Your search keyword '"Jarhad, Dnyandev B."' showing total 47 results

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. Stereochemical influence of 4ʹ-methyl substitutions on truncated 4ʹ-thioadenosine derivatives: Impact on A3 adenosine receptor binding and antagonism

Author

Kim, Minjae, Naik, Siddhi D., Jarhad, Dnyandev B., Aswar, Vikas R., Tripathi, Sushil Kumar, Aslam, Muhammad Arif, Huh, Joo Young, and Jeong, Lak Shin

Published

2024

3. 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

4. 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

5. Identification of 6′-β-fluoro-homoaristeromycin as a potent inhibitor of chikungunya virus replication

Author

Shin, Young Sup, Jarhad, Dnyandev B., Jang, Min Hwan, Kovacikova, Kristina, Kim, Gyudong, Yoon, Ji-seong, Kim, Hong-Rae, Hyun, Young Eum, Tipnis, Amol S., Chang, Tong-Shin, van Hemert, Martijn J., and Jeong, Lak Shin

Published

2020

6. 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

7. 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

8. Stereoselective Approach for the Synthesis of Diverse 1′-Modified Carbanucleosides

Author

Sung, Kisu, primary, Aswar, Vikas R., additional, Song, Jiyoon, additional, Jarhad, Dnyandev B., additional, and Jeong, Lak Shin, additional

Published

2023

9. Design, synthesis and anticancer activity of fluorocyclopentenyl-purines and – pyrimidines

Author

Yoon, Ji-seong, Jarhad, Dnyandev B., Kim, Gyudong, Nayak, Akshata, Zhao, Long Xuan, Yu, Jinha, Kim, Hong-Rae, Lee, Ji Yun, Mulamoottil, Varughese A., Chandra, Girish, Byun, Woong Sub, Lee, Sang Kook, Kim, Yong-Chul, and Jeong, Lak Shin

Published

2018

10. Synthesis and anti-HIV activity of l-2′,3′-Dideoxy-4′-selenonucleosides (l-4′-Se-ddNs)

Author

Yu, Jinha, Kim, Gyudong, Jarhad, Dnyandev B., Kim, Hong-Rae, and Jeong, Lak Shin

Published

2019

11. Correlation study between A3 adenosine receptor binding affinity and anti-renal interstitial fibrosis activity of truncated adenosine derivatives

Author

Yu, Jinha, Kim, Gyudong, Jarhad, Dnyandev B., Lee, Hyuk Woo, Lee, Jiyoun, Park, Chong Woo, Ha, Hunjoo, and Jeong, Lak Shin

Published

2019

12. 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

13. Molecular complexity and diversity from aromatics. Intramolecular cycloaddition of cyclohexa-2,4-dienones and sigmatropic shift in excited state: a unified approach towards synthesis of polycyclic frameworks related to crotogoudin, conidiogenol, and crinipellins

Author

Behera, Tarun Kumar, Jarhad, Dnyandev B., Mobin, Shaikh M., and Singh, Vishwakarma

Published

2016

14. 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

15. Benzofuran as a dienophile in π4s+π2s cycloaddition with cyclohexa-2,4-dienones. Studies on synthesis and photoreaction of dihydrobenzofuran annulated bicyclo[2.2.2]octenones

Author

Jarhad, Dnyandev B., Behera, Tarun Kumar, and Singh, Vishwakarma

Published

2015

16. Molecular diversity from aromatics. Cycloaddition of cyclohexa-2,4-dienones, ring-closing metathesis and sigmatropic shifts: a general and stereoselective route to novel spirocarbocyclics

Author

Singh, Vishwakarma, Das, Beauty, Jarhad, Dnyandev B., and Mobin, Shaikh M.

Published

2015

17. Synthesis of Enantiomerically Pure Pyrimidine Ribonucleosides Locked in the South Conformation

Author

Hyun, Young Eum, primary, Jarhad, Dnyandev B., additional, Kim, Minjae, additional, Yang, Ayeon, additional, Kim, Gyudong, additional, Kim, Hong-Rae, additional, and Jeong, Lak Shin, additional

Published

2022

18. 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

19. Catalyst-controlled regioselective Sonogashira coupling of 9-substituted-6-chloro-2,8-diiodopurines

Author

Kim, Gibae, primary, Lee, Grim, additional, Kim, Gyudong, additional, Seo, Yeonseong, additional, Jarhad, Dnyandev B., additional, and Jeong, Lak Shin, additional

Published

2022

20. 4′‐Selenonucleosides: Regio‐ and Stereoselective Synthesis of Novel Ribavirin and Acadesine Analogs as Anti‐Hepatitis C Virus (HCV) Agents

Author

Lee, Hyejin, primary, Jarhad, Dnyandev B., additional, Lee, Ahrim, additional, Lee, Choongho, additional, and Jeong, Lak Shin, additional

Published

2021

21. 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

Published

2022

22. 6′,6′-Difluoro-aristeromycin is a potent inhibitor of MERS-coronavirus replication

