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Structure-guided engineering of tick evasins for targeting chemokines in inflammatory diseases.


ABSTRACT: As natural chemokine inhibitors, evasin proteins produced in tick saliva are potential therapeutic agents for numerous inflammatory diseases. Engineering evasins to block the desired chemokines and avoid off-target side effects requires structural understanding of their target selectivity. Structures of the class A evasin EVA-P974 bound to human CC chemokine ligands 7 and 17 (CCL7 and CCL17) and to a CCL8-CCL7 chimera reveal that the specificity of class A evasins for chemokines of the CC subfamily is defined by conserved, rigid backbone-backbone interactions, whereas the preference for a subset of CC chemokines is controlled by side-chain interactions at four hotspots in flexible structural elements. Hotspot mutations alter target preference, enabling inhibition of selected chemokines. The structure of an engineered EVA-P974 bound to CCL2 reveals an underlying molecular mechanism of EVA-P974 target preference. These results provide a structure-based framework for engineering evasins as targeted antiinflammatory therapeutics.

SUBMITTER: Bhusal RP 

PROVIDER: S-EPMC8892493 | biostudies-literature | 2022 Mar

REPOSITORIES: biostudies-literature

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Structure-guided engineering of tick evasins for targeting chemokines in inflammatory diseases.

Bhusal Ram Prasad RP   Aryal Pramod P   Devkota Shankar Raj SR   Pokhrel Rina R   Gunzburg Menachem J MJ   Foster Simon R SR   Lim Herman D HD   Payne Richard J RJ   Wilce Matthew C J MCJ   Stone Martin J MJ  

Proceedings of the National Academy of Sciences of the United States of America 20220301 9


As natural chemokine inhibitors, evasin proteins produced in tick saliva are potential therapeutic agents for numerous inflammatory diseases. Engineering evasins to block the desired chemokines and avoid off-target side effects requires structural understanding of their target selectivity. Structures of the class A evasin EVA-P974 bound to human CC chemokine ligands 7 and 17 (CCL7 and CCL17) and to a CCL8-CCL7 chimera reveal that the specificity of class A evasins for chemokines of the CC subfam  ...[more]

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