Search CORE

365 research outputs found

282: Efficient Induction and Isolation of a Primary CMV-specific CD8+ T Cell Response from CMV Seronegative Donors for the Treatment of Serious CMV-Related Complications in CMV Seropositive Patients Transplanted with a CMV Seronegative Donor

Author: Falkenburg J.H.F.
Jedema I.
Marijt E.W.A.
Meij P.
van de Meent M.
van der Heiden P.L.J.
Willemze R.
Publication venue: American Society for Blood and Marrow Transplantation. Published by Elsevier Inc.
Publication date: 29/02/2008
Field of study

Elsevier - Publisher Connector

Randomized controlled trial on the effects of a supervised high intensity exercise program in patients with a hematologic malignancy treated with autologous stem cell transplantation:Results from the EXIST study

Author: Brug J.
Buffart L.M.
ChinAPaw M.J.M.
Kersten M.J.
Koene H.R.
Liu R.D.K.
Lugtenburg P.J.
Marijt E.W.A.
Minnema M.C.
Nollet F.
Persoon S.
Wijermans P.
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 20/07/2017
Field of study

International Migration, Integration and Social Cohesion online publications

Minor histocompatibility antigen HA-1, -2, -4 and HY specific cytotoxic T cell clones inhibit human hematopoietic progenitor cell growth by a mechanism that is dependent on direct cell-cell contact.

Author: Falkenburg J.H.F.
Goulmy E.A.J.M.
Marijt W.A.F.
Rood J.J. van
Veenhof W.F.J.
Willemze R.
Publication venue
Publication date: 01/01/1993
Field of study

Leiden University Scholary Publications

Cross-presentation of a TAP-independent signal peptide induces CD8 T immunity to escaped cancers but necessitates anchor replacement

Author: Blijleven L.
Burg S.H. van der
Griffioen L.
Hall T. van
Marijt K.A.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 17/06/2021
Field of study

Cancer cells frequently display defects in their antigen-processing pathway and thereby evade CD8 T cell immunity. We described a novel category of cancer antigens, named TEIPP, that emerge on cancers with functional loss of the peptide pump TAP. TEIPPs are non-mutated neoantigens despite their 'self' origin by virtue of their absence on normal tissues. Here, we describe the development of a synthetic long peptide (SLP) vaccine for the most immunogenic TEIPP antigen identified thus far, derived from the TAP-independent LRPAP1 signal sequence. LRPAP1(21-30)-specific CD8 T cells were present in blood of all tested healthy donors as well as patients with non-small cell lung adenocarcinoma. SLPs with natural flanking, however, failed to be cross-presented by monocyte-derived dendritic cells. Since the C-terminus of LRPAP1(21-30) is an unconventional and weakly binding serine (S), we investigated if replacement of this anchor would result in efficient cross-presentation. Exchange into a valine (V) resulted in higher HLA-A2 binding affinity and enhanced T cell stimulation. Importantly, CD8 T cells isolated using the V-variant were able to bind tetramers with the natural S-variant and respond to TAP-deficient cancer cells. A functional screen with an array of N-terminal and C-terminal extended SLPs pointed at the 24-mer V-SLP, elongated at the N-terminus, as most optimal vaccine candidate. This SLP was efficiently cross-presented and consistently induced a strong polyclonal LRPAP1(21-30)-specific CD8 T cells from the endogenous T cell repertoire. Thus, we designed a TEIPP SLP vaccine from the LRPAP1 signal sequence ready for validation in clinical trials.Experimental cancer immunology and therap

Leiden University Scholary Publications