Your search keyword '"Kang, Dongwan"' showing total 18 results

1. Investigation of the Efficacy of Benzylidene-3-methyl-2-thioxothiazolidin-4-one Analogs with Antioxidant Activities on the Inhibition of Mushroom and Mammal Tyrosinases.

Author

Kim, Hye Jin, Jung, Hee Jin, Kim, Young Eun, Jeong, Daeun, Park, Hyeon Seo, Park, Hye Soo, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Chung, Hae Young, and Moon, Hyung Ryong

Subjects

PHENOL oxidase, MUSHROOMS, ANTIOXIDANTS, MAMMALS, DOPA, BINDING sites, MELANINS

Abstract

Based on the fact that substances with a β-phenyl-α,β-unsaturated carbonyl (PUSC) motif confer strong tyrosinase inhibitory activity, benzylidene-3-methyl-2-thioxothiazolidin-4-one (BMTTZD) analogs 1–8 were prepared as potential tyrosinase inhibitors. Four analogs (1–3 and 5) inhibited mushroom tyrosinase strongly. Especially, analog 3 showed an inhibitory effect that was 220 and 22 times more powerful than kojic acid in the presence of l-tyrosine and l-dopa, respectively. A kinetic study utilizing mushroom tyrosinase showed that analogs 1 and 3 competitively inhibited tyrosinase, whereas analogs 2 and 5 inhibited tyrosinase in a mixed manner. A docking simulation study indicated that analogs 2 and 5 could bind to both the tyrosinase active and allosteric sites with high binding affinities. In cell-based experiments using B16F10 cells, analogs 1, 3, and 5 effectively inhibited melanin production; their anti-melanogenic effects were attributed to their ability to inhibit intracellular tyrosinase activity. Moreover, analogs 1, 3, and 5 inhibited in situ B16F10 cellular tyrosinase activity. In three antioxidant experiments, analogs 2 and 3 exhibited strong antioxidant efficacy, similar to that of the positive controls. These results suggest that the BMTTZD analogs are promising tyrosinase inhibitors for the treatment of hyperpigmentation-related disorders. [ABSTRACT FROM AUTHOR]

Published

2024

2. Anti-Browning Effect of 2-Mercaptobenzo[ d ]imidazole Analogs with Antioxidant Activity on Freshly-Cut Apple Slices and Their Highly Potent Tyrosinase Inhibitory Activity.

Author

Lee, Jieun, Park, Hye Soo, Jung, Hee Jin, Park, Yu Jung, Kang, Min Kyung, Kim, Hye Jin, Yoon, Dahye, Ullah, Sultan, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Chung, Hae Young, and Moon, Hyung Ryong

Subjects

PHENOL oxidase, IMIDAZOLES, REACTIVE oxygen species, COPPER ions, CULTIVATED mushroom

Abstract

Ten 2-mercaptobenzimidazole (2-MBI) analogs were synthesized as potential tyrosinase inhibitors because mercapto-containing compounds can bind to copper ions at the active site of tyrosinase to inhibit enzyme activity. Nine 2-MBI analogs showed sub-micromolar IC50 values for mushroom tyrosinase monophenolase activity; analog 4 was 280-fold more potent than kojic acid, and in diphenolase activity, 6 was 970-fold more potent than kojic acid. The inhibition mode of the 2-MBI analogs was investigated using kinetic studies supported by docking simulations. Benzimidazoles without the 2-mercapto substituent of the 2-MBI analogs lost their tyrosinase inhibitory activity, implying that the 2-mercapto substituent plays an important role in tyrosinase inhibition. The 2-MBI analogs exerted potent antioxidant effects against 2,2′-azino-bis(3-ethylbenzothiazoline-6-sulfonic acid (ABTS), 2,2-diphenyl-1-picrylhydrazyl (DPPH), and reactive oxygen species (ROS). The results obtained from apple slices and human embryonic kidney cells (HEK-293) suggest that most 2-MBI analogs are sufficiently safe candidates to delay the browning of apple slices effectively. Thus, these results support the potential use of 2-MBI analogs as anti-browning agents in foods such as mushrooms, vegetables, and fruits. [ABSTRACT FROM AUTHOR]

Published

2023

3. Design, Synthesis, In Vitro, and In Silico Insights of 5-(Substituted benzylidene)-2-phenylthiazol-4(5 H)-one Derivatives: A Novel Class of Anti-Melanogenic Compounds.

Author

Yoon, Dahye, Kang, Min Kyung, Jung, Hee Jin, Ullah, Sultan, Lee, Jieun, Jeong, Yeongmu, Noh, Sang Gyun, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Chung, Hae Young, and Moon, Hyung Ryong

Subjects

PHENOL oxidase, COUPLING constants, RADICAL cations, RADICALS (Chemistry), WESTERN immunoblotting, MELANINS

Abstract

(Z)-5-Benzylidene-2-phenylthiazol-4(5H)-one ((Z)-BPT) derivatives were designed by combining the structural characteristics of two tyrosinase inhibitors. The double-bond geometry of trisubstituted alkenes, (Z)-BPTs 1–14, was determined based on the 3JC,Hβ coupling constant of 1H-coupled 13C NMR spectra. Three (Z)-BPT derivatives (1–3) showed stronger tyrosinase inhibitory activities than kojic acid; in particular, 2 was to be 189-fold more potent than kojic acid. Kinetic analysis using mushroom tyrosinase indicated that 1 and 2 were competitive inhibitors, whereas 3 was a mixed-type inhibitor. The in silico results revealed that 1–3 could strongly bind to the active sites of mushroom and human tyrosinases, supporting the kinetic results. Derivatives 1 and 2 decreased the intracellular melanin contents in a concentration-dependent manner in B16F10 cells, and their anti-melanogenic efficacy exceeded that of kojic acid. The anti-tyrosinase activity of 1 and 2 in B16F10 cells was similar to their anti-melanogenic effects, suggesting that their anti-melanogenic effects were primarily owing to their anti-tyrosinase activity. Western blotting of B16F10 cells revealed that the derivatives 1 and 2 inhibited tyrosinase expression, which partially contributes to their anti-melanogenic ability. Several derivatives, including 2 and 3, exhibited potent antioxidant activities against ABTS cation radicals, DPPH radicals, ROS, and peroxynitrite. These results suggest that (Z)-BPT derivatives 1 and 2 have promising potential as novel anti-melanogenic agents. [ABSTRACT FROM AUTHOR]

Published

2023

4. Design and Synthesis of (Z)-2-(Benzylamino)-5-benzylidenethiazol-4(5 H)-one Derivatives as Tyrosinase Inhibitors and Their Anti-Melanogenic and Antioxidant Effects.

