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107 results on '"Hou, Xiyan"'

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

2. Structural Modification and Biological Evaluation of 2,8-Disubstituted Adenine and Its Nucleosides as A2A Adenosine Receptor Antagonists: Exploring the Roles of Ribose at Adenosine Receptors

Author

Kim, Gibae, primary, Jarhad, Dnyandev B., additional, Lee, Grim, additional, Kim, Gyudong, additional, Hou, Xiyan, additional, Yu, Jinha, additional, Lee, Chang Soo, additional, Warnick, Eugene, additional, Gao, Zhan-Guo, additional, Ahn, Sang Yeop, additional, Kwak, Dongik, additional, Park, Kichul, additional, Lee, Summer Dabin, additional, Park, Tae-uk, additional, Jung, So-young, additional, Lee, Jong Hyun, additional, Choi, Jong-Ryoul, additional, Kim, Myeongjoong, additional, Kim, Donghyun, additional, Kim, Bongtae, additional, Jacobson, Kenneth A., additional, and Jeong, Lak Shin, additional

Published
2024
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6. Structural Modification and Biological Evaluation of 2,8-Disubstituted Adenine and Its Nucleosides as A2A Adenosine Receptor Antagonists: Exploring the Roles of Ribose at Adenosine Receptors.

Author

Kim, Gibae, Jarhad, Dnyandev B., Lee, Grim, Kim, Gyudong, Hou, Xiyan, Yu, Jinha, Lee, Chang Soo, Warnick, Eugene, Gao, Zhan-Guo, Ahn, Sang Yeop, Kwak, Dongik, Park, Kichul, Lee, Summer Dabin, Park, Tae-uk, Jung, So-young, Lee, Jong Hyun, Choi, Jong-Ryoul, Kim, Myeongjoong, Kim, Donghyun, and Kim, Bongtae

Published
2024
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7. 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
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8. Structural Modification and Biological Evaluation of 2,8-Disubstituted Adenine and Its Nucleosides as A2AAdenosine Receptor Antagonists: Exploring the Roles of Ribose at Adenosine Receptors

Author

Kim, Gibae, Jarhad, Dnyandev B., Lee, Grim, Kim, Gyudong, Hou, Xiyan, Yu, Jinha, Lee, Chang Soo, Warnick, Eugene, Gao, Zhan-Guo, Ahn, Sang Yeop, Kwak, Dongik, Park, Kichul, Lee, Summer Dabin, Park, Tae-uk, Jung, So-young, Lee, Jong Hyun, Choi, Jong-Ryoul, Kim, Myeongjoong, Kim, Donghyun, Kim, Bongtae, Jacobson, Kenneth A., and Jeong, Lak Shin

Abstract

Building on the preceding structural analysis and a structure–activity relationship (SAR) of 8-aryl-2-hexynyl nucleoside hA2AAR antagonist 2a, we strategically inverted C2/C8 substituents and eliminated the ribose moiety. These modifications aimed to mitigate potential steric interactions between ribose and adenosine receptors. The SAR findings indicated that such inversions significantly modulated hA3AR binding affinities depending on the type of ribose, whereas removal of ribose altered the functional efficacy via hA2AAR. Among the synthesized derivatives, 2-aryl-8-hexynyl adenine 4ademonstrated the highest selectivity for hA2AAR (Ki,hA2A= 5.0 ± 0.5 nM, Ki,hA3/Ki,hA2A= 86) and effectively blocked cAMP production and restored IL-2 secretion in PBMCs. Favorable pharmacokinetic properties and a notable enhancement of anticancer effects in combination with an mAb immune checkpoint blockade were observed upon oral administration of 4a. These findings establish 4aas a viable immune-oncology therapeutic candidate.

