| 发明名称 |
Recombinant toxin fragments |
| 摘要 |
A single polypeptide is provided which comprises first and second domains. The first domain enables the polypeptide to cleave one or more vesicle or plasma-membrane associated proteins essential to exocytosis, and the second domain enables the polypeptide to be translocated into a target cell or increases the solubility of the polypeptide, or both. The polypeptide thus combines useful properties of a clostridial toxin, such as a botulinum or tetanus toxin, without the toxicity associated with the natural molecule. The polypeptide can also contain a third domain that targets it to a specific cell, rendering the polypeptide useful in inhibition of exocytosis in target cells. Fusion proteins comprising the polypeptide, nucleic acids encoding the polypeptide and methods of making the polypeptide are also provided. Controlled activation of the polypeptide is possible and the polypeptide can be incorporated into vaccines and toxin assays.
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| 申请公布号 |
US2003166238(A1) |
申请公布日期 |
2003.09.04 |
| 申请号 |
US20020241596 |
申请日期 |
2002.09.12 |
| 申请人 |
MICROBIOLOGICAL RESEARCH AUTHORITY AND THE SPEYWOOD LABORATORY LIMITED |
发明人 |
SHONE CLIFFORD CHARLES;QUINN CONRAD PADRAIG;FOSTER KEITH ALAN;CHADDOCK JOHN;MARKS PHILIP;SUTTON J. MARK;STANCOMBE PATRICK;WAYNE JONATHAN |
| 分类号 |
C12N15/09;A61K;A61K38/00;A61K38/16;A61K39/00;A61K39/08;A61K47/48;A61K48/00;A61P31/04;C07K14/33;C07K14/65;C07K19/00;C12N1/19;C12N1/21;C12N5/10;C12N9/52;C12N15/31;C12N15/62;C12P21/02;C12P21/04;C12R1/145;C12R1/19;(IPC1-7):C12N9/50;C07H21/04 |
主分类号 |
C12N15/09 |
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