Search

Your search keyword '"Hyun, Young Eum"' showing total 23 results
Start Over Author "Hyun, Young Eum"
23 results on '"Hyun, Young Eum"'

1. GPCR Agonist-to-Antagonist Conversion: Enabling the Design of Nucleoside Functional Switches for the A2A Adenosine Receptor.

Author

Shiriaeva, Anna, Park, Daejin, Kim, Gyudong, Lee, Yoonji, Hou, Xiyan, Jarhad, Dnyandev B, Kim, Gibae, Yu, Jinha, Hyun, Young Eum, Kim, Woomi, Gao, Zhan-Guo, Jacobson, Kenneth A, Han, Gye Won, Stevens, Raymond C, Jeong, Lak Shin, Choi, Sun, and Cherezov, Vadim

Subjects
Thiophenes, Nucleosides, Receptor, Adenosine A2A, Crystallography, X-Ray, Molecular Conformation, Adenosine A2 Receptor Antagonists, Neurosciences, Medicinal and Biomolecular Chemistry, Organic Chemistry, Pharmacology and Pharmaceutical Sciences, Medicinal & Biomolecular Chemistry
Abstract

Modulators of the G protein-coupled A2A adenosine receptor (A2AAR) have been considered promising agents to treat Parkinson's disease, inflammation, cancer, and central nervous system disorders. Herein, we demonstrate that a thiophene modification at the C8 position in the common adenine scaffold converted an A2AAR agonist into an antagonist. We synthesized and characterized a novel A2AAR antagonist, 2 (LJ-4517), with Ki = 18.3 nM. X-ray crystallographic structures of 2 in complex with two thermostabilized A2AAR constructs were solved at 2.05 and 2.80 Å resolutions. In contrast to A2AAR agonists, which simultaneously interact with both Ser2777.42 and His2787.43, 2 only transiently contacts His2787.43, which can be direct or water-mediated. The n-hexynyl group of 2 extends into an A2AAR exosite. Structural analysis revealed that the introduced thiophene modification restricted receptor conformational rearrangements required for subsequent activation. This approach can expand the repertoire of adenosine receptor antagonists that can be designed based on available agonist scaffolds.

Published
2022

4. Correction to “Structure–Activity Relationship of Truncated 2,8-Disubstituted-Adenosine Derivatives as Dual A2A/A3 Adenosine Receptor Antagonists and Their Cancer Immunotherapeutic Activity”

Author

Kim, Gibae, primary, Hou, Xiyan, additional, Byun, Woong Sub, additional, Kim, Gyudong, additional, Jarhad, Dnyandev B., additional, Lee, Grim, additional, Hyun, Young Eum, additional, Yu, Jinha, additional, Lee, Chang Soo, additional, Qu, Shuhao, additional, Warnick, Eugene, additional, Gao, Zhan-Guo, additional, Kim, Ji Yong, additional, Ji, Seunghee, additional, Shin, Hyunwoo, additional, Choi, Jong-Ryoul, additional, Jacobson, Kenneth A., additional, Lee, Hyuk Woo, additional, Lee, Sang Kook, additional, and Jeong, Lak Shin, additional

Published
2024
Full Text
View/download PDF

5. Structure–Activity Relationship of Truncated 2,8-Disubstituted-Adenosine Derivatives as Dual A2A/A3 Adenosine Receptor Antagonists and Their Cancer Immunotherapeutic Activity

Author

Kim, Gibae, primary, Hou, Xiyan, additional, Byun, Woong Sub, additional, Kim, Gyudong, additional, Jarhad, Dnyandev B., additional, Lee, Grim, additional, Hyun, Young Eum, additional, Yu, Jinha, additional, Lee, Chang Soo, additional, Qu, Shuhao, additional, Warnick, Eugene, additional, Gao, Zhan-Guo, additional, Kim, Ji Yong, additional, Ji, Seunghee, additional, Shin, Hyunwoo, additional, Choi, Jong-Ryoul, additional, Jacobson, Kenneth A., additional, Lee, Hyuk Woo, additional, Lee, Sang Kook, additional, and Jeong, Lak Shin, additional