Author

Ogando, Natacha S., primary, Zevenhoven-Dobbe, Jessika C., additional, Jarhad, Dnyandev B., additional, Tripathi, Sushil Kumar, additional, Lee, Hyuk Woo, additional, Jeong, Lak Shin, additional, Snijder, Eric J., additional, and Posthuma, Clara C., additional

Published

2021

23. Antiproliferative and Antimigration Activities of Fluoro-Neplanocin A via Inhibition of Histone H3 Methylation in Triple-Negative Breast Cancer

Author

Byun, Woong Sub, primary, Kim, Won Kyung, additional, Yoon, Ji-seong, additional, Jarhad, Dnyandev B., additional, Jeong, Lak Shin, additional, and Lee, Sang Kook, additional

Published

2020

24. 6′-β-Fluoro-Homoaristeromycin and 6′-Fluoro-Homoneplanocin A Are Potent Inhibitors of Chikungunya Virus Replication through Their Direct Effect on Viral Nonstructural Protein 1

Author

Kovacikova, Kristina, primary, Morren, Bas M., additional, Tas, Ali, additional, Albulescu, Irina C., additional, van Rijswijk, Robin, additional, Jarhad, Dnyandev B., additional, Shin, Young Sup, additional, Jang, Min Hwan, additional, Kim, Gyudong, additional, Lee, Hyuk Woo, additional, Jeong, Lak Shin, additional, Snijder, Eric J., additional, and van Hemert, Martijn J., additional

Published

2020

25. Asymmetric Synthesis of Fluoro‐MLN4924 as a Selective NEDD8‐Activating Enzyme (NAE) Inhibitor

Author

Kim, Hong‐Rae, primary, Jarhad, Dnyandev B., additional, Sahu, Pramod K., additional, Sung, Kisu, additional, An, Dayoung, additional, Hyun, Young Eum, additional, Yu, Jinha, additional, and Jeong, Lak Shin, additional

Published

2019

26. Design, Synthesis, and Anti-RNA Virus Activity of 6′-Fluorinated-Aristeromycin Analogues

Author

Yoon, Ji-seong, primary, Kim, Gyudong, additional, Jarhad, Dnyandev B., additional, Kim, Hong-Rae, additional, Shin, Young-Sup, additional, Qu, Shuhao, additional, Sahu, Pramod K., additional, Kim, Hea Ok, additional, Lee, Hyuk Woo, additional, Wang, Su Bin, additional, Kong, Yun Jeong, additional, Chang, Tong-Shin, additional, Ogando, Natacha S., additional, Kovacikova, Kristina, additional, Snijder, Eric J., additional, Posthuma, Clara C., additional, van Hemert, Martijn J., additional, and Jeong, Lak Shin, additional

Published

2019

27. An efficient synthesis of fluoro-neplanocin A analogs using electrophilic fluorination and palladium-catalyzed dehydrosilylation

Author

Jarhad, Dnyandev B., primary, Jang, Min Hwan, additional, Shin, Young Sup, additional, Kim, Gyudong, additional, Kim, Hong-Rae, additional, Hyun, Young Eum, additional, Yoon, Ji-seong, additional, and Jeong, Lak Shin, additional

Published

2019

28. An alternative and efficient synthesis of MLN4924, a selective NEDD8 inhibitor

Author

Kim, Hong-Rae, primary, Hyun, Young Eum, additional, Jarhad, Dnyandev B., additional, Yu, Jinha, additional, and Jeong, Lak Shin, additional

Published

2019

29. Design, Synthesis, and Anti-RNA Virus Activity of 6′-Fluorinated-Aristeromycin Analogues.

Author

Yoon, Ji-seong, Kim, Gyudong, Jarhad, Dnyandev B., Kim, Hong-Rae, Shin, Young-Sup, Qu, Shuhao, Sahu, Pramod K., Kim, Hea Ok, Lee, Hyuk Woo, Wang, Su Bin, Kong, Yun Jeong, Chang, Tong-Shin, Ogando, Natacha S., Kovacikova, Kristina, Snijder, Eric J., Posthuma, Clara C., van Hemert, Martijn J., and Jeong, Lak Shin

Published

2020

30. Correlation study between A3 adenosine receptor binding affinity and anti-renal interstitial fibrosis activity of truncated adenosine derivatives

Author

Yu, Jinha, primary, Kim, Gyudong, additional, Jarhad, Dnyandev B., additional, Lee, Hyuk Woo, additional, Lee, Jiyoun, additional, Park, Chong Woo, additional, Ha, Hunjoo, additional, and Jeong, Lak Shin, additional

Published

2018

31. Dual-Specificity Tyrosine Phosphorylation-Regulated Kinase 1A (DYRK1A) Inhibitors as Potential Therapeutics

Author

Jarhad, Dnyandev B., primary, Mashelkar, Karishma K., additional, Kim, Hong-Rae, additional, Noh, Minsoo, additional, and Jeong, Lak Shin, additional

