Your search keyword '"Drug Screening Assays"' showing total 132 results

1. Tumor Genomic Profiling and Ex Vivo Drug Sensitivity Testing for Pediatric Leukemia and Lymphoma Patients

Author

Eaton, Aubrie, Wong, Victor, Schiff, Deborah, Anderson, Eric, Ding, Hilda, Capparelli, Edmund V, Determan, Deb, and Kuo, Dennis John

Subjects

Pediatric, Pediatric Research Initiative, Lymphoma, Pediatric Cancer, precision medicine, Human Genome, acute lymphoblastic leukemia, pediatric oncology, Hematology, acute myeloid leukemia, Rare Diseases, Orphan Drug, Good Health and Well Being, Clinical Research, 5.1 Pharmaceuticals, Pediatrics, Perinatology and Child Health, drug screening assays, Genetics, Pharmacology (medical), genomic profiling, Development of treatments and therapeutic interventions, antitumor, Biotechnology, Cancer

Abstract

OBJECTIVE To describe the frequency of use of tumor genomic profiling and functional ex vivo drug sensitivity testing in pediatric patients with hematologic malignancies at our institution, and to determine how the results affected treatment selection. METHODS A retrospective chart review was conducted to analyze the frequency of tumor genomic profiling and functional drug sensitivity screening in our institution in pediatric patients with hematologic malignancies and to ask if the results were used to direct treatment. A case series of patients for whom these testing recommendations resulted in therapeutic interventions is reported. RESULTS Thirty-three patients underwent tumor genomic profiling assays, functional ex vivo testing, or both. Nineteen patients (58%) had genomic profiling assays performed alone, 3 (9%) had functional ex vivo testing performed alone, and 11 (33%) had both tests performed. Twenty-one (64%) patients had potentially actionable mutations detected by the genomic profiling assay. Seven (21%) patients received at least 1 chemotherapeutic agent in accordance with the tumor genomic profiling or functional ex vivo drug sensitivity testing results. Three (43%) of the 7 patients who were treated with testing directed therapy had a favorable treatment response (PR or CR) to treatments selected based upon results of genomic or functional ex vivo testing. CONCLUSIONS This retrospective case series demonstrates that precision medicine techniques such as genomic profiling and drug sensitivity testing can positively inform treatment selection in pediatric patients with relapsed or refractory leukemia and lymphoma.

Published

2022

2. New 1,2,3-triazole linked ciprofloxacin-chalcones induce DNA damage by inhibiting human topoisomerase I& II and tubulin polymerization

Author

Hamada H. H. Mohammed, Amer Ali Abd El-Hafeez, Kareem Ebeid, Aml I. Mekkawy, Mohammed A. S. Abourehab, Emad I. Wafa, Suhaila O. Alhaj-Suliman, Aliasger K. Salem, Pradipta Ghosh, Gamal El-Din A. Abuo-Rahma, Alaa M. Hayallah, and Samar H. Abbas

Subjects

Medicinal & Biomolecular Chemistry, Type I, chalcone, Antineoplastic Agents, HCT116 cells, Drug Screening Assays, Type II, topoisomerase I and II inhibitors, Cell Line, Polymerization, Structure-Activity Relationship, Medicinal and Biomolecular Chemistry, Chalcone, Chalcones, Ciprofloxacin, Tubulin, ciprofloxacin, tubulin polymerisation inhibition, Cell Line, Tumor, Drug Discovery, Humans, Cell Proliferation, Cancer, Pharmacology, Tumor, Molecular Structure, General Medicine, Antitumor, Triazoles, Click synthesis, Colo-Rectal Cancer, DNA Topoisomerases, Type II, DNA Topoisomerases, Type I, Doxorubicin, DNA damage, cytotoxicity, Biochemistry and Cell Biology, Drug Screening Assays, Antitumor, Caco-2 Cells, Digestive Diseases, DNA Topoisomerases, DNA Damage

Abstract

A series of novel 1,2,3-triazole-linked ciprofloxacin-chalcones 4a-j were synthesised as potential anticancer agents. Hybrids 4a-j exhibited remarkable anti-proliferative activity against colon cancer cells. Compounds 4a-j displayed IC50s ranged from 2.53-8.67 µM, 8.67–62.47 µM, and 4.19–24.37 µM for HCT116, HT29, and Caco-2 cells; respectively, whereas the doxorubicin, showed IC50 values of 1.22, 0.88, and 4.15 µM. Compounds 4a, 4b, 4e, 4i, and 4j were the most potent against HCT116 with IC50 values of 3.57, 4.81, 4.32, 4.87, and 2.53 µM, respectively, compared to doxorubicin (IC50 = 1.22 µM). Also, hybrids 4a, 4b, 4e, 4i, and 4j exhibited remarkable inhibitory activities against topoisomerase I, II, and tubulin polymerisation. They increased the protein expression level of γH2AX, indicating DNA damage, and arrested HCT116 in G2/M phase, possibly through the ATR/CHK1/Cdc25C pathway. Thus, the novel ciprofloxacin hybrids could be exploited as potential leads for further investigation as novel anticancer medicines to fight colorectal carcinoma.

Published

2022

3. Are Pt(IV) Prodrugs That Release Combretastatin A4 True Multi-action Prodrugs?

Author

Ingo Ott, Valentina Gandin, Claudia Schmidt, Annika Timm, Viktor Brabec, Uttara Basu, Hana Kostrhunova, Dan Gibson, and Tomer Babu

Subjects

Organoplatinum Compounds, Stereochemistry, Antineoplastic Agents, Drug Screening Assays, Ligands, Cell Line, Dose-Response Relationship, Structure-Activity Relationship, Carbonic Anhydrase IV, Cricetulus, Prohibitins, Drug Discovery, medicine, Animals, Humans, Moiety, Prodrugs, Cytotoxicity, IC50, Cell Proliferation, Cisplatin, Dose-Response Relationship, Drug, Molecular Structure, Ligand, Chemistry, Lewis lung carcinoma, Antitumor, Prodrug, In vitro, Molecular Medicine, Drug Screening Assays, Antitumor, Drug, medicine.drug

Abstract

"Multi-action" Pt(IV) derivatives of cisplatin with combretastatin A4 (CA4) bioactive ligands that are conjugated to Pt(IV) by carbonate are unique because the ligand (IC50 < 10 nM) is dramatically 1000-folds more cytotoxic than cisplatin in vitro. The Pt(IV)-CA4 prodrugs were as cytotoxic as CA4 itself, indicating that the platinum moiety probably plays an insignificant role in triggering cytotoxicity, suggesting that the Pt(IV)-CA4 complexes act as prodrugs for CA4 rather than as true multi-action prodrugs. In vivo tests (Lewis lung carcinoma) show that ctc-[Pt(NH3)2(PhB)(CA4)Cl2] inhibited tumor growth by 93% compared to CA4 (67%), cisplatin (84%), and 1:1:1 cisplatin/CA4/PhB (85%) while displaying

Published

2021

4. Sensitivity of Oncogenic KRAS-Expressing Cells to CDK9 Inhibition

Author

Nicolas Muzet, Matthew Holderfield, Kanika Sharma, Eamonn Rooney, Bertrand Vivet, Renaud Morales, Christophe Marcireau, Ming Yi, Laurent Debussche, Frederic Lacroix, Walter Englaro, Julia Frappier, Dwight V. Nissley, Emilie Schell, Lick Pui Lai, Frank McCormick, Viviane Brel, Nicolas Basse, and Nadia Le-Henanf

Subjects

0301 basic medicine, phenotypic high-throughput screen, Phenotypic screening, CDK9, Synthetic lethality, Drug Screening Assays, medicine.disease_cause, Biochemistry, Article, Analytical Chemistry, Proto-Oncogene Proteins p21(ras), Mice, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, KRAS, medicine, isogenic cell panel, 2.1 Biological and endogenous factors, Animals, Viability assay, Aetiology, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Cancer, Neoplastic, Kinase, Chemistry, Antitumor, Cyclin-Dependent Kinase 9, synthetic lethality, Colo-Rectal Cancer, High-Throughput Screening Assays, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Gene Expression Regulation, 5.1 Pharmaceuticals, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, Cyclin-dependent kinase 9, Development of treatments and therapeutic interventions, Drug Screening Assays, Antitumor, Digestive Diseases, Biotechnology

Abstract

Oncogenic forms of KRAS proteins are known to be drivers of pancreatic, colorectal, and lung cancers. The goal of this study is to identify chemical leads that inhibit oncogenic KRAS signaling. We first developed an isogenic panel of mouse embryonic fibroblast (MEF) cell lines that carry wild-type RAS, oncogenic KRAS, and oncogenic BRAF. We validated these cell lines by screening against a tool compound library of 1402 annotated inhibitors in an adenosine triphosphate (ATP)-based cell viability assay. Subsequently, this MEF panel was used to conduct a high-throughput phenotypic screen in a cell viability assay with a proprietary compound library. All 126 compounds that exhibited a selective activity against mutant KRAS were selected and prioritized based on their activities in secondary assays. Finally, five chemical clusters were chosen. They had specific activity against SW620 and LS513 over Colo320 colorectal cancer cell lines. In addition, they had no effects on BRAF(V600E), MEK1, extracellular signal-regulated kinase 2 (ERK2), phosphoinositide 3-kinase alpha (PI3Kα), AKT1, or mammalian target of rapamycin (mTOR) as tested in in vitro enzymatic activity assays. Biophysical assays demonstrated that these compounds did not bind directly to KRAS. We further identified the mechanism of action and showed that three of them have CDK9 inhibitory activity. In conclusion, we have developed and validated an isogenic MEF panel that was used successfully to identify RAS oncogenic or wild-type allele-specific vulnerabilities. Furthermore, we identified sensitivity of oncogenic KRAS-expressing cells to CDK9 inhibitors, which warrants future studies of treating KRAS-driven cancers with CDK9 inhibitors.