Author

Lee, Jieun, Park, Yu Jung, Jung, Hee Jin, Ullah, Sultan, Yoon, Dahye, Jeong, Yeongmu, Kim, Ga Young, Kang, Min Kyung, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Chung, Hae Young, and Moon, Hyung Ryong

Subjects

PHENOL oxidase, MICROPHTHALMIA-associated transcription factor, MELANINS, PROTEIN expression

Abstract

In this study, (Z)-2-(benzylamino)-5-benzylidenethiazol-4(5H)-one (BABT) derivatives were designed as tyrosinase inhibitors based on the structure of MHY2081, using a simplified approach. Of the 14 BABT derivatives synthesized, two derivatives ((Z)-2-(benzylamino)-5-(3-hydroxy-4-methoxybenzylidene)thiazol-4(5H)-one [7] and (Z)-2-(benzylamino)-5-(2,4-dihydroxybenzylidene)thiazol-4(5H)-one [8]) showed more potent mushroom tyrosinase inhibitory activities than kojic acid, regardless of the substrate used; in particular, compound 8 was 106-fold more potent than kojic acid when l-tyrosine was used as the substrate. Analysis of Lineweaver–Burk plots for 7 and 8 indicated that they were competitive inhibitors, which was confirmed via in silico docking. In experiments using B16F10 cells, 8 exerted a greater ability to inhibit melanin production than kojic acid, and it inhibited cellular tyrosinase activity in a concentration-dependent manner, indicating that the anti-melanogenic effect of 8 is attributable to its ability to inhibit tyrosinase. In addition, 8 exhibited strong antioxidant activity to scavenge 2,2-diphenyl-1-picrylhydrazyl and 2,2′-azino-bis(3-ethylbenzothiazoline-6-sulfonic acid) radicals and peroxynitrite and inhibited the expression of melanogenesis-associated proteins (tyrosinase and microphthalmia-associated transcription factor). These results suggest that BABT derivative 8 is a promising candidate for the treatment of hyperpigmentation-related diseases, owing to its inhibition of melanogenesis-associated protein expression, direct tyrosinase inhibition, and antioxidant activity. [ABSTRACT FROM AUTHOR]

Published

2023

5. Design and Synthesis of (Z)-5-(Substituted benzylidene)-3-cyclohexyl-2-thioxothiazolidin-4-one Analogues as Anti-Tyrosinase and Antioxidant Compounds: In Vitro and In Silico Insights.

Author

Ko, Jeongin, Lee, Jieun, Jung, Hee Jin, Ullah, Sultan, Jeong, Yeongmu, Hong, Sojeong, Kang, Min Kyung, Park, Yu Jung, Hwang, YeJi, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Yoo, Jin-Wook, Chung, Hae Young, and Moon, Hyung Ryong

Subjects

MELANINS, PHENOL oxidase, PROTEIN expression, FUNCTIONAL groups, ANTIOXIDANTS, STEREOCHEMISTRY

Abstract

Many compounds containing the β-phenyl-α,β-unsaturated carbonyl (PUSC) scaffold, including cinnamamide derivatives, have been shown to inhibit tyrosinase potently in vitro and in vivo. Structural changes to cinnamamide derivatives were produced by adding a dithionate functional group to provide eight (Z)-5-(substituted benzylidene)-3-cyclohexyl-2-thioxothiazolidin-4-one analogs with high log p values for skin. These analogs were synthesized using a two-step reaction, and their stereochemistry was confirmed using the 3JC4-Hβ values of C4 measured in proton-coupled 13C mode. Analogs 2 (IC50 = 5.21 ± 0.86 µM) and 3 (IC50 = 1.03 ± 0.14 µM) more potently inhibited mushroom tyrosinase than kojic acid (IC50 = 25.26 ± 1.10 µM). Docking results showed 2 binds strongly to the active site of tyrosinase, while 3 binds strongly to an allosteric site. Kinetic studies using l-tyrosine as substrate indicated 2 and 3 competitively and non-competitively inhibit tyrosinase, respectively, which was supported by our docking results. In B16F10 cells, 3 significantly and concentration-dependently reduced α–MSH plus IBMX induced increases in cellular tyrosinase activity and melanin production and the similarity between these inhibitory patterns implied that the anti-melanogenic effect of 3 might be due to its tyrosinase-inhibitory ability. In addition, 2 and 3 exhibited strong antioxidant effects; for example, they reduced ROS and ONOO– levels and exhibited radical scavenging activities, suggesting that these effects might underlie their anti-melanogenic effects. Furthermore, 3 suppressed the expressions of melanogenesis-associated proteins and genes in B16F10 cells. These results suggest (Z)-5-(substituted benzylidene)-3-cyclohexyl-2-thioxothiazolidin-4-one analogs offer a means of producing novel anti-melanogenesis agents. [ABSTRACT FROM AUTHOR]

Published

2022

6. Urolithin and Reduced Urolithin Derivatives as Potent Inhibitors of Tyrosinase and Melanogenesis: Importance of the 4-Substituted Resorcinol Moiety.

