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Homing to solid cancers: a vascular checkpoint in adoptive cell therapy using CAR T-cells

期刊

BIOCHEMICAL SOCIETY TRANSACTIONS
卷 44, 期 -, 页码 377-385

出版社

PORTLAND PRESS LTD
DOI: 10.1042/BST20150254

关键词

chemokine receptors; endothelial cell anergy; extravasation; high endothelial venules; homing; integrins; selectins; tumour blood vessels; tumouricidal T-lymphocytes; vessel normalization

资金

  1. Wellcome Trust [094511/Z/10/Z]
  2. Medical Research Council UK [MR/L008742/1]
  3. Ministry of Higher Education and Scientific Research, Kurdistan Regional Government, Iraq
  4. Wellcome Trust [094511/Z/10/Z] Funding Source: Wellcome Trust
  5. Medical Research Council [MR/L008742/1, 1180095] Funding Source: researchfish
  6. MRC [MR/L008742/1] Funding Source: UKRI

向作者/读者索取更多资源

The success of adoptive T-cell therapies for the treatment of cancer patients depends on transferred T-ymphocytes 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. This depends on co-ordinated signalling of selectins, integrins and chemokine receptors on T-cells by their respective ligands which are up-regulated on inflamed blood vessels. Clinical data and experimental studies in mice suggest that tumour blood vessels are anergic to inflammatory stimuli and the recruitment of cytotoxic CD8(+) T-lymphocytes is not very efficient. Interestingly, and somewhat counter-intuitively, anti-angiogenic therapy can promote CD8(+) T-cell infiltration of tumours and increase the efficacy of adoptive CD8(+) T-cell therapy. Rather than inhibit tumour angiogenesis, anti-angiogenic therapy 'normalizes' (matures) tumour blood vessels by promoting pericyte recruitment, increasing tumour blood vessel perfusion and sensitizing tumour blood vessels to inflammatory stimuli. A number of different approaches are currently being explored to increase recruitment by manipulating the expression of homing-associated molecules on T-cells and tumour blood vessels. Future studies should address whether these approaches improve the efficacy of adoptive T-cell therapies for solid, vascularized cancers in patients.

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