Your search keyword '"Acha-Orbea H"' showing total 8 results

1. CD4+CD3− Cells Induce Peyer's Patch Development: Role of α4β1 Integrin Activation by CXCR5

Author

Finke, D., Acha-Orbea, H., Mattis, A., Lipp, M., and Kraehenbuhl, J.P.

Subjects

*HEMATOPOIETIC stem cells, *CHEMOKINES, *CELL adhesion

Abstract

CD4+CD3− cells are the predominant hematopoietic cells found in mouse fetal intestine. We prove their role as Peyer''s patch (PP)-inducing cells by transfer into neonatal PP-deficient mice. To test the requirement of chemokines and adhesion molecules in induction of PP, we studied mice deficient in CXCR5 and/or α4β1 integrin-mediated adhesion. CXCR5−/− mice have CD4+CD3− cells, which are inefficient in inducing PP formation. We show here that CXCR5/CXCL13 signaling activates α4β1 integrin on CD4+CD3− cells. Blocking of β1 integrin or VCAM-1, the ligand of α4β1 integrin, inhibits PP formation. This study demonstrates the link between chemokine receptors and adhesion molecules that regulates stromal/hematopoietic cell interaction leading to PP formation. [Copyright &y& Elsevier]

Published

2002

2. The primary <em>in vivo</em> immune response to Mls-1 (<em>Mtv-7 sag</em>). Route of injection determines the immune response pattern.

Author

Andersson, M. and Acha-Orbea, H.

Subjects

*SUPERANTIGENS, *IMMUNE response, *IMMUNE system, *B cells, *IMMUNITY, *IMMUNOLOGY

Abstract

Injection of cells expressing the retroviral superantigen Mls-1 (Mtv-7 sag) into adult Mls-1 — mice induces a strong immune response including both T- and B-cell activation. This model was used for studying qualitative aspects of the immune response in normal mice with a defined antigen-presenting cell (the B cell) and without the use of adjuvant. BALB/c mice were injected locally or systemically with Mis-l-expressing spleen cells from Mis-l-congenic BALB.D2 mice. Intravenous injection led to an initially strong expansion of Mis-l-reactive Vβ6+ CD4+ cells mainly in the spleen, to a large degree explained by the trapping of reactive cells, and a rapid down-regulation of interleukin-2 (IL-2) and interferon-γ (IFN-γ) production, consistent with the proposed tolerogenic property of B cells as antigen-presenting cells. However, these mice developed a slowly appearing but persistent B-cell response dominated by IgG1-producing cells, suggesting a shift in lymphokines produced rather than complete unresponsiveness. Subcutaneous injection into the hind footpad with the same number of cells led to a strong local response in the draining lymph node, characterized by a dramatic increase of Vβ6+ CD4+ T cells, local production of IL-2 and IFN-γ, and a strong but short-lived antibody response dominated by IgG2a-producing cells, characteristic of a T-helper type 1 (Th 1) type of response. Both routes of injection led ultimately to deletion of reactive T cells and anergy, as defined by the inability to produce IL-2 upon in vitro stimulation with Mis-1. It is concluded that Mls-1 presented by B cells induces qualitatively different responses in vivo dependent on the route of injection. We propose that the different responses result from the migration of the injected cells to different micro-anatomical sites in the lymphoid tissue. Furthermore, these results suggest that B cells may function as professional antigen-presenting cells in vivo if present in an appropriate environment. [ABSTRACT FROM AUTHOR]

Published

1994

3. A comparative study of T-cell receptor Vβ usage in non-obese diabetic (NOD) and I-E transgenic NOD mice.

Author

Parish, N. M., Acha-Orbea, H., Simpson, E., Qin, S.-X., Lund, T., and Cooke, A.

Subjects

*T cells, *PEOPLE with diabetes, *TRANSGENIC animals, *IMMUNOGLOBULINS, *DIABETES, *CARBOHYDRATE intolerance

Abstract

The non-obese diabetic (NOD) mouse is a model for the study of insulin-dependent diabetes mellitus (IDDM). Recently transgenic NOD mice have been derived (NOD-E) that express the major histocompatibility complex (MHC) class III-E molecule. NOD-E do not become diabetic and show negligible pancreatic insulins. The possibility pertained that NOD-E mice are protected from disease by a process of T-cell deletion or anergy. This paper describes our attempts to discover whether this was so, by comparing NOD and NOD-E mouse T-cell receptor Vβ usage. Splenocytes and lymph node cells were therefore tested for their ability to proliferate iii response to monoclonal anti-Vβ antibodies. We were unable to show any consistent differences between NOD and NOD-E responses to the panel of antibodies used. Previously proposed Vβ were shown to be unlikely candidates for deletion or anergy. T cells present at low frequency (Vβ5+) in both NOD and NOD-E mice were shown to be as capable of expansion in response to antigenic stimulation as were more frequently expressed Vβ. Our data therefore do not support deletion or anergy as mechanisms which could account for the observed disease protection in NOD-E mice. [ABSTRACT FROM AUTHOR]

Published

1993

4. Clonal deletion of V beta 14-bearing T cells in mice transgenic for mammary tumour virus.

Author

Acha-Orbea, H. and Shakhov, A.N.

