Expression in transgenic mice of class I histocompatibility antigens controlled by the metallothionein promoter.

Morahan, Grant; Brennan, Francine E.; Bhathal, Prithi S.; Allison, James P.; Cox, K.O.; Miller, J. F. A. P.

doi:10.1073/pnas.86.10.3782

Cited by 94 publications

(61 citation statements)

References 29 publications

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“…16,17 Support for a role of hepatocytes as APCs in vivo comes from studies performed using transgenic mouse models. When Alb-K b and Met-K b transgenic mice, expressing the allo-MHC H-2K b molecule on hepatocytes, 18,19 were adoptively transferred with TCR transgenic T cells specific for H-2K b , T cell primary activation occurred in the liver independently of lymphoid tissues, thus supporting the thesis that hepatocytes can interact with circulating T cells in vivo. 6,8 Such results suggest that hepatocytes can present antigen to both CD8 ϩ T lymphocytes and possibly also NKT lymphocytes, and thus play a major role in antigen-specific recruitment of these cells to the liver.…”

mentioning

confidence: 82%

“…B10.BR and C57BL/6 mice were purchased from the Animal Resources Centre (Perth, Australia). Met-K b and Alb-K b transgenic mice expressing H-2K b on hepatocytes under the control of the sheep metallothionein 19 or the mouse albumin promoters, 18 respectively, were kindly provided by Drs Grant Morahan and Jacques Miller (WEHI, Australia) and Dr Bernd Arnold (DKZ, Germany). Des-TCR, which express an H-2K b -specific TCR, 25 were a gift of Dr. Bernd Arnold.…”

Section: Methodsmentioning

confidence: 99%

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T lymphocytes interact with hepatocytes through fenestrations in murine liver sinusoidal endothelial cells

et al. 2006

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The liver has an established ability to induce tolerance. Recent evidence indicates that this unique property might be related to its distinctive architecture allowing T cells to be activated in situ independently of lymphoid tissues. Unlike lymph node-activated T cells, liver-activated T cells are shortlived, a mechanism that might contribute to the "liver tolerance effect." Although the potential role of hepatocytes as tolerogenic antigen-presenting cells has been demonstrated, the question as to whether these cells are able to interact with CD8 ؉ T cells in physiological settings remains controversial. Contradicting the immunological dogma stating that naïve T lymphocytes are prevented from interacting with parenchymal cells within non-lymphoid organs by an impenetrable endothelial barrier, we show here that the unique morphology of the liver sinusoidal endothelial cell (LSEC) permits interactions between lymphocytes and hepatocytes. Using electron microscopy, we demonstrate that liver resident lymphocytes as well as circulating naïve CD8 ؉ T cells make direct contact with hepatocytes through cytoplasmic extensions penetrating the endothelial fenestrations that perforate the LSECs. Furthermore, the expression of molecules required for primary T cell activation, MHC class I and ICAM-1, is polarized on hepatocytes to the perisinusoidal cell membrane, thus maximizing the opportunity for interactions with circulating lymphocytes. In conclusion, this study has identified, at the ultrastructural level, a unique type of interaction between naïve T lymphocytes and liver parenchymal cells in vivo. These results hold implications for the pathogenesis of viral hepatitis in which hepatocytes may represent the main antigen-presenting cell, and for the development of immune tolerance as lymphocytes pass through the liver.

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confidence: 82%

Section: Methodsmentioning

confidence: 99%

T lymphocytes interact with hepatocytes through fenestrations in murine liver sinusoidal endothelial cells

et al. 2006

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“…The more intense the stimulation, the greater the number of activated T cells and hence bystander suppression of the ongoing T cell response. Indeed in many in vivo models, continuous high-dose Ag results in a state of immune paralysis, in which T cells become unresponsive to stimulation (31)(32)(33)(34)(35). Bystander suppression by activated T cells may provide balance in immune responses so as to prevent immune exhaustion and thereby allow effective memory T cell development (36,37).…”

Section: Discussionmentioning

confidence: 99%

Antigen Nonspecific Suppression of T Cell Responses by Activated Stimulation-Refractory CD4+ T Cells

Duthoit

Nguyen

Geiger

2004

The Journal of Immunology

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Several classes of anergic T cells are capable of suppressing naive T cell proliferation and thereby limiting immune responses. Activated T cells, although not anergic, are transiently refractory to restimulation with Ag. We examine in this study whether activated refractory murine T cells can also suppress naive T cell responses. We find that they can, and that they exhibit many of the suppressive properties of anergic T cells. The activated cells strongly diminish Ag-mediated T cell proliferation, an activity that correlates with their refractory period. Suppression is independent of APC numbers and requires cell contact or proximity. Naive T cells stimulated in the presence of activated refractory cells up-regulate CD25 and CD69, but fail to produce IL-2. The addition of IL-2 to culture medium, however, does not prevent the suppression, which is therefore not solely due to the absence of this growth factor. Persistence of the suppressor cells is also not essential. T cells stimulated in their presence and then isolated from them and cultured do not divide. The suppressive cells, however, do not confer a refractory or anergic state on the target T lymphocytes, which can fully respond to antigenic stimulation if removed from the suppressors. Our results therefore provide evidence that activated T cells act as transient suppressor cells, severely constraining bystander T cell stimulation and thereby restricting their response. These results have potentially broad implications for the development and regulation of immune responses.