Published

2021

5. Scalable Total Synthesis, IP3R Inhibitory Activity of Desmethylxestospongin B, and Effect on Mitochondrial Function and Cancer Cell Survival

Author

Paula Farias, Armen Zakarian, Jordi Molgó, Artur K. Mailyan, Maša Podunavac, Jeffrey J. Jackson, Cesar Cardenas, Hernan Huerta, Alenka Lovy, CEA- Saclay (CEA), and Commissariat à l'énergie atomique et aux énergies alternatives (CEA)

Subjects

Cell type, Cell Survival, [SDV]Life Sciences [q-bio], Antineoplastic Agents, 010402 general chemistry, Drug Screening Assays, 01 natural sciences, Catalysis, Article, Cell Line, chemistry.chemical_compound, Cell Line, Tumor, medicine, Inositol 1,4,5-Trisphosphate Receptors, [CHIM]Chemical Sciences, Humans, cancer, IP3R receptor, total synthesis, ComputingMilieux_MISCELLANEOUS, 5-Trisphosphate Receptors, Calcium signaling, Cell Proliferation, Biological Products, Natural product, Tumor, xestospongins, Molecular Structure, 010405 organic chemistry, Organic Chemistry, Cancer, Total synthesis, General Chemistry, Antitumor, General Medicine, medicine.disease, Inositol 1, 0104 chemical sciences, Cell biology, Mitochondria, chemistry, Cancer cell, Chemical Sciences, Lactam, Drug Screening Assays, Antitumor, metabolism, Function (biology)

Abstract

The scalable synthesis of the oxaquinolizidine marine natural product desmethylxestospongin B is based on the early application of Ireland-Claisen rearrangement, macrolactamization, and a late-stage installation of the oxaquinolizidine units by lactam reduction. The synthesis serves as the source of material to investigate calcium signaling and its effect on mitochondrial metabolism in various cell types, including cancer cells.

Published

2021

6. Tutuilamides A–C: Vinyl-Chloride-Containing Cyclodepsipeptides from Marine Cyanobacteria with Potent Elastase Inhibitory Properties

Author

Anthony J. O’Donoghue, Hendrik Luesch, Brian M. Suzuki, K.M. Canuto, Brendan M. Duggan, Jehad Almaliti, Evgenia Glukhov, Asfandyar Sikandar, C. Liu, Jesko Koehnke, William H. Gerwick, Dan Luo, Lena Keller, C. B. Naman, and HZI,Helmholtz-Zentrum für Infektionsforschung GmbH, Inhoffenstraße 7, 38124 Braunschweig, Germany.

Subjects

0301 basic medicine, Lung Neoplasms, Drug Screening Assays, 01 natural sciences, Biochemistry, chemistry.chemical_compound, Models, Tandem Mass Spectrometry, Depsipeptides, Amino Acids, Enzyme Inhibitors, chemistry.chemical_classification, Cyclic, Chromatography, Tumor, Pancreatic Elastase, Molecular Structure, Aminobutyrates, Elastase, General Medicine, Biological Sciences, Cyclic peptide, Amino acid, High Pressure Liquid, Molecular Medicine, Two-dimensional nuclear magnetic resonance spectroscopy, Protein Binding, Cell Survival, Stereochemistry, Antiparasitic, medicine.drug_class, Vinyl Chloride, Antineoplastic Agents, Cyanobacteria, Cell Line, 03 medical and health sciences, Residue (chemistry), Hydrolase, medicine, Humans, Piperidones, Natural product, 010405 organic chemistry, Organic Chemistry, Molecular, Antitumor, 0104 chemical sciences, 030104 developmental biology, chemistry, Chemical Sciences, Peptides

Abstract

Marine cyanobacteria (blue-green algae) have been shown to possess an enormous capacity to produce structurally diverse natural products that exhibit a broad spectrum of potent biological activities, including cytotoxic, antifungal, antiparasitic, antiviral, and antibacterial activities. Using mass-spectrometry-guided fractionation together with molecular networking, cyanobacterial field collections from American Samoa and Palmyra Atoll yielded three new cyclic peptides, tutuilamides A-C. Their structures were established by spectroscopic techniques including 1D and 2D NMR, HR-MS, and chemical derivatization. Structure elucidation was facilitated by employing advanced NMR techniques including nonuniform sampling in combination with the 1,1-ADEQUATE experiment. These cyclic peptides are characterized by the presence of several unusual residues including 3-amino-6-hydroxy-2-piperidone and 2-amino-2-butenoic acid, together with a novel vinyl chloride-containing residue. Tutuilamides A-C show potent elastase inhibitory activity together with moderate potency in H-460 lung cancer cell cytotoxicity assays. The binding mode to elastase was analyzed by X-ray crystallography revealing a reversible binding mode similar to the natural product lyngbyastatin 7. The presence of an additional hydrogen bond with the amino acid backbone of the flexible side chain of tutuilamide A, compared to lyngbyastatin 7, facilitates its stabilization in the elastase binding pocket and possibly explains its enhanced inhibitory potency.

Published

2020

7. Oxazole-Based Compounds As Anticancer Agents

Author

Salvatore V. Giofrè, Giuseppe Lanza, Roberto Romeo, Daniela Iannazzo, Ugo Chiacchio, Maria A. Chiacchio, Laura Legnani, Chiacchio, M, Lanza, G, Chiacchio, U, Giofre, S, Romeo, R, Iannazzo, D, and Legnani, L

Subjects

Oxazolidine, Antineoplastic Agents, Oxazoline, Drug Screening Assays, 010402 general chemistry, 01 natural sciences, Biochemistry, Anticancer activity, Oxazole, Cell Line, Synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Isoxazole, Cell Line, Tumor, Drug Discovery, Humans, Oxazoles, Pharmacology, Tumor, 010405 organic chemistry, Drug discovery, Synthesi, Organic Chemistry, Biological activity, Antitumor, Combinatorial chemistry, 0104 chemical sciences, Drug Screening Assays, Antitumor, chemistry, Chemical diversity, Molecular Medicine, Anticancer activity, Isoxazole, Oxazole, Oxazolidine, Oxazoline, Synthesis

Abstract

Heterocyclic compounds represent a significant target for anti-cancer research and drug discovery, due to their structural and chemical diversity. Oxazoles, with oxygen and nitrogen atoms present in the core structure, enable various types of interactions with different enzymes and receptors, favoring the discovery of new drugs. Aim of this review is to describe the most recent reports on the use of oxazole-based compounds in anticancer research, with reference to the newly discovered iso/oxazole-based drugs, to their synthesis and to the evaluation of the most biologically active derivatives. The corresponding dehydrogenated derivatives, i.e. iso/oxazolines and iso/oxazolidines, are also reported.

Published

2020

8. The anticancer activity of an air-stable Pd(<scp>i</scp>)-NHC (NHC = N-heterocyclic carbene) dimer

Author

Busra Dereli, Stefano Palazzolo, Enrica Bortolamiol, Tiziana Perin, Manoj V. Mane, Flavio Rizzolio, Nicola Demitri, Vincenzo Canzonieri, Steven P. Nolan, Isabella Caligiuri, Thomas Scattolin, Fabiano Visentin, and Luigi Cavallo

Subjects

ISOCYANIDES, Cell Survival, Stereochemistry, Dimer, SUPPORTED PRECATALYSTS, BRIDGING ALLYL, Antineoplastic Agents, Drug Screening Assays, Catalysis, Cell Line, Dose-Response Relationship, Structure-Activity Relationship, chemistry.chemical_compound, CYCLOPENTADIENYL, Coordination Complexes, Heterocyclic Compounds, Cell Line, Tumor, Cell Proliferation, Dimerization, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Methane, Molecular Structure, Palladium, Materials Chemistry, Settore CHIM/03 - Chimica Generale e Inorganica, Tumor, Chemistry, Metals and Alloys, Antitumor, General Chemistry, REACTIVITY, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, UNUSUAL COORDINATION BEHAVIOR, DINUCLEAR PALLADIUM(I), Ceramics and Composites, BINUCLEAR PALLADIUM(I) COMPLEXES, LIGANDS, Drug, BOND, Carbene

Abstract

A new dinuclear Pd(i) complex coordinating two bis(NHC) ligands revealed an unsuspected stability despite the unsaturation of the two metal centres. Even more surprisingly, the compound showed high and selective antiproliferative activity against different cancer cell lines and ovarian cancer tumoroids, and the mechanism of action was different from that of cisplatin.

Published

2020

9. A first-in-class anticancer dual HDAC2/FAK inhibitors bearing hydroxamates/benzamides capped by pyridinyl-1,2,4-triazoles

Author

Mustafa, Muhamad, Abd El-Hafeez, Amer Ali, Abdelhamid, Dalia, Katkar, Gajanan D, Mostafa, Yaser A, Ghosh, Pradipta, Hayallah, Alaa M, and Abuo-Rahma, Gamal El-Din A

Subjects

Medicinal & Biomolecular Chemistry, Histone Deacetylase 2, Antineoplastic Agents, Apoptosis, Hydroxamic Acids, Drug Screening Assays, Dose-Response Relationship, Structure-Activity Relationship, Medicinal and Biomolecular Chemistry, Humans, Protein Kinase Inhibitors, Cell Proliferation, Cancer, 4-Triazoles, Cultured, Molecular Structure, FAK, Organic Chemistry, Antitumor, Pharmacology and Pharmaceutical Sciences, Triazoles, Tumor Cells, HDAC2, Histone Deacetylase Inhibitors, Anticancer, 5.1 Pharmaceuticals, Focal Adhesion Kinase 1, Benzamides, Molecular docking, Drug, Development of treatments and therapeutic interventions

Abstract

Novel 5-pyridinyl-1,2,4-triazoles were designed as dual inhibitors of histone deacetylase 2 (HDAC2) and focal adhesion kinase (FAK). Compounds 5d, 6a, 7c, and 11c were determined as potential inhibitors of both HDAC2 (IC50=0.09-1.40μM) and FAK (IC50=12.59-36.11nM); 6a revealed the highest activity with IC50 values of 0.09μM and 12.59nM for HDAC2 and FAK, respectively. Compound 6a was superior to reference drugs vorinostat and valproic acid in its ability to inhibit growth/proliferation of A-498 and Caki-1 renal cancer cells. Further investigation proved that 6a strongly arrests the cell cycle at the G2/M phase and triggers apoptosis in both A-498 and Caki-1cells. Moreover, the enhanced Akt activity that is observed upon chronic application of HDAC inhibitors was effectively suppressed by the dual HDAC2/FAK inhibitor. Finally, the high potency and selectivity of 6a towards HDAC2 and FAK proteins were rationalized by molecular docking. Taken together, these findings highlight the potential of 6a as a promising dual-acting HDAC2/FAK inhibitor that could benefit from further optimization.

