–9.1
–7.2
–7.6
–8.5
–9.3
G-6-O-CH
2
COOH
–7.4
–7.5
–8.0
–8.2
–8.7
G-6,6
-O-di-CH
2
COOH
–7.3
–7.5
–7.5
–8.0
–8.9
G-6-O-CH
2
CONH
2
–8.7
–7.3
–7.8
–8.5
–9.1
G-6,6
-di-O-CH
2
CONH
2
–7.5
–7.3
–7.6
–8.1
–8.9
The 3D structures of the proteins (or enzymes) EGFR (transferase/transferase
inhibitor, PDB ID: 4RJ8 with resolution of 2.50 Å), HNE (hydrolase, ID: 1H1B, 2.00
Å) and MMP 2 (gelatinase, ID: 1QIB, 2.80 Å), MMP 9 (hydrolase/hydrolase inhibitor,
ID: 4H1Q, 1.59 Å) and Tyrosinase (oxidoreductase, ID: 2Y9W, 2.30 Å) were
downloaded from Protein Data Bank (PDB) server.
In conclusion, gossypol derivatives have shown potential to dock with all the five
selected proteins. The present docking investigation has shown mono-substituted alkyl
derivatives of gossypol are exhibited lower (stronger binding) energy for selected
enzymes than di-substituted derivatives. Gossypol exhibits lower (stronger binding)
energy then its
O
6-mono- and
O
6,
O
6
-di-alkyl derivatives, exception for HNE (1H1B).
References:
1. Y. Wang, H. Lai, X. Fan, L. Luo, F. Duan, Z. Jiang, Q. Wang, E.L.H. Leung, L.
Liu, and X. Yao.
Front. Pharmacol
., 2018,
9
, 728.
2. V. Ragavan, A. Ramesh, and R. Narayanaswamy.
Rasayan J. Chem.
, 2020,
13(1)
,
469–475.
Poster presentation
152
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