Author

Lee, Sanggwon, Choi, Heejeong, Park, Yujin, Jung, Hee Jin, Ullah, Sultan, Choi, Inkyu, Kang, Dongwan, Park, Chaeun, Ryu, Il Young, Jeong, Yeongmu, Hwang, YeJi, Hong, Sojeong, Chun, Pusoon, and Moon, Hyung Ryong

Subjects

PHENOL oxidase, RESORCINOL, MELANOGENESIS, MOIETIES (Chemistry), HUMAN skin color, HYDROXYL group

Abstract

We previously reported (E)-β-phenyl-α,β-unsaturated carbonyl scaffold ((E)-PUSC) played an important role in showing high tyrosinase inhibitory activity and that derivatives with a 4-substituted resorcinol moiety as the β-phenyl group of the scaffold resulted in the greatest tyrosinase inhibitory activity. To examine whether the 4-substituted resorcinol moiety could impart tyrosinase inhibitory activity in the absence of the α,β-unsaturated carbonyl moiety of the (E)-PUSC scaffold, 10 urolithin derivatives were synthesized. To obtain more candidate samples, the lactone ring in synthesized urolithins was reduced to produce nine reduced urolithins. Compounds 1c (IC50 = 18.09 ± 0.25 μM), 1h (IC50 = 4.14 ± 0.10 μM), and 2a (IC50 = 15.69 ± 0.40 μM) had greater mushroom tyrosinase-inhibitory activities than kojic acid (KA) (IC50 = 48.62 ± 3.38 μM). The SAR results suggest that the 4-substituted resorcinol motif makes an important contribution to tyrosinase inhibition. To investigate whether these compounds bind to human tyrosinase, a human tyrosinase homology model was developed. Docking simulations with mushroom and human tyrosinases showed that 1c, 1h, and 2a bind to the active site of both tyrosinases with higher binding affinities than KA. Pharmacophore analyses showed that two hydroxyl groups of the 4-substituted resorcinol entity act as hydrogen bond donors in both mushroom and human tyrosinases. Kinetic analyses indicated that these compounds were all competitive inhibitors. Compound 2a inhibited cellular tyrosinase activity and melanogenesis in α-MSH plus IBMX-stimulated B16F10 melanoma cells more strongly than KA. These results suggest that 2a is a promising candidate for the treatment of skin pigment disorders, and show the 4-substituted resorcinol entity importantly contributes to tyrosinase inhibition. [ABSTRACT FROM AUTHOR]

Published

2021

7. Evaluation of the Novel Synthetic Tyrosinase Inhibitor (Z)-3-(3-bromo-4-hydroxybenzylidene)thiochroman-4-one (MHY1498) In Vitro and In Silico.

Author

Bang, EunJin, Noh, Sang-Gyun, Ha, Sugyeong, Jung, Hee Jin, Kim, Dae Hyun, Lee, A Kyoung, Hyun, Min Kyung, Kang, Dongwan, Lee, Sanggwon, Park, Chaeun, Moon, Hyung Ryong, and Chung, Hae Young

Subjects

PHENOL oxidase, MELANOGENESIS, BIOSYNTHESIS, SKIN diseases, MELANOMA treatment, BENZYLIDENE compounds, CHEMICAL structure

Abstract

Tyrosinase is a key enzyme in melanin synthesis, catalyzing the initial rate-limiting steps of melanin synthesis. Abnormal and excessive melanin synthesis is the primary cause of serious skin disorders including melasma, senile lentigo, freckles, and age spots. In attempts to find potent and safe tyrosinase inhibitors, we designed and synthesized a novel compound, (Z)-3-(3-bromo-4-hydroxybenzylidene)thiochroman-4-one (MHY1498), and evaluated its tyrosinase inhibitory activity in vitro and in silico. The chemical structures of (Z)-3-benzylidenethiochroman-4-one analogues, including the novel compound MHY1498, were rationally designed and synthesized as hybrid structures of reported potent tyrosinase inhibitors, which were confirmed both in vitro and in vivo: (Z)-5-(substituted benzylidene)thiazolidine-2,4-diones (Compound A) and 2-(substituted phenyl)benzo[d]thiazoles (Compound B). During screening, MHY1498 showed a strong dose-dependent inhibitory effect on mushroom tyrosinase. The IC50 value of MHY1498 (4.1 ± 0.6 μM) was significantly lower than that of the positive control, kojic acid (22.0 ± 4.7 μM). In silico molecular multi-docking simulation and inhibition mechanism studies indicated that MHY1498 interacts competitively with the tyrosinase enzyme, with greater affinity for the active site of tyrosinase than the positive control. Furthermore, in B16F10 melanoma cells treated with α-melanocyte-stimulating hormone, MHY1498 suppressed both melanin production and tyrosinase activity. In conclusion, our data demonstrate that MHY1498, a synthesized novel compound, effectively inhibits tyrosinase activity and has potential for treating hyperpigmentation and related disorders. [ABSTRACT FROM AUTHOR]

Published

2018

8. A Potent Tyrosinase Inhibitor, (E)-3-(2,4-Dihydroxyphenyl)-1-(thiophen-2-yl)prop-2-en-1-one, with Anti-Melanogenesis Properties in α-MSH and IBMX-Induced B16F10 Melanoma Cells.

