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Follow-up
of individual T cell mobilization through TCR integration
Principal Investigator: Jean Paul Soullilou, Institut
de Transplantation, Nantes, France
Abstract | Investigators
| Background
| Resources
Abstract
Autoimmune diseases are characterized by autoreactive
T cells which can be identified by their function or
phenotypes. Complex alterations of chain T cell receptor
(TCR) repertoires for antigens (including auto-antigens)
can be detected during auto immune response and tolerance
states. The following in time of these changes can
theoretically provide important information for diagnostic,
disease activity and the effect of treatment, including
regimens aimed at inducing immune tolerance against
auto antigens (deletion of autoreactive clones for
instance). However, because of the flexibility and
adaptability of TCR recognition (cross recognition),
auto immune T cells are not clonally distributed and
strongly selected T cell cohorts without apparent clonality
are also important to consider. To date, analysis of
auto-antigen induced biases in TCR V(beta) segment
usage can be routinely identified by Immunoscope/ Spectratype
methods. However, these methods do not provide information
on the amount of mRNA concerned (reflecting the size
and the activation of the autoreactive T cell pools).
In addition they only provide independent information
for each of the V(beta) family. New tools such as tetramers
will be very useful but require a precise knowledge
of a dominant peptide and a specific restricting MHC.
We propose a new approach that integrates qualitative
and quantitative variations of T cell receptor antigens
in T lymphocytes. In addition, we express these integrated
alterations as a global landscape (Tc Land© including
all V(beta) transcriptome). This approach, that we
have validated in man in vitro and in vitro/in vivo
in the rat (rejection/tolerance of allograft) has never
been used before. Using this method, we want to study
landscape of blood T lymphocytes in a cohort of 30
patients with active forms of MS, an auto immune disease
in which T cells reacting against myelin determinants
are believed to be instrumental. We hope to demonstrate,
at the level of each patient (since the T cell receptor
usage is individually shaped), patterns specific for
their disease and to relate them to the disease activity.
If we can obtain such " TCR signature ",
we will, in a second time, use it to follow regulation
of auto reactive T cells, particularly during tolerance
induction. The approach can be theoretically extended
to other auto immune diseases and to transplantation.
 Participating
Investigators
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Jean Paul Soulillou,
Institut de Transplantation, Nantes, France |
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Marc-André
Delsuc, University
Hospital, Montpellier, France |
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Samia Khoury, Brigham
& Women's Hospital, Boston, MA |
Background
Articles
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Different
qualitative and quantitative regulation of V beta
TCR transcripts during early acute allograft rejection
and tolerance induction - J Immunol [go ] |
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Highly altered
V beta repertoire of T cells infiltrating long-term
rejected kidney allografts - J Immunol [go]
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TCR usage in naive
and committed alloreactive cells: implications
for the understanding of TCR biases in transplantation – Curr.
Op in Immuno [go] |
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T cell
receptor repertoire usage in allotransplantation:
an overview - Transplantation [go] |
Resources
& Interesting Links
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TcLand
[go] |
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