Publications by authors named "Sophie Wehenkel"

Article Synopsis
  • L-selectin on T-cells helps naïve and memory cells enter lymph nodes, but it also plays a role in directing activated T-cells to infection sites after being shed.
  • Research shows that activated T-cells can re-express L-selectin to locate virus-infected areas, and while the enzyme ADAM17 is crucial for L-selectin's proteolysis, this process does not affect general T-cell activation markers.
  • Importantly, L-selectin cleavage enhances the early expansion of cytotoxic T-cells during viral infections, leading to significantly increased immune responses compared to T-cells that can't cleave L-selectin.
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Adoptive transfer of tumor-specific cytotoxic T cells is a promising advance in cancer therapy. Similarly, checkpoint inhibition has shown striking clinical results in some patients. Here we combine adoptive cell transfer with ablation of the checkpoint protein Src homology 2-domain-containing phosphatase 1 (SHP-1, Ptpn6).

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The success of adoptive T-cell therapies for the treatment of cancer patients depends on transferred T-lymphocytes finding and infiltrating cancerous tissues. For intravenously transferred T-cells, this means leaving the bloodstream (extravasation) from tumour blood vessels. In inflamed tissues, a key event in extravasation is the capture, rolling and arrest of T-cells inside blood vessels which precedes transmigration across the vessel wall and entry into tissues.

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The immense power of the immune system is harnessed in healthy individuals by a range of negative regulatory signals and checkpoints. Manipulating these checkpoints through inhibition has resulted in striking immune-mediated clearance of otherwise untreatable tumours and metastases; unfortunately, not all patients respond to treatment with the currently available inhibitors of cytotoxic T-lymphocyte-associated protein 4 (CTLA-4) and programmed cell death protein 1 (PD-1). Combinatorial studies using both anti-CTLA-4 and anti-PD-1 demonstrate synergistic effects of targeting multiple checkpoints, paving the way for other immune checkpoints to be targeted.

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