Potent memapsin 2 (β-secretase) inhibitors: Design, synthesis, protein-ligand X-ray structure, and in vivo evaluation

Ghosh, Arun K.; Kumaragurubaran, Nagaswamy; Lin, Hong; Kulkarni, Sarang; Xu, Xiaoming; Miller, Heather B.; Reddy, D. Srinivasa; Weerasena, Vajira; Turner, Robert T.; Chang, Wan‐Pin; Koelsch, Gerald; Tang, Jordan

doi:10.1016/j.bmcl.2007.12.028

Cited by 90 publications

(88 citation statements)

References 29 publications

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“…Coburn provided a possible explanation for the unexpected phenomena [23] that the α-methyl of (4-fluorophenyl)ethyl of 3 at the 3-position packs firmly against Ile110 of BACE-1, which orients the 4-fluorophenyl ring toward S 3 and creates a novel S 3 subpocket (S 3 SP ). The subpocket is unique, different from other reported BACE-1 complexed structures, which may make (4-fluorophenyl) ethyl as a suitable substituent as R 3 , even for HE-based inhibitors [14,15] , although it is relatively large for the S 3 pocket. The special orientation of the molecules in the active pockets of BACE-1 is closely associated with the groups of the 5-position of N-terminal isophthalamide, which may result in N-methyl(methylsulfonyl)amino being more preferable than the nitro group at this site when (4-fluorophenyl)ethyl group is selected as R 3 .…”

Section: Discussionmentioning

confidence: 77%

“…Compounds 10 and 11, which contain the substituent, did show nanomolar activities. The unexpected results pushed us to carefully study the complex crystal structures of 3 and 4 [14,15,23,24] . Coburn provided a possible explanation for the unexpected phenomena [23] that the α-methyl of (4-fluorophenyl)ethyl of 3 at the 3-position packs firmly against Ile110 of BACE-1, which orients the 4-fluorophenyl ring toward S 3 and creates a novel S 3 subpocket (S 3 SP ).…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, BACE-1 gene knockout mice showed no Aβ production and appeared healthy, which offered further powerful in vivo evidence for the opinion that BACE-1 was an attractive AD target and inhibition of the protease could effectively reduce Aβ formation, thereby halting the progression of AD [11,12] . Since first discovered in 1999, numerous BACE-1 inhibitors have been designed, synthesized and evaluated the biological activities, in which some molecules caused an in vivo decrease of amyloids when used in animal models (eg, 1, 2) [13][14][15] , especially compound GRL-7234 bearing the HE scaffold, which has been shown to induce a reduction of Aβ 40 production in transgenic mice after a single intraperitoneal administration ( Figure 1) [14] . However, the majority of these compounds are peptide-based analogs [16][17][18][19][20][21] that, if used as drug agents, will face formidable difficulties due to their vulnerability to degradative enzymes, rapid biliary clearance and poor oral absorption [22] .…”

Section: Introductionmentioning

confidence: 99%

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Discovery of potent β-secretase (bace-1) inhibitors by the synthesis of isophthalamide-containing hybrids

Zhu

Xiao

et al. 2009

Acta Pharmacol Sin

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Aim:The aim of this study was to design and synthesize a series of high activity compounds against aspartyl protease β-secretase (BACE-1) bearing hydroxyethylene (HE) framework.Methods: First, we designed the small library based on our previous work and rational analysis. Subsequently, thirteen compounds were selected and synthesized using skilled solid phase synthetic methods to explore the relationship between structure and activity. We then used molecular modeling to explain the possible binding mode. Results:Thirteen new compounds (6-18) have been designed, synthesized and bioassayed. Their structures were determined by nuclear magnetic resonance (NMR) spectra, low-and high-resolution mass spectra and optical rotation. Most compounds have shown moderate to excellent activities, and compound 10, which contains fewer amino acids and amide bonds than GRL-7234, was about 5-fold more potent than the control compound 4 discovered by Merck. The molecular modeling results have indicated the possible binding mode and explained the difference between compounds 10 and 16, providing direction for further study. Conclusion:This study yielded several high activity compounds bearing fewer amino acids and amide bonds than previous compounds, providing insight into the further development of potent BACE-1 inhibitors for the treatment of Alzheimer's disease.

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Section: Discussionmentioning

confidence: 77%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Discovery of potent β-secretase (bace-1) inhibitors by the synthesis of isophthalamide-containing hybrids

Zhu

Xiao

et al. 2009

Acta Pharmacol Sin

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“…Several examples are shown in Figure 10. These can be roughly classified by their transition state mimic and include: (1) peptidomimetic designs incorporating statine Hu et al, 2003Hu et al, , 2004Lamar et al, 2004;Tung et al, 2002], hydroxymethylcarbonyl [Hamada et al, 2006[Hamada et al, , 2008aShuto et al, 2003], or hydroxyethylene [Brady et al, 2004;Ghosh et al, 2006;Hanessian et al, 2005;Hom et al, 2004;Xiao et al, 2006]; (2) nonpeptidic designs incorporating a reduced amide , hydroxymethylcarbonyl [Hamada et al, 2008a,b] hydroxyethylene [Ghosh et al, 2007], hydroxyethylamine Freskos et al, 2007a,b;Ghosh et al, 2008;Kortum et al, 2007;Maillard et al, 2007;Park et al, 2008;Stachel et al, 2004Stachel et al, , 2006Stauffer et al, 2007], aminoethylene , or tertiary carbinamine [Lindsley et al, 2007;Rajapakse et al, 2006]; (3) arylpiperazines [Garino et al, 2006]; (4) acylguanidines Fobare et al, 2007;Jennings et al, 2008]; (5) dihydroquinazolines [Baxter et al, 2007]; (6) isocytosines Geschwindner et al, 2007]; (7) pyrrolidine/piperidines [Iserloh et al,Fig. 9.…”

Section: Structure-based Designmentioning

confidence: 99%

Structure and modeling in the design of β‐ and γ‐secretase inhibitors

Holloway

Hunt

McGaughey

2009

Drug Development Research

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This review discusses the involvement of structure and modeling in the design of b-secretase (BACE-1) and g-secretase inhibitors as putative Alzheimer's Disease therapeutics. The early and broad availability of structural information for BACE-1, a membrane-tethered aspartyl protease, has led to the use of in silico methods in the overall design and optimization process. However, for g-secretase, an integral membrane protein, the lack of a detailed 3D structure has limited the application of computational methods. Drug Dev Res 70 : 70-93, 2009.