Published

2018

32. 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

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

Author

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

Published

2017

34. Stereoselective Synthesis of 4′‐Selenonucleosides via the Seleno‐Michael Reaction

Author

Sahu, Pramod K., primary, Jarhad, Dnyandev B., additional, Kim, Gyudong, additional, and Jeong, Lak Shin, additional

Published

2017

35. Asymmetric Synthesis of 2′‑C‑Methyl-4′-selenonucleosides as Anti-Hepatitis C Virus Agents.

Author

Lee, Hyejin, Jarhad, Dnyandev B., Yu, Jinha, Lee, Choongho, and Jeong, Lak Shin

Published

2019

36. Correlation study between A3 adenosine receptor binding affinity and anti-renal interstitial fibrosis activity of truncated adenosine derivatives.

Author

Yu, Jinha, Kim, Gyudong, Jarhad, Dnyandev B., Lee, Hyuk Woo, Lee, Jiyoun, Park, Chong Woo, Ha, Hunjoo, and Jeong, Lak Shin

Abstract

Truncated 4′-thionucleosides 1–4 and 4′-oxonucleosides 5–8 as potent and selective A3AR antagonists were synthesized from d-mannose and d-erythronic acid γ-lactone, respectively. These nucleosides were evaluated for their anti-fibrotic renoprotective activity in TGF-β1-treated murine proximal tubular (mProx) cells. Their antagonistic activities for A3AR were proportional to their inhibitory activities against TGF-β1-induced collagen I upregulation in mProx cells. This result suggests that the binding affinity of A3AR antagonists is closely correlated with their anti-fibrotic activity. Thus, A3AR antagonists might be novel therapeutic candidates for treating chronic kidney disease. [ABSTRACT FROM AUTHOR]

Published

2019

37. 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

38. 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

39. π4s + π2s Cycloaddition of Spiroepoxycyclohexa-2,4-dienone, Radical Cyclization, and Oxidation–Aldol–Oxidation Cascade: Synthesis of BCDE Ring of Atropurpuran

Author

Jarhad, Dnyandev B., primary and Singh, Vishwakarma, additional

Published

2016

40. Asymmetric Synthesis of (-)-6'-β-Fluoro-aristeromycin via Stereoselective Electrophilic Fluorination.

Author

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

Published

2017

41. π4s + π²s Cycloaddition of Spiroepoxycyclohexa-2,4-dienone, Radical Cyclization, and Oxidation-Aldol-Oxidation Cascade: Synthesis of BCDE Ring of Atropurpuran.

Author

Jarhad, Dnyandev B. and Singh, Vishwakarma

Abstract

Synthesis of a tetracyclic ring system (BCDE) of atropurpuran is described. Oxidative dearomatization, cycloaddition of spiroepoxycyclohexa-2,4-dienone, radical cyclization, and a tandem oxidation-aldol-oxidation are the key features of our methodology. [ABSTRACT FROM AUTHOR]

Published

2016

42. 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

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

Author

Kim G, Jarhad DB, Lee G, Kim G, Hou X, Yu J, Lee CS, Warnick E, Gao ZG, Ahn SY, Kwak D, Park K, Lee SD, Park TU, Jung SY, Lee JH, Choi JR, Kim M, Kim D, Kim B, Jacobson KA, and Jeong LS

Subjects

Humans, Structure-Activity Relationship, Animals, Mice, Molecular Structure, Rats, Female, Cell Line, Tumor, Adenine pharmacology, Adenine chemistry, Adenine analogs & derivatives, Adenosine A2 Receptor Antagonists pharmacology, Adenosine A2 Receptor Antagonists chemistry, Adenosine A2 Receptor Antagonists chemical synthesis, Nucleosides chemistry, Nucleosides pharmacology, Nucleosides chemical synthesis, Ribose chemistry, Ribose metabolism, Receptor, Adenosine A2A metabolism

Abstract

Building on the preceding structural analysis and a structure-activity relationship (SAR) of 8-aryl-2-hexynyl nucleoside hA 2A AR 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 hA 3 AR binding affinities depending on the type of ribose, whereas removal of ribose altered the functional efficacy via hA 2A AR. Among the synthesized derivatives, 2-aryl-8-hexynyl adenine 4a demonstrated the highest selectivity for hA 2A AR ( K i ,hA2A = 5.0 ± 0.5 nM, K i ,hA3 / K i ,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 4a as a viable immune-oncology therapeutic candidate.

Published

2024

44. Correction to "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

Published

2024

45. 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

46. 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

47. Asymmetric Synthesis of (-)-6'-β-Fluoro-aristeromycin via Stereoselective Electrophilic Fluorination.

Author

Kim G, Yoon JS, Jarhad DB, Shin YS, Majik MS, Mulamoottil VA, Hou X, Qu S, Park J, Baik MH, and Jeong LS

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

2017