Published

2021

10. Identification of Active Compounds against Melanoma Growth by Virtual Screening for Non-Classical Human DHFR Inhibitors

Author

Andrés Felipe Vásquez, Luis Alberto Gómez, Andrés González Barrios, and Diego M. Riaño-Pachón

Subjects

Organic Chemistry, Antineoplastic Agents, General Medicine, PROTEÍNAS, Catalysis, Computer Science Applications, Inorganic Chemistry, Tetrahydrofolate Dehydrogenase, Methotrexate, DHFR inhibitors, pharmacophore modeling, molecular docking simulations, virtual screening, melanoma, drug screening assays, drug discovery, Humans, Folic Acid Antagonists, Physical and Theoretical Chemistry, Melanoma, Molecular Biology, Spectroscopy

Abstract

Antifolates such as methotrexate (MTX) have been largely known as anticancer agents because of their role in blocking nucleic acid synthesis and cell proliferation. Their mechanism of action lies in their ability to inhibit enzymes involved in the folic acid cycle, especially human dihydrofolate reductase (hDHFR). However, most of them have a classical structure that has proven ineffective against melanoma, and, therefore, inhibitors with a non-classical lipophilic structure are increasingly becoming an attractive alternative to circumvent this clinical resistance. In this study, we conducted a protocol combining virtual screening (VS) and cell-based assays to identify new potential non-classical hDHFR inhibitors. Among 173 hit compounds identified (average logP = 3.68; average MW = 378.34 Da), two—herein, called C1 and C2—exhibited activity against melanoma cell lines B16 and A375 by MTT and Trypan-Blue assays. C1 showed cell growth arrest (39% and 56%) and C2 showed potent cytotoxic activity (77% and 51%) in a dose-dependent manner. The effects of C2 on A375 cell viability were greater than MTX (98% vs 60%) at equivalent concentrations and times. Our results indicate that the integrated in silico/in vitro approach provided a benchmark to identify novel promising non-classical DHFR inhibitors showing activity against melanoma cells.

Published

2022

11. Innovative C2-symmetric testosterone and androstenedione dimers: Design, synthesis, biological evaluation on prostate cancer cell lines and binding study to recombinant CYP3A4

Author

Paquin, Alexis, Oufqir, Yassine, Sevrioukova, Irina F, Reyes-Moreno, Carlos, and Bérubé, Gervais

Subjects

Male, Urologic Diseases, Aging, CYP3A4, Cell Survival, Medicinal & Biomolecular Chemistry, Antineoplastic Agents, Drug Screening Assays, Dose-Response Relationship, Structure-Activity Relationship, Medicinal and Biomolecular Chemistry, Humans, Cytochrome P-450 CYP3A, Testosterone, Dimers, Cell Proliferation, Cancer, Cultured, Molecular Structure, Prostate Cancer, Organic Chemistry, Androstenedione, Prostatic Neoplasms, Dihydrotestosterone, Antitumor, Pharmacology and Pharmaceutical Sciences, Recombinant Proteins, Tumor Cells, Drug Design, Drug, Dimerization

Abstract

The synthesis of two isomeric testosterone dimers and an androstenedione dimer is reported. The design takes advantage of an efficient transformation of testosterone leading to the synthesis of the key diene, 7α-(buta-1,3-dienyl)-4-androsten-17β-ol-3-one, through an elimination reaction. It was found that in some instances the same reaction led to partial epimerization of the 17β-hydroxyl group into the 17α-hydroxyl group. The specific orientation of the hydroxyl function was confirmed by NMR spectroscopy. Capitalizing on this unforeseen side reaction, several dimers were assembled using an olefin metathesis reaction with Hoveyda-Grubbs catalyst. This led to the formation of two isomeric testosterone dimers with 17α-OH or 17β-OH (14α and 14β) as well as an androstenedione dimer (14). The new dimers and their respective precursors were tested on androgen-dependent (LNCaP) and androgen independent (PC3 and DU145) prostate cancer cells. It was discovered that the most active dimer was made of the natural hormone testosterone (14β) with an average IC50 of 13.3μM. In LNCaP cells, 14β was ∼5 times more active than the antiandrogen drug cyproterone acetate (IC50 of 12.0μM vs. 59.6μM, respectively). At low concentrations (0.25-0.5μM), 14α and 14β were able to completely inhibit LNCaP cell growth induced by testosterone or dihydrotestosterone. Furthermore, cross-reactivity of androgen-based dimers with sterol-metabolizing cytochrome P450 3A4 was explored and the results are disclosed herein.

Published

2021

12. Hetero-Bis-Conjugation of Bioactive Molecules to Half-Sandwich Ruthenium(II) and Iridium(III) Complexes Provides Synergic Effects in Cancer Cell Cytotoxicity

Author

Stefano Zacchini, Guido Pampaloni, Viktor Brabec, Hana Kostrhunova, Lorenzo Biancalana, Mouna Hadiji, Paul J. Dyson, Fabio Marchetti, Ilaria Degano, Lucinda K. Batchelor, Biancalana L., Kostrhunova H., Batchelor L.K., Hadiji M., Degano I., Pampaloni G., Zacchini S., Dyson P.J., Brabec V., and Marchetti F.

Subjects

Pyridines, Pyridine, cisplatin, platinum(iv) prodrug, scaffold, Drug Screening Assays, Iridium, Ligands, 01 natural sciences, Antineoplastic Agent, chemistry.chemical_compound, Biotin, Coordination Complexes, Tumor Cells, Cultured, Cytotoxicity, chemistry.chemical_classification, Cultured, Aqueous solution, Coordination Complexe, Molecular Structure, Tumor Cells, Ruthenium, inhibitor, Dicarboxylic acid, acid, Drug, strategy, Human, Metalation, Cell Survival, rational design, chemistry.chemical_element, Ligand, Antineoplastic Agents, 010402 general chemistry, Dose-Response Relationship, Inorganic Chemistry, anticancer agents, Humans, Physical and Theoretical Chemistry, Cell Proliferation, Dose-Response Relationship, Drug, 010405 organic chemistry, crystal-structure, Antitumor, Combinatorial chemistry, 0104 chemical sciences, chemistry, DNA Damage, Drug Screening Assays, Antitumor, derivatives

Abstract

Four bipyridine-Type ligands variably derivatized with two bioactive groups (taken from ethacrynic acid, flurbiprofen, biotin, and benzylpenicillin) were prepared via sequential esterification steps from commercial 2,2′-bipyridine-4,4′-dicarboxylic acid and subsequently coordinated to ruthenium(II) p-cymene and iridium(III) pentamethylcyclopentadienyl scaffolds. The resulting complexes were isolated as nitrate salts in high yields and fully characterized by analytical and spectroscopic methods. NMR and MS studies in aqueous solution and in cell culture medium highlighted a substantial stability of ligand coordination and a slow release of the bioactive fragments in the latter case. The complexes were assessed for their antiproliferative activity on four cancer cell lines, showing cytotoxicity to the low micromolar level (equipotent with cisplatin). Additional biological experiments revealed a multimodal mechanism of action of the investigated compounds, involving DNA metalation and enzyme inhibition. Synergic effects provided by specific combinations of metal and bioactive fragments were identified, pointing toward an optimal ethacrynic acid/flurbiprofen combination for both Ru(II) and Ir(III) complexes.

Published

2021

13. DNA methyltransferase inhibitors upregulate CD38 protein expression and enhance daratumumab efficacy in multiple myeloma

Author

Jeffrey L. Wolf, Huimin Geng, Arun P. Wiita, Thomas G. Martin, Sandy W. Wong, Margarette C. Mariano, Nina Shah, and Priya Choudhry

Subjects

DNA (Cytosine-5-)-Methyltransferase 1, 0301 basic medicine, Cancer Research, Letter, Plasma Cells, Clinical Sciences, Oncology and Carcinogenesis, Immunology, DNA Methyltransferase Inhibitor, Myeloma, Cancer immunotherapy, Biology, CD38, Drug Screening Assays, Antibodies, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Monoclonal, medicine, Humans, Multiple myeloma, Regulation of gene expression, Neoplastic, Tumor, Antibodies, Monoclonal, Daratumumab, Drug Synergism, Antitumor, Hematology, medicine.disease, ADP-ribosyl Cyclase 1, Gene Expression Regulation, Neoplastic, Cancer therapeutic resistance, 030104 developmental biology, Gene Expression Regulation, Oncology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Immunotherapy, Drug Screening Assays, Antitumor, Antibody, Multiple Myeloma

Abstract

Author(s): Choudhry, Priya; Mariano, Margarette C; Geng, Huimin; Martin, Thomas G; Wolf, Jeffrey L; Wong, Sandy W; Shah, Nina; Wiita, Arun P

Published

2019

14. Distinct biological responses of metastatic castration resistant prostate cancer cells upon exposure to G-quadruplex interacting naphthalenediimide derivatives

Author

Marta Recagni, Maria Laura Greco, Andrea Milelli, Marco Folini, Anna Minarini, Claudia Sissi, Nadia Zaffaroni, Recagni M., Greco M.L., Milelli A., Minarini A., Zaffaroni N., Folini M., and Sissi C.