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“…[8][9][10] Segundo a hipótese da cascata amiloide, os níveis elevados de proteínas insolúveis b-Amiloides (Ab) são responsáveis pela formação de placas amiloides e emaranhados neurofibrilares que estão relacionados com morte celular, processos inflamatórios, demência e DA. 11 Embora o desenvolvimento de fárma-cos que bloqueiem ou revertam a formação de proteínas insolúveis bAmiloides seja uma área de grande interesse, 12,13 as terapias disponíveis atualmente para o tratamento de DA visam manter e facilitar a atividade dos sistemas colinérgicos sobreviventes. 14 Nesse sentido, a principal estratégia terapêutica disponível se baseia na inibição das colinesterases (ChEIs), uma vez que a modulação dos níveis de ACh é feita por duas enzimas, a acetilcolinesterase (AChE -EC 3.1.1.7) e butirilcolinesterase (BuChE -EC 3.1.1.8).…”

Section: Introductionunclassified

Estudos de QSAR 3D para um conjunto de inibidores de butirilcolinesterase humana

Freitas¹,

Paz²,

Castilho³

2009

Quím. Nova

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Recebido em 9/12/08; aceito em 14/4/09; publicado na web em 22/9/09 QSAR 3D STUDIES OF A SERIES OF HUMAN BUTYRYLCHOLINESTERASE INHIBITORS. Alzheimer's disease (AD) is considered the main cause of cognitive decline in adults. The available therapies for AD treatment seek to maintain the activity of cholinergic system through the inhibition of the enzyme acetylcholinesterase. However, butyrylcholinesterase (BuChE) can be considered an alternative target for AD treatment. Aiming at developing new BuChE inhibitors, robust QSAR 3D models with high predictive power were developed. INTRODUÇÃOA doença ou mal de Alzheimer (DA), descrita primeiramente por Alois Alzheimer 1 acomete cerca de 37 milhões de pessoas em todo o mundo, 2 sendo considerada a principal causa de declínio cognitivo em adultos.3 De fato, 50 a 70% dos casos de demência entre idosos acima de 65 anos está relacionada à DA e aproximadamente 5% desta população será afetada pelo mal de Alzheimer. 4 De acordo com a OMS, a prevalência da doença dobra a cada 5 anos, passando de 3% aos 70 anos para 20-30% aos 85 anos.3 Dessa forma, esperase que o número de casos aumente para 114 milhões até 2050.5 De fato, em função do número crescente de pacientes com DA, os custos diretos e indiretos associados ao tratamento dessa doença são de, no mínimo, 100 bilhões de dólares, nos EUA. 2O mal de Alzheimer caracteriza-se por diversos eventos metabólicos que culminam no aparecimento dos sinais característicos da doença. Entre esses eventos estão a deposição de placas de proteínas insolúveis b-Amiloides (Ab), como resultado do metabolismo anormal da proteína precursora de b-Amiloide (PPA) e formação de emaranhados neurofibrilares, em função do colapso do citoesqueleto neuronal, decorrente da hiperfosforilação da proteína Tau, em regiões do lobo temporal e neocórtex.6 Soma-se a isso, o processo de disfunção simpática e neuroquímica relacionada à redução da atividade colinérgica central. 7 Como consequência desses eventos neuropatológicos, há perda de memória, grandes variações de humor, depressão associada a distúrbios de linguagem, perda de poder de julgamento etc.Atualmente, as principais estratégias terapêuticas para o tratamento de DA baseiam-se na hipótese colinérgica ou na hipótese amiloide. De acordo com a hipótese colinérgica, processos neurodegenerativos levam à destruição de neurônios colinérgicos da região frontal do cérebro resultando em déficit da transmissão colinérgica central, 4 provocando declínio cognitivo e perda da capacidade de execução das tarefas diárias, redução da atenção e da memória.8-10 Segundo a hipótese da cascata amiloide, os níveis elevados de proteínas insolúveis b-Amiloides (Ab) são responsáveis pela formação de placas amiloides e emaranhados neurofibrilares que estão relacionados com morte celular, processos inflamatórios, demência e DA.11 Embora o desenvolvimento de fárma-cos que bloqueiem ou revertam a formação de proteínas insolúveis bAmiloides seja uma área de grande interesse, 12,13 as terapias disponíveis atualmente para o tratamento ...

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Potent memapsin 2 (β-secretase) inhibitors: Design, synthesis, protein-ligand X-ray structure, and in vivo evaluation

Cited by 90 publications

References 29 publications

Discovery of potent β-secretase (bace-1) inhibitors by the synthesis of isophthalamide-containing hybrids

Discovery of potent β-secretase (bace-1) inhibitors by the synthesis of isophthalamide-containing hybrids

Structure and modeling in the design of β‐ and γ‐secretase inhibitors

Estudos de QSAR 3D para um conjunto de inibidores de butirilcolinesterase humana

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