In CD4+ T-Cell-Induced Diabetes, Macrophages Are the Final Effector Cells that Mediate Islet β-Cell Killing

In an accompanying paper, we find specific localization of diabetogenic T cells only to islets of Langerhans bearing the specific antigen. Instrumental in the specific localization was the presence of intraislet dendritic cells bearing the β-cell-peptide-MHC complex. Here, we report that the entry of diabetogenic CD4 T cells very rapidly triggered inflammatory gene expression changes in islets and vessels by up-regulating chemokines and adhesion molecules. Vascular cell adhesion molecule-1 (VCAM-1) expression was notable in blood vessels, as was intercellular adhesion molecule-1 (ICAM-1). ICAM-1 was also found on β-cells. These expression changes induced the entry of nonspecific T cells that otherwise did not localize to the islets. In contrast to the entry of diabetogenic CD4 T cells, the entrance of nonspecific T cells required a chemokine response and VCAM-1 expression by the islets. IFN-γ was important for the early gene expression changes in the islets. By microarray analysis, we detected up-regulation of a group of IFNinducible genes as early as 8 h post-T-cell transfer. These studies establish that entry of diabetogenic T cells induces a state of receptivity of islets to subsequent immunological insults.T-cell migration | autoimmunity | type 1 diabetes T he entry of T cells to tissues containing antigen-presenting cells (APCs) bearing their protein antigen leads to an inflammatory response. Within a few days, specific cells are difficult to distinguish among the many inflammatory cells made up of various leukocytes: macrophages, dendritic cells (DC), natural killer cells, and neutrophils. These events have been extensively examined, mainly in the case of the central nervous system (CNS) autoreactivity, where activated myelin antigen-specific T cells migrate to the CNS, leading to autoimmune encephalomyelitis (1). Flow of specific and nonspecific T cells into the capillaries of the cerebral vasculature and adherence to endothelial cells has been shown, particularly after inflammation (2-4). The retention of the circulating autoreactive T cells that allows the passage across the blood-brain barrier depends on the presence of class II MHC bearing APC within the perivascular or Virchow-Robin space (5, 6). After specific T cells are in play, they dictate the migration of nonspecific T cells into the CNS (4, 6, 7). Moreover, a random nonspecific entry and exit of T cells has been described in the mouse and rat (4,(8)(9)(10).In the case of autoimmune diabetes, activated diabetogenic CD4 T cells localized only to islets bearing their cognate antigen; thus, in mice bearing hen-egg white lysozyme (HEL) under the insulin promoter (IP-HEL), T cells bearing a transgenic T-cell receptor for HEL peptides only localized to islets bearing HEL. The same was true for the localization of diabetogenic T cells in the NOD model of spontaneous diabetes (11). In both cases, the intraislet DCs were instrumental in the presentation of the peptide-MHC complexes and in the localization of the CD4 T cells. We did not obtain evidence t...

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“…For experiments using STZ, a dose of 50 mg/kg i.p. was administered for two consecutive days (24). PTx treatment was performed as in ref.…”

Section: Methodsmentioning

confidence: 99%

Entry of diabetogenic T cells into islets induces changes that lead to amplification of the cellular response

Calderon

Carrero

Miller

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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“…ROS mediates apoptosis [49]. The importance of proinflammatory macrophages in T1D was demonstrated by clodronate depletion of macrophages in diabetogenic CD4 + T-cells in NOD mice that inhibit activation and differentiation of monocytes into effector macrophage by reducing the macrophage islet β-cell lytic capacity and prevents severe diabetes development [98]. Entry of the macrophages into the T1D islets is dependent on complement receptor 3 interactions as complement 3 antibody inhibition markedly delay disease development [99].…”

Section: Involvement Of Macrophages In Type 1 Diabetesmentioning

confidence: 99%

Polarization of Macrophages in Metabolic Diseases

Rosendah¹

2015

J Clin Cell Immunol

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Monocytes originate from progenitor cells in the bone marrow and traffic via the bloodstream to peripheral tissues. During both homeostasis and in responses to clear pathogens, circulating monocytes leave the bloodstream and migrate into tissues where they, following exposure to local growth factors, pro-inflammatory cytokines and microbial products, differentiate into macrophage or dendritic cell sub-populations. Type 1 diabetes (T1D) is a disease characterised by the elimination of the insulin producing β-cells in the pancreatic tissue through activation mainly of the adaptive immune system. In metabolic diseases, i.e. obesity, Type 2 diabetes (T2D) and diabetic complications, inflammation is mostly driven by macrophages and has been shown pivotal for disease progression even when blood glucose levels are well controlled. This review describes some current ideas and trends regarding the monocyte and macrophage involvement and their polarization in metabolic diseases that might open up novel therapeutic areas for the growing diabetic population.

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“…Given the role of macrophages and islet inflammation in initiating T1D (Oschilewski et al 1985, Charlton et al 1988, Lee et al 1988a,b, Chung et al 1997, Jun et al 1999a,b, Calderon et al 2006, it seems plausible that hIAPP aggregates, via induction of islet inflammation, could be a trigger or accelerator of autoimmunity in T1D. Amyloid has not been thoroughly investigated in T1D pancreas, and the deficiency of IAPP (along with insulin) associated with beta cell loss makes development of extensive amyloid plaques in T1D seem unlikely.…”

Section: Could Iapp-induced Inflammation Play a Role Type 1 Diabetes?mentioning

confidence: 99%

IAPP and type 1 diabetes: implications for immunity, metabolism and islet transplants

Denroche

Verchere

2018

Journal of Molecular Endocrinology

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Islet amyloid polypeptide (IAPP), the main component of islet amyloid in type 2 diabetes and islet transplants, is now recognized as a contributor to beta cell dysfunction. Increasingly, evidence warrants its investigation in type 1 diabetes owing to both its immunomodulatory and metabolic actions. Autoreactive T cells to IAPP-derived epitopes have been described in humans, suggesting that IAPP is an islet autoantigen in type 1 diabetes. In addition, although aggregates of IAPP have not been implicated in type 1 diabetes, they are potent pro-inflammatory stimuli to innate immune cells, and thus, could influence autoimmunity. IAPP aggregates also occur rapidly in transplanted islets and likely contribute to islet transplant failure in type 1 diabetes through sterile inflammation. In addition, since type 1 diabetes is a disease of both insulin and IAPP deficiency, clinical trials have examined the potential benefits of IAPP replacement in type 1 diabetes with the injectable IAPP analogue, pramlintide. Pramlintide limits postprandial hyperglycemia by delaying gastric emptying and suppressing hyperglucagonemia, underlining the possible role of IAPP in postprandial glucose metabolism. Here, we review IAPP in the context of type 1 diabetes: from its potential involvement in type 1 diabetes pathogenesis, through its role in glucose metabolism and use of IAPP analogues as therapeutics, to its potential role in clinical islet transplant failure and considerations in this regard for future beta cell replacement strategies.

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In CD4+ T-Cell-Induced Diabetes, Macrophages Are the Final Effector Cells that Mediate Islet β-Cell Killing

Cited by 112 publications

References 48 publications

Entry of diabetogenic T cells into islets induces changes that lead to amplification of the cellular response

Entry of diabetogenic T cells into islets induces changes that lead to amplification of the cellular response

Polarization of Macrophages in Metabolic Diseases

IAPP and type 1 diabetes: implications for immunity, metabolism and islet transplants

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