Published
2023
Full Text
View/download PDF

6. Structure–Activity Relationships of Truncated 1′-Homologated Carbaadenosine Derivatives as New PPARγ/δ Ligands: A Study on Sugar Puckering Affecting Binding to PPARs

Author

Hyun, Young Eum, primary, An, Seungchan, additional, Kim, Minjae, additional, Park, In Guk, additional, Yoon, Sanghee, additional, Javaid, Hafiz Muhammad Ahmad, additional, Vu, Thi Ngoc Lan, additional, Kim, Gyudong, additional, Choi, Hongseok, additional, Lee, Hyuk Woo, additional, Noh, Minsoo, additional, Huh, Joo Young, additional, Choi, Sun, additional, Kim, Hong-Rae, additional, and Jeong, Lak Shin, additional

Published
2023
Full Text
View/download PDF

7. Structure–Activity Relationship of Truncated 2,8-Disubstituted-Adenosine Derivatives as Dual A2A/A3 Adenosine Receptor Antagonists and Their Cancer Immunotherapeutic Activity.

Author

Kim, Gibae, Hou, Xiyan, Byun, Woong Sub, Kim, Gyudong, Jarhad, Dnyandev B., Lee, Grim, Hyun, Young Eum, Yu, Jinha, Lee, Chang Soo, Qu, Shuhao, Warnick, Eugene, Gao, Zhan-Guo, Kim, Ji Yong, Ji, Seunghee, Shin, Hyunwoo, Choi, Jong-Ryoul, Jacobson, Kenneth A., Lee, Hyuk Woo, Lee, Sang Kook, and Jeong, Lak Shin

Published
2023
Full Text
View/download PDF

9. Structure–Activity Relationship of Truncated 2,8-Disubstituted-Adenosine Derivatives as Dual A2A/A3Adenosine Receptor Antagonists and Their Cancer Immunotherapeutic Activity

Author

Kim, Gibae, Hou, Xiyan, Byun, Woong Sub, Kim, Gyudong, Jarhad, Dnyandev B., Lee, Grim, Hyun, Young Eum, Yu, Jinha, Lee, Chang Soo, Qu, Shuhao, Warnick, Eugene, Gao, Zhan-Guo, Kim, Ji Yong, Ji, Seunghee, Shin, Hyunwoo, Choi, Jong-Ryoul, Jacobson, Kenneth A., Lee, Hyuk Woo, Lee, Sang Kook, and Jeong, Lak Shin

Abstract

Based on hA2AAR structures, a hydrophobic C8-heteroaromatic ring in 5′-truncated adenosine analogues occupies the subpocket tightly, converting hA2AAR agonists into antagonists while maintaining affinity toward hA3AR. The final compounds of 2,8-disubstituted-N6-substituted 4′-thionucleosides, or 4′-oxo, were synthesized from d-mannose and d-erythrono-1,4-lactone, respectively, using a Pd-catalyst-controlled regioselective cross-coupling reaction. All tested compounds completely antagonized hA2AAR, including 5dwith the highest affinity (Ki,A2A= 7.7 ± 0.5 nM). The hA2AAR–5dX-ray structure revealed that C8-heteroaromatic rings prevented receptor activation-associated conformational changes. However, the C8-substituted compounds still antagonized hA3AR. Structural SAR features and docking studies supported different binding modes at A2AAR and A3AR, elucidating pharmacophores for receptor activation and selectivity. Favorable pharmacokinetics were demonstrated, in which 5ddisplayed high oral absorption, moderate half-life, and bioavailability. Also, 5dsignificantly improved the antitumor effect of anti-PD-L1 in vivo. Overall, this study suggests that the novel dual A2AAR/A3AR nucleoside antagonists would be promising drug candidates for immune-oncology.

