Novel four-disulfide insulin analog with high aggregation stability and potency† †Electronic supplementary information (ESI) available: Detailed synthesis procedure and mass spectrometry data along with biological experiment protocol. See DOI: 10.1039/c9sc04555d

A novel four-disulfide insulin analog was designed with retained bioactivity and increased fibrillation stability. Although insulin was first purified and used therapeutically almost a century ago, there is still a need to improve therapeutic efficacy and patient convenience. A key challenge is the...

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Veröffentlicht in:Chemical science (Cambridge) 2019-11, Vol.11 (1), p.195-200
Hauptverfasser: Xiong, Xiaochun, Blakely, Alan, Karra, Prasoona, VandenBerg, Michael A., Ghabash, Gabrielle, Whitby, Frank, Zhang, Yi Wolf, Webber, Matthew J., Holland, William L., Hill, Christopher P., Chou, Danny Hung-Chieh
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Sprache:eng
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Zusammenfassung:A novel four-disulfide insulin analog was designed with retained bioactivity and increased fibrillation stability. Although insulin was first purified and used therapeutically almost a century ago, there is still a need to improve therapeutic efficacy and patient convenience. A key challenge is the requirement for refrigeration to avoid inactivation of insulin by aggregation/fibrillation. Here, in an effort to mitigate this problem, we introduced a 4 th disulfide bond between a C-terminal extended insulin A chain and residues near the C-terminus of the B chain. Insulin activity was retained by an analog with an additional disulfide bond between residues A22 and B22, while other linkages tested resulted in much reduced potency. Furthermore, the A22-B22 analog maintains the native insulin tertiary structure as demonstrated by X-ray crystal structure determination. We further demonstrate that this four-disulfide analog has similar in vivo potency in mice compared to native insulin and demonstrates higher aggregation stability. In conclusion, we have discovered a novel four-disulfide insulin analog with high aggregation stability and potency.
ISSN:2041-6520
2041-6539
DOI:10.1039/c9sc04555d