Please use this identifier to cite or link to this item: doi:10.22028/D291-43610
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Title: Synthetic intracellular nanostructures enhance cytotoxic T cell function via 2 assembly-driven chemical engineering
Author(s): Chagri, Sarah
Burgstaller, Anna
Schirra, Claudia
Link, Julian
Zhou, Zhixuan
Wenderoth, Patrick
Meyer, Raphael
Fetzer, Jana
Ren, Yong
Si, Shutian
Mazzotta, Francesca
Wagner, Manfred
Lieberwirth, Ingo
Landfester, Katharina
Ng, David Y. W.
Staufer, Oskar
Weil, Tanja
Language: English
Publisher/Platform: ChemRxiv
Year of Publication: 2024
Free key words: T cells
Intracellular nanostructures
Peptide self-assembly
DDC notations: 540 Chemistry
Publikation type: Other
Abstract: Nature achieves diverse biological functions through structure formation. Inspired by the controlled formation of polypeptide nanostructures in cells, synthetic methods have been developed to assemble artificial nanostructures and organelle-like compartments within living cells. While these synthetic intracellular assemblies have mostly been used to disrupt cellular processes, their potential to induce a gain of function within cells remains unexplored. Here, we introduce redox-sensitive isopeptides that transform into self-assembling linear peptides inside human cytotoxic T cells in response to intracellular levels of glutathione. The in situ formation of synthetic peptide nanostructures in cytotoxic T cells leads to cellular stiffening, establishing a direct interface between biochemically driven peptide assembly and mechanobiological effects. This change in biophysical properties, along with increased phosphorylation of signaling proteins associated with T cell activation, correlates with a significant enhancement in the efficacy of cytotoxic T cells to eliminate cancer cells. Our findings elucidate the cellular impact of synthetic peptide nanostructures assembled within living cytotoxic T cells and demonstrate their ability to modulate and enhance effector immune cell responses.
DOI of the first publication: 10.26434/chemrxiv-2024-3lxgk
URL of the first publication: https://chemrxiv.org/engage/chemrxiv/article-details/66fa4e6c12ff75c3a1eabf18
Link to this record: urn:nbn:de:bsz:291--ds-436109
hdl:20.500.11880/39077
http://dx.doi.org/10.22028/D291-43610
Date of registration: 2-Dec-2024
Notes: Preprint
Faculty: NT - Naturwissenschaftlich- Technische Fakultät
Department: NT - Chemie
Professorship: NT - Keiner Professur zugeordnet
Collections:SciDok - Der Wissenschaftsserver der Universität des Saarlandes

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