Document details

IgG autoantibody to brain beta tubulin III associated with cytokine cluster-II ...

Author(s): Bansal, D. cv logo 1 ; Herbert, F. cv logo 2 ; Lim, P. cv logo 3 ; Deshpande, P. cv logo 4 ; Becavin, C. cv logo 5 ; Guiyedi, V. cv logo 6 ; de Maria, I. cv logo 7 ; Rousselle, J.C. cv logo 8 ; Namane, A. cv logo 9 ; Jain, R. cv logo 10 ; Cazenave, P.A. cv logo 11 ; Mishra, G.C. cv logo 12 ; Ferlini, C. cv logo 13 ; Fesel, C. cv logo 14 ; Benecke, A. cv logo 15 ; Pied, S. cv logo 16

Date: 2009

Persistent ID: http://hdl.handle.net/10400.7/213

Origin: ARCA - Access to Research and Communication Annals

Subject(s): Antigens, Protozoan/immunology; Autoantibodies/blood; Brain/immunology; Cytokines/blood; Immunoglobulin G/immunology; Immunoglobulin M/immunology


Description
We investigated the significance of these self-reactive antibodies in clinically well-defined groups of P. falciparum infected patients manifesting mild malaria (MM), severe non-cerebral malaria (SM), or cerebral malaria (CM) and in control subjects from Gondia, a malaria epidemic site in central India using quantitative immunoprinting and multivariate statistical analyses. A two-fold complete-linkage hierarchical clustering allows classifying the different patient groups and to distinguish the CM from the others on the basis of their profile of IgG reactivity to brain proteins defined by PANAMA Blot. We identified beta tubulin III (TBB3) as a novel discriminant brain antigen in the prevalence of CM. In addition, circulating IgG from CM patients highly react with recombinant TBB3. Overall, correspondence analyses based on singular value decomposition show a strong correlation between IgG anti-TBB3 and elevated concentration of cluster-II cytokine (IFNγ, IL1β, TNFα, TGFβ) previously demonstrated to be a predictor of CM in the same population
Document Type Article
Language English
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