Dilly, J. J., Morgan, A. L., Bedding, M., Low, J., Mackay, J., Conibear, A. C., Bhusal, R. P., Stone, M. J., Franck, C. K. M., & Payne, R. J. (2024). Tyrosine Sulfation Modulates the Binding Affinity of Chemokine-Targeting Nanobodies. ACS Chemical Biology, 19(7), 1426–1432. https://doi.org/10.1021/acschembio.4c00230
E163-03-2 - Forschungsgruppe Molekulare Chemie und Chemische Biologie
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Journal:
ACS Chemical Biology
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ISSN:
1554-8929
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Date (published):
19-Jul-2024
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Number of Pages:
7
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Publisher:
AMER CHEMICAL SOC
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Peer reviewed:
No
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Keywords:
Humans; Protein Binding; Sulfates; Tyrosine; Single-Domain Antibodies; Chemokines
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Abstract:
Chemokines are an important family of small proteins integral to leukocyte recruitment during inflammation. Dysregulation of the chemokine-chemokine receptor axis is implicated in many diseases, and both chemokines and their cognate receptors have been the targets of therapeutic development. Analysis of the antigen-binding regions of chemokine-binding nanobodies revealed a sequence motif suggestive of tyrosine sulfation. Given the well-established importance of post-translational tyrosine sulfation of receptors for chemokine affinity, it was hypothesized that the sulfation of these nanobodies may contribute to chemokine binding and selectivity. Four nanobodies (16C1, 9F1, 11B1, and 11F2) were expressed using amber codon suppression to incorporate tyrosine sulfation. The sulfated variant of 16C1 demonstrated significantly improved chemokine binding compared to the non-sulfated counterpart, while the other nanobodies displayed equipotent or reduced affinity upon sulfation. The ability of tyrosine sulfation to modulate chemokine binding, both positively and negatively, could be leveraged for chemokine-targeted sulfo-nanobody therapeutics in the future.
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Project title:
Erweiterung des Zugangs zu modifizierten Proteinen über eine neuartige halbsynthetische Plattform: DP220101037 (Australian Research Council)
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Research Areas:
Biological and Bioactive Materials: 60% Structure-Property Relationsship: 40%