Thymic self-antigens for the design of a negative/tolerogenic self-vaccination against type 1 diabetes

Geenen, Vincent; Mottet, Marie; Dardenne, Olivier; Kermani, Hamid; Martens, Henri; François, Jean-Marie; Galleni, Moreno; Hober, Didier; Rahmouni, Souad; Moutschen, Michel

doi:10.1016/j.coph.2010.04.005

Cited by 21 publications

(13 citation statements)

References 107 publications

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“…Ins2 was not expressed by MTE cells or was expressed at a very low level below the detection threshold of our RT-qPCR. The latter observation is not so surprising, since a very low degree of insulin gene transcription in healthy murine and human thymus had already been described and correlated to the poor tolerogenicity of insulin protein evidenced in many studies (20). In contrast, Igf1 transcripts were detectable, and a decreased level of these transcripts was observed in CV-B4 E2-infected MTE cultures as well, but to a lesser extent than Igf2 transcripts.…”

Section: Cd8mentioning

confidence: 66%

“…Indeed, administration of IGF-2-derived self-antigens (B11-25 sequence) to peripheral blood mononuclear cells from DQ8 ϩ type 1 diabetic patients seems to be an efficient approach in T1D prevention, since it elicits a tolerogenic/regulatory cytokine profile (interleukin-10 [IL-10], IL-10/ gamma interferon [IFN-␥], and IL-4) statistically different from the one induced by Ins B9-23 (19). This issue is currently investigated by vaccination of NOD mice with recombinant human IGF-2 alone or in combination with adjuvants (20). The association between CV-B4 infection and the loss of immune self-tolerance is still unclear.…”

mentioning

confidence: 99%

“…Besides, Igf2 could be employed both in the reprogramming of immunological tolerance to islet ␤ cells and in the regeneration of a functional ␤-cell mass (20). On the basis of the close homology and cross-tolerance between insulin and IGF-2, a novel type of negative/tolerogenic self-vaccination is currently developed for prevention and cure of T1D (23).…”

mentioning

confidence: 99%

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Persistent Infection of Thymic Epithelial Cells with Coxsackievirus B4 Results in Decreased Expression of Type 2 Insulin-Like Growth Factor

Jaïdane

Caloone

Lobert

et al. 2012

J Virol

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Section: Cd8mentioning

confidence: 66%

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confidence: 99%

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Persistent Infection of Thymic Epithelial Cells with Coxsackievirus B4 Results in Decreased Expression of Type 2 Insulin-Like Growth Factor

Jaïdane

Caloone

Lobert

et al. 2012

J Virol

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“…We proposed that IGF-2 could be a safer and more valuable basis for developing a specific “negative/tolerogenic self-vaccination,” on the basis that Igf2 transcription is defective in the thymus of BBDP rats (Kecha-Kamoun et al, 2001) and that IGF-2 mediates significant cross-tolerance to insulin (Hansenne et al, 2006). The concept of negative self-vaccination implies both the competition between IGF-2 and insulin-derived epitopes for presentation by DQ2 and DQ8 alleles, as well as a tolerogenic response—including recruitment of Treg cells–induced by MHC-presentation of IGF-2 self-peptides (Geenen et al, 2004, 2010). …”

Section: The Concept Of “Negative/tolerogenic Self-vaccination”mentioning

confidence: 99%

Programming of neuroendocrine self in the thymus and its defect in the development of neuroendocrine autoimmunity