Subjects

Male, MAPK/ERK pathway, Cell, Drug Screening Assays, Ligands, Castration-Resistant, 01 natural sciences, C-circle DNA, Prostate cancer, Drug Discovery, Epidermal growth factor receptor, Receptor, 0303 health sciences, Tumor, G-quadruplex, biology, Chemistry, General Medicine, Gene promoter, Naphthalenediimide, Cell Line, Tumor, DNA, Drug Screening Assays, Antitumor, ErbB Receptors, G-Quadruplexes, Gene Expression Regulation, Neoplastic, Humans, MAP Kinase Signaling System, Naphthalimides, Prostatic Neoplasms, Castration-Resistant, medicine.anatomical_structure, Cell Line, 03 medical and health sciences, DU145, medicine, Protein kinase B, PI3K/AKT/mTOR pathway, 030304 developmental biology, Pharmacology, Neoplastic, 010405 organic chemistry, Organic Chemistry, Prostatic Neoplasms, Antitumor, medicine.disease, 0104 chemical sciences, Gene Expression Regulation, Cancer research, biology.protein

Abstract

Small molecules able to bind non-canonical G-quadruplex DNA structures (G4) have been recently tested as novel potential agents for the treatment of prostate cancer thanks to their repression of aberrant androgen receptor gene. However, metastatic castration-resistant prostate cancer (mCRPC), a letal form of prostate cancer, is still incurable. Here we tested two naphthalenediimide derivatives, previously reported as multitarget agents, on a couple of relevant mCRPC cell models (DU145 and PC-3). We showed that these compounds interfere with the RAS/MEK/ERK and PI3K/AKT pathways. Interestingly, both these two biological processes depend upon Epidermal Growth Factor Receptor (EGFR) activation. By means of biological and analytical tools we showed that our compounds are efficient inducers of the structural transition of the EGFR promoter towards a G-quadruplex conformation, ultimately leading to a reduction of the receptor production. The overall result is an interesting cytotoxic profile for these two derivatives. Thanks to their activity at different steps, these compounds can open the way to novel therapeutic approaches for mCRPC that could contribute to escape resistance to selective treatments.

Published

2019

15. Exploiting the 1-(4-fluorobenzyl)piperazine fragment for the development of novel tyrosinase inhibitors as anti-melanogenic agents: Design, synthesis, structural insights and biological profile

Author

Antonio Rapisarda, Laura De Luca, Sonia Floris, Yael Pazy, Antonella Fais, Maria Paola Germanò, Batel Deri, Ayelet Fishman, Serena Vittorio, Rosaria Gitto, Salvatore Mirabile, Laura Ielo, and Simone Ronsisvalle

Subjects

Models, Molecular, Agaricus, Tyrosinase, Crystallography, X-Ray, Drug Screening Assays, 01 natural sciences, Piperazines, B16F10 melanoma cells, Melanin, chemistry.chemical_compound, Models, Drug Discovery, Docking studies, Enzyme Inhibitors, Cytotoxicity, chemistry.chemical_classification, 0303 health sciences, anti-melanogenic effects, Tyrosinase inhibitors, X-ray crystallography, Antineoplastic Agents, Cell Line, Tumor, Cell Proliferation, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Molecular Structure, Monophenol Monooxygenase, Structure-Activity Relationship, Drug Design, Tumor, Crystallography, General Medicine, Biochemistry, Drug, In silico, Cell Line, Dose-Response Relationship, 03 medical and health sciences, Oxidoreductase, 030304 developmental biology, Pharmacology, 010405 organic chemistry, Organic Chemistry, Molecular, Antitumor, 0104 chemical sciences, Piperazine, chemistry, Design synthesis, X-Ray, Kojic acid, anti-melanogenic effects, B16F10 melanoma cells, Docking studies, Tyrosinase inhibitors, X-ray crystallography

Abstract

The development of Tyrosinase inhibitors (TYRIs) could represent an efficacious strategy for pharmacological intervention on skin pathologies related to aberrant production of melanin. Based on in silico studies we designed and tested a library of twenty-four compounds bearing the 4-(4-fluorobenzyl)piperazin-1-yl]-fragment. As result, we identified several compounds with excellent inhibit effects at low micromolar concentration against TYR from Agaricus bisporus (TyM). Among them, compound 25 (IC50 = 0.96 μM) proved to be ∼20-fold more potent than the reference compound kojic acid (IC50 = 17.76 μM) having wide applications in the cosmetics and pharmaceutical industries. The mode of interaction of active inhibitor 25 was deciphered by means of crystallography as well as molecular docking and these results were consistent with kinetic experiments. Moreover, the identified compound 25 exhibited no considerable cytotoxicity and showed anti-melanogenic effects on B16F10 melanoma cells. Therefore, a combination of computational and biochemical approaches could represent a rational guidelines for further structural modification of this class of compounds as future anti-melanogenic agents.

Published

2019

16. A Syngeneic ErbB2 Mammary Cancer Model for Preclinical Immunotherapy Trials

Author

Matthew T. Silvestrini, Clifford G. Tepper, Alexander D. Borowsky, Zsófia Pénzváltó, Jane Qian Chen, Ryan R. Davis, Maxine Umeh-Garcia, and Colleen A Sweeney

Subjects

0301 basic medicine, Cancer Research, Receptor, ErbB-2, animal diseases, medicine.medical_treatment, Drug Screening Assays, Transgenic, B7-H1 Antigen, Mice, Breast cancer, ErbB-2, Antineoplastic Agents, Immunological, 0302 clinical medicine, Immunophenotyping, Antineoplastic Combined Chemotherapy Protocols, Cancer, Tumor, Syngeneic, Immunological, Oncology, 030220 oncology & carcinogenesis, Female, Immunotherapy, Receptor, Biotechnology, PD-L1, Clinical Sciences, Primary Cell Culture, Antineoplastic Agents, Breast Neoplasms, Mice, Transgenic, Biology, Article, Cell Line, Mouse model, Vaccine Related, Experimental, 03 medical and health sciences, Immune system, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Oncology & Carcinogenesis, Transplantation, Mammary Neoplasms, Carcinoma, Mammary Neoplasms, Experimental, Reproducibility of Results, Antitumor, In vitro, 030104 developmental biology, Erbb2, Cell culture, biology.protein, Cancer research, Feasibility Studies, Immunization, Drug Screening Assays, Antitumor

Abstract

In order to develop a practical model of breast cancer, with in vitro and syngeneic,immune-intact, in vivo growth capacity, we established a primary cell line derived from a mammary carcinoma in the transgenic FVB/N-Tg(MMTV-ErbB2*)NDL2-5Mul mouse, referred to as "NDLUCD". The cellline is adapted to standard cell culture and can be transplanted into syngeneic FVB/N mice. The line maintains a stable phenotype over multiple in vitro passages and rounds of in vivo transplantation. NDLUCD tumors in FVB/N mice exhibit high expression of ErbB2 and ErbB3 and signaling molecules downstream of ErbB2. The syngeneic transplant tumors elicit an immune reaction in the adjacent stroma, detected and characterized using histology, immunophenotyping, and gene expression. NDLUCD cells also express PD-L1 in vivo and in vitro, and in vivo transplants are reactive to anti-immune checkpoint therapy with responses conducive to immunotherapy studies. This new NDLUCD cell line model is a practical alternative to the more commonly used 4T1 cells, and our previously described FVB/N-Tg(MMTV-PyVT)634Mul derived Met-1fvb2 and FVB/NTg(MMTV-PyVTY315F/Y322F) derived DB-7fvb2 cell lines. The NDLUCD cells have, so far, remained genetically and phenotypically stable over many generations, with consistent and reproducible results in immune intact preclinical cohorts.

Published

2019

17. Exploration of the carmaphycins as payloads in antibody drug conjugate anticancer agents

Author

Bailey W. Miller, C. Benjamin Naman, Jeffrey A. Hanson, Toni Kline, Frederick A. Valeriote, Halina Pietraszkiewicz, Jehad Almaliti, William H. Gerwick, Evgenia Glukhov, Xiaofan Li, and Sihong Zhou

Subjects

Carmaphycins, Drug Screening Assays, 01 natural sciences, Monoclonal, Drug Discovery, Amines, Cytotoxicity, Cancer, 0303 health sciences, Oligopeptide, Tumor, Aniline Compounds, Molecular Structure, Chemistry, Antibodies, Monoclonal, Pharmacology and Pharmaceutical Sciences, General Medicine, 5.1 Pharmaceuticals, Amine gas treating, Drug, Development of treatments and therapeutic interventions, Proteasome Inhibitors, Oligopeptides, 4-Sulfonylaniline, Biotechnology, Proteasome Endopeptidase Complex, Antibody-drug conjugate, Cell Survival, Medicinal & Biomolecular Chemistry, Antineoplastic Agents, Proteasome inhibitors, Anticancer drugs, Article, Antibodies, Cell Line, Dose-Response Relationship, Structure-Activity Relationship, Medicinal and Biomolecular Chemistry, 03 medical and health sciences, Rare Diseases, Cell Line, Tumor, Humans, Structure–activity relationship, Cell Proliferation, 030304 developmental biology, Pharmacology, Dose-Response Relationship, Drug, 010405 organic chemistry, Organic Chemistry, Antitumor, Combinatorial chemistry, 0104 chemical sciences, Orphan Drug, Proteasome, Amine basicity optimization, Drug Screening Assays, Antitumor, Linker, Conjugate

Abstract

Antibody-drug conjugates (ADCs) represent a new dimension of anticancer chemotherapeutics, with warheads to date generally involving either antitubulin or DNA-directed agents to achieve low-to sub-nanomolar potency. However, other potent cytotoxins working by different pharmacological mechanisms are under investigation, such as α,β-epoxyketone based proteasome inhibitors. These proteasome active agents are an emerging class of anticancer drug that possesses ultra-potent cytotoxicity to some cancer cell lines. The carmaphycins are representatives of this latter class that we isolated and characterized from a marine cyanobacterium, and these as well as several synthetic analogues exhibit this level of potency. In the current work, we investigated the use of these highly potent cytotoxic compounds as warheads in the design of novel ADCs. We designed and synthesized a library of carmaphycin B analogues that contain amine handles, enabling their attachment to an antibody linker. The basicity of these incorporated amine handles was shown to strongly affect their cytotoxic properties. Linear amines resulted in the greatest reduction in cytotoxicity whereas less basic aromatic amines retained potent activity as demonstrated by a 4-sulfonylaniline derivative. These investigations resulted in identifying the P2 residue in the carmaphycins as the most suitable site for linker attachment point, and hence, we synthesized a highly potent analogue of carmaphycin B that contained a 4-sulfonylaniline handle as an attachment point for the linker antibody.

