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Literature DB >> 18718526

Commonalities of genetic resistance to spontaneous autoimmune and free radical--mediated diabetes.

Jing Chen¹, Ying Lu, Chul-Ho Lee, Renhua Li, Edward H Leiter, Clayton E Mathews.

Abstract

ALR/Lt, a NOD-related mouse strain, was selected for resistance to alloxan free radical-mediated diabetes (ALD). Despite extensive genomic identity with NOD (>70%), ALR mice display strong resistance to autoimmune type 1 diabetes (T1D) due to both an unusual elevation in systemic antioxidant defenses and a reduction in cellular ROS production that extends to the beta cell level. Reciprocal backcross to NOD previously linked the ALR-derived T1D resistance to Chr. 3, 8, and 17 as well as to the ALR mt-Nd2(a) allele encoded by the mitochondrial genome (mtDNA). To determine whether any of the ALR-derived loci protecting against T1D also protected against ALD, 296 six-week-old F2 mice from reciprocal outcrosses were alloxan-treated and assessed for diabetes onset, and a genome-wide scan (GWS) was conducted. GWS linked mt-Nd2 as well as three nuclear loci with alloxan-induced diabetes. A dominant ALR-derived ALD resistance locus on Chr. 8 colocalized with the ALR-derived T1D resistance locus identified in the previous backcross analysis. In contrast, whereas ALR contributed a novel T1D resistance locus on Chr. 3 marked by Susp, a more proximal ALR-derived region marked by Il-2 contributed ALD susceptibility, not resistance. In addition, a locus was mapped on Chr. 2, where heterozygosity provided heightened susceptibility. Tests for alloxan sensitivity in ALR conplastic mice encoding the NOD mt-Nd2(c) allele and NOD mice congenic for the protective Chr. 8 locus supported our mapping results. Alloxan sensitivity was increased in ALR.mt(NOD) mice, whereas it was decreased by congenic introduction of ALR genome on Chr. 8 into NOD. These data demonstrate both similarities and differences in the genetic control of T1D versus ROS-induced diabetes.

Entities: CellLine Chemical Disease Gene Mutation Species

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Year: 2008 PMID： 18718526 PMCID： PMC2872108 DOI： 10.1016/j.freeradbiomed.2008.07.020

Source DB: PubMed Journal: Free Radic Biol Med ISSN： 0891-5849 Impact factor: 7.376

65 in total

1. An inhibitor of inducible nitric oxide synthase and scavenger of peroxynitrite prevents diabetes development in NOD mice.

Authors: W L Suarez-Pinzon; J G Mabley; K Strynadka; R F Power; C Szabó; A Rabinovitch
Journal: J Autoimmun Date: 2001-06 Impact factor: 7.094

2. Interleukin-2 gene variation impairs regulatory T cell function and causes autoimmunity.

Authors: Jun Yamanouchi; Dan Rainbow; Pau Serra; Sarah Howlett; Kara Hunter; Valerie E S Garner; Andrea Gonzalez-Munoz; Jan Clark; Riitta Veijola; Rose Cubbon; Show-Ling Chen; Raymond Rosa; Anne Marie Cumiskey; David V Serreze; Simon Gregory; Jane Rogers; Paul A Lyons; Barry Healy; Luc J Smink; John A Todd; Laurence B Peterson; Linda S Wicker; Pere Santamaria
Journal: Nat Genet Date: 2007-02-04 Impact factor: 38.330

3. COX-2 inhibition prevents insulin-dependent diabetes in low-dose streptozotocin-treated mice.

Authors: T Tabatabaie; A M Waldon; J M Jacob; R A Floyd; Y Kotake
Journal: Biochem Biophys Res Commun Date: 2000-07-05 Impact factor: 3.575

4. Supplementation of N-acetylcysteine inhibits NFkappaB activation and protects against alloxan-induced diabetes in CD-1 mice.

Authors: E Ho; G Chen; T M Bray
Journal: FASEB J Date: 1999-10 Impact factor: 5.191

5. Nuclear and mitochondrial interaction involving mt-Nd2 leads to increased mitochondrial reactive oxygen species production.

