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The contacting details of the individual residues involved in binding were shown in Figure 6.
PER-dependent rhythms of CLK phosphorylation and E-box binding were shown in Drosophila, and PER-DBT (doubletime kinase) interaction is required for the transcriptional repression process.
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The MDs involved in DnaK binding are shown in green, and those that cannot bind to DnaK are shown in red.
A brief summary of reagents used and the general effects on immune complex binding is shown in Table 1.
The linkage for a model-free binding and a model-dependent binding is shown in Figure 5, where the relationship of macroscopic (stepwise or stoichimetric) binding constants (K1 and K2), overall binding constants (β1 and β2) and microscopic association biding constants, KI and KII is shown.
Representative titrations for SRC-1 NR2 binding are shown in Figure S3.
Physiological relevance of TIRC7 and HLA-DR α2 binding is shown in acute inflammatory setting in vivo after LPS.
The sensorgrams and the kinetic data of the binding are shown in Fig. 3 and Table S4, respectively.
The geometry of PA-CD4 with a highest score is shown in Figure 1A, and crystal structure of gp120-CD4 (PDB code 1GC1) binding is shown in Figure 1B.
The key residues involved in the pyridine ring binding are shown in red.
Surfaces involved in RNA and P binding are shown in purple and green, respectively.
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