Your search keyword '"José C. Crispín"' showing total 2 results

1. De NovoDonor-Specific HLA Antibody Development and PeripheralCD4+CD25highCells in Kidney Transplant Recipients: A Place for Interaction?

Author

Norma O. Uribe-Uribe, Luis E. Morales-Buenrostro, Gabriel Carrasco, Diana Gómez-Martín, José C. Crispín, Jorge Alcocer-Varela, María Inés Vargas-Rojas, Josefina Alberú, and Roxana Rodríguez-Romo

Subjects

medicine.medical_specialty, biology, medicine.diagnostic_test, business.industry, Gastroenterology, Kidney transplant, Peripheral, Flow cytometry, Cd4 cd25, Immune system, Internal medicine, Immunology, biology.protein, Medicine, Hla antibodies, IL-2 receptor, Antibody, business

Abstract

The aim of this study was to determine whether the abundance of regulatory T cells (Tregs) (CD4+CD25high) affects thede novodevelopment of anti-HLA donor-specific antibodies (DSAs) in kidney transplant recipients (KTRs).Methods. Unsensitized (PRA ≤ 10%, no DSA) adult primary KTRs who received a living (83%) or deceased (17%) KT in our Institution during 2004/2005 were included. DSA testing was performed monthly, and Tregs were quantified by flow cytometry every 3 months, during the 1st year after KT. All patients received triple drug immunosuppressive therapy (CNI + MMF or AZA + PDN); 83% received anti-CD25.Results. 53 KTRs were included; 32% developed DSA during the 1st year after KT. Significantly lower 7-year graft survival was observed in those who developed DSA. No difference was observed in Treg numbers up to 9 months after KT, between DSA positive and negative. However, at 12 months after KT, DSA-negative patients had significantly higher numbers of Treg.Conclusions. Early development of DSA was not associated to variations in Treg abundance. The differences in Treg numbers observed at the late time point may reflect better immune acceptance of the graft and may be associated to long-term effects. Additional inhibitory mechanisms participating earlier in DSA development after KT deserve to be sought.

Published

2012

2. IL-17 in Systemic Lupus Erythematosus

Author

George C. Tsokos and José C. Crispín

Subjects

lcsh:Biotechnology, Health, Toxicology and Mutagenesis, medicine.medical_treatment, Lupus nephritis, lcsh:Medicine, Review Article, lcsh:Chemical technology, lcsh:Technology, Immune system, Blisibimod, immune system diseases, lcsh:TP248.13-248.65, Genetics, medicine, Animals, Humans, Lupus Erythematosus, Systemic, lcsh:TP1-1185, skin and connective tissue diseases, Molecular Biology, Autoimmune disease, Lupus erythematosus, lcsh:T, business.industry, Interleukin-17, lcsh:R, General Medicine, medicine.disease, Cytokine, Immunology, Molecular Medicine, Interleukin 17, business, Biotechnology, Anti-SSA/Ro autoantibodies

Abstract

IL-17 is a cytokine with powerful proinflammatory activity. Production of IL-17 is abnormally increased in patients with systemic lupus erythematosus (SLE), a multiorgan chronic autoimmune disease. In patients with SLE,CD3+CD4−CD8−(double negative) T cells are an important source of IL-17. IL-17 produced by double negative and CD4 T cells participates in the pathogenesis of the disease. IL-17-producing T cells are present in the kidneys of patients with lupus nephritis. IL-17 increased production in patients with SLE can amplify the immune response by increasing target organ inflammation and damage and by augmenting the production of antibodies by B cells.

Published

2010