Sains Malaysiana 50(9)(2021): 2603-2614
http://doi.org/10.17576/jsm-2021-5009-09
Synthesis, Molecular Docking and
Tyrosinase Inhibitory Activity of the Decorated Methoxy Sulfonamide Chalcones: in
vitro Inhibitory Effects and the
Possible Binding Mode
(Sintesis, Penyambungan Molekul dan Aktiviti
Perencatan Tirosinase dari Metoksi Sulfonamida Kalkon: Kesan Perencatan in
vitro dan Mod Pengikatan Mungkin)
THAWANRAT
KOBKEATTHAWIN1, SUCHADA CHANTRAPROMMA1*, THITIPONE
SUWUNWONG2, LYDIA RHYMAN3,4, YEE SIEW CHOONG5 &
PONNADURAI RAMASAMI3,4
1Division of Physical Science, Faculty of
Science, Prince of Songkla University, Songkhla
90110, Thailand
2School of Science, Mae Fah Luang University, Chiang Rai 57100, Thailand
3Computational Chemistry Group, Department
of Chemistry, Faculty of Science, University of Mauritius, Réduit 80837, Mauritius
4Centre for Natural Product Research,
Department of Chemical Sciences,
University of Johannesburg
Doornfontein Campus, Johannesburg 2028, South Africa
5Computational Institute for Research in
Molecular Medicine (INFORMM), Universiti Sains Malaysia, USM 11800, Malaysia
Diserahkan: 17 Mei 2020/Diterima: 13 Januari 2021
ABSTRACT
In this
study, a series of sulfonamide chalcones derivatives was synthesized and its
chemical structures were confirmed by spectral characteristics. The
synthesized compounds were evaluated for their tyrosinase inhibitory activities
along with molecular docking study. The
tyrosinase inhibitory results indicated that compounds 5b, 5c, 5f, 5g and 5h
displayed the significant tyrosinase inhibitory activity and comparable to the
standard drug (kojic acid). Compound 5c exhibits the most potent tyrosinase
inhibition among the synthesized compounds with IC50 = 0.43±0.07
mM, L-DOPA as the substrate, and better than that of the standard kojic
acid (IC50 = 0.60±0.20
mM). Molecular docking studies showed that the
binding mode of some compounds is in the tyrosinase binding pocket surrounding
the copper in the active site. The
correlation between the docking results with IC50 values showed that
the binding mode prediction of the test compounds would also be convincing. This
comprehensive study allows for a possible mechanism for the antityrosinase
activity of the sulfonamide chalcones. These
sulfonamide chalcones bind to copper atoms of tyrosinase which responsible for the catalytic
activity of tyrosinase. These compounds may be used as a lead for
rational drug designing for the multi-functional tyrosinase inhibitor.
Keywords: Binding mode; molecular docking; sulfonamide chalcones; tyrosinase inhibitor
ABSTRAK
Dalam kajian ini, satu siri terbitan sulfonamida kalkon disintesis dan struktur kimianya disahkan oleh pencirian spektrum. Sebatian yang disintesis dinilai untuk aktiviti penghambatan tirosinasenya bersama dengan kajian mengedok molekul. Hasil perencatan tirosinase menunjukkan bahawa sebatian 5b, 5c, 5f, 5g
dan 5h menunjukkan aktiviti penghambatan tirosinase yang signifikan dan setanding dengan ubat piawai (asid kojik). Sebatian 5c menunjukkan perencatan tirosinase yang paling kuat antara sebatian yang disintesis dengan IC50 = 0.43 ± 0.07 mM, L-DOPA sebagai substrat dan lebih baik daripada asid kojik piawai (IC50 = 0.60 ± 0.20 mM). Kajian mengedok molekul menunjukkan bahawa kaedah pengikatan sebilangan sebatian terdapat di dalam poket pengikat tirosinase yang mengelilingi tembaga di tapak aktif. Hubungan antara hasil dok dengan nilai IC50 menunjukkan bahawa ramalan mod pengikat sebatian ujian juga akan meyakinkan. Kajian komprehensif ini memungkinkan adanya mekanisme untuk aktiviti anti-tirosinase sulfonamida kalkon. Kalkon sulfonamida ini mengikat atom tembaga tirosinase yang bertanggungjawab untuk aktiviti pemangkin tirosinase. Sebatian ini boleh digunakan sebagai petunjuk untuk mereka bentuk ubat yang rasional untuk perencat tirosinase pelbagai fungsi.
Kata kunci: Dok molekul;
mod pengikat; perencat tirosinase; sulfonamida kalkon
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*Pengarang untuk surat-menyurat; email:
suchada.c@psu.ac.th
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