Published
2023
Full Text
View/download PDF

13. Discovery and Structure–Activity Relationships of Novel Template, Truncated 1′-Homologated Adenosine Derivatives as Pure Dual PPARγ/δ Modulators

Author

An, Seungchan, primary, Kim, Gyudong, additional, Kim, Hyun Jin, additional, Ahn, Sungjin, additional, Kim, Hyun Young, additional, Ko, Hyejin, additional, Hyun, Young Eum, additional, Nguyen, Mai, additional, Jeong, Juri, additional, Liu, Zijing, additional, Han, Jinhe, additional, Choi, Hongseok, additional, Yu, Jinha, additional, Kim, Ji Won, additional, Lee, Hyuk Woo, additional, Jacobson, Kenneth A., additional, Cho, Won Jea, additional, Kim, Young-Mi, additional, Kang, Keon Wook, additional, Noh, Minsoo, additional, and Jeong, Lak Shin, additional

Published
2020
Full Text
View/download PDF

17. Correction to "Structure–Activity Relationship of Truncated 2,8-Disubstituted-Adenosine Derivatives as Dual A2A/A3 Adenosine Receptor Antagonists and Their Cancer Immunotherapeutic Activity".

Author

Kim, Gibae, Hou, Xiyan, Byun, Woong Sub, Kim, Gyudong, Jarhad, Dnyandev B., Lee, Grim, Hyun, Young Eum, Yu, Jinha, Lee, Chang Soo, Qu, Shuhao, Warnick, Eugene, Gao, Zhan-Guo, Kim, Ji Yong, Ji, Seunghee, Shin, Hyunwoo, Choi, Jong-Ryoul, Jacobson, Kenneth A., Lee, Hyuk Woo, Lee, Sang Kook, and Jeong, Lak Shin

Published
2024
Full Text
View/download PDF

19. Correction to “Structure–Activity Relationship of Truncated 2,8-Disubstituted-Adenosine Derivatives as Dual A2A/A3Adenosine Receptor Antagonists and Their Cancer Immunotherapeutic Activity”

Author

Kim, Gibae, Hou, Xiyan, Byun, Woong Sub, Kim, Gyudong, Jarhad, Dnyandev B., Lee, Grim, Hyun, Young Eum, Yu, Jinha, Lee, Chang Soo, Qu, Shuhao, Warnick, Eugene, Gao, Zhan-Guo, Kim, Ji Yong, Ji, Seunghee, Shin, Hyunwoo, Choi, Jong-Ryoul, Jacobson, Kenneth A., Lee, Hyuk Woo, Lee, Sang Kook, and Jeong, Lak Shin

Published
2024
Full Text
View/download PDF

20. GPCR Agonist-to-Antagonist Conversion: Enabling the Design of Nucleoside Functional Switches for the A2AAdenosine Receptor

Author

Shiriaeva, Anna, Park, Daejin, Kim, Gyudong, Lee, Yoonji, Hou, Xiyan, Jarhad, Dnyandev B., Kim, Gibae, Yu, Jinha, Hyun, Young Eum, Kim, Woomi, Gao, Zhan-Guo, Jacobson, Kenneth A., Han, Gye Won, Stevens, Raymond C., Jeong, Lak Shin, Choi, Sun, and Cherezov, Vadim

Abstract

Modulators of the G protein-coupled A2Aadenosine receptor (A2AAR) have been considered promising agents to treat Parkinson’s disease, inflammation, cancer, and central nervous system disorders. Herein, we demonstrate that a thiophene modification at the C8 position in the common adenine scaffold converted an A2AAR agonist into an antagonist. We synthesized and characterized a novel A2AAR antagonist, 2(LJ-4517), with Ki= 18.3 nM. X-ray crystallographic structures of 2in complex with two thermostabilized A2AAR constructs were solved at 2.05 and 2.80 Å resolutions. In contrast to A2AAR agonists, which simultaneously interact with both Ser2777.42and His2787.43, 2only transiently contacts His2787.43, which can be direct or water-mediated. The n-hexynyl group of 2extends into an A2AAR exosite. Structural analysis revealed that the introduced thiophene modification restricted receptor conformational rearrangements required for subsequent activation. This approach can expand the repertoire of adenosine receptor antagonists that can be designed based on available agonist scaffolds.