Published

2019

18. A Circulating Tumor Cell-RNA Assay for Assessment of Androgen Receptor Signaling Inhibitor Sensitivity in Metastatic Castration-Resistant Prostate Cancer

Author

Pin Jung Chen, Sungyong You, Nu Yao, Jasmine J. Wang, Beatrice S. Knudsen, Hsian-Rong Tseng, Gina C.Y. Chu, Shirley Cheng, Michael R. Freeman, Minhyung Kim, Howard Chung, Yu Jen Jan, Edwin M. Posadas, Felix Y. Feng, Yi-Tsung Lu, Jie Fu Chen, Pai Chi Teng, Yi Te Lee, Yazhen Zhu, Isla P. Garraway, Allen C. Gao, Amber Lozano, Leland W.K. Chung, and Junhee Yoon

Subjects

Male, 0301 basic medicine, Aging, Medicine (miscellaneous), Cancer RNA Profiling, Drug resistance, Drug Screening Assays, Neoplastic Cells, Castration-Resistant, Androgen Receptor Signaling Inhibitors, Prostate cancer, 0302 clinical medicine, Circulating tumor cell, Metastatic Castration-Resistant Prostate Cancer, Circulating, Circulating Tumor Cell, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Cancer, Prostate Cancer, Neoplastic Cells, Circulating, 3. Good health, Prostatic Neoplasms, Castration-Resistant, 030220 oncology & carcinogenesis, Research Paper, Signal Transduction, Urologic Diseases, Oncology and Carcinogenesis, Antineoplastic Agents, Castration resistant, 03 medical and health sciences, Clinical Research, Androgen Receptor Antagonists, Genetics, medicine, Humans, Gene, business.industry, Computational Biology, Prostatic Neoplasms, RNA, Antitumor, medicine.disease, Androgen receptor, 030104 developmental biology, Cell culture, Cancer research, Drug Screening Assays, Antitumor, Transcriptome, business

Abstract

Rationale: Our objective was to develop a circulating tumor cell (CTC)-RNA assay for characterizing clinically relevant RNA signatures for the assessment of androgen receptor signaling inhibitor (ARSI) sensitivity in metastatic castration-resistant prostate cancer (mCRPC) patients. Methods: We developed the NanoVelcro CTC-RNA assay by combining the Thermoresponsive (TR)-NanoVelcro CTC purification system with the NanoString nCounter platform for cellular purification and RNA analysis. Based on the well-validated, tissue-based Prostate Cancer Classification System (PCS), we focus on the most aggressive and ARSI-resistant PCS subtype, i.e., PCS1, for CTC analysis. We applied a rigorous bioinformatic process to develop the CTC-PCS1 panel that consists of prostate cancer (PCa) CTC-specific RNA signature with minimal expression in background white blood cells (WBCs). We validated the NanoVelcro CTC-RNA assay and the CTC-PCS1 panel with well-characterized PCa cell lines to demonstrate the sensitivity and dynamic range of the assay, as well as the specificity of the PCS1 Z score (the likelihood estimate of the PCS1 subtype) for identifying PCS1 subtype and ARSI resistance. We then selected 31 blood samples from 23 PCa patients receiving ARSIs to test in our assay. The PCS1 Z scores of each sample were computed and compared with ARSI treatment sensitivity. Results: The validation studies using PCa cell line samples showed that the NanoVelcro CTC-RNA assay can detect the RNA transcripts in the CTC-PCS1 panel with high sensitivity and linearity in the dynamic range of 5-100 cells. We also showed that the genes in CTC-PCS1 panel are highly expressed in PCa cell lines and lowly expressed in background WBCs. Using the artificial CTC samples simulating the blood sample conditions, we further demonstrated that the CTC-PCS1 panel is highly specific in identifying PCS1-like samples, and the high PCS1 Z score is associated with ARSI resistance samples. In patient bloods, ARSI-resistant samples (ARSI-R, n=14) had significantly higher PCS1 Z scores as compared with ARSI-sensitive samples (ARSI-S, n=17) (Rank-sum test, P=0.003). In the analysis of 8 patients who were initially sensitive to ARSI (ARSI-S) and later developed resistance (ARSI-R), we found that the PCS1 Z score increased from the time of ARSI-S to the time of ARSI-R (Pairwise T-test, P=0.016). Conclusions: Using our new methodology, we developed a first-in-class CTC-RNA assay and demonstrated the feasibility of transforming clinically-relevant tissue-based RNA profiling such as PCS into CTC tests. This approach allows for detecting RNA expression relevant to clinical drug resistance in a non-invasive fashion, which can facilitate patient-specific treatment selection and early detection of drug resistance, a goal in precision oncology.

Published

2019

19. Acceptability and feasibility study of patient-specific ‘tumouroids’ as personalised treatment screening tools: Protocol for prospective tissue and data collection of participants with confirmed or suspected renal cell carcinoma

Author

Jack Grierson, Joana B. Neves, Katerina Stamati, Umber Cheema, Norman R. Williams, Mark Emberton, Maxine G. B. Tran, Patricia de Albuquerque Garcia Redondo, Alethea Cope, Marilena Loizidou, and Chris Brew-Graves

Subjects

medicine.medical_specialty, 3D in vitro cancer models, Psychological intervention, 030230 surgery, In vitro techniques, 03 medical and health sciences, 0302 clinical medicine, Renal cell carcinoma, medicine, Screening tool, 030212 general & internal medicine, Personalised cancer treatment, Intensive care medicine, Protocol (science), Data collection, business.industry, Precision medicine, Cancer, Patient specific, medicine.disease, Drug screening assays, Surgery, business, Research Paper

Abstract

Highlights • First study on patient acceptability of patient derived cell culture models. • First study to assess the feasibility of using patient derived kidney cancer 3D tumour models. • Study will inform the design of a clinical trial in personalised tumouroid response to therapy., Introduction ‘Personalised medicine’ aims to tailor interventions to the individual, and has become one of the fastest growing areas of cancer research. One of these approaches is to harvest cancer cells from patients and grow them in the laboratory, which can then be subjected to treatments and the response assessed. We have developed a 3D tumour model with a complex protein matrix that mimics the tumour stroma, cell to cell and cell-matrix interactions seen in vivo, called a tumouroid. In this study, we test the acceptability and feasibility of using this model to establish patient-derived tumouroids. Methods and analysis This is a first in-human study using prospective tissue and data collection of adult participants with confirmed or suspected renal cell carcinoma. The goals of the study are to assess patient acceptability to the use of patient-derived tumour models for future treatment decisions, and to assess the feasibility of generating patient-specific renal cancer tumouroids that can be challenged with drugs. These goals will be realised through the collection of tumour samples (expected n = 10), participant-completed questionnaires (expected n = 10), and in-depth semi-structured interviews with patients (expected n = 5). Collected multiregional tumour samples will be dissociated to isolate primary cells which are then expanded in vitro and incorporated into tumouroids. Drug challenge will ensue and the response will be categorised into “responder”, “weak responder”, and “non-responder”. Statistical analysis will be descriptive. Ethics and dissemination The study has ethical approval (REC reference 17/LO/1744). Findings will be made available to patients, clinicians, funders, and the National Health Service (NHS) through presentations at national and international meetings, peer-reviewed publications, social media and patient support groups. Trial registration Registered on ClinicalTrials.gov (NCT03300102).

Published

2019

20. Exploring the Biological Activity of a Library of 1,2,5-Oxadiazole Derivatives Endowed With Antiproliferative Activity

Author

Arianna Gelain, Fiorella Meneghetti, Aída Nelly García-Argáez, M. Mori, F. Porta, Lisa Dalla Via, Akira Asai, Salvatore Guccione, Stefania Villa, Livia Basile, Gaetano Marverti, and Mariafrancesca Hyeraci

Subjects

Cancer Research, Cytotoxicity, HCT-116, Type I, Oxadiazole, Drug Screening Assays, HeLa, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, Humans, Structure–activity relationship, MTT assay, Docking studies, Cell Proliferation, Oxadiazoles, biology, Topoisomerase, Biological activity, Antitumor, General Medicine, HCT116 Cells, biology.organism_classification, Topoisomerase I, Molecular Docking Simulation, DNA Topoisomerases, Type I, Oncology, chemistry, Biochemistry, Docking (molecular), 030220 oncology & carcinogenesis, biology.protein, Drug Screening Assays, Antitumor, HeLa Cells, DNA Topoisomerases

Abstract

BACKGROUND/AIM The identification of a series of oxadiazole-based compounds, as promising antiproliferative agents, has been previously reported. The aim of this study was to explore the SAR of newly-synthesized oxadiazole derivatives and identify their molecular targets. MATERIALS AND METHODS A small library of 1,2,5-oxadiazole derivatives was synthetized and their antiproliferative activity was tested by the MTT assay. Their interaction with topoisomerase I was evaluated and a molecular docking study was performed. RESULTS Several candidates showed cytotoxicity towards two human tumor cell lines, HCT-116 (colorectal carcinoma) and HeLa (cervix adenocarcinoma). Some derivatives exhibited inhibitory effects on the catalytic activity of topoisomerase I and this effect was supported by docking studies. CONCLUSION The enzyme inhibition results, although not directly related to cytotoxicity, suggest that a properly modified 1,2,5 oxadiazole scaffold could be considered for the development of new anti-topoisomerase agents.

Published

2018

21. Human estrogen receptor α antagonists, part 2: Synthesis driven by rational design, in vitro antiproliferative, and in vivo anticancer evaluation of innovative coumarin-related antiestrogens as breast cancer suppressants

Author

Nezrina Kurtanović, Nevena Tomašević, Lorenzo Antonini, Milan Mladenović, Manuela Sabatino, Danijela A. Kostić, Marina Mitrovic, Sanja Matić, and Rino Ragno

Subjects

MAPK/ERK pathway, In silico, In vitro antiproliferative evaluation, Wistar, Estrogen receptor, Antineoplastic Agents, Breast Neoplasms, Drug Screening Assays, Dose-Response Relationship, Synthesis, Experimental, Structure-Activity Relationship, Breast cancer, In vivo, Coumarins, Drug Discovery, medicine, Animals, Humans, Rats, Wistar, Cell Proliferation, Pharmacology, Dose-Response Relationship, Drug, Molecular Structure, Coumarin-based ERα antagonists, Chemistry, Mammary Neoplasms, Organic Chemistry, Estrogen Receptor alpha, In vivo anticancer evaluation, Drug Screening Assays, Antitumor, Estrogen Receptor Antagonists, Female, MCF-7 Cells, Mammary Neoplasms, Experimental, Rats, Drug Design, Antitumor, General Medicine, medicine.disease, Mechanism of action, Selective estrogen receptor modulator, Cancer research, Drug, medicine.symptom, Signal transduction

Abstract

New twelve in silico designed coumarin-based ERα antagonists, namely 3DQ-1a to 3DQ-1е, were synthesized and confirmed as selective ERα antagonists, showing potencies ranging from single-digit nanomolar to picomolar. The hits were confirmed as selective estrogen receptor modulators and validated as antiproliferative agents using MCF-7 breast cancer cell lines exerting from picomolar to low nanomolar potency, at the same time showing no agonistic activity within endometrial cell lines. Their mechanism of action was inspected and revealed to be through the inhibition of the Raf-1/MAPK/ERK signal transduction pathway, preventing hormone-mediated gene expression on either genomic direct or genomic indirect level, and stopping the MCF-7 cells proliferation at G0/G1 phase. In vivo experiments, by means of the per os administration to female Wistar rats with pre-induced breast cancer, distinguished six derivatives, 3DQ-4a, 3DQ-2a, 3DQ-1a, 3DQ-1b, 3DQ-2b, and 3DQ-3b, showing remarkable potency as tumor suppressors endowed with optimal pharmacokinetic profiles and no significant histopathological profiles. The presented data indicate the new compounds as potential candidates to be submitted in clinical trials for breast cancer therapy.

