340) positive epithelial cells, stained with Hyb213-6, was significantly up regulated in inflammatory colon tissue sections from patients with ulcerative colitis (p<0.0001) and Crohn's disease (p?=?0.006) compared to normal colon tissue. Immunohistochemical analysis of trefoil factor TFF1, 2 and 3 showed that TFF1 and 3 localized to goblet cells in both normal colon tissue and in tissue from patients with ulcerative colitis or Crohn's disease. No staining for TFF2 was seen in goblet cells in normal colon tissue whereas the majority of tissue sections in ulcerative colitis and Crohn's disease showed sparse and scattered TFF2 positive goblet cells. DMBT1 and TFF proteins did therefore not co-localize in the same cells but localized in adjacent cells in the colon. The interaction between DMBT1(gp340) and trefoil TFFs proteins was investigated using an ELISA assay. DMBT1(gp340) bound to solid-phase bound recombinant dimeric TFF3 in a calcium dependent manner (p<0.0001) but did not bind to recombinant forms of monomeric TFF3, TFF2 or glycosylated TFF2. This implies a role for DMBT1 and TFF3 together in inflammatory bowel disease.
e64441
Madsen, Jens
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Sorensen, Grith Lykke
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Nielsen, Ole
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Tornoe, Ida
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Thim, Lars
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Fenger, Claus
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Mollenhauer, Jan
7280cbd1-7e49-4f84-badf-ab560b782750
Holmskov, Uffe
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15 May 2013
Madsen, Jens
b5d8ae35-00ac-4d19-930e-d8ddec497359
Sorensen, Grith Lykke
fa12b2d9-d771-43ce-8264-f163edbb2464
Nielsen, Ole
7656790a-07fc-44bc-bb1e-e8507cb3b30e
Tornoe, Ida
1843a350-ebeb-409a-92a0-c581fb9fa449
Thim, Lars
9fb8ab9c-7da2-4d3b-ab7d-c98874c52118
Fenger, Claus
4f869489-09c5-47f7-a5fb-c5cda1ca82ae
Mollenhauer, Jan
7280cbd1-7e49-4f84-badf-ab560b782750
Holmskov, Uffe
8a55aecd-694c-4d61-849b-9cf32da8ba39
Madsen, Jens, Sorensen, Grith Lykke, Nielsen, Ole, Tornoe, Ida, Thim, Lars, Fenger, Claus, Mollenhauer, Jan and Holmskov, Uffe
(2013)
A variant form of the human Deleted in Malignant Brain Tumor 1 (DMBT1) gene shows increased expression in inflammatory bowel diseases and interacts with dimeric trefoil factor 3 (TFF3).
PLoS ONE, 8 (5), .
(doi:10.1371/journal.pone.0064441).
(PMID:23691218)
Abstract
The protein deleted in malignant brain tumors (DMBT1) and the trefoil factor (TFF) proteins have all been proposed to have roles in epithelial cell growth and cell differentiation and shown to be up regulated in inflammatory bowel diseases. A panel of monoclonal antibodies was raised against human DMBT1(gp340). Analysis of lung washings and colon tissue extracts by Western blotting in the unreduced state, two antibodies (Hyb213-1 and Hyb213-6) reacted with a double band of 290 kDa in lung lavage. Hyb213-6, in addition, reacted against a double band of 270 kDa in colon extract while Hyb213-1 showed no reaction. Hyb213-6 showed strong cytoplasmic staining in epithelial cells of both the small and large intestine whereas no staining was seen with Hyb213-1. The number of DMBT1(gp340) positive epithelial cells, stained with Hyb213-6, was significantly up regulated in inflammatory colon tissue sections from patients with ulcerative colitis (p<0.0001) and Crohn's disease (p?=?0.006) compared to normal colon tissue. Immunohistochemical analysis of trefoil factor TFF1, 2 and 3 showed that TFF1 and 3 localized to goblet cells in both normal colon tissue and in tissue from patients with ulcerative colitis or Crohn's disease. No staining for TFF2 was seen in goblet cells in normal colon tissue whereas the majority of tissue sections in ulcerative colitis and Crohn's disease showed sparse and scattered TFF2 positive goblet cells. DMBT1 and TFF proteins did therefore not co-localize in the same cells but localized in adjacent cells in the colon. The interaction between DMBT1(gp340) and trefoil TFFs proteins was investigated using an ELISA assay. DMBT1(gp340) bound to solid-phase bound recombinant dimeric TFF3 in a calcium dependent manner (p<0.0001) but did not bind to recombinant forms of monomeric TFF3, TFF2 or glycosylated TFF2. This implies a role for DMBT1 and TFF3 together in inflammatory bowel disease.
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MADSEN - PLoS One - A variant form of the human deleted....pdf
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Published date: 15 May 2013
Organisations:
Clinical & Experimental Sciences
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Local EPrints ID: 351204
URI: http://eprints.soton.ac.uk/id/eprint/351204
ISSN: 1932-6203
PURE UUID: 8ec13494-d0b7-4da2-8318-cc6540b31c90
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Date deposited: 16 Apr 2013 11:35
Last modified: 15 Mar 2024 03:29
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Author:
Jens Madsen
Author:
Grith Lykke Sorensen
Author:
Ole Nielsen
Author:
Ida Tornoe
Author:
Lars Thim
Author:
Claus Fenger
Author:
Jan Mollenhauer
Author:
Uffe Holmskov
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