Your search keyword '"Lin, Pin-Fang"' showing total 6 results

1. Inhibitors of HIV-1 attachment. Part 11: The discovery and structure–activity relationships associated with 4,6-diazaindole cores

Author

Bender, John A., Yang, Zhong, Eggers, Betsy, Gong, Yi-Fei, Lin, Pin-Fang, Parker, Dawn D., Rahematpura, Sandhya, Zheng, Ming, Meanwell, Nicholas A., and Kadow, John F.

Subjects

*HIV, *DRUG development, *STRUCTURE-activity relationships, *AZAINDOLES, *HIV-1 glycoprotein 120, *CLINICAL trials

Abstract

Abstract: A series of HIV-1 attachment inhibitors containing a 4,6-diazaindole core were examined in an effort to identify a compound which improved upon the potency and oral exposure of BMS-488043 (2). BMS-488043 (2) is a 6-azaindole-based HIV-1 attachment inhibitor which established proof-of-concept for this mechanism in human clinical studies but required high doses and concomitant administration of a high fat meal to achieve efficacious exposures. Based on previous studies in indole and azaindole scaffolds, SAR investigation was concentrated around the key 7-position in the 4,6-diazaindole series and led to the discovery of molecules with 5- to 20-fold increases in potency and three- to seven-fold increases in exposure over 2 in a rat PK studies. [Copyright &y& Elsevier]

Published

2013

2. Inhibitors of HIV-1 attachment. Part 10. The discovery and structure–activity relationships of 4-azaindole cores

Author

Wang, Tao, Yang, Zhong, Zhang, Zhongxing, Gong, Yi-Fei, Riccardi, Keith A., Lin, Pin-Fang, Parker, Dawn D., Rahematpura, Sandhya, Mathew, Marina, Zheng, Ming, Meanwell, Nicholas A., Kadow, John F., and Bender, John A.

Subjects

*HIV, *STRUCTURE-activity relationships, *AZAINDOLES, *DRUG development, *PIPERAZINE, *BENZAMIDE, *PHARMACOKINETICS, *BIOAVAILABILITY, *HIV-1 glycoprotein 120

Abstract

Abstract: A series of 4-azaindole oxoacetic acid piperazine benzamides was synthesized and evaluated in an effort to identify an oral HIV-1 attachment inhibitor with the potential to improve upon the pre-clinical profile of BMS-378806 (7), an initial clinical compound. Modifications at the 7-position of the 4-azaindole core modulated potency significantly and SAR showed that certain compounds with a 5-membered ring heteroaryl group at that position were the most potent. Four of the compounds with the best profiles were evaluated in a rat pharmacokinetic model and all had superior oral bioavailability and lower clearance when compared with 7. [Copyright &y& Elsevier]

Published

2013

3. Inhibitors of Human ImmunodeficiencyVirus Type 1(HIV-1) Attachment 6. Preclinical and Human Pharmacokinetic Profilingof BMS-663749, a Phosphonooxymethyl Prodrug of the HIV-1 AttachmentInhibitor 2-(4-Benzoyl-1-piperazinyl)-1-(4,7-dimethoxy-1H-pyrrolo[2,3-c]pyridin-3-yl)-2-oxoethanone (BMS-488043)

Author

Kadow, John F., Ueda, Yasutsugu, Meanwell, Nicholas A., Connolly, Timothy P., Wang, Tao, Chen, Chung-Pin, Yeung, Kap-Sun, Zhu, Juliang, Bender, John A., Yang, Zhong, Parker, Dawn, Lin, Pin-Fang, Colonno, Richard J., Mathew, Marina, Morgan, Daniel, Zheng, Ming, Chien, Caly, and Grasela, Dennis

Subjects

*HIV, *VIRUS inhibitors, *PHARMACOKINETICS, *METHYL groups, *PRODRUGS, *DRUG dosage

Abstract

BMS-663749, a phosphonooxymethyl prodrug 4of theHIV-1 attachment inhibitor 2-(4-benzoyl-1-piperazinyl)-1-(4,7-dimethoxy-1H-pyrrolo[2,3-c]pyridin-3-yl)-2-oxoethanone(BMS-488043) (2) was prepared and profiled in a varietyof preclinical in vitro and in vivo models designed to assess itsability to deliver parent drug following oral administration. Thedata showed that prodrug 4had excellent potential tosignificantly reduce dissolution rate-limited absorption followingoral dosing in humans. Clinical studies in normal healthy subjectsconfirmed the potential of 4, revealing that the prodrugsignificantly increased both the AUC and Cmaxof 2compared to a solid capsule formulation containingthe parent drug upon dose escalation. These data provided guidancefor further efforts to obtain an effective HIV-1 attachment inhibitor. [ABSTRACT FROM AUTHOR]