Published

2021

22. Discovery of antiproliferative and anti-FAK inhibitory activity of 1,2,4-triazole derivatives containing acetamido carboxylic acid skeleton

Author

Pradipta Ghosh, Alaa M. Hayallah, Esam R. Ahmed, Muhamad Mustafa, Gamal El-Din A. Abuo-Rahma, Amer Ali Abd El-Hafeez, and Dalia Abdelhamid

Subjects

Cell cycle checkpoint, Clinical Biochemistry, Pharmaceutical Science, Apoptosis, Drug Screening Assays, 01 natural sciences, Biochemistry, Anticancer activity, Synthesis, Drug Discovery, Aminobenzoates, Phosphorylation, Cancer, Tumor, medicine.diagnostic_test, Kinase, Chemistry, FAK inhibitors, Pharmacology and Pharmaceutical Sciences, Molecular Docking Simulation, 5.1 Pharmaceuticals, S Phase Cell Cycle Checkpoints, Molecular Medicine, Development of treatments and therapeutic interventions, Docking study, Protein Binding, Medicinal & Biomolecular Chemistry, Antineoplastic Agents, Article, Cell Line, Focal adhesion, Medicinal and Biomolecular Chemistry, Rare Diseases, Western blot, Cell Line, Tumor, 4-triazoles, medicine, Humans, Molecular Biology, Protein kinase B, IC50, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Cell Proliferation, 5-Pyridinyl-1, Binding Sites, 010405 organic chemistry, Organic Chemistry, Antitumor, Triazoles, G1 Phase Cell Cycle Checkpoints, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Focal Adhesion Kinase 1, Cancer research, Acetanilides, Drug Screening Assays, Antitumor

Abstract

Small molecule inhibitors of the focal adhesion kinase are regarded as promising tools in our armamentarium for treating cancer. Here, we identified four 1,2,4-triazole derivatives that inhibit FAK kinase significantly and evaluated their therapeutic potential. Most tested compounds revealed potent antiproliferative activity in HepG2 and Hep3B liver cancer cells, in which 3c and 3d were the most potent (IC50 range; 2.88~4.83µM). Compound 3d possessed significant FAK inhibitory activity with IC50 value of 18.10nM better than the reference GSK-2256098 (IC50=22.14nM). The preliminary mechanism investigation by Western blot analysis showed that both 3c and 3d repressed FAK phosphorylation comparable to GSK-2256098 in HepG2 cells. As a result of FAK inhibition, 3c and 3d inhibited the pro-survival pathways by decreasing the phosphorylation levels of PI3K, Akt, JNK, and STAT3 proteins. This effect led to apoptosis induction and cell cycle arrest. Taken together, these results indicate that 3d could serve as a potent preclinical candidate for the treatment of cancers.

Published

2021

23. Phytochemical Investigations and In Vitro Bioactivity Screening on Melia azedarach L. Leaves Extract from Nepal

Author

Gokhan Zengin, Sangeeta Rajbhandary, Sara Grana, Irene Ferrarese, Gunes Ak, Stefania Sut, Shyam Sharan Shrestha, Deepak Raj Pant, and Stefano Dall'Acqua

Subjects

Melia azedarach, Phytochemicals, Drug Screening Assays, 01 natural sciences, Biochemistry, Antioxidants, Rutin, chemistry.chemical_compound, enzyme inhibitory assays, Phytogenic, Tumor, Traditional medicine, biology, Phytosterol, General Medicine, Phytochemical, Skin hyperpigmentation, Acetylcholinesterase, Molecular Medicine, medicine.drug, Cell Survival, phytosterols, Antineoplastic Agents, Bioengineering, Limonoid, Cell Line, Picrates, traditional Nepalese medicine, Cell Line, Tumor, medicine, Humans, Benzothiazoles, Molecular Biology, polyphenols, Cell Proliferation, Antineoplastic Agents, Phytogenic, Biphenyl Compounds, Butyrylcholinesterase, Cholinesterase Inhibitors, Drug Screening Assays, Antitumor, Plant Extracts, Plant Leaves, Sulfonic Acids, 010405 organic chemistry, Antitumor, General Chemistry, biology.organism_classification, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, chemistry, Polyphenol, Kojic acid

Abstract

Melia azedarach is a common tree used in the traditional medicine of Nepal. In this work, leaves were considered as source of bioactive constituents and composition of methanol extract was evaluated and compared with starting plant material. Flavonoid glycosides and limonoids were identified and quantified by HPLC-DAD-MSn approaches in dried leaves and methanolic extract, while HPLC-APCI-MSn and GC/MS analysis were used to study phytosterol and lipid compositions. β-Sitosterol and rutin were the most abundant constituents. HPLC-APCI-MSn and HPLC-DAD-MSn analysis revealed high levels of phytosterols and flavonoids in methanolic extract accounting 9.6 and 7.5 % on the dried weight, respectively. On the other hand, HPLC/MSn data revealed that limonoid constituents were in minor amount in the extract

Published

2021

24. A facile synthesis of diaryl pyrroles led to the discovery of potent colchicine site antimitotic agents

Author

Giampietro Viola, Paola Oliva, Stefano Manfredini, Elena Mariotto, Ernest Hamel, Roberta Bortolozzi, Maria Kimatrai Salvador, Federica Maccarinelli, Salvatore Ferla, Chiara Padroni, Fatlum Rruga, Andrea Brancale, Roberto Ronca, and Romeo Romagnoli

Subjects

Antimitotic agents, Antiproliferative activity, Drug Screening Assays, 01 natural sciences, Polymerization, chemistry.chemical_compound, Tubulin, Drug Discovery, Colchicine, Pyrrole, 0303 health sciences, Tumor, Molecular Structure, biology, 1H-pyrrole, Structure-activity relationship, Tubulin polymerization, General Medicine, Cell cycle, Tubulin Modulators, Drug, Stereochemistry, Antineoplastic Agents, Antimitotic Agents, Cell Line, Tumor, Cell Proliferation, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Pyrroles, Structure-Activity Relationship, NO, Cell Line, Dose-Response Relationship, 03 medical and health sciences, In vivo, Structure–activity relationship, 030304 developmental biology, Pharmacology, Combretastatin, 010405 organic chemistry, Organic Chemistry, Antitumor, 0104 chemical sciences, chemistry, Cell culture, biology.protein

Abstract

Three different series of cis-restricted analogues of combretastatin A-4 (CA-4), corresponding to thirty-nine molecules that contained a pyrrole nucleus interposed between the two aryl rings, were prepared by a palladium-mediated coupling approach and evaluated for their antiproliferative activity against six human cancer cell lines. In the two series of 1,2-diaryl pyrrole derivatives, results suggested that the presence of the 3′,4′,5′-trimethoxyphenyl moiety at the N-1 position of the pyrrole ring was more favorable for antiproliferative activity. In the series of 3,4-diarylpyrrole analogues, three compounds (11i-k) exhibited maximal antiproliferative activity, showing excellent antiproliferative activity against the CA-4 resistant HT-29 cells. Inhibition of tubulin polymerization of selected 1,2 pyrrole derivatives (9a, 9c, 9o and 10a) was similar to that observed with CA-4, while the isomeric 3,4-pyrrole analogues 11i-k were generally from 1.5- to 2-fold more active than CA-4. Compounds 11j and 11k were the only compounds that showed activity as inhibitors of colchicine binding comparable to that CA-4. Compound 11j had biological properties consistent with its intracellular target being tubulin. This compound was able to block the cell cycle in metaphase and to induce significant apoptosis at a concentration of 25 nM, following the mitochondrial pathway, with low toxicity for normal cells. More importantly, compound 11j exerted activity in vivo superior to that of CA-4P, being able to significantly reduce tumor growth in a syngeneic murine tumor model even at the lower dose tested (5.0 mg/kg).