et al. 2013

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For centuries after its first description by Galen, the thymus was considered as only a vestigial endocrine organ until the discovery in 1961 by Jacques FAP Miller of its essential role in the development of T (thymo-dependent) lymphocytes. A unique thymus first appeared in cartilaginous fishes some 500 million years ago, at the same time or shortly after the emergence of the adaptive (acquired) immune system. The thymus may be compared to a small brain or a computer highly specialized in the orchestration of central immunological self-tolerance. This was a necessity for the survival of species, given the potent evolutionary pressure imposed by the high risk of autotoxicity inherent in the stochastic generation of the diversity of immune cell receptors that characterize the adaptive immune response. A new paradigm of “neuroendocrine self-peptides” has been proposed, together with the definition of “neuroendocrine self.” Neuroendocrine self-peptides are secreted by thymic epithelial cells (TECs) not according to the classic model of neuroendocrine signaling, but are processed for presentation by, or in association with, the thymic major histocompatibility complex (MHC) proteins. The autoimmune regulator (AIRE) gene/protein controls the transcription of neuroendocrine genes in TECs. The presentation of self-peptides in the thymus is responsible for the clonal deletion of self-reactive T cells, which emerge during the random recombination of gene segments that encode variable parts of the T cell receptor for the antigen (TCR). At the same time, self-antigen presentation in the thymus generates regulatory T (Treg) cells that can inhibit, in the periphery, those self-reactive T cells that escaped negative selection in the thymus. Several arguments indicate that the origin of autoimmunity directed against neuroendocrine glands results primarily from a defect in the intrathymic programming of self-tolerance to neuroendocrine functions. This defect may be genetic or acquired, for example during an enteroviral infection. This novel knowledge of normal and pathologic functions of the thymus constitutes a solid basis for the development of a novel type of tolerogenic/negative self-vaccination against type 1 diabetes (T1D).

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“…According to the novel knowledge gained in type 1 diabetes pathogenesis and the central role of a thymus dysfunction in its development, the control of the autoimmune process could be obtained by (re)programming ␤ -cells through the potent tolerogenic properties of the thymus, in particular the repertoire of thymic type 1 diabetes-related self-antigens. Contrary to insulin, the 'altered self IGF-2', IGF-2 and derived epitopes might be a much more appropriate choice for a novel type of negative self-vaccination that associates competition for major histocompatibility complex presentation and regulatory responses downstream, as well as potential bystander suppression of autoimmune responses to other type 1 diabetes-related autoantigens [41] . This hypothesis is currently being investigated by vaccination of NOD mice with recombinant human IGF-2 alone or in combination with tolerogenic adjuvants.…”

Section: Prospective: the Concept Of Negative Self-vaccinationmentioning

confidence: 99%

The Role of the Thymus in the Integrated Evolution of the Recombinase-Dependent Adaptive Immune Response and the Neuroendocrine System

Mottet¹,

Goffinet²,

Beckers³

et al. 2011

Neuroimmunomodulation

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Before being able to react against infectious non-self-antigens, the immune system has to be educated in recognition and tolerance of neuroendocrine self-proteins. This sophisticated educational process takes place only in the thymus. The development of an autoimmune response directed to neuroendocrine glands has been shown to result from a thymus dysfunction in programming immunological self-tolerance to neuroendocrine-related antigens. This thymus dysfunction leads to a breakdown of immune homeostasis with an enrichment of ‘forbidden’ self-reactive T cells and a deficiency in self-antigen-specific natural regulatory T cells in the peripheral T lymphocyte repertoire. A large number of neuroendocrine self-antigens are expressed by the thymic epithelium, under the control of the autoimmune regulator (AIRE) gene/protein in the medulla. Based on the close homology and cross-tolerance between thymic type 1 diabetes-related self-antigens and peripheral antigens targeted in β-cells by autoimmunity, a novel type of vaccination is currently developed for the prevention and cure of type 1 diabetes. If this approach were found to be effective in reprogramming immunological tolerance that is absent or broken in this disease, it could pave the way for the design of negative/tolerogenic self-vaccines against other endocrine and organ-specific autoimmune disorders.

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Thymic self-antigens for the design of a negative/tolerogenic self-vaccination against type 1 diabetes

Cited by 21 publications

References 107 publications

Persistent Infection of Thymic Epithelial Cells with Coxsackievirus B4 Results in Decreased Expression of Type 2 Insulin-Like Growth Factor

Persistent Infection of Thymic Epithelial Cells with Coxsackievirus B4 Results in Decreased Expression of Type 2 Insulin-Like Growth Factor

Programming of neuroendocrine self in the thymus and its defect in the development of neuroendocrine autoimmunity

The Role of the Thymus in the Integrated Evolution of the Recombinase-Dependent Adaptive Immune Response and the Neuroendocrine System

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