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CD1d-restricted peripheral T cell lymphoma in mice and humans.
- Bachy, Emmanuel;
- Urb, Mirjam;
- Chandra, Shilpi;
- Robinot, Rémy;
- Bricard, Gabriel;
- de Bernard, Simon;
- Traverse-Glehen, Alexandra;
- Gazzo, Sophie;
- Blond, Olivier;
- Khurana, Archana;
- Baseggio, Lucile;
- Heavican, Tayla;
- Ffrench, Martine;
- Crispatzu, Giuliano;
- Mondière, Paul;
- Schrader, Alexandra;
- Taillardet, Morgan;
- Thaunat, Olivier;
- Martin, Nadine;
- Dalle, Stéphane;
- Le Garff-Tavernier, Magali;
- Salles, Gilles;
- Lachuer, Joel;
- Hermine, Olivier;
- Asnafi, Vahid;
- Roussel, Mikael;
- Lamy, Thierry;
- Herling, Marco;
- Iqbal, Javeed;
- Buffat, Laurent;
- Marche, Patrice;
- Gaulard, Philippe;
- Kronenberg, Mitchell;
- Defrance, Thierry;
- Genestier, Laurent
- et al.
Published Web Location
https://doi.org/10.1084/jem.20150794Abstract
Peripheral T cell lymphomas (PTCLs) are a heterogeneous entity of neoplasms with poor prognosis, lack of effective therapies, and a largely unknown pathophysiology. Identifying the mechanism of lymphomagenesis and cell-of-origin from which PTCLs arise is crucial for the development of efficient treatment strategies. In addition to the well-described thymic lymphomas, we found that p53-deficient mice also developed mature PTCLs that did not originate from conventional T cells but from CD1d-restricted NKT cells. PTCLs showed phenotypic features of activated NKT cells, such as PD-1 up-regulation and loss of NK1.1 expression. Injections of heat-killed Streptococcus pneumonia, known to express glycolipid antigens activating NKT cells, increased the incidence of these PTCLs, whereas Escherichia coli injection did not. Gene expression profile analyses indicated a significant down-regulation of genes in the TCR signaling pathway in PTCL, a common feature of chronically activated T cells. Targeting TCR signaling pathway in lymphoma cells, either with cyclosporine A or anti-CD1d blocking antibody, prolonged mice survival. Importantly, we identified human CD1d-restricted lymphoma cells within Vδ1 TCR-expressing PTCL. These results define a new subtype of PTCL and pave the way for the development of blocking anti-CD1d antibody for therapeutic purposes in humans.
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