Published

2021

25. A high-content screen identifies drugs that restrict tumor cell extravasation across the Endothelial Barrier

Author

Adam D. Langenbacher, Matteo Pellegrini, M. Luisa Iruela-Arispe, Jonathan Freshman, Georg Hilfenhaus, Vanessa Morais Freitas, Feiyang Ma, Divya P. Prajapati, Byoung Kyu Cho, Ana Mompeon, Robert Damoiseaux, Young Ah Goo, Dana Song, Jau-Nian Chen, Snezana Mirkov, and Gloria Hernandez

Subjects

0301 basic medicine, Proteomics, Male, Cancer Research, Lung Neoplasms, Cell, Cell Communication, Inbred C57BL, Drug Screening Assays, Neoplastic Cells, Cell junction, Metastasis, RATOS, Mice, 0302 clinical medicine, Circulating tumor cell, Circulating, 2.1 Biological and endogenous factors, Aetiology, Barrier function, Niclosamide, Inbred BALB C, Zebrafish, Cancer, Mice, Inbred BALB C, Tumor, Chemistry, Neoplastic Cells, Circulating, Extravasation, medicine.anatomical_structure, Oncology, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Female, Signal transduction, Development of treatments and therapeutic interventions, medicine.drug, Oncology and Carcinogenesis, Article, Cell Line, 03 medical and health sciences, Rare Diseases, Cell Line, Tumor, Vascular, medicine, Human Umbilical Vein Endothelial Cells, Animals, Humans, Metabolomics, Neoplasm Invasiveness, Endothelium, Oncology & Carcinogenesis, Cell Proliferation, Kininogens, Colforsin, Transendothelial and Transepithelial Migration, Endothelial Cells, Antitumor, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, Cancer research, Endothelium, Vascular, Drug Screening Assays, Antitumor

Abstract

Metastases largely rely on hematogenous dissemination of tumor cells via the vascular system and significantly limit prognosis of patients with solid tumors. To colonize distant sites, circulating tumor cells must destabilize the endothelial barrier and transmigrate across the vessel wall. Here we performed a high-content screen to identify drugs that block tumor cell extravasation by testing 3,520 compounds on a transendothelial invasion coculture assay. Hits were further characterized and validated using a series of in vitro assays, a zebrafish model enabling three-dimensional (3D) visualization of tumor cell extravasation, and mouse models of lung metastasis. The initial screen advanced 38 compounds as potential hits, of which, four compounds enhanced endothelial barrier stability while concurrently suppressing tumor cell motility. Two compounds niclosamide and forskolin significantly reduced tumor cell extravasation in zebrafish, and niclosamide drastically impaired metastasis in mice. Because niclosamide had not previously been linked with effects on barrier function, single-cell RNA sequencing uncovered mechanistic effects of the drug on both tumor and endothelial cells. Importantly, niclosamide affected homotypic and heterotypic signaling critical to intercellular junctions, cell–matrix interactions, and cytoskeletal regulation. Proteomic analysis indicated that niclosamide-treated mice also showed reduced levels of kininogen, the precursor to the permeability mediator bradykinin. Our findings designate niclosamide as an effective drug that restricts tumor cell extravasation through modulation of signaling pathways, chemokines, and tumor–endothelial cell interactions. Significance: A high-content screen identified niclosamide as an effective drug that restricts tumor cell extravasation by enhancing endothelial barrier stability through modulation of molecular signaling, chemokines, and tumor–endothelial cell interactions.

Published

2021

26. A comprehensive assessment of a new series of 5',6'-difluorobenzotriazole-acrylonitrile derivatives as microtubule targeting agents (MTAs)

Author

Roberta Ibba, Valentina Bordoni, Luigi Bagella, Simona Sestito, Michele Lai, Sanna L, M. Andrea Scorciapino, Federico Riu, Antonio Carta, and Sandra Piras

Subjects

Cell growth inhibition, Benzotriazoles, Extrusion pump inhibition, Microtubule targeting agents, Molecular docking, Tubulin, Acrylonitrile, Antineoplastic Agents, Cell Proliferation, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, HeLa Cells, Humans, Microtubules, Mitosis, Molecular Docking Simulation, Molecular Structure, Structure-Activity Relationship, Triazoles, Drug Screening Assays, 01 natural sciences, Dose-Response Relationship, HeLa, 03 medical and health sciences, chemistry.chemical_compound, Microtubule, Drug Discovery, Binding site, 030304 developmental biology, Pharmacology, 0303 health sciences, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Antitumor, General Medicine, biology.organism_classification, 0104 chemical sciences, Biochemistry, Docking (molecular), Cancer cell, biology.protein, Drug, Lead compound

Abstract

Microtubules (MTs) are the principal target for drugs acting against mitosis. These compounds, called microtubule targeting agents (MTAs), cause a mitotic arrest during G2/M phase, subsequently inducing cell apoptosis. MTAs could be classified in two groups: microtubule stabilising agents (MSAs) and microtubule destabilising agents (MDAs). In this paper we present a new series of (E) (Z)-2-(5,6-difluoro-(1H)2H-benzo[d] [1,2,3]triazol-1(2)-yl)-3-(R)acrylonitrile (9a-j, 10e, 11a,b) and (E)-2-(1H-benzo[d] [1,2,3]triazol-1-yl)-3-(R)acrylonitrile derivatives (13d,j), which were recognised to act as MTAs agents. They were rationally designed, synthesised, characterised and subjected to different biological assessments. Computational docking was carried out in order to investigate the potential binding to the colchicine-binding site on tubulin. From this first prediction, the di-fluoro substitution seemed to be beneficial for the binding affinity with tubulin. The new fluorine derivatives, here presented, showed an improved antiproliferative activity when compared to the previously reported compounds. The biological evaluation included a preliminary antiproliferative screening on NCI60 cancer cells panel (1–10 μM). Compound 9a was selected as lead compound of the new series of derivatives. The in vitro XTT assay, flow cytometry analysis and immunostaining performed on HeLa cells treated with 9a showed a considerable antiproliferative effect, (IC50 = 3.2 μM), an increased number of cells in G2/M-phase, followed by an enhancement in cell division defects. Moreover, β-tubulin staining confirmed 9a as a MDA triggering tubulin disassembly, whereas colchicine-9a competition assay suggested that compound 9a compete with colchicine for the binding site on tubulin. Then, the co-administration of compound 9a and an extrusion pump inhibitor (EPI) was investigated: the association resulted beneficial for the antiproliferative activity and compound 9a showed to be client of extrusion pumps. Finally, structural superimposition of different colchicine binding site inhibitors (CBIs) in clinical trial and our MDA, provided an additional confirmation of the targeting to the predicted binding site. Physicochemical, pharmacokinetic and druglikeness predictions were also conducted and all the newly synthesised derivatives showed to be drug-like molecules.

Published

2020

27. 1,2,4-Oxadiazole Topsentin Analogs with Antiproliferative Activity against Pancreatic Cancer Cells, Targeting GSK3β Kinase

Author

Elisa Giovannetti, Veronica Di Sarno, Daniela Carbone, Camilla Pecoraro, Patrizia Diana, Giulia Auriemma, Barbara Parrino, Girolamo Cirrincione, Stella Cascioferro, Simona Musella, Daniela Carbone, Barbara Parrino, Stella Cascioferro, Camilla Pecoraro, Elisa Giovannetti, Veronica Di Sarno, Simona Musella, Giulia Auriemma, Girolamo Cirrincione, Patrizia Diana, Medical oncology laboratory, CCA - Cancer biology and immunology, and Amsterdam Gastroenterology Endocrinology Metabolism

Subjects

Models, Molecular, Indoles, 1,2,4-oxadiazole topsentin analogs, GSK3β kinase, inhibition of migration, PDAC antiproliferative activity, proapoptotic activity, Apoptosis, Drug Screening Assays, 01 natural sciences, Biochemistry, chemistry.chemical_compound, Antineoplastic Agents, Cell Proliferation, Cell Survival, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Glycogen Synthase Kinase 3 beta, Humans, Imidazoles, Molecular Structure, Oxadiazoles, Pancreatic Neoplasms, Protein Kinase Inhibitors, Structure-Activity Relationship, Tumor Cells, Cultured, Models, Annexin, Drug Discovery, General Pharmacology, Toxicology and Pharmaceutics, 4-oxadiazole topsentin analogs, Cultured, Chemistry, Kinase, Cell migration, Tumor Cells, Molecular Medicine, Drug, Intracellular, Dose-Response Relationship, Pancreatic cancer, medicine, Propidium iodide, Pharmacology, 010405 organic chemistry, Organic Chemistry, Molecular, Antitumor, medicine.disease, Settore CHIM/08 - Chimica Farmaceutica, Molecular biology, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Cell culture, 1,2,4-oxadiazole topsentin analog

Abstract

A new series of topsentin analogs, in which the central imidazole ring of the natural lead was replaced by a 1,2,4- oxadiazole moiety, was efficiently synthesized. All derivatives were pre-screened for antiproliferative activity against the National Cancer Institute (NCI-60) cell lines panel. The five most potent compounds were further investigated in various pancreatic ductal adenocarcinoma (PDAC) cell lines, including SUIT-2, Capan-1, and Panc-1 cells, eliciting EC50 values in the micromolar and sub-micromolar range, associated with significant reduction of cell migration. These remarkable results might be explained by the effects of these new topsentin analogues on epithelial-to-mesenchymal transition markers, including SNAIL-1/2 and metalloproteinase-9. Moreover, flow cytometric analysis after Annexin V-FITC and propidium iodide staining demonstrated that these derivatives enhanced apoptosis of PDAC cells. Keeping with these data, the PathScan intracellular signaling and ELISA array revealed cleavage of caspase-3 and PARP and a significant inhibition of GSK3β phosphorylation, suggesting this kinase as a potential downstream target of our novel compounds. This was further supported by a specific assay for the evaluation of GSK3β activity, showing IC50 values for the most active compounds against this enzyme in the micromolar range.

Published

2020

28. In vivo modeling of metastatic human high-grade serous ovarian cancer in mice

Author

Kim, Olga, Park, Eun Young, Klinkebiel, David L, Pack, Svetlana D, Shin, Yong-Hyun, Abdullaev, Zied, Emerson, Robert E, Coffey, Donna M, Kwon, Sun Young, Creighton, Chad J, Kwon, Sanghoon, Chang, Edmund C, Chiang, Theodore, Yatsenko, Alexander N, Chien, Jeremy, Cheon, Dong-Joo, Yang-Hartwich, Yang, Nakshatri, Harikrishna, Nephew, Kenneth P, Behringer, Richard R, Fernández, Facundo M, Cho, Chi-Heum, Vanderhyden, Barbara, Drapkin, Ronny, Bast, Robert C, Miller, Kathy D, Karpf, Adam R, Kim, Jaeyeon, and Kwiatkowski, David J

Subjects

Ribonuclease III, DNA Repair, Knockout, Primary Cell Culture, Cystadenocarcinoma, Drug Resistance, Antineoplastic Agents, Drug Screening Assays, Cell Line, DEAD-box RNA Helicases, Mice, Rare Diseases, Chromosomal Instability, Genetics, Animals, Humans, 2.1 Biological and endogenous factors, Neoplasm Metastasis, Aetiology, Peritoneal Neoplasms, Cancer, Ovarian Neoplasms, Tumor, Animal, PTEN Phosphohydrolase, Serous, Antitumor, Ovarian Cancer, Disease Models, Mutation, Feasibility Studies, Neoplasm, Female, Tumor Suppressor Protein p53, Neoplasm Grading, Developmental Biology

Abstract

Metastasis is responsible for 90% of human cancer mortality, yet it remains a challenge to model human cancer metastasis in vivo. Here we describe mouse models of high-grade serous ovarian cancer, also known as high-grade serous carcinoma (HGSC), the most common and deadliest human ovarian cancer type. Mice genetically engineered to harbor Dicer1 and Pten inactivation and mutant p53 robustly replicate the peritoneal metastases of human HGSC with complete penetrance. Arising from the fallopian tube, tumors spread to the ovary and metastasize throughout the pelvic and peritoneal cavities, invariably inducing hemorrhagic ascites. Widespread and abundant peritoneal metastases ultimately cause mouse deaths (100%). Besides the phenotypic and histopathological similarities, mouse HGSCs also display marked chromosomal instability, impaired DNA repair, and chemosensitivity. Faithfully recapitulating the clinical metastases as well as molecular and genomic features of human HGSC, this murine model will be valuable for elucidating the mechanisms underlying the development and progression of metastatic ovarian cancer and also for evaluating potential therapies.