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“…Genes for a foreign antigen can be placed under the control of the insulin promoter [33, 341, thus targeting gene expression to the insulin-secreting cells of the pancreatic islets of Langerhans. Alternatively, targeting can be chiefly to the liver, through using the metallothionein promoter [35] or to the exocrine portion of the pancreas through use of the elastase promoter (361. If, as is usually the case in most founder lines, the transgene is expressed early in ontogeny, T cell tolerance to the antigen in question can develop (reviewed in [37,381).…”

Section: Peripheral Tolerance Induction Among T Lymphocytesmentioning

confidence: 99%

“…Any specific B cells found to be present can then be placed singly into clonal microcultures with appropriately strong immunogens to ask whether the cell can develop into an antibody-forming clone. It turns out that, depending on the strength of the negative signal, both clonal abortion and clonal anergy can be induced [14,35,171 and indeed one and the same reagent can cause clonal abortion at high concentration and clonal anergy at low [17].…”

Section: Clonal Analysis Of Tolerance In Conventional Micementioning

confidence: 99%

Molecular and cellular aspects of immunologic tolerance

Nossal

1991

European Journal of Biochemistry

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This review seeks to explain the most exciting recent data concerning the nature of self/non-self discrimination by the immune system in a manner accessible to a biochemical readership. The nature of recognition in the two great lymphocyte families, B cells and T cells, is described with special emphasis on the nature of the ligands recognized by each. The history of the field of immunologic tolerance is surveyed, as are the key experiments on conventional mice which provided a conceptual framework. This suggested that tolerance was essentially due to 'holes' in the recognition repertoires of both the T and B cell populations so that lymphocytes competent to react to self antigens were not part of the immunologic dictionary. There were essentially two ways to achieve this situation. On the one hand, self antigens might 'catch' developing lymphocytes early in their ontogeny and delete the cell, a process of clonal abortion. On the other hand, self antigens might signal lymphocytes (particularly immature cells) in a negative manner, reducing or abolishing their capacity for later responses, without causing death. This process is referred to as clonal anergy. Evidence for both processes exists.Special emphasis is placed on a wave of experimentation beginning in 1988 which imaginatively uses transgenic mouse technology to study tolerance. Transgenic manipulations can produce mice which synthesize foreign antigens in a constitutive and/or inducible manner, sometimes only in specific locations; mice which possess T or B lymphocytes almost all expressing a given receptor of known specificity; and mice which are an immunologic time bomb in that the antigen is present and so too are lymphocytes all endowed with receptors for that antigen. These experiments have vindicated the possibility of both clonal abortion and clonal anergy in both T and B cell populations, the choice of which phenomenon occurs depending on a number of operational circumstances. For T cell tolerance, clonal abortion occurs if the self antigenic determinant concerned is present within the thymus; if not, clonal anergy is more likely. For B cell tolerance, the strength of the negative signal and therefore the choice between abortion and anergy depends on the molar concentration of the self antigen, the capacity for multivalent presentation to a B cell, and the affinity of the B cell's receptor for the antigen in question. Some B cells with low affinity for self antigens certainly escape censorship and remain capable of secreting low affinity anti-self antibodies, which however do no harm. Mechanisms which prevent the emergence of hypermutated, high-affinity anti-self B cells are discussed.Lt is an honour and also a considerable challenge to be asked to summarize an essentially immunological topic, and an important and rapidly moving one, for a biochemical readership. The task is worthwhile because biochemistry and molecular biology have revolutionized immunology over the last quarter century, and because immunologic tolerance remains the single most i...

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Expression in transgenic mice of class I histocompatibility antigens controlled by the metallothionein promoter.

Cited by 94 publications

References 29 publications

T lymphocytes interact with hepatocytes through fenestrations in murine liver sinusoidal endothelial cells

T lymphocytes interact with hepatocytes through fenestrations in murine liver sinusoidal endothelial cells

Antigen Nonspecific Suppression of T Cell Responses by Activated Stimulation-Refractory CD4+ T Cells

Molecular and cellular aspects of immunologic tolerance

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