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PDBsum entry 7bs7
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PDB id:
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Hydrolase
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Title:
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Bovine pancreatic trypsin with aniline (cryo)
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Structure:
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Cationic trypsin. Chain: a. Synonym: beta-trypsin. Ec: 3.4.21.4
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Source:
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Bos taurus. Bovine. Organism_taxid: 9913
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Resolution:
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1.04Å
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R-factor:
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0.159
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R-free:
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0.169
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Authors:
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M.Maeki,S.Ito,R.Takeda,T.Funakubo,G.Ueno,A.Ishida,H.Tani,M.Yamamoto, M.Tokeshi
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Key ref:
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M.Maeki
et al.
(2020).
Room-temperature crystallography using a microfluidic protein crystal array device and its application to protein-ligand complex structure analysis.
Chem Sci,
11,
9072-9087.
PubMed id:
DOI:
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Date:
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30-Mar-20
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Release date:
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26-Aug-20
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PROCHECK
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Headers
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References
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P00760
(TRY1_BOVIN) -
Serine protease 1 from Bos taurus
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Seq:
Struc:
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246 a.a.
223 a.a.
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Key: |
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PfamA domain |
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Secondary structure |
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Enzyme class:
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E.C.3.4.21.4
- trypsin.
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Reaction:
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Preferential cleavage: Arg-|-Xaa, Lys-|-Xaa.
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DOI no:
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Chem Sci
11:9072-9087
(2020)
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PubMed id:
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Room-temperature crystallography using a microfluidic protein crystal array device and its application to protein-ligand complex structure analysis.
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M.Maeki,
S.Ito,
R.Takeda,
G.Ueno,
A.Ishida,
H.Tani,
M.Yamamoto,
M.Tokeshi.
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ABSTRACT
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Room-temperature (RT) protein crystallography provides significant information
to elucidate protein function under physiological conditions. In particular,
contrary to typical binding assays, X-ray crystal structure analysis of a
protein-ligand complex can determine the three-dimensional (3D) configuration of
its binding site. This allows the development of effective drugs by
structure-based and fragment-based (FBDD) drug design. However, RT
crystallography and RT crystallography-based protein-ligand complex analyses
require the preparation and measurement of numerous crystals to avoid the X-ray
radiation damage. Thus, for the application of RT crystallography to
protein-ligand complex analysis, the simultaneous preparation of protein-ligand
complex crystals and sequential X-ray diffraction measurement remain
challenging. Here, we report an RT crystallography technique using a
microfluidic protein crystal array device for protein-ligand complex structure
analysis. We demonstrate the microfluidic sorting of protein crystals into
microwells without any complicated procedures and apparatus, whereby the sorted
protein crystals are fixed into microwells and sequentially measured to collect
X-ray diffraction data. This is followed by automatic data processing to
calculate the 3D protein structure. The microfluidic device allows the
high-throughput preparation of the protein-ligand complex solely by the
replacement of the microchannel content with the required ligand solution. We
determined eight trypsin-ligand complex structures for the proof of concept
experiment and found differences in the ligand coordination of the corresponding
RT and conventional cryogenic structures. This methodology can be applied to
easily obtain more natural structures. Moreover, drug development by FBDD could
be more effective using the proposed methodology.
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