Subjects

*TUMORS

Abstract

Presents research that explored a role for mouse mammary tumor virus (MMTV) gene products in the clonal deletion of autoreactive cells. Analyzes lines of transgenic mice bearing either the complete exogenous provirus MMTV or only the open reading frame present in the long terminal repeat of the provirus.

Published

1991

5. Role of major histocompatibility complex class II expression by non-hematopoietic cells in autoimmune and inflammatory disorders: facts and fiction.

Author

Duraes, F. V., Thelemann, C., Sarter, K., Acha‐Orbea, H., Hugues, S., and Reith, W.

Subjects

*HISTOCOMPATIBILITY, *GENE expression, *HEMATOPOIETIC agents, *AUTOIMMUNE diseases, *INFLAMMATION, *CD4 antigen, *T cells

Abstract

It is well established that interactions between CD4+ T cells and major histocompatibility complex class II ( MHCII) positive antigen-presenting cells ( APCs) of hematopoietic origin play key roles in both the maintenance of tolerance and the initiation and development of autoimmune and inflammatory disorders. In sharp contrast, despite nearly three decades of intensive research, the functional relevance of MHCII expression by non-hematopoietic tissue-resident cells has remained obscure. The widespread assumption that MHCII expression by non-hematopoietic APCs has an impact on autoimmune and inflammatory diseases has in most instances neither been confirmed nor excluded by indisputable in vivo data. Here we review and put into perspective conflicting in vitro and in vivo results on the putative impact of MHCII expression by non-hematopoietic APCs-in both target organs and secondary lymphoid tissues-on the initiation and development of representative autoimmune and inflammatory disorders. Emphasis will be placed on the lacunar status of our knowledge in this field. We also discuss new mouse models-developed on the basis of our understanding of the molecular mechanisms that regulate MHCII expression-that constitute valuable tools for filling the severe gaps in our knowledge on the functions of non-hematopoietic APCs in inflammatory conditions. [ABSTRACT FROM AUTHOR]

Published

2013

6. Passive Immunization with Neutralizing Antibodies Interrupts the Mouse Mammary Tumor Virus Life Cycle.

Author

Mpandi, M., Otten, L.A., Lavanchy, C., Acha-Orbea, H., and Finke, D.

Subjects

*MOUSE mammary tumor virus, *MONOCLONAL antibodies, *GLYCOPROTEINS, *LABORATORY rats

Abstract

Mouse mammary tumor virus (MMTV) infects the host via mucosal surfaces and exploits the host immune system for systemic spread and chronic infection. We have tested a neutralizing rat monoclonal antibody specific for the retroviral envelope glycoprotein gp52 for its efficiency in preventing acute and chronic mucosal and systemic infection. The antibody completely inhibits the superantigen response and chronic viral infection following systemic or nasal infection. Surprisingly however, the antibody only partially inhibits the early infection of antigen-presenting cells in the draining lymph node. Despite this initially inefficient protection from infection, superantigen-specific B- and T-cell responses and systemic viral spread are abolished, leading to complete clearance of the retroviral infection and hence interruption of the viral life cycle. In conclusion, systemic neutralizing monoclonal antibodies can provide an efficient protection against chronic retroviral amplification and persistence. [ABSTRACT FROM AUTHOR]

Published

2003

7. Tissue distribution of the Ankara strain of vaccinia virus (MVA) after mucosal or systemic administration.

Author

Ramirez, J. C., Finke, D., Esteban, M., Kraehenbuhl, J. P., and Acha-Orbea, H.

Subjects

*VIROLOGY, *INJECTIONS, *TISSUES, *IMMUNIZATION, *VACCINATION, *VIRUSES, *CARDIOPULMONARY system

Abstract

Summary. MVA is a candidate vector for vaccination against pathogens and tumors. Little is known about its behaviour in mucosal tissues. We have investigated the fate and biosafety of MVA, when inoculated by different routes in C57BL/6 mice. Intranasal inoculation targeted the virus to the nasal associated lymphoid tissue and the lungs, whereas systemic inoculation led to distribution of MVA in almost all lymphoid organs, lungs and ovaries. Intravaginal, intrarectal and intragastric inoculations failed to induce efficient infection. After 48 h no virus was detectable any more in the organs analyzed. Upon intranasal inoculation, no inflammatory reactions were detected in the central nervous system as well as the upper and lower airways. These results show the tropism of MVA and indicate that high doses of recombinant MVA are safe when nasally administered, a vaccination route known to elicit strong cellular and humoral immune responses in the female genital tract. [ABSTRACT FROM AUTHOR]

Published

2003

8. MHC class II transactivator is an in vivo regulator of osteoclast differentiation and bone homeostasis co-opted from adaptive immunity

Author

⁎, E., Mariani, E., Scolari, M., Perilli, E., Barras, E., Fazzalari, N.L., Campana, L., Otten, L., Particelli, F., Acha-Orbea, H., Baruffaldi, F., Faccio, R., Sitia, R., Reith, W., and Cenci, S.

Published

2012