Author

Kim, Chang Seok, Noh, Sang Gyun, Park, Yujin, Kang, Dongwan, Chun, Pusoon, Chung, Hae Young, Jung, Hee Jin, and Moon, Hyung Ryong

Subjects

CHALCONES, MUSHROOMS, HYDROXYLASES, ENZYME kinetics, PHENOL oxidase, HYPERPIGMENTATION, MELANINS, MOLECULAR docking

Abstract

In this study, we designed and synthesized eight thiophene chalcone derivatives (1a–h) as tyrosinase inhibitors and evaluated their mushroom tyrosinase inhibitory activities. Of these eight compounds, (E)-3-(2,4-dihydroxyphenyl)-1-(thiophen-2-yl)prop-2-en-1-one (1c) showed strong competitive inhibition activity against mushroom tyrosinase with IC50 values of 0.013 μM for tyrosine hydroxylase and 0.93 μM for dopa oxidase. In addition, we used enzyme kinetics study and docking program to further evaluate the inhibitory mechanism of 1c toward tyrosinase. As an underlying mechanism of 1c mediated anti-melanogenic effect, we investigated the inhibitory activity against melanin contents and cellular tyrosinase in B16F10 melanoma cells. As the results, the enzyme kinetics and docking results supports that 1c highly interacts with tyrosinase residues in the tyrosinase active site and it can directly inhibit tyrosinase as competitive inhibitor. In addition, 1c exhibited dose-dependent inhibitory effects in melanin contents and intracellular tyrosinase on α-MSH and IBMX-induced B16F10 cells. Overall, our results suggested that 1c might be considered potent tyrosinase inhibitor for use in the development of therapeutic agents for diseases associated with hyperpigment disorders. [ABSTRACT FROM AUTHOR]

Published

2018

9. Highly potent anti-melanogenic effect of 2-thiobenzothiazole derivatives through nanomolar tyrosinase activity inhibition.

Author

Jin Jung, Hee, Jin Kim, Hye, Soo Park, Hye, Young Kim, Ga, Jung Park, Yu, Lee, Jieun, Kyung Kang, Min, Yoon, Dahye, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Young Chung, Hae, and Ryong Moon, Hyung

Subjects

*PHENOL oxidase, *MELANINS, *MOLECULAR dynamics, *COPPER ions, *THIOLS

Abstract

[Display omitted] • 2-TBT derivatives inhibited mushroom tyrosinase with IC 50 values of 0.02–0.83 μM. • Melanin production was inhibited by their B16F10 cellular tyrosinase inhibition. • 2-TBT derivatives effectively inhibit melanogenesis in cells and zebrafish embryos. • 2-TBT derivatives mimic PTU, chelating copper ions in tyrosinase active site. • Their copper-chelating ability was demonstrated in two experiments. Compounds with sulfhydryl substituents and azole compounds exhibit potent anti-tyrosinase potency. 2-Thiobenzothiazole (2-TBT), a hybrid structure of sulfhydryl and azole, exists in two tautomeric forms, with the thione form being predominant according to several studies. 2-TBT derivatives were synthesized as potential tyrosinase inhibitors as the thione tautomeric form has the same N -C S moiety as phenylthiourea (PTU), which is suitable for chelation with the copper ions present in the tyrosinase active site. Eight of the ten 2-TBT derivatives inhibited the monophenolase and diphenolase activities of mushroom tyrosinase, with IC 50 values of 0.02–0.83 μM. Kinetic studies and molecular dynamics simulations were performed to determine their mode of action and confirm that the 2-TBT derivatives bind to the tyrosinase active site with high stability. Derivatives 3 , 4 , 8 , and 10 strongly inhibited melanogenesis in B16F10 cells in a pattern similar to the results of cellular tyrosinase inhibition, thereby suggesting that their ability to inhibit melanogenesis was due to their tyrosinase inhibitory activity. In a depigmentation experiment using zebrafish embryos, all 2-TBT derivatives showed better potency than kojic acid, even at 400 to 2000 times lower concentration, and 1 and 10 reduced zebrafish larva pigmentation more strongly than PTU even at 20 times lower concentration. Experiments investigating the changes in tyrosinase inhibitory activity of 2-TBT derivatives in the presence and absence of CuSO 4 and their copper chelating ability supported that these derivatives exert their anti-melanogenic effect by chelating the copper ions of tyrosinase. These results suggest that 2-TBT derivatives are promising candidates for the treatment of hyperpigmentation-related disorders. [ABSTRACT FROM AUTHOR]

Published

2024

10. Design, synthesis, and anti-melanogenic efficacy of 2-mercaptobenzoxazoles with nanomolar tyrosinase activity inhibition.

Author

Park, Yu Jung, Jung, Hee Jin, Kang, Min Kyung, Lee, Jieun, Yoon, Dahye, Park, Hye Soo, Jin Kim, Hye, Kim, Ga Young, Kang, Dongwan, Park, Yujin, Chung, Hae Young, and Moon, Hyung Ryong

Subjects

*PHENOL oxidase, *COPPER ions, *THIOLS, *COPPER, *CHELATING agents, *FUNCTIONAL groups, *CHELATION

Abstract

[Display omitted] • 2-MBO analogs showed stronger tyrosinase inhibition potency than phenylthiourea. • In B16F10 cells, 2-MBO analogs strongly inhibited melanin production. • Their anti-melanogenic effect was due to inhibition of cellular tyrosinase activity. • Their tyrosinase inhibitory activity was due to chelation of tyrosinase copper ions. • 2-MBO analogs are promising candidates for treating skin-pigmentation disorders. Tyrosinase is a metalloenzyme that contains copper(II) ions. We designed and synthesized eight known low-molecular-weight 2-mercaptobenzoxazole (2-MBO) analogs as tyrosinase inhibitors. Our focus was on the mercapto functional group, which interacts with copper ions. Analogs 1 – 3 exhibited mushroom tyrosinase inhibitory activity at the nanomolar level and demonstrated strong potency with extremely low half-maximal inhibitory concentration (IC 50) values of 80–90 nM for l -dopa and 100–240 nM for l -tyrosine. Analogs 2 , 4 , and 5 showed the most potent anti-melanogenic effects in B16F10 cells, and their mode of action was demonstrated by kinetic analysis. Their anti-melanogenic effects were similar to the tyrosinase inhibition results, suggesting that their anti-melanogenic effects could be attributed to their tyrosinase inhibitory ability. Experiments using copper-chelating activity assays and changes in tyrosinase inhibitory activity with and without CuSO 4 demonstrated that 2-MBO analogs inhibit tyrosinase activity by chelating the copper ions of tyrosinase. In conclusion, the 2-MBO analogs show potential as anti-melanogenic agents with potent tyrosinase inhibitory activity. [ABSTRACT FROM AUTHOR]

Published

2024

11. In vitro and in vivo anti-pigmentation effects of 2-mercaptobenzimidazoles as nanomolar tyrosinase inhibitors on mammalian cells and zebrafish embryos: Preparation of pigment-free zebrafish embryos.