Published
2024
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9. 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
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11. 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
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13. 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
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16. Subtle Chemical Changes Cross the Boundary between Agonist and Antagonist: New A3 Adenosine Receptor Homology Models and Structural Network Analysis Can Predict This Boundary

Author

Lee, Yoonji, primary, Hou, Xiyan, additional, Lee, Jin Hee, additional, Nayak, Akshata, additional, Alexander, Varughese, additional, Sharma, Pankaz K., additional, Chang, Hyerim, additional, Phan, Khai, additional, Gao, Zhan-Guo, additional, Jacobson, Kenneth A., additional, Choi, Sun, additional, and Jeong, Lak Shin, additional

Published
2021
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19. Urchin-Like Cobalt-Copper (Hydr)oxides as an Efficient Water Oxidation Electrocatalyst

Author

Ye, Qilun, Hou, Xiyan, Lee, Husileng, Liu, Hongzhen, Lu, Liangjie, Wu, Xiujuan, Sun, Licheng, Ye, Qilun, Hou, Xiyan, Lee, Husileng, Liu, Hongzhen, Lu, Liangjie, Wu, Xiujuan, and Sun, Licheng

Abstract

The development of e & xfb03;cient and low-cost oxygen evolution reaction (OER) catalysts is essential for the generation of clean hydrogen energy from water splitting. Herein, a novel hierarchical urchin-like cobalt-copper (hydr)oxide in situ grown on copper foam (CoCuOxHy(S)/CF) was synthesized through the electrochemical transformation of cobalt-copper sulfides (Co9S8-Cu1.81S) via anodization process. This CoCuOxHy(S)/CF anode exhibited a low overpotential (eta) of 274 mV at a current density of 100 mA cm(-2)with a robust durability over a period of 40 h when operated at 10 mA cm(-2). Further investigations imply that the unique nanowires aggregated urchin-like structure of CoCuOxHy(S) derived from the in situ anion exchange process could facilitate the exposure of active sites and accelerate electron transfer. More importantly, the incorporation of copper resulted in an electronic delocalization around the cobalt species, which contributed to reach a high-valent catalytically active cobalt species and further improved the OER performance., QC 20200720

Published
2020
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20. Copper Selenide-Derived Copper Oxide Nanoplates as a Durable and Efficient Electrocatalyst for Oxygen Evolution Reaction

Author

Wang, Xiaoxiao, Hou, Xiyan, Lee, Husileng, Lu, Liangjie, Wu, Xiujuan, Sun, Licheng, Wang, Xiaoxiao, Hou, Xiyan, Lee, Husileng, Lu, Liangjie, Wu, Xiujuan, and Sun, Licheng

Abstract

Earth-abundant transition metal-based nanomaterials play a signi?cant role in oxygen evolution reaction (OER). Among them, copper has attracted signi?cant attention due to its excellent electrocatalytic activity, low price, and abundance. Herein, a nanostructured copper oxide (CuO-A) is generated in situ from a cuprous selenide (Cu2Se) precursor under oxygen evolution reaction conditions. The as-prepared CuO-A/copper foam (CF) electrode delivers a current density of 10 mA cm(-2) at an overpotential of 297 mV with good stability for over 50 h in 1 m KOH solution, which is superior to most recently reported copper-based water oxidation catalysts. The high catalytic performance of CuO-A is mainly attributed to the improved surface area offered by the morphology reconstruction during the in situ transformation process. As a result, it paves a way to synthesize effective and stable transition metal oxide catalysts via the in situ conversion of transition metal chalcogenides for energy conversion and storage applications., QC 20210915

Published
2020
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25. Widespread Existence of Quorum Sensing Inhibitors in Marine Bacteria: Potential Drugs to Combat Pathogens with Novel Strategies

