A Transformable Supramolecular Bispecific Cell Engager for Augmenting Natural Killer and T Cell‐Based Cancer Immunotherapy

A Transformable Supramolecular Bispecific Cell Engager for Augmenting Natural Killer and T Cell‐Based Cancer Immunotherapy

Immune cells are pivotal in cancer immunotherapy, yet their therapeutic effectiveness is often hampered by limited tumor infiltration and inhibitory tumor microenvironments. An alkaline phosphatase (ALP)‐responsive and transformable supramolecular bis‐specific cell engager (Supra‐BiCE) to harness na...

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Veröffentlicht in:Advanced materials (Weinheim) 2024-01, Vol.36 (3), p.e2306736-n/a
Hauptverfasser: Chen, Yumiao, Li, Wei, Wang, Zhongqiu, Yu, Yingying, Li, Jie, Ding, Yinghao, Hu, Zhiwen, Liu, Qian, Yang, Zhimou, Gao, Jie
Format: Artikel
Sprache:eng
Schlagworte:
Alkaline phosphatase
bispecific cell engager
Cancer
cancer immunotherapy
Cell death
Combinatorial analysis
Immune system
Immunotherapy
Lymphocytes
Nanoribbons
natural killer cells
Peptides
self‐assembling peptides
T cells
Tumors
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Zusammenfassung:Immune cells are pivotal in cancer immunotherapy, yet their therapeutic effectiveness is often hampered by limited tumor infiltration and inhibitory tumor microenvironments. An alkaline phosphatase (ALP)‐responsive and transformable supramolecular bis‐specific cell engager (Supra‐BiCE) to harness natural killer (NK)/T cells for effective cancer immunotherapy is introduced here. The Supra‐BiCE, consisting of both SA‐P (a phosphorylated peptide targeting and blocking programmed cell death ligand 1 (PD‐L1)) and SA‐T (a phosphorylated peptide targeting and blocking T cell immunoglobulin and ITIM domain (TIGIT)) is constructed by a simple co‐assembling strategy. Upon intravenous administration, Supra‐BiCE self‐assembles into nanoribbons and interacts with NK/T cells via TIGIT. Notably, these nanoribbons undergo transformation into long nanofibrils within ALP‐overexpressing tumor regions, resulting in enhanced binding affinities of Supra‐BiCE to both PD‐L1 and TIGIT. Consequently, this leads to the accumulation and retention of NK/T cells within tumor regions. Furthermore, the combinatorial blockade of checkpoints by Supra‐BiCE activates infiltrating NK/T cells. Moreover, the adjustable peptide ratio in Supra‐BiCE enables customization for optimal therapeutic effects against distinct tumor types. Particularly, Supra‐BiCE (T:P = 1:3) achieved 98.27% tumor suppression rate against colon carcinoma model. Overall, this study offers a promising tool for engaging NK and T cells for cancer immunotherapy. A supramolecular bispecific‐cell‐engager (Supra‐BiCE) that simultaneously targets TIGIT on NK/T cells and PD‐L1 on tumor cells is fabricated by co‐assembly of two immune checkpoint blocking peptides. Supra‐BiCE creates artificial connections between NK/T cells with tumor cells as well as blocking both check points, thus increasing infiltration and activation of NK and T cells at tumor site and boosting tumor inhibition rate.
ISSN:0935-9648
1521-4095
DOI:10.1002/adma.202306736