Author

Yoon, Dahye, Jung, Hee Jin, Lee, Jieun, Kim, Hye Jin, Park, Hye Soo, Park, Yu Jung, Kang, Min Kyung, Kim, Ga Young, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Chung, Hae Young, and Moon, Hyung Ryong

Subjects

*PHENOL oxidase, *MELANINS, *MELANOGENESIS, *QUATERNARY structure, *AMINO acid sequence, *BRACHYDANIO, *EMBRYOS

Abstract

Recently, 10 2-mercaptobenzo[ d ]imidazole (2-MBI) compounds (1 – 10) were synthesized. Although all 2-MBI compounds are tyrosinase inhibitors that inhibit mushroom tyrosinase at extremely low concentrations (IC 50 values: 20–740 nM) and effectively inhibit the browning of apples, to our knowledge, no studies have determined whether 2-MBI compounds inhibit mammalian tyrosinase. Mammalian tyrosinase is different from mushroom tyrosinase in its distribution within the cell and has structural characteristics that are different from mushroom tyrosinase in amino acid sequence and in the presence of a quaternary structure. Thus, the effect of the 10 2-MBI compounds on mammalian tyrosinase activity was investigated in B16F10 cells. Six compounds (1 – 6) exhibited stronger intracellular tyrosinase inhibition than that of kojic acid and phenylthiourea (PTU), which are known to be the most potent tyrosinase inhibitors; their strong tyrosinase inhibitory activity robustly inhibited intracellular melanin production in B16F10 cells. None of the tested 2-MBI compounds exhibited appreciable cytotoxicity in HaCaT and B16F10 cells. To confirm the anti -melanogenic efficacy of the 2-MBI compounds in vivo , a zebrafish embryo model was used. At concentrations 100 times lower than kojic acid, most 2-MBI compounds demonstrated much stronger depigmentation efficacy than that of kojic acid, and three 2-MBI compounds (2 – 4) showed depigmentation activity similar to or more potent than that of PTU, resulting in nearly pigment-free zebrafish embryos. These results suggest that 2-MBI compounds may be potential therapeutic agents for hyperpigmentation-related disorders. [Display omitted] • 2-Mercaptobenzo[ d ]imidazole (2-MBI) derivatives (1 – 10) greatly inhibited mammalian cell tyrosinase in B16F10 cells. • Four 2-MBI derivatives inhibited intracellular melanin production in B16F10 cells more potently than kojic acid and PTU. • Depigmentation experiments of 2-MBI derivatives using zebrafish embryos resulted in pigment-free zebrafish embryos. • These 2-MBI derivatives did not exhibit significant cytotoxicity in B16F10 cells and HaCaT cells at concentrations ≤20 μM. • These results suggest that 2-MBI derivatives may be potential therapeutic agents for hyperpigmentation-related disorders. [ABSTRACT FROM AUTHOR]

Published

2024

12. Thiazol-4(5H)-one analogs as potent tyrosinase inhibitors: Synthesis, tyrosinase inhibition, antimelanogenic effect, antioxidant activity, and in silico docking simulation.

Author

Jung Park, Yu, Jin Jung, Hee, Jin Kim, Hye, Soo Park, Hye, Lee, Jieun, Yoon, Dahye, Kyung Kang, Min, Young Kim, Ga, Ullah, Sultan, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Young Chung, Hae, and Ryong Moon, Hyung

Subjects

*PHENOL oxidase, *MOLECULAR docking, *OXIDANT status, *RADICALS (Chemistry), *MELANOGENESIS, *CATECHOL

Abstract

[Display omitted] • 14 analogs with a PUSC structure built on a thiazol-4(5 H)-one scaffold were synthesized. • Analog 11 showed 26-fold stronger inhibition against mushroom tyrosinase than kojic acid (KA). • Analogs 9 and 11 inhibited tyrosinase competitively and mixedly, respectively, which was supported by docking results. • Analogs 9 and 11 inhibited tyrosinase activity and melanin production in B16F10 cells more effectively than KA. • These analogs showed strong antioxidant ability to scavenge ABTS+, DPPH, and ROS radicals. As the β-phenyl-α,β-unsaturated carbonyl (PUSC) structure was previously identified to play a key role in tyrosinase inhibition, 14 analogs with a PUSC structure built on a thiazol-4(5 H)-one scaffold were synthesized using Knoevenagel condensation to serve as potential tyrosinase inhibitors. Through mushroom tyrosinase inhibition experiments, two analogs 9 and 11 were identified as potent tyrosinase inhibitors, with 11 exhibiting an IC 50 value of 0.4 ± 0.01 μM, which indicates its 26-fold greater potency than kojic acid. Kinetic studies using Lineweaver-Burk plots revealed that 9 and 11 are competitive and mixed-type inhibitors, respectively; these kinetic results were supported by docking simulations. According to the B16F10 cell-based experiments, 9 and 11 inhibited melanogenesis more effectively than kojic acid due to their potent cellular tyrosinase inhibitory activity. In addition, analogs 9 and 11 exhibited moderate-to-strong antioxidant capacity, scavenging ABTS+, DPPH, and ROS radicals. In particular, analog 12 with a catechol moiety exhibited very strong ROS-scavenging activity, similar to Trolox. These results suggest that analogs 9 and 11 , which exhibit potent tyrosinase inhibitory activity in mushroom and mammalian cells and anti-melanogenic effects in B16F10 cells, are promising antibrowning agents for crops and skin lightening agents for hyperpigmentation-related diseases. [ABSTRACT FROM AUTHOR]

Published

2024

13. Identification and molecular mechanism of novel 5-alkenyl-2-benzylaminothiazol-4(5H)-one analogs as anti-melanogenic and antioxidant agents.