Published

2020

29. Neutral analogs of the heat shock protein 70 (Hsp70) inhibitor, JG-98

Author

Hao Shao and Jason E. Gestwicki

Subjects

Aging, Clinical Biochemistry, Pharmaceutical Science, Drug Screening Assays, medicine.disease_cause, 01 natural sciences, Biochemistry, chemistry.chemical_compound, Breast cancer, Drug Discovery, Moiety, Cancer, Tumor, Prostate cancer, Molecular Structure, Pharmacology and Pharmaceutical Sciences, Molecular Docking Simulation, Benzothiazole, Molecular chaperone, Molecular Medicine, Pyridinium, Protein Binding, Allosteric inhibitor, Medicinal & Biomolecular Chemistry, Allosteric regulation, Anti-cancer agents, Antineoplastic Agents, Fluorescence, Article, Cell Line, Medicinal and Biomolecular Chemistry, Structure-Activity Relationship, Cell Line, Tumor, medicine, Chemical probe, Humans, HSP70 Heat-Shock Proteins, Benzothiazoles, Molecular Biology, Cell Proliferation, Fluorescent Dyes, Binding Sites, 010405 organic chemistry, Organic Chemistry, Antitumor, 0104 chemical sciences, Hsp70, 010404 medicinal & biomolecular chemistry, Proteostasis, chemistry, Cancer cell, Drug Screening Assays, Antitumor, Carcinogenesis

Abstract

The heat shock protein 70 (Hsp70) family of molecular chaperones are highly expressed in tumors. Inhibitors containing a pyridinium-modified benzothiazole, such as JG-98, bind to a conserved, allosteric site in Hsp70, showing promising anti-proliferative activity in cancer cells. When bound to Hsp70, the charged pyridinium makes favorable contacts; however, this moiety also increases the inhibitor’s fluorescence, giving rise to undesirable interference in biochemical and cell-based assays. Here, we explore whether the pyridinium can be replaced with a neutral pyridine. We report that pyridine-modified benzothiazoles, such as compound 17h (JG2-38), have reduced fluorescence, yet retain promising anti-proliferative activity (EC50 values ~0.1 to 0.07 µM) in breast and prostate cancer cell lines. These chemical probes are expected to be useful in exploring the roles of Hsp70s in tumorigenesis and cell survival.

Published

2019

30. Kinome rewiring reveals AURKA limits PI3K-pathway inhibitor efficacy in breast cancer

Author

Andrei Goga, Rebecca S. Levin, Khyati N. Shah, Roman Camarda, Sourav Bandyopadhyay, Nora Bayani, Kevan M. Shokat, James T. Webber, Olga Momcilovic, John D. Gordan, James E. Korkola, and Hayley J. Donnella

Subjects

0301 basic medicine, Pediatric Research Initiative, Biochemistry & Molecular Biology, Cell signaling, Breast Neoplasms, Antineoplastic Agents, Apoptosis, Drug Screening Assays, Article, Phosphatidylinositol 3-Kinases, Medicinal and Biomolecular Chemistry, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, In vivo, Breast Cancer, Humans, Medicine, Chemoproteomics, Kinome, Molecular Biology, Protein kinase B, PI3K/AKT/mTOR pathway, Cancer, Plant Proteins, Cell Proliferation, Aurora Kinase A, Phosphoinositide-3 Kinase Inhibitors, business.industry, Azepines, Antitumor, Cell Biology, medicine.disease, 3. Good health, Pyrimidines, 030104 developmental biology, 5.1 Pharmaceuticals, 6.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Cancer research, Female, Biochemistry and Cell Biology, Drug Screening Assays, Antitumor, business

Abstract

Dysregulation of the PI3K-AKT-mTOR signaling network is a prominent feature of breast cancers. However, clinical responses to drugs targeting this pathway have been modest, possibly because of dynamic changes in cellular signaling that drive resistance and limit drug efficacy. Using a quantitative chemoproteomics approach, we mapped kinome dynamics in response to inhibitors of this pathway and identified signaling changes that correlate with drug sensitivity. Maintenance of AURKA after drug treatment was associated with resistance in breast cancer models. Incomplete inhibition of AURKA was a common source of therapy failure, and combinations of PI3K, AKT or mTOR inhibitors with the AURKA inhibitor MLN8237 were highly synergistic and durably suppressed mTOR signaling, resulting in apoptosis and tumor regression in vivo. This signaling map identifies survival factors whose presence limits the efficacy of targeted therapies and reveals new drug combinations that may unlock the full potential of PI3K-AKT-mTOR pathway inhibitors in breast cancer.

Published

2018

31. New 6- and 7-heterocyclyl-1H-indole derivatives as potent tubulin assembly and cancer cell growth inhibitors

Author

Giuseppe La Regina, Antonio Coluccia, Ruoli Bai, Carmela Mazzoccoli, Giulio Dondio, Ernest Hamel, Chiara Cavallini, Stefania Vultaggio, Romano Silvestri, Annalisa Verrico, Valentina Naccarato, Paola Rovella, Marianna Nalli, Eleonora Da Pozzo, Claudia Martini, Domiziana Masci, Valeria Famiglini, Ciro Mercurio, Mario Varasi, and Patrizia Lavia

Subjects

0301 basic medicine, Indoles, Microtubule Tubulin Cancer cell Inhibitor Indole, Cancer cell, Drug Screening Assays, Polymerization, HeLa, 0302 clinical medicine, Tubulin, Drug Discovery, Tumor Cells, Cultured, Mic, Cultured, Molecular Structure, biology, Chemistry, General Medicine, Tubulin Modulators, Tumor Cells, inhibitor, Biochemistry, 030220 oncology & carcinogenesis, Indole, Microtubule, Cell Proliferation, Cell Survival, Dose-Response Relationship, Structure-Activity Relationship, Drug, microtubule, tubulin, cancer cell, inhibitor, indole, Antineoplastic Agents, [object Object], 03 medical and health sciences, Humans, Settore CHIM/08 - CHIMICA FARMACEUTICA, Pharmacology, Indole test, Dose-Response Relationship, Drug, Cell growth, Organic Chemistry, Antitumor, biology.organism_classification, 030104 developmental biology, Cell culture, biology.protein, Drug Screening Assays, Antitumor

Abstract

We designed new 3-arylthio- and 3-aroyl-1H-indole derivatives 3–22 bearing a heterocyclic ring at position 5, 6 or 7 of the indole nucleus. The 6- and 7-heterocyclyl-1H-indoles showed potent inhibition of tubulin polymerization, binding of colchicine to tubulin and growth of MCF-7 cancer cells. Compounds 13 and 19 inhibited a panel of cancer cells and the NCI/ADR-RES multidrug resistant cell line at low nanomolar concentrations. Compound 13 at 50 nM induced 77% G2/M in HeLa cells, and at 20 nM caused 50% stable arrest of mitosis. As an inhibitor of HepG2 cells (IC50 = 20 nM), 13 was 4-fold superior to 19. Compound 13 was a potent inhibitor of the human U87MG glioblastoma cells at nanomolar concentrations, being nearly one order of magnitude superior to previously reported arylthioindoles. The present results highlight 13 as a robust scaffold for the design of new anticancer agents.

Published

2018

32. Samholides, Swinholide-Related Metabolites from a Marine Cyanobacterium cf. Phormidium sp

Author

Daojing Zhang, Lena Gerwick, Yiwen Tao, Pinglin Li, William H. Gerwick, Thomas F. Murray, Chen Zhang, and Evgenia Glukhov

Subjects

Cyanobacteria, Double bond, Stereochemistry, Antineoplastic Agents, Drug Screening Assays, 010402 general chemistry, 01 natural sciences, Cell Line, Medicinal and Biomolecular Chemistry, Cell Line, Tumor, Humans, Cytotoxicity, Lung, Cancer, chemistry.chemical_classification, Tumor, biology, 010405 organic chemistry, Organic Chemistry, Antitumor, Methylation, Featured Article, biology.organism_classification, 0104 chemical sciences, chemistry, Marine Toxins, Drug Screening Assays, Antitumor, Isomerization, Two-dimensional nuclear magnetic resonance spectroscopy, Marine toxin, Lactone

Abstract

Cancer cell cytotoxicity was used to guide the isolation of nine new swinholide-related compounds, named samholides A–I (1–9), from an American Samoan marine cyanobacterium cf. Phormidium sp. Their structures were determined by extensive analysis of 1D and 2D NMR spectroscopic data. The new compounds share an unusual 20-demethyl 44-membered lactone ring composed of two monomers, and they demonstrate structural diversity arising from geometric isomerization of double bonds, sugar units with unique glyceryl moieties and varied methylation patterns. All of the new samholides were potently active against the H-460 human lung cancer cell line with IC50 values ranging from 170 to 910 nM. The isolation of these new swinholide-related compounds from a marine cyanobacterium reinvigorates questions concerning the evolution and biosynthetic origin of these natural products.

Published

2018

33. Towards an Improvement of Anticancer Activity of Benzyl Adenosine Analogs

Author

Manuela Grimaldi, Maurizio Bifulco, Maria Proto, Verdiana Covelli, Mohammad Firoznezhad, Rosario Randino, Anna Maria D'Ursi, Patrizia Gazzerro, Manuela Rodriquez, Veronica De Simone, Gianluca Matteoli, Covelli, V., Grimaldi, M., Randino, R., Firoznezhad, M., Proto, M. C., De Simone, V., Matteoli, G., Gazