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Dive into the research topics where Christian Taube is active.

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Featured researches published by Christian Taube.


Journal of Immunology | 2009

Vaccine-Induced CD8+ T Cell-Dependent Suppression of Airway Hyperresponsiveness and Inflammation

Katsuyuki Takeda; Steven W. Dow; Nobuaki Miyahara; Taku Kodama; Toshiyuki Koya; Christian Taube; Anthony Joetham; Jung-Won Park; Azzeddine Dakhama; Ross M. Kedl; Erwin W. Gelfand

Suppressing the abnormalities associated with asthma has been difficult to accomplish using immunotherapy or vaccination once the disease is established. The effector cells necessary for effective immunization/vaccination and immunotherapy of asthma are also not well understood. Therefore, we vaccinated allergen (OVA)-sensitized mice to determine whether therapeutic immunization could suppress airway hyperresponsiveness (AHR) and inflammation and to identify key immune effector cells and cytokines. Mice were immunized with a vaccine comprised of Ag and cationic liposome-DNA complexes (CLDC), a vaccine which has previously been shown to elicit strong CD4+ and CD8+ T cell responses and activation of Th1 immunity. We showed that immunization with the OVA-CLDC vaccine significantly suppressed AHR, eosinophilia, goblet cell metaplasia, and Th2 cytokine production. In contrast, immunization with CLDC alone suppressed eosinophilia and Th2 cytokine production, but failed to suppress AHR and goblet cell changes. Using adoptive transfer experiments, we found that suppression of AHR was mediated by Ag-specific CD8+ T cells and was dependent on IFN-γ production by the transferred T cells. Thus, we conclude that generation of strong, allergen-specific CD8+ T cell responses by immunization may be capable of suppressing AHR and allergic airway inflammation, even in previously sensitized and challenged mice.


Journal of Immunology | 2009

Allergic Airway Hyperresponsiveness-Enhancing γδ T Cells Develop in Normal Untreated Mice and Fail to Produce IL-4/13, Unlike Th2 and NKT Cells

Niyun Jin; Christina L. Roark; Nobuaki Miyahara; Christian Taube; M. Kemal Aydintug; J. M. Wands; Yafei Huang; Youn Soo Hahn; Erwin W. Gelfand; Rebecca L. O'Brien; Willi K. Born

Allergic airway hyperresponsiveness (AHR) in OVA-sensitized and challenged mice, mediated by allergen-specific Th2 cells and Th2-like invariant NKT (iNKT) cells, develops under the influence of enhancing and inhibitory γδ T cells. The AHR-enhancing cells belong to the Vγ1+ γδ T cell subset, cells that are capable of increasing IL-5 and IL-13 levels in the airways in a manner like Th2 cells. They also synergize with iNKT cells in mediating AHR. However, unlike Th2 cells, the AHR enhancers arise in untreated mice, and we show here that they exhibit their functional bias already as thymocytes, at an HSAhigh maturational stage. In further contrast to Th2 cells and also unlike iNKT cells, they could not be stimulated to produce IL-4 and IL-13, consistent with their synergistic dependence on iNKT cells in mediating AHR. Mice deficient in IFN-γ, TNFRp75, or IL-4 did not produce these AHR-enhancing γδ T cells, but in the absence of IFN-γ, spontaneous development of these cells was restored by adoptive transfer of IFN-γ-competent dendritic cells from untreated donors. The i.p. injection of OVA/aluminum hydroxide restored development of the AHR enhancers in all of the mutant strains, indicating that the enhancers still can be induced when they fail to develop spontaneously, and that they themselves need not express TNFRp75, IFN-γ, or IL-4 to exert their function. We conclude that both the development and the cytokine potential of the AHR-enhancing γδ T cells differs critically from that of Th2 cells and NKT cells, despite similar influences of these cell populations on AHR.


Archive | 2003

SP-D Regulates Airway Function and Allergic Inflammation Through Regulation of Macrophage Function

Katsuyuki Takeda; Nobuaki Miyahara; Y. H. Rah; Christian Taube; Eun Seok Yang; Anthony Joetham; Tatsuhiko Kodama; Annette Balhorn; Azzeddine Dakhama; Catherine Duez; Amanda Evans; Dennis R. Voelker; Erwin W. Gelfand


Archive | 2013

Determined at the Age of Initial Sensitization Responsiveness to Allergen Challenge Are Induction and Maintenance of Airway

Katsuyuki Takeda; Christian Taube; Erwin W. Gelfand; Anthony Joetham; Zhi-Hua Cui


Archive | 2013

Depends on IL-10 Induction of TGF- Cell Regulation of Airway Allergic Responses Naturally Occurring Lung CD4+CD25+ T

Yeong-Ho Rha; Azzeddine Dakhama; Erwin W. Gelfand; Nobuaki Miyahara; Satoko Matsubara; Toshiyuki Koya; Anthony Joetham; Katsuyuki Takada; Christian Taube


Archive | 2013

Ovalbumin-Sensitized and Challenged Mice Hyperreactivity to Methacholine in T Cells Regulate Airway

Erwin W. Gelfand; Willi K. Born; Christina L. Roark; Michael Lahn; Rebecca L. O'Brien; J. M. Wands; M. Kemal Aydintug; Youn-Soo Hahn; Christian Taube; Niyun Jin


Archive | 2013

Antibodies and Fc Allergen Challenge Is Dependent on Specific Transient Neutrophil Infiltration After

Erwin W. Gelfand; Annette Balhorn; Toshiyuki Takai; Katie R. Poch; Anthony Joetham; Christian Taube; Azzeddine Dakhama; Yeong-Ho Rha


アレルギー | 2007

P156 CD8T細胞およびロイコトリエンB4受容体の気道過敏性における役割の検討(動物モデル1, 第19回日本アレルギー学会春季臨床大会)

信明 宮原; Christian Taube; 勝行 武田; 元洋 池田; 康子 渕本; 光 古賀; 安 谷本; 有彦 金廣; 光音 谷本; Erwin W. Gelfand


Archive | 2005

Inhibition du facteur B et de la voie du complément alternative et procédés associés

Vernon Michael Holers; Joshua M. Thurman; Christian Taube; Erwin W. Gelfand; Gary S. Gilkeson


Archive | 2005

Inhibition of factor B, the alternative komplemenpathway and related method

Vernon Michael Holers; Joshua M. Thurman; Erwin W. Gelfand; Gary S. Gilkeson; Christian Taube

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Erwin W. Gelfand

University of Colorado Hospital

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Anthony Joetham

University of Colorado Denver

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Azzeddine Dakhama

University of Colorado Denver

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Katsuyuki Takeda

University of Colorado Denver

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Gary S. Gilkeson

Medical University of South Carolina

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J. M. Wands

University of Colorado Denver

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Joshua M. Thurman

University of Colorado Denver

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