Method for preparing swine O-type foot-and-mouth disease synthetic peptide antigen 2600 by solid-phase fragment method
A technology for foot-and-mouth disease and synthetic peptides, which is applied to peptide preparation methods, chemical instruments and methods, and peptides, and can solve problems such as incomplete core sequences, pollution, and unreachable yields.
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Embodiment 1
[0069] This embodiment relates to the preparation of SEQ ID No: 3 modified by 9-fluorenylmethoxycarbonyl at the amino end, comprising the following steps:
[0070] (1) Preparation of Fmoc-Pro-2-chlororityl resin
[0071] Weigh 100g of 2-chlororityl resin (100-200 mesh, 1.1mmol / g, 110mmol) into the EST-50 polypeptide synthesizer, swell with 1L of DCM for 30min, filter to dryness, add 1L to dissolve 37.1g of Fmoc-Pro- OH (110mmol) and 14.2g of DIEA (18.7ml, 110mmol of DCM solution, react at 20-25°C for 60min. Filter to dryness, add 1L of MeOH / DIEA (9:1) solution for blocking reaction for 30min, after filtration, the resins are sequentially Wash several times with NMP, MeOH, and NMP, and drain to obtain Fmoc-Pro-2-chlororityl resin. Take a small amount of resin and wash it several times with MeOH to measure the load by removing Fmoc method, and the measured load is 0.70mmol / g .
[0072] (2) Preparation of Fmoc-Leu-Pro-2-chlorotrityl resin
[0073] Add 1L of 20% piperidine / NMP ...
Embodiment 2
[0079] This embodiment relates to the preparation of SEQ ID No: 4 modified by 9-fluorenylmethoxycarbonyl at the amino end, comprising the following steps:
[0080] (1) Preparation of Fmoc-Pro-2-chlororityl resin
[0081] Weigh 100g of 2-chlororityl resin (100-200 mesh, 1.1mmol / g, 110mmol) into the EST-50 polypeptide synthesizer, swell with 1L of DCM for 30min, filter to dryness, add 1L to dissolve 37.1g of Fmoc-Pro- OH (110mmol) and 14.2g of DIEA (18.7ml, 110mmol) in DCM were reacted at 20-25°C for 60min. After filtering to dryness, add 1L of MeOH / DIEA (9:1) solution to carry out blocking reaction for 30min. After filtering, the resin was washed several times with NMP, MeOH, and NMP in turn, and then drained to obtain Fmoc-Pro-2-chlorotrityl resin. Take a small amount of resin and wash it several times with MeOH to measure the loading by removing Fmoc method, and the measured loading is 0.70mmol / g.
[0082] (2) Preparation of Fmoc-Thr(tBu)-Pro-2-chlorotrityl resin
[0083] ...
Embodiment 3
[0089] This embodiment relates to the preparation of SEQ ID No: 5 modified by 9-fluorenylmethoxycarbonyl at the amino end, comprising the following steps:
[0090] (1) Preparation of Fmoc-Gly-2-chlororityl resin
[0091] Weigh 100g of 2-chlororityl resin (100-200 mesh, 1.1mmol / g, 110mmol) into the EST-50 peptide synthesizer, swell with 1L of DCM for 30min, filter to dryness, add 1L to dissolve 32.7g of Fmoc-Gly- OH (110mmol) and 14.2g of DIEA (18.7ml, 110mmol) in DCM were reacted at 20-25°C for 60min. After filtering to dryness, add 1L of MeOH / DIEA (9:1) solution for blocking reaction for 30min. After filtering, the resin was washed several times with NMP, MeOH, and NMP in sequence, and then drained to obtain Fmoc-Gly-2-chlorotrityl resin. Take a small amount of resin and wash it several times with MeOH to measure the loading by removing Fmoc method, and the measured loading is 0.65mmol / g.
[0092] (2) Preparation of Fmoc-Arg(Pbf)-Gly-2-chlorotrityl resin
[0093] Add 1L of...
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