Journal ArticleDOI
Interleukin-1 inhibits glucose-modulated insulin and glucagon secretion in rat islet monolayer cultures.
TLDR
IL-1 causes a reversible decrease in the insulin content of islet cells and an irreversible decrease in glucagon content, and these actions of IL-1 do not appear to account for the beta-cell-specific destruction of islets characteristic of type 1 diabetes.Abstract:
Recent observations suggest a role for interleukin-1 (IL-1), a polypeptide product of macrophage/monocytic cells, in the immune-mediated destruction of pancreatic islet beta-cells observed in type 1 diabetes. In this study, we investigated the effects of IL-1 on both alpha- and beta-cell secretory functions in rat islet cell monolayer cultures. Insulin release was 97% inhibited after 6 h of incubation in RPMI-1640 medium (11 mM glucose) containing 1 U/ml IL-1 and 96% inhibited after 24 h of incubation in medium containing 0.1 U/ml IL-1. The cell content of insulin in the monolayers was decreased by 66% (P less than 0.01) after 4 days of incubation in 10 U/ml IL-1; however, after a further 8-day incubation in IL-1-free medium, cell insulin content recovered fully. In contrast, cell glucagon content was decreased by 77% (P less than 0.001) after 4 days of incubation in 10 U/ml IL-1 and did not recover after a further 8-day incubation in IL-1-free medium. After an 18-h preincubation in medium with 0.1 and 1 U/ml IL-1, insulin release responses to 16.7 mM glucose were abolished in 4-h incubations, whereas responses to 0.1 mM 3-isobutyl-1-methylxanthine were normal, and after a further 2 and 5 days of incubation in IL-1-free medium, insulin responses to 16.7 mM glucose recovered fully. Similarly, the inhibitory effect of 16.7 mM glucose on glucagon release was lost after an 18-h preincubation in 0.1 and 1 U/ml IL-1, and did not recover fully after 2 and 5 days in IL-1-free medium, whereas the stimulatory effect of 3-isobutyl-1-methylxanthine on glucagon release was not affected by IL-1. We conclude that 1) IL-1 inhibits glucose-dependent and not cAMP-dependent mechanisms of insulin and glucagon release; 2) inhibition of glucose-stimulated insulin release by IL-1 is reversible, whereas the effect on glucose-modulated glucagon release is not; and 3) IL-1 causes a reversible decrease in the insulin content of islet cells and an irreversible decrease in glucagon content. These actions of IL-1 do not appear to account for the beta-cell-specific destruction of islets characteristic of type 1 diabetes.read more
Citations
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Journal ArticleDOI
A Taql polymorphism in the human interleukin-1β (IL-1β) gene correlates with IL-1β secretion in vitro
TL;DR: It is concluded that the 13.4 kb allele represents an IL‐1β‘high‐secretor’ phenotype, that the observed RFLP may be a genetic susceptibility marker for IDDM in non‐DR3 and non-DR4 individuals and that high IL‐ 1β secretory capacity may be an pathogenic factor for ID DM in these patients.
Journal ArticleDOI
The role of interleukin-1 in the pathogenesis of IDDM.
TL;DR: "It is perhaps today, where a certain underevaluation well, even disrespect o f scientific research is growing useful again and again to refer to the fact how well suited the discovery of insulin is to demonstrate that unprejudiced scientific research sooner or later will be fruitful also to clinical practice".
Journal ArticleDOI
Autoimmune diabetes mellitus in the BB rat.
Book ChapterDOI
Cytokine and free radicals as effector molecules in the destruction of pancreatic beta cells.
Thomas Mandrup-Poulsen,S. Helqvist,Lise Wogensen,J. Mølvig,Flemming Pociot,Jesper Johannesen,J Nerup +6 more
Journal ArticleDOI
On the pathogenesis of IDDM
Jørn Nerup,T. Mandrap-Poulsen,S. Helqvist,Henrik U. Andersen,Flemming Pociot,Jesper I. Reimers,B. G. Cuartero,Allan E. Karlsen,Ulla Bjerre,T. Lorenzen +9 more
TL;DR: A model of the pathogenesis of insulin-dependent diabetes mellitus is proposed: in a cascade-like fashion efficient antigen presentation, unbalanced cytokine, secretion and poor beta-cell defence result in beta- cell destruction by toxic free radicals produced by the beta cells themselves.
References
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Journal ArticleDOI
Coated charcoal immunoassay of insulin.
TL;DR: The procedure here described yields a straight line graph when insulin added is plotted against insulin recovered, and makes simpler and more rapid the immunoassay of insulin in biologic fluids, using radioisotope dilution with 131I-insulin and "biopsy" of the insulin pool by antibody to insulin.
Journal ArticleDOI
Breeding of a non-obese, diabetic strain of mice.
Susumu Makino,Kikuko Kunimoto,Yoshihiro Muraoka,Yukio Mizushima,Ken Katagiri,Yoshihiro Tochino +5 more
TL;DR: The nod mouse may be a useful animal model for investigating the human juvenile type diabetes because of the high frequency of lymphocyte infiltration around and/or into the Langerhans' islet.
Journal ArticleDOI
Pathologic Anatomy of the Pancreas in Juvenile Diabetes Mellitus
TL;DR: Quantitative study of insular tissue has revealed that the number of B cells is greatly diminished in Patients with acute juvenile diabetes from the time of clinical onset of the disease, and may be assumed that during the preclinical phase of juvenile diabetes, an extrapancreatic factor has exerted a strong stimulant action on theinsular tissue.
Journal ArticleDOI
Cytotoxicity of human pI 7 interleukin-1 for pancreatic islets of Langerhans.
Klaus Bendtzen,Thomas Mandrup-Poulsen,Jørn Nerup,Jens Høiriis Nielsen,Charles A. Dinarello,M. Svenson +5 more
TL;DR: Monocyte-derived pI 7 IL-1 may contribute to islet cell damage and therefore to the development of insulin-dependent diabetes mellitus.
Journal ArticleDOI
Destruction of Rat Islet Cell Monolayers by Cytokines: Synergistic Interactions of Interferon-γ, Tumor Necrosis Factor, Lymphotoxin, and Interleukin 1
TL;DR: Results indicate that the cytokine products of mononuclear cells of the immune system, IFN-γ, TNF, LT, and IL-1 have strong synergistic cytotoxic effects on islet cells and therefore may act as direct chemical mediators of islet β-cell destruction in type I (insulin-dependent) diabetes.