Your search keyword '"Ditt, Vanessa"' showing total 3 results

1. High‐resolution analysis of individual spike peptide‐specific CD4+ T‐cell responses in vaccine recipients and COVID‐19 patients.

Author

Karsten, Hendrik, Cords, Leon, Westphal, Tim, Knapp, Maximilian, Brehm, Thomas Theo, Hermanussen, Lennart, Omansen, Till Frederik, Schmiedel, Stefan, Woost, Robin, Ditt, Vanessa, Peine, Sven, Lütgehetmann, Marc, Huber, Samuel, Ackermann, Christin, Wittner, Melanie, Addo, Marylyn Martina, Sette, Alessandro, Sidney, John, and Schulze zur Wiesch, Julian

Subjects

COVID-19, VACCINE effectiveness, T cells, COVID-19 vaccines, PEPTIDES, HISTOCOMPATIBILITY antigens

Abstract

Objectives: Potential differences in the breadth, distribution and magnitude of CD4+ T‐cell responses directed against the SARS‐CoV‐2 spike glycoprotein between vaccinees, COVID‐19 patients and subjects who experienced both ways of immunisation have not been comprehensively compared on a peptide level. Methods: Following virus‐specific in vitro cultivation, we determined the T‐cell responses directed against 253 individual overlapping 15‐mer peptides covering the entire SARS‐CoV‐2 spike glycoprotein using IFN‐γ ELISpot and intracellular cytokine staining. In vitro HLA binding was determined for selected peptides. Results: We mapped 955 single peptide‐specific CD4+ T‐cell responses in a cohort of COVID‐19 patients (n = 8), uninfected vaccinees (n = 16) and individuals who experienced both infection and vaccination (n = 11). Patients and vaccinees (two‐time and three‐time vaccinees alike) had a comparable number of CD4+ T‐cell responses (median 26 vs. 29, P = 0.7289). Most of these specificities were conserved in B.1.1.529 and the BA.4 and BA.5 sublineages. The highest magnitude of these in vitro IFN‐γ CD4+ T‐cell responses was observed in COVID‐19 patients (median 0.35%), and three‐time vaccinees showed a higher magnitude than two‐time vaccinees (median 0.091% vs. 0.175%, P < 0.0001). Twelve peptide specificities were each detected in at least 40% of subjects. In vitro HLA binding showed promiscuous presentation by DRB1 molecules for several peptides. Conclusion: Both SARS‐CoV‐2 infection and vaccination prime broadly directed T‐cell responses directed against the SARS‐CoV‐2 spike glycoprotein. This comprehensive high‐resolution analysis of spike peptide specificities will be a useful resource for further investigation of spike‐specific T‐cell responses. [ABSTRACT FROM AUTHOR]

Published

2022

2. IMPACT OF DE NOVO ANTI-HLA DSA ON ALLOGRAFT SURVIVAL IN A COHORT OF LIVING-DONOR RENAL TRANSPLANT RECIPIENTS: A FOLLOW-UP OF A RETROSPECTIVE STUDY

Author

Dieplinger, Georg, Ditt, Vanessa, Arns, Wolfgang, Cingoez, Tuelay, Wahba, Roger, Bauerfeind, Ursula, Stippel, Dirk, Dieplinger, Georg, Ditt, Vanessa, Arns, Wolfgang, Cingoez, Tuelay, Wahba, Roger, Bauerfeind, Ursula, and Stippel, Dirk

Published

2015

3. Impact of de novo donor-specific HLA antibodies detected by Luminex solid-phase assay after transplantation in a group of 88 consecutive living-donor renal transplantations

Author

Dieplinger, Georg, Ditt, Vanessa, Arns, Wolfgang, Huppertz, Andrea, Kisner, Tuelay, Hellmich, Martin, Bauerfeind, Ursula, Stippel, Dirk L., Dieplinger, Georg, Ditt, Vanessa, Arns, Wolfgang, Huppertz, Andrea, Kisner, Tuelay, Hellmich, Martin, Bauerfeind, Ursula, and Stippel, Dirk L.

Abstract

De novo donor-specific HLA antibodies (DSA) after renal transplantation are known to be correlated with poor graft outcome and the development of acute and chronic rejection. Currently, data for the influence of de novo DSA in patient cohorts including only living-donor renal transplantations (LDRT) are limited. A consecutive cohort of 88 LDRT was tested for the occurrence of de novo DSA by utilizing the highly sensitive Luminex solid-phase assay for antibody detection. Data were analyzed for risk factors for de novo DSA development and correlated with acute rejection (AR) and graft function. Patients with de novo DSA [31 (35%)] showed a trend for inferior graft function [mean creatinine change (mg/dL/year) after the first year: 0.15 DSA (+) vs. 0.02 DSA (-) (P=0.10)] and a higher rate of AR episodes, especially in case of de novo DSA of both class I and II [6 (55%), (P=0.05)]. Antibody-mediated rejection (AMR) appeared in five patients and was significantly correlated with de novo DSA (P=0.05). Monitoring for de novo DSA after LDRT may help to identify patients at risk of declining renal function. Especially patients with simultaneous presence of de novo DSA class I and class II are at a high risk to suffer AR episodes.

Published

2014