Author

Kang, Min Kyung, Yoon, Dahye, Jung, Hee Jin, Ullah, Sultan, Lee, Jieun, Park, Hye Soo, Kim, Hye Jin, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Young Chung, Hae, and Moon, Hyung Ryong

Subjects

*AMINO acid sequence, *MOLECULAR recognition, *PHENOL oxidase, *REARRANGEMENTS (Chemistry), *REACTIVE oxygen species, *CHEMICAL synthesis

Abstract

[Display omitted] • The 5-alkenyl-2-benzylaminothiazol-4(5 H)-ones 1 – 14 were synthesized as anti-melanogenic agents. via a rearrangement reaction. • Two analogs showed stronger mushroom tyrosinase inhibitory activity in the presence of l -tyrosine and l -dopa than kojic acid. • Kinetic studies indicated that 6 and 9 are a mixed type inhibitor and a competitive inhibitor, respectively. • In B16F10 murine cells, 6 and 9 effectively decreased melanin contents due to their ability to inhibit tyrosinase. • Considering strong antioxidant capacities, analogs 6 and 9 are potent anti-melanogenic agents with antioxidant ability. Mushroom tyrosinase is a tetramer, whereas mammalian tyrosinase is a monomeric glycoprotein. In addition, the amino acid sequence of mushroom tyrosinases differs from that of mammalian tyrosinases. MHY2081 exhibits potent inhibitory activity against both mushroom and mammalian tyrosinases. Accordingly, based on the MHY2081 structure, 5-alkenyl-2-benzylaminothiazol-4(5 H)-one analogs were designed as a novel anti-tyrosinase agent and synthesized using 2-((3,4-dimethoxybenzyl)amino)thiazol-4(5 H)-one (16), a key intermediate obtained via the rearrangement of a benzylamino group. Compounds 6 and 9 (IC 50 = 1.5–4.6 µM) exhibited higher mushroom tyrosinase inhibitory activity than kojic acid (IC 50 = 20–21 µM) in the presence of l -tyrosine and/or l -dopa. Based on kinetic analysis using Lineweaver-Burk plots, 6 was a mixed inhibitor, whereas 9 was a competitive inhibitor, and docking simulation results supported that these compounds could bind to the active site of mushroom tyrosinase. Using B16F10 mammalian cells, we demonstrated that these compounds inhibited melanogenesis more potently than kojic acid, and their anti-melanogenic effects could be attributed to tyrosinase inhibition. All synthesized compounds could scavenge reactive oxygen species (ROS), with five compounds exhibiting mild-to-strong ABTS+ and DPPH radical-scavenging abilities. Compounds 6 and 9 were potent tyrosinase inhibitors with strong antioxidant activities against ROS, ABTS+, and DPPH radicals. Moreover, the compounds significantly suppressed tyrosinase expression in a dose-dependent manner. Collectively, these results suggest that the novel 5-alkenyl-2-benzylaminothiazol-4(5 H)-one analogs, especially 6 and 9 , are potential anti-melanogenic agents with antioxidant activity. [ABSTRACT FROM AUTHOR]

Published

2023

14. Inhibitory effects of N-(acryloyl)benzamide derivatives on tyrosinase and melanogenesis.

Author

Lee, Sanggwon, Ullah, Sultan, Park, Chaeun, Won Lee, Hee, Kang, Dongwan, Yang, Jungho, Akter, Jinia, Park, Yujin, Chun, Pusoon, and Moon, Hyung Ryong

Subjects

*MELANINS, *PHENOL oxidase, *ACID derivatives

Abstract

• Ten NAB derivatives were synthesized via Horner-Wadsworth-Emmons olefination. • 1a and 1j exhibited potent anti-melanogenic effects compared to kojic acid. • 1a and 1j showed stronger binding affinities for tyrosinase than kojic acid. Targeting of tyrosinase has proven to be the best means of identifying safe, efficacious, and potent tyrosinase inhibitors for whitening skin. We designed and synthesized ten NAB (N -(acryloyl)benzamide) derivatives (1a–1j) using the Horner-Wadsworth-Emmons olefination of diethyl (2-benzamido-2-oxoethyl)phosphonate and appropriate benzaldehydes. A mushroom tyrosinase inhibitory assay showed compounds 1a (36.71 ± 2.14% inhibition) and 1j (25.99 ± 2.77% inhibition) inhibited tyrosinase more than the other eight NAB derivatives and kojic acid (21.56 ± 2.93% inhibition), and docking studies indicated 1a (−6.9 kcal/mole) and 1j (−7.5 kcal/mole) had stronger binding affinities for tyrosinase than kojic acid (−5.7 kcal/mole). At a concentration of 25 μM, 1a and 1j were nontoxic in B16F10 melanoma cells and exhibited stronger tyrosinase inhibition (59.70% and 76.77%, respectively) than kojic acid (50.30% inhibition) or arbutin (41.78% inhibition at 400 μM). Similarly, in B16F10 melanoma cells, compounds 1a and 1j at 25 μM decreased total melanin content by 47.97% and 61.77%, respectively (kojic acid; 38.98%). Similarities between inhibitions of tyrosinase activity and melanin contents suggested the anti-melanogenic effects of 1a and 1j were due to tyrosinase inhibition. The excellent DPPH scavenging activity of 1j suggests it might enhance in vivo effect on melanin contents. The study suggests compound 1j offers a potential starting point for the development of safe, potent tyrosinase inhibitors. [ABSTRACT FROM AUTHOR]

