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Solution synthesis of a biologically active fragment (33–41) of thymosin β9

✍ Scribed by Kalbacher, Hubert ;Jahan, Meeno ;Mihelić, Mirna ;Zaman, Fakhar ;Voelter, Wolfgang


Publisher
John Wiley and Sons
Year
1990
Tongue
English
Weight
423 KB
Volume
1990
Category
Article
ISSN
0947-3440

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✦ Synopsis


Abstract

The C‐terminal fragment 33–41 of thymosin β~9~ is synthesized by solution synthesis, using the strategy of maximum side‐chain protection with acid‐labile tert‐butyl groups and temporary N^α^‐benzyloxycarbonyl protection during the elongation steps. Part of this peptide is deprotected, coupled to KLH and the conjugate used for the production of antibodies. The biological activities of two fragments and of the nonapeptide are tested in our α‐amanitin‐inhibited E‐rosette assay.


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