Identification of Dipeptidyl Nitriles as Potent and Selective Inhibitors of Cathepsin B through Structure-Based Drug Design

Greenspan, Paul D.; Clark, Kirk; Tommasi, Rubén; Cowen, Scott D.; Mcquire, L.; Farley, David; Duzer, John H. van; Goldberg, R.L.; Zhou, Huanghai; Du, Zengming; Fitt, John J.; Coppa, David E.; Zheng, Fang; Macchia, William; Zhu, Lijuan; Capparelli, Michael; Goldstein, Robert J.; Wigg, A.M.; Doughty, John; Bohacek, Regine S.; Knap, Anna K.

doi:10.1021/jm010206q

Cited by 117 publications

(110 citation statements)

References 35 publications

(84 reference statements)

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“…In this work, the synthesis of a small library of chalcones and a study of their role as inhibitors of cathepsin B was carried out. First, the protocol of the docking was validated by reproducing the binding structure of the DPN ligand to active site of cathepsin B protein in the crystal complex (PDB code: 1GMY) (Greenspan et al, 2001), fig. 5.…”

Section: Docking Studiesmentioning

confidence: 99%

“…High mortality rate in patients could be mainly attributed to the invasiveness and metastasis in the prostate cancer progression. Generally, malignant cells show an increased rate of proteolytic activity, thus resulting in enhanced invasion and metastasis (Heidenreich et al, 2008;Fidler 1990). Many proteolytic enzymes are involved in the degradation of the extracellular matrices.…”

Section: Introductionmentioning

confidence: 99%

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Design, Synthesis and In-Silico Studies of Novel Chalcones as Anti-Prostate Cancer and Cathepsin B Inhibitors

Soliman¹,

Farrag²,

Omran³

2017

J App Pharm Sci

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In the present study a series of novel N-(4-3-(pheny)-1-prop-2-en-1-one phenyl) benzamide derivatives (5a-p) were synthesized, characterized and evaluated for their anti-prostate cancer activities against PC-3 prostate adenocarcinoma cell line using the SRB method. The cathepsin B inhibition potential was further tested by the using enzyme-linked immunosorbent assay. The furyl derivative 5p was the most active candidate, (IC50 = 5.597μΜ), against prostate cancer cell line, PC-3. This derivative also demonstrated 50.4% reduction in concentration of cathepsin B, additionally, compounds 5b and 5m showed 53.2 and 56.6% reduction in concentration of cathepsin B, respectively. In conclusion, compounds 5b, 5m and 5p showed good activity both as antiproliferative and as inhibitors of Cathepsin B production. Moreover, a pharmacophore model was constructed, a QSAR study was carried out where a model was successfully built from which the physicochemical parameters were correlated to the activity. This developed QSAR model was found statistically significant and had good predictive power. Furthermore, molecular docking studies of the active derivatives were also carried out, where they were found to maintain the essential key interactions, specially with the cysteine residue, Cys29.

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Section: Docking Studiesmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Design, Synthesis and In-Silico Studies of Novel Chalcones as Anti-Prostate Cancer and Cathepsin B Inhibitors

Soliman¹,

Farrag²,

Omran³

2017

J App Pharm Sci

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“…A wide variety of these inhibitors were obtained using computer-aided design. For example, high-resolution X-ray crystallographic data and molecular modeling studies were used to find out one of the most potent inhibitors of cathepsin B (K i =7nM) -dipeptide nitrile shown in Figure 8 (Greenspan et al, 2001). In the Figure www.intechopen.com…”

Section: Reversible Inhibitorsmentioning

confidence: 99%

Inhibitors of Proteinases as Potential Anti-Cancer Agents

Gluza¹,

Kafarski²

2011

Drug Development - A Case Study Based Insight Into Modern Strategies

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“…The lysosomal cysteine protease, Cathepsin B, hereafter Cat B, is responsible for the degradation and processing of proteins in living organisms [1,2]. The structure is characterised by a thiol in the cysteine residue, Cys29, and a histidine, His199, in the catalytic site [3,4], and therefore, in the context of metal-based drugs, offers the opportunity for coordination to metal centres.…”

Section: Introductionmentioning

confidence: 99%

Crystallographic, DFT and docking (cathepsin B) studies on an organotellurium(IV) compound

Caracelli

Zukerman-Schpector

Madureira

et al. 2016

Zeitschrift Für Kristallographie - Crystalline Materials

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Identification of Dipeptidyl Nitriles as Potent and Selective Inhibitors of Cathepsin B through Structure-Based Drug Design

Cited by 117 publications

References 35 publications

Design, Synthesis and In-Silico Studies of Novel Chalcones as Anti-Prostate Cancer and Cathepsin B Inhibitors

Design, Synthesis and In-Silico Studies of Novel Chalcones as Anti-Prostate Cancer and Cathepsin B Inhibitors

Inhibitors of Proteinases as Potential Anti-Cancer Agents

Crystallographic, DFT and docking (cathepsin B) studies on an organotellurium(IV) compound

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