Published

2012

4. Increased sensitivity of HIV variants selected by attachment inhibitors to broadly neutralizing antibodies

Author

Zhou, Nannan, Fan, Li, Ho, Hsu-Tso, Nowicka-Sans, Beata, Sun, Yongnian, Zhu, Yingjie, Hu, Yanhua, McAuliffe, Brian, Rose, Burt, Fang, Hua, Wang, Tao, Kadow, John, Krystal, Mark, Alexander, Louis, Colonno, Richard, and Lin, Pin-Fang

Subjects

*HIV, *MICROBIAL sensitivity tests, *MICROBIAL mutation, *IMMUNOGLOBULINS, *HOST-virus relationships, *ANTIVIRAL agents, *EPITOPES

Abstract

Abstract: Treatment with HIV attachment inhibitors (AIs) can select for escape mutants throughout the viral envelope. We report on three such mutations: F423Y (gp120 CD4 binding pocket) and I595F and K655E (gp41 ectodomain). Each displayed decreased sensitivity to the AI BMS-488043 and earlier generation AIs, along with increased sensitivity to the broadly neutralizing antibodies 2F5 and 4E10, without affecting the rate of viral entry or sensitivity to the entry inhibitors AMD-3100 and Enfuvirtide. We also observed that I595F did not substantially increase envelope sensitivity to HIV-infected patient sera. Based on these observations, we propose that although F423Y, I595F and K655E may all affect the presentation of the 2F5 and 4E10 epitopes, natural immune mimicry is rare only for the I595F effect. Thus, it seems that in addition to restricting AI resistance development, incorporation of I595F into an appropriate vehicle could elicit a novel antiviral response to improve vaccine efficacy. [Copyright &y& Elsevier]

Published

2010

5. Inhibitors of HIV-1 attachment. Part 4: A study of the effect of piperazine substitution patterns on antiviral potency in the context of indole-based derivatives

Author

Wang, Tao, Kadow, John F., Zhang, Zhongxing, Yin, Zhiwei, Gao, Qi, Wu, Dedong, Parker, Dawn DiGiugno, Yang, Zheng, Zadjura, Lisa, Robinson, Brett A., Gong, Yi-Fei, Blair, Wade S., Shi, Pei-Yong, Yamanaka, Gregory, Lin, Pin-Fang, and Meanwell, Nicholas A.

Subjects

*VIRUS inhibitors, *HIV, *PIPERAZINE, *SUBSTITUTION reactions, *ANTIVIRAL agents, *INDOLE, *KETONES, *GLYCOPROTEINS, *CELL receptors, *BINDING sites

Abstract

Abstract: 4-Fluoro- and 4-methoxy-1-(4-benzoylpiperazin-1-yl)-2-(1H-indol-3-yl)ethane-1,2-dione (2 and 3, respectively) have been characterized as potent inhibitors of HIV-1 attachment that interfere with the interaction of viral gp120 with the host cell receptor CD4. As part of an effort to understand fundamental aspects of this pharmacophore, discovered originally using a high throughput cell-based screen, modification and substitution of the piperazine ring was examined in the context of compounds 6a–ah. The piperazine ring was shown to be a critical element of the HIV-1 attachment inhibiting pharmacophore, acting as a scaffold to deploy the indole glyoxamide and benzamide in a topographical relationship that complements the binding site on gp120. [Copyright &y& Elsevier]

Published

2009

6. Inhibitors of HIV-1 attachment. Part 3: A preliminary survey of the effect of structural variation of the benzamide moiety on antiviral activity

Author

Meanwell, Nicholas A., Wallace, Owen B., Wang, Henry, Deshpande, Milind, Pearce, Bradley C., Trehan, Ashok, Yeung, Kap-Sun, Qiu, Zhilei, Wright, J.J. Kim, Robinson, Brett A., Gong, Yi-Fei, Wang, Hwei-Gene Heidi, Blair, Wade S., Shi, Pei-Yong, and Lin, Pin-fang

Subjects

*VIRUS inhibitors, *HIV, *STRUCTURAL analysis (Science), *BENZAMIDE, *ANTIVIRAL agents, *GLYCOPROTEINS, *STRUCTURE-activity relationships, *CELL receptors, *PHENYL compounds, *INDOLE, *THERAPEUTICS

Abstract

Abstract: 1-(4-Benzoylpiperazin-1-yl)-2-(1H-indol-3-yl)ethane-1,2-dione (1a) has been characterized as an inhibitor of HIV-1 attachment that interferes with the interaction of viral gp120 with the host cell receptor CD4. In previous studies, the effect of indole substitution pattern on antiviral activity was probed. In this Letter, the effect of structural variation of the benzamide moiety is described, a study that reveals the potential or the phenyl moiety to be replaced by five-membered heterocyclic rings and a restricted tolerance for the introduction of substituents to the phenyl ring. [Copyright &y& Elsevier]

Published

2009