Abstract

Pancreatitis is an important clinical problem for which treatment is still largely supportive. We have identified the transcription factor NF-KappaB as a molecule that is activated early in the disease contributing to the initiation of an inflammatory cascade.
Specific aim #1 is to determine the mechanisms and role of NF-KappaB activation in acute pancreatitis. We will extend our understanding of the significance of NF-KappaB activation by directly activating and inhibiting NF-KappaB within the pancreas using adenoviral expression of active and dominant negative subunits. We hypothesize that NF-KappaB plays a pro-inflammatory role and specifically drives expression of mob-1 and gro-alpha, two important chemokines. We will identify other genes activated by NF-KappaB within pancreatic acinar cells using a combination of adenovirus mediated delivery of an active subunit and oligonucleotide-directed microarray analysis. We will also test the hypothesis that trypsin activation is able to activate NF-KappaB within acinar cells using an adenoviral approach to directly active trypsin within acinar cells.
Specific aim #2 is to identify the genes that are induced early in the course of acute pancreatitis. To further identify new molecules that are important in acute pancreatitis, we will utilize oligonucleotide directed microarrays to profile gene expression in rapid onset models of acute pancreatitis. We will specifically focus our search on genes for transcription factors and inflammatory mediators, as these may become targets of therapy for the disease.
Specific aim #3 is to determine the mechanisms and role of the transcription factor EGR-1 in acute pancreatitis. Preliminary experiments have shown that the transcription factor EGR-1 is highly induced early in the course of caerulein induced acute pancreatitis. EGR-1 plays an important role in other inflammatory diseases and is a know regulator of tissue factor (TF). We will determine if this transcription factor is also induced in other models of acute pancreatitis, investigate the cellular mechanisms involved in its regulation, and determine the relationship between its activation and the severity of acute pancreatitis. We will also test the hypothesis that EGR-1 drives expression of TF in the pancreas, and identify other targets of this important transcription factor.
Specific aim #4 is to determine the roles of pro-inflammatory effectors, mob-1, gro-alpha, TF and CGRP in acute pancreatitis. Of the pro-inflammatory molecules identified as up-regulated after treatment of animals with high concentrations of caerulein, we have selected these four as being especially likely to contribute to the severity of acute pancreatitis based upon their known functions in other diseases. Specifically, we will test the hypothesis that mob-1 and gro-alpha are important for chemoattraction of T-cells and neutrophils respectively, that TF is important for initiating blood coagulation in the pancreas, and that CGRP expression in acinar cells contributes to alterations in pancreatic and systemic blood flow.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
7R01DK052067-07
Application #
6797193
Study Section
General Medicine A Subcommittee 2 (GMA)
Program Officer
Serrano, Jose
Project Start
1998-05-10
Project End
2006-07-31
Budget Start
2004-09-15
Budget End
2006-07-31
Support Year
7
Fiscal Year
2004
Total Cost
$255,663
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Biology
Type
Other Domestic Higher Education
DUNS #
800772139
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Gomez-Chou, Sobeyda B; Swidnicka-Siergiejko, Agnieszka Katarzyna; Badi, Niharika et al. (2017) Lipocalin-2 Promotes Pancreatic Ductal Adenocarcinoma by Regulating Inflammation in the Tumor Microenvironment. Cancer Res 77:2647-2660
Swidnicka-Siergiejko, A K; Gomez-Chou, S B; Cruz-Monserrate, Z et al. (2017) Chronic inflammation initiates multiple forms of K-Ras-independent mouse pancreatic cancer in the absence of TP53. Oncogene 36:3149-3158
Gaziova, Ivana; Jackson, Daniel; Boor, Paul J et al. (2016) The MET Receptor Tyrosine Kinase Confers Repair of Murine Pancreatic Acinar Cells following Acute and Chronic Injury. PLoS One 11:e0165485
Logsdon, Craig D; Lu, Weiqin (2016) The Significance of Ras Activity in Pancreatic Cancer Initiation. Int J Biol Sci 12:338-46
Logsdon, Craig D; Arumugam, Thiruvengadam; Ramachandran, Vijaya (2015) Animal Models of Gastrointestinal and Liver Diseases. The difficulty of animal modeling of pancreatic cancer for preclinical evaluation of therapeutics. Am J Physiol Gastrointest Liver Physiol 309:G283-91
Fu, Yong; Cruz-Monserrate, Zobeida; Helen Lin, H et al. (2015) Ductal activation of oncogenic KRAS alone induces sarcomatoid phenotype. Sci Rep 5:13347
Cruz-Monserrate, Zobeida; Roland, Christina L; Deng, Defeng et al. (2014) Targeting pancreatic ductal adenocarcinoma acidic microenvironment. Sci Rep 4:4410
Huang, H; Daniluk, J; Liu, Y et al. (2014) Oncogenic K-Ras requires activation for enhanced activity. Oncogene 33:532-5
Roland, Christina L; Arumugam, Thiruvengadam; Deng, Defeng et al. (2014) Cell surface lactate receptor GPR81 is crucial for cancer cell survival. Cancer Res 74:5301-10
Charo, Chantale; Holla, Vijaykumar; Arumugam, Thiruvengadam et al. (2013) Prostaglandin E2 regulates pancreatic stellate cell activity via the EP4 receptor. Pancreas 42:467-74

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