Author

Jing Zhao, Ming Chen, Chunshan Quan, Li Xinyun, and Hou Xiyan

Subjects
Marine conservation, QS inhibition mechanisms, Pharmaceutical Science, Computational biology, Crop cultivation, Review, 03 medical and health sciences, Marine bacteriophage, Anti-Infective Agents, Drug Development, small molecule QS inhibitors, Drug Discovery, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), lcsh:QH301-705.5, quorum quenching enzymes, 030304 developmental biology, structural modification, 0303 health sciences, biology, Bacteria, Molecular Structure, 030306 microbiology, Quorum Sensing, biology.organism_classification, Enzymes, Quorum sensing, Drug development, lcsh:Biology (General), marine bacteria, Quorum Quenching, QS inhibitors, Virulence gene expression, application
Abstract

Quorum sensing (QS) is a phenomenon of intercellular communication discovered mainly in bacteria. A QS system consisting of QS signal molecules and regulatory protein components could control physiological behaviors and virulence gene expression of bacterial pathogens. Therefore, QS inhibition could be a novel strategy to combat pathogens and related diseases. QS inhibitors (QSIs), mainly categorized into small chemical molecules and quorum quenching enzymes, could be extracted from diverse sources in marine environment and terrestrial environment. With the focus on the exploitation of marine resources in recent years, more and more QSIs from the marine environment have been investigated. In this article, we present a comprehensive review of QSIs from marine bacteria. Firstly, screening work of marine bacteria with potential QSIs was concluded and these marine bacteria were classified. Afterwards, two categories of marine bacteria-derived QSIs were summarized from the aspects of sources, structures, QS inhibition mechanisms, environmental tolerance, effects/applications, etc. Next, structural modification of natural small molecule QSIs for future drug development was discussed. Finally, potential applications of QSIs from marine bacteria in human healthcare, aquaculture, crop cultivation, etc. were elucidated, indicating promising and extensive application perspectives of QS disruption as a novel antimicrobial strategy.

Published
2019

30. 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
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36. Asymmetric Synthesis of (−)-6′-β-Fluoro-aristeromycin via Stereoselective Electrophilic Fluorination

Author

Kim, Gyudong, Yoon, Ji-seong, Jarhad, Dnyandev B., Shin, Young Sup, Majik, Mahesh S., Mulamoottil, Varughese A., Hou, Xiyan, Qu, Shuhao, Park, Jiyong, Baik, Mu-Hyun, and Jeong, Lak Shin

Abstract

(−)-6′-β-Fluoro-aristeromycin (2), a potent inhibitor of S-adenosylhomocysteine (AdoHcy) hydrolase, has been synthesized via stereoselective electrophilic fluorination followed by a purine base build-up approach. Interestingly, purine base condensation using a cyclic sulfate resulted in a synthesis of (+)-5′-β-fluoro-isoaristeromycin (2a). Computational analysis indicates that the fluorine atom controlled the regioselectivity of the purine base substitution.

Published
2024
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37. 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
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41. Structure-Activity Relationships of Truncated D- and L-4′-Thioadenosine Derivatives as Species-Independent A3 Adenosine Receptor Antagonists1

Author

Jeong, Lak Shin, Pal, Shantanu, Choe, Seung Ah, Choi, Won Jun, Jacobson, Kenneth A., Gao, Zhan-Guo, Klutz, Athena M., Hou, Xiyan, Kim, Hea Ok, Lee, Hyuk Woo, Lee, Sang Kook, Tosh, Dilip K., and Moon, Hyung Ryong

Subjects
Structure-Activity Relationship, Adenosine, Thionucleosides, Molecular Structure, Receptor, Adenosine A3, Adenosine A3 Receptor Antagonists, Animals, Humans, Article, Rats
Abstract

Novel D- and l-4'-thioadenosine derivatives lacking the 4'-hydroxymethyl moiety were synthesized, starting from d-mannose and d-gulonic gamma-lactone, respectively, as potent and selective species-independent A 3 adenosine receptor (AR) antagonists. Among the novel 4'-truncated 2-H nucleosides tested, a N(6)-(3-chlorobenzyl) derivative 7c was the most potent at the human A 3 AR (K i = 1.5 nM), but a N(6)-(3-bromobenzyl) derivative 7d showed the optimal species-independent binding affinity.