Published

2019

15. Tyrosinase inhibition and anti-melanin generation effect of cinnamamide analogues.

Author

Ullah, Sultan, Park, Chaeun, Ikram, Muhammad, Kang, Dongwan, Lee, Sanggwon, Yang, Jungho, Park, Yujin, Yoon, Sik, Chun, Pusoon, and Moon, Hyung Ryong

Subjects

*PHENOL oxidase, *MELANINS, *HORNER-Emmons reaction, *CINNAMIC acid, *PIGMENTATION disorders, *GROUP rings, *CHEMICAL inhibitors

Abstract

• Twenty cinnamamide derivatives were synthesized as potential tyrosinase inhibitors. • Four cinnmamides exhibited over 90% mushroom tyrosinase inhibitions than kojic acid. • In B16F10 cells, four compounds strongly decreased tyrosinase activity and melanin. • In docking study, four cinnamamides bind to tyrosinase strongerly than kojic acid. Abnormal melanogenesis results in excessive production of melanin, leading to pigmentation disorders. As a key and rate-limiting enzyme for melanogenesis, tyrosinase has been considered an important target for developing therapeutic agents of pigment disorders. Despite having an (E)-β-phenyl-α,β-unsaturated carbonyl scaffold, which plays an important role in the potent inhibition of tyrosinase activity, cinnamic acids have not attracted attention as potential tyrosinase inhibitors, due to their low tyrosinase inhibitory activity and relatively high hydrophilicity. Given that cinnamic acids' structure intrinsically features this (E)-scaffold and following our experience that minute changes in the chemical structure can powerfully affect tyrosinase activity, twenty less hydrophilic cinnamamide derivatives were designed as potential tyrosinase inhibitors and synthesised using a Horner-Wadsworth-Emmons reaction. Four of these cinnmamides (4 , 9 , 14 , and 19) exhibited much stronger mushroom tyrosinase inhibition (over 90% inhibition) at 25 µM compared to kojic acid (20.57% inhibition); crucially, all four have a 2,4-dihydroxy group on the β-phenyl ring of the scaffold. A docking simulation using tyrosinase indicated that the four cinnamamides exceeded the binding affinity of kojic acid, and bound more strongly to the active site of tyrosinase. Based on the strength of their tyrosinase inhibition, these four cinnamamides were further evaluated in B16F10 melanoma cells. All four cinnamamides, without cytotoxicity, exhibited higher tyrosinase inhibitory activity (67.33 – 79.67% inhibition) at 25 μM than kojic acid (38.11% inhibition), with the following increasing inhibitory order: morpholino (9) = cyclopentylamino (14) < cyclohexylamino (19) < N -methylpiperazino (4) cinnamamides. Analysis of tyrosinase activity and melanin content in B16F10 cells showed that the four cinnamamides dose-dependently inhibited both cellular tyrosinase activity and melanin content and that their inhibitory activity at 25 μM was much better than that of kojic acid. The results of melanin content analysis well matched those of the cellular tyrosinase activity analysis, indicating that tyrosinase inhibition by the four cinnamamides is a major factor in the reduction of melanin production. These results imply that these four cinnamamides with a 2,4-dihydroxyphenyl group can act as excellent anti-melanogenic agents in the treatment of pigmentation disorders. [ABSTRACT FROM AUTHOR]

Published

2019

16. Antioxidant, anti-tyrosinase and anti-melanogenic effects of (E)-2,3-diphenylacrylic acid derivatives.

Author

Ullah, Sultan, Park, Yujin, Park, Chaeun, Lee, Sanggwon, Kang, Dongwan, Yang, Jungho, Akter, Jinia, Chun, Pusoon, and Moon, Hyung Ryong

Subjects

*MELANINS, *ACID derivatives, *PHENYLACETIC acid, *PHENOL oxidase

Abstract

• Fifteen 2,3-DPA derivatives were designed and synthesized via Perkin reaction. • (Z)-2,3-DPA derivative (1l′) was reported for the first time as a major product. • Mushroom tyrosinase and B16F10 cells were used for in vitro studies. • 1c significantly decreased the activity of mushroom and cellular tyrosinase. • In docking studies, 1c strongly binds to tyrosinase than kojic acid. During our continued search for strong skin whitening agents over the past ten years, we have investigated the efficacies of many tyrosinase inhibitors containing a common (E)-β-phenyl-α,β-unsaturated carbonyl scaffold, which we found to be essential for the effective inhibition of mushroom and mammalian tyrosinases. In this study, we explored the tyrosinase inhibitory effects of 2,3-diphenylacrylic acid (2,3-DPA) derivatives, which also possess the (E)-β-phenyl-α,β-unsaturated carbonyl motif. We synthesized fourteen (E)-2,3-DPA derivatives 1a – 1n and one (Z)-2,3-DPA-derivative 1l′ using a Perkin reaction with phenylacetic acid and appropriate substituted benzaldehydes. In our mushroom tyrosinase assay, 1c showed higher tyrosinase inhibitory activity (76.43 ± 3.53%, IC 50 = 20.04 ± 1.91 µM) with than the other 2,3-DPA derivatives or kojic acid (21.56 ± 2.93%, IC 50 = 30.64 ± 1.27 μM). Our mushroom tyrosinase inhibitory results were supported by our docking study, which showed compound 1c (−7.2 kcal/mole) exhibited stronger binding affinity for mushroom tyrosinase than kojic acid (−5.7 kcal/mole). In B16F10 melanoma cells (a murine cell-line), 1c showed no cytotoxic effect up to a concentration of 25 μM and exhibited greater tyrosinase inhibitory activity (68.83%) than kojic acid (49.39%). In these cells, arbutin (a well-known tyrosinase inhibitor used as the positive control) only inhibited tyrosinase by 42.67% even at a concentration of 400 μM. Furthermore, at 25 µM, 1c reduced melanin contents in B16F10 melanoma cells by 24.3% more than kojic acid (62.77% vs. 38.52%). These results indicate 1c is a promising candidate treatment for pigmentation-related diseases and potential skin whitening agents. [ABSTRACT FROM AUTHOR]

