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Query: UMLS:C0003615 (
appendicitis
)
4,439
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The appendix contains abundant lymphoid tissue and is constantly exposed to gut flora. When completed at a young age,
appendicitis
followed by appendectomy (AA) prevents or significantly ameliorates Inflammatory Bowel Diseases (IBDs) in later life. Inflammatory bowel disease comprises Crohn's disease and ulcerative colitis. Our murine AA model is the only existing experimental model of AA. In our unique model, AA performed in the most proximal colon limits colitis pathology in the most distal colon by curbing T-helper 17 cell activity, diminishing autophagy, modulating interferon activity-associated molecules, and suppressing endothelin vaso-activity-mediated immunopathology. In the research presented in this paper, we have examined the role of chemokines in colitis pathology with our murine AA model. Chemokines are a family of small cytokines with four conserved cysteine residues. Chemokines induce chemotaxis in adjacent cells with corresponding receptors. All 40 known chemokine genes and 24 chemokine receptor genes were examined for gene expression levels in distal colons three days post-AA and 28 days post-AA. At 28 days post-AA, the chemokine gene
CCL5
was significantly upregulated. Furthermore, Gene Set Enrichment Analysis (GSEA) showed upregulation of seven
CCL5
-associated gene-sets 28 days post-AA in contrast to just one gene-set downregulated at the same time-point. The chemokine gene
CXCL11
was significantly upregulated three days post-AA and 28 days post-AA. Evaluation using GSEA showed upregulation of six
CXCL11
-associated gene sets but no downregulation of any gene set. At 28 days post-AA,
CCL17
gene expression was significantly downregulated. There was no expression of any chemokine receptor gene three days post-AA, but
CCR10
was the only chemokine receptor gene that displayed differential gene expression (upregulation) 28 days post-AA. No
CCR10
-associated gene set was upregulated in GSEA in contrast to one downregulated gene set. Our analysis resulted in identifying three new therapeutic targets towards ameliorating colitis: CCL5, CXCL11, and
CCL17
. While CCL5 and CXCL11 are good therapeutic chemokine candidates to be exogenously administered,
CCL17
is a good candidate chemokine to competitively inhibit or limit colitis pathology.
...
PMID:The Role of Specific Chemokines in the Amelioration of Colitis by Appendicitis and Appendectomy. 3003 25
The appendix contains copious lymphoid tissue and is constantly exposed to gut flora.
Appendicitis
followed by appendectomy (AA), when done at a young age, prevents or significantly ameliorates inflammatory bowel diseases (IBDs) in later life. Inflammatory bowel disease comprises Crohn's disease and ulcerative colitis. Our unique murine AA model is the only existing experimental model of AA. Herein, the appendiceal pathology closely resembles the pathological features of human
appendicitis
. Our AA model protects against experimental colitis in an age-, bacteria- and antigen-dependent manner.
Appendicitis
-appendectomy performed in the most proximal colon curbs T helper 17 (Th17) cell activity, diminishes autophagy, modulates interferon activity-associated molecules, and suppresses endothelin vasoactivity-mediated immunopathology in the most distal colon. These changes induced by AA contribute to limiting colitis pathology. Manipulating and modulating various aspects of these pathways, pathophysiology, and molecular interactions will assist the development of novel therapeutic options to manage IBD. Competitive inhibition of the Th17 cell recruitment factor CCL20 or the chemokine
CCL17
with antibodies, combinatorial peptides, or small molecules may limit colitic pathology. The chemokines CCL5 and CXCL11 could be investigated as potential therapies. Inhibition of the autophagy-associated molecules VPS15, LAMP2, LC3A, XBP1, or ULK1 may decrease colitic pathology. Curtailing endothelin-activity may decrease colitic impact. The antiproliferative, immunomodulatory molecules IFIT1, IFIT2, IFIT3, and IFI44 may have direct therapeutic value in ameliorating colitis. The molecules IRF4, IRF8, IRF2BP1, IFRD1, and IFRD2 are potentially good target molecules to competitively inhibit towards curbing colitis.
...
PMID:Identification of New Potential Therapies for Colitis Amelioration Using an Appendicitis-Appendectomy Model. 3032 49