Published
2008

42. Synthesis and Anti-Renal Fibrosis Activity of Conformationally Locked Truncated 2-Hexynyl-N6-Substituted-(N)-Methanocarba-nucleosides as A3 Adenosine Receptor Antagonists and Partial Agonists

Author

Nayak, Akshata, primary, Chandra, Girish, additional, Hwang, Inah, additional, Kim, Kyunglim, additional, Hou, Xiyan, additional, Kim, Hea Ok, additional, Sahu, Pramod K., additional, Roy, Kuldeep K., additional, Yoo, Jakyung, additional, Lee, Yoonji, additional, Cui, Minghua, additional, Choi, Sun, additional, Moss, Steven M., additional, Phan, Khai, additional, Gao, Zhan-Guo, additional, Ha, Hunjoo, additional, Jacobson, Kenneth A., additional, and Jeong, Lak Shin, additional

Published
2014
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43. Structure–Activity Relationships of Truncated C2- or C8-Substituted Adenosine Derivatives as Dual Acting A2A and A3 Adenosine Receptor Ligands

Author

Hou, Xiyan, primary, Majik, Mahesh S., additional, Kim, Kyunglim, additional, Pyee, Yuna, additional, Lee, Yoonji, additional, Alexander, Varughese, additional, Chung, Hwa-Jin, additional, Lee, Hyuk Woo, additional, Chandra, Girish, additional, Lee, Jin Hee, additional, Park, Seul-gi, additional, Choi, Won Jun, additional, Kim, Hea Ok, additional, Phan, Khai, additional, Gao, Zhan-Guo, additional, Jacobson, Kenneth A., additional, Choi, Sun, additional, Lee, Sang Kook, additional, and Jeong, Lak Shin, additional

Published
2011
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47. Structure−Activity Relationships of Truncatedd- andl-4′-Thioadenosine Derivatives as Species-Independent A3Adenosine Receptor Antagonists(1)

Author

Jeong, Lak Shin, primary, Pal, Shantanu, additional, Choe, Seung Ah, additional, Choi, Won Jun, additional, Jacobson, Kenneth A., additional, Gao, Zhan-Guo, additional, Klutz, Athena M., additional, Hou, Xiyan, additional, Kim, Hea Ok, additional, Lee, Hyuk Woo, additional, Lee, Sang Kook, additional, Tosh, Dilip K., additional, and Moon, Hyung Ryong, additional

Published
2008
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49. Synthesis and Anti-Renal FibrosisActivity of ConformationallyLocked Truncated 2-Hexynyl-N6-Substituted-(N)-Methanocarba-nucleosidesas A3Adenosine Receptor Antagonists and Partial Agonists.

Author

Nayak, Akshata, Chandra, Girish, Hwang, Inah, Kim, Kyunglim, Hou, Xiyan, Kim, Hea Ok, Sahu, Pramod K., Roy, Kuldeep K., Yoo, Jakyung, Lee, Yoonji, Cui, Minghua, Choi, Sun, Moss, Steven M., Phan, Khai, Gao, Zhan-Guo, Ha, Hunjoo, Jacobson, Kenneth A., and Jeong, Lak Shin

Published
2014
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50. Alternative and improved syntheses of highly potent and selective A3 adenosine receptor agonists, CI-IB-MECA and Thio-CI-IB-MECA.

Author

Hou, Xiyan, Lee, Hyuk, Tosh, Dilip, Zhao, Long, and Jeong, Lak

Abstract

Improved syntheses of potent and selective A3 adenosine receptor agonists, CI-IB-MECA and thio-CI-IB-MECA were accomplished from cheap stating material, D-ribose. New synthetic methods were found to be superior to old methods from the viewpoint of use of cheap starting material, number of steps, and overall yields. [ABSTRACT FROM AUTHOR]

Published
2007
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