Published

2019

17. Design, synthesis and anti-melanogenic effect of cinnamamide derivatives.

Author

Ullah, Sultan, Park, Yujin, Ikram, Muhammad, Lee, Sanggwon, Park, Chaeun, Kang, Dongwan, Yang, Jungho, Akter, Jinia, Yoon, Sik, Chun, Pusoon, and Moon, Hyung Ryong

Subjects

*MELANINS, *PHENOL oxidase, *MELANOMA, *CANCER cells, *PIGMENTATION disorders, *CINNAMIC acid

Abstract

Graphical abstract Abstract Pigmentation disorders are attributed to excessive melanin which can be produced by tyrosinase. Therefore, tyrosinase is supposed to be a vital target for the treatment of disorders associated with overpigmentation. Based on our previous findings that an (E)-β-phenyl-α,β-unsaturated carbonyl scaffold can play a key role in the inhibition of tyrosinase activity, and the fact that cinnamic acid is a safe natural substance with a scaffolded structure, it was speculated that appropriate cinnamic acid derivatives may exhibit potent tyrosinase inhibitory activity. Thus, ten cinnamamides were designed, and synthesized by using a Horner-Emmons olefination as the key step. Cinnamamides 4 (93.72% inhibition), 9 (78.97% inhibition), and 10 (59.09% inhibition) with either a 2,4-dihydroxyphenyl, or 4-hydroxy-3-methoxyphenyl substituent showed much higher mushroom tyrosinase inhibition at 25 µM than kojic acid (18.81% inhibition), used as a positive control. Especially, the two cinnamamides 4 and 9 having a 2,4-dihydroxyphenyl group showed the strongest inhibition. Docking simulation with tyrosinase revealed that these three cinnamamides, 4 , 9 , and 10 , bind to the active site of tyrosinase more strongly than kojic acid. Cell-based experiments carried out using B16F10 murine skin melanoma cells demonstrated that all three cinnamamides effectively inhibited cellular tyrosinase activity and melanin production in the cells without cytotoxicity. There was a close correlation between cellular tyrosinase activity and melanin content, indicating that the inhibitory effect of the three cinnamamides on melanin production is mainly attributed to their capability for cellular tyrosinase inhibition. These results imply that cinnamamides having the (E)-β-phenyl-α,β-unsaturated carbonyl scaffolds are promising candidates for skin-lighting agents. [ABSTRACT FROM AUTHOR]

Published

2018

18. Anti-tyrosinase flavone derivatives and their anti-melanogenic activities: Importance of the β-phenyl-α,β-unsaturated carbonyl scaffold.

Author

Lee, Jieun, Jeong, Yeongmu, Jin Jung, Hee, Ullah, Sultan, Ko, Jeongin, Young Kim, Ga, Yoon, Dahye, Hong, Sojeong, Kang, Dongwan, Park, Yujin, Chun, Pusoon, Young Chung, Hae, and Ryong Moon, Hyung

Subjects

*FLAVONES, *MOLECULAR structure, *PHENOL oxidase, *GENE expression, *OXIDANT status, *RADICALS (Chemistry)

Abstract

[Display omitted] • Flavone derivatives with an intrinsic β-phenyl-α,unsaturated carbonyl (PUSC) scaffold were synthesized as potential anti-tyrosinase compounds. • In B16F10 murine cells, 1a and 1e inhibited melanin production more strongly than kojic acid, and this anti-melanogenesis effect was attributable to the inhibition of cellular tyrosinase. • These flavones also exhibited strong antioxidant activities (scavenging intracellular ROS and ABTS and DPPH radicals) and inhibited melanogenesis-related gene expression. • Flavone derivatives may be promising melanogenesis inhibitors via (i) their direct tyrosinase inhibition, (ii) antioxidant capacity, and (iii) the inhibition of melanogenesis-related gene expression. • Flavones are excellent natural potential anti-melanogenic compounds as they have a PUSC scaffold in their internal molecular structure that plays an important role in anti-tyrosinase effect. Flavone derivatives were designed and synthesized based on the hypothesis that flavones containing the β-phenyl-α,β-unsaturated carbonyl (PUSC) scaffold have potential anti-tyrosinase activity. Flavones 1a and 1e inhibited mushroom tyrosinase more potently than kojic acid, and 1e inhibited monophenolase and diphenolase 61- and 28-fold more than kojic acid, respectively. Kinetic studies on mushroom tyrosinase indicated that 1a and 1e competitively inhibit monophenolase and diphenolase, and docking results supported these results. In an in vitro assay using B16F10 murine cells, 1a and 1e inhibited melanin production more potently than kojic acid, and this was attributed to the inhibition of tyrosinase. Furthermore, 1a and 1e strongly scavenged DPPH and ABTS radicals and ROS, which suggested that their antioxidant properties were at least partly responsible for their anti-melanogenic effects. Moreover, flavone 1a also inhibited the gene expressions of the melanogenesis-related genes tyrosinase , tyrosinase-related protein (TRP)-1 , and TRP-2. Our findings that flavone derivatives (i) directly inhibit tyrosinase, (ii) act as antioxidants, and (iii) inhibit the expressions of melanogenesis-related genes suggest their potential use as natural melanogenesis inhibitors. Furthermore, the study confirms that the PUSC scaffold confers anti-tyrosinase activity. [ABSTRACT FROM AUTHOR]

Published

2023