Published
2022
Full Text
View/download PDF

22. Structure-Activity Relationship of Truncated 2,8-Disubstituted-Adenosine Derivatives as Dual A 2A /A 3 Adenosine Receptor Antagonists and Their Cancer Immunotherapeutic Activity.

Author

Kim G, Hou X, Byun WS, Kim G, Jarhad DB, Lee G, Hyun YE, Yu J, Lee CS, Qu S, Warnick E, Gao ZG, Kim JY, Ji S, Shin H, Choi JR, Jacobson KA, Lee HW, Lee SK, and Jeong LS

Subjects
Humans, Androgen Receptor Antagonists, Immunotherapy, Purinergic P1 Receptor Antagonists, Structure-Activity Relationship, Thionucleosides chemistry, Thionucleosides pharmacology, Adenosine pharmacology, Neoplasms
Abstract

Based on hA 2A AR structures, a hydrophobic C8-heteroaromatic ring in 5'-truncated adenosine analogues occupies the subpocket tightly, converting hA 2A AR agonists into antagonists while maintaining affinity toward hA 3 AR. The final compounds of 2,8-disubstituted- N 6 -substituted 4'-thionucleosides, or 4'-oxo, were synthesized from d-mannose and d-erythrono-1,4-lactone, respectively, using a Pd-catalyst-controlled regioselective cross-coupling reaction. All tested compounds completely antagonized hA 2A AR, including 5d with the highest affinity ( K i,A 2A = 7.7 ± 0.5 nM). The hA 2A AR- 5d X-ray structure revealed that C8-heteroaromatic rings prevented receptor activation-associated conformational changes. However, the C8-substituted compounds still antagonized hA 3 AR. Structural SAR features and docking studies supported different binding modes at A 2A AR and A 3 AR, elucidating pharmacophores for receptor activation and selectivity. Favorable pharmacokinetics were demonstrated, in which 5d displayed high oral absorption, moderate half-life, and bioavailability. Also, 5d significantly improved the antitumor effect of anti-PD-L1 in vivo . Overall, this study suggests that the novel dual A 2A AR/A 3 AR nucleoside antagonists would be promising drug candidates for immune-oncology.

Published
2023
Full Text
View/download PDF

23. GPCR Agonist-to-Antagonist Conversion: Enabling the Design of Nucleoside Functional Switches for the A 2A Adenosine Receptor.

Author

Shiriaeva A, Park D, Kim G, Lee Y, Hou X, Jarhad DB, Kim G, Yu J, Hyun YE, Kim W, Gao ZG, Jacobson KA, Han GW, Stevens RC, Jeong LS, Choi S, and Cherezov V

Subjects
Adenosine A2 Receptor Antagonists chemistry, Adenosine A2 Receptor Antagonists pharmacology, Crystallography, X-Ray, Molecular Conformation, Thiophenes, Nucleosides, Receptor, Adenosine A2A chemistry
Abstract

Modulators of the G protein-coupled A 2A adenosine receptor (A 2A AR) have been considered promising agents to treat Parkinson's disease, inflammation, cancer, and central nervous system disorders. Herein, we demonstrate that a thiophene modification at the C8 position in the common adenine scaffold converted an A 2A AR agonist into an antagonist. We synthesized and characterized a novel A 2A AR antagonist, 2 (LJ-4517), with K i = 18.3 nM. X-ray crystallographic structures of 2 in complex with two thermostabilized A 2A AR constructs were solved at 2.05 and 2.80 Å resolutions. In contrast to A 2A AR agonists, which simultaneously interact with both Ser277 7.42 and His278 7.43 , 2 only transiently contacts His278 7.43 , which can be direct or water-mediated. The n -hexynyl group of 2 extends into an A 2A AR exosite. Structural analysis revealed that the introduced thiophene modification restricted receptor conformational rearrangements required for subsequent activation. This approach can expand the repertoire of adenosine receptor antagonists that can be designed based on available agonist scaffolds.

Published
2022
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results