Authors: Aaron M Gusdon; Tatyana V Votyakova; Ian J Reynolds; Clayton E Mathews
Journal: J Biol Chem Date: 2006-12-21 Impact factor: 5.157

6. Genetic control of neutrophil superoxide production in diabetes-resistant ALR/Lt mice.

Authors: Clayton E Mathews; Brian D Dunn; Michael O Hannigan; Chi-Kuang Huang; Edward H Leiter
Journal: Free Radic Biol Med Date: 2002-04-15 Impact factor: 7.376

7. Glutathione is implied in the control of 7-ketocholesterol-induced apoptosis, which is associated with radical oxygen species production.

Authors: G Lizard; S Gueldry; O Sordet; S Monier; A Athias; C Miguet; G Bessede; S Lemaire; E Solary; P Gambert
Journal: FASEB J Date: 1998-12 Impact factor: 5.191

8. Reactive oxygen intermediates in autoimmune islet cell destruction of the NOD mouse induced by peritoneal exudate cells (rich in macrophages) but not T cells.

Authors: F Horio; M Fukuda; H Katoh; M Petruzzelli; N Yano; C Rittershaus; S Bonner-Weir; M Hattori
Journal: Diabetologia Date: 1994-01 Impact factor: 10.122

9. Alpha-phenyl-tert-butylnitrone (PBN) inhibits NFkappaB activation offering protection against chemically induced diabetes.

Authors: E Ho; G Chen; T M Bray
Journal: Free Radic Biol Med Date: 2000-02-15 Impact factor: 7.376

10. Streptozocin- and alloxan-induced H2O2 generation and DNA fragmentation in pancreatic islets. H2O2 as mediator for DNA fragmentation.

Authors: N Takasu; I Komiya; T Asawa; Y Nagasawa; T Yamada
Journal: Diabetes Date: 1991-09 Impact factor: 9.461

9 in total

Review 1. Use of nonobese diabetic mice to understand human type 1 diabetes.

Authors: Terri C Thayer; S Brian Wilson; Clayton E Mathews
Journal: Endocrinol Metab Clin North Am Date: 2010-07-08 Impact factor: 4.741

Review 2. Comparative genetics: synergizing human and NOD mouse studies for identifying genetic causation of type 1 diabetes.

Authors: John P Driver; Yi-Guang Chen; Clayton E Mathews
Journal: Rev Diabet Stud Date: 2012-12-28

Commonalities of genetic resistance to spontaneous autoimmune and free radical--mediated diabetes.

1. An inhibitor of inducible nitric oxide synthase and scavenger of peroxynitrite prevents diabetes development in NOD mice.

2. Interleukin-2 gene variation impairs regulatory T cell function and causes autoimmunity.

3. COX-2 inhibition prevents insulin-dependent diabetes in low-dose streptozotocin-treated mice.

4. Supplementation of N-acetylcysteine inhibits NFkappaB activation and protects against alloxan-induced diabetes in CD-1 mice.

5. Nuclear and mitochondrial interaction involving mt-Nd2 leads to increased mitochondrial reactive oxygen species production.

6. Genetic control of neutrophil superoxide production in diabetes-resistant ALR/Lt mice.

7. Glutathione is implied in the control of 7-ketocholesterol-induced apoptosis, which is associated with radical oxygen species production.

8. Reactive oxygen intermediates in autoimmune islet cell destruction of the NOD mouse induced by peritoneal exudate cells (rich in macrophages) but not T cells.

9. Alpha-phenyl-tert-butylnitrone (PBN) inhibits NFkappaB activation offering protection against chemically induced diabetes.

10. Streptozocin- and alloxan-induced H2O2 generation and DNA fragmentation in pancreatic islets. H2O2 as mediator for DNA fragmentation.

Review 1. Use of nonobese diabetic mice to understand human type 1 diabetes.

Review 2. Comparative genetics: synergizing human and NOD mouse studies for identifying genetic causation of type 1 diabetes.

3. Is There a Role for Bioactive Lipids in the Pathobiology of Diabetes Mellitus?

Review 4. Mitochondrial Reactive Oxygen Species and Type 1 Diabetes.

5. NADPH oxidase deficiency regulates Th lineage commitment and modulates autoimmunity.

6. Association of the mt-ND2 5178A/C polymorphism with Parkinson's disease.

7. Mitochondrial polymorphisms in rat genetic models of hypertension.

Review 8. Role of increased ROS dissipation in prevention of T1D.

9. mt-Nd2(a) Modifies resistance against autoimmune type 1 diabetes in NOD mice at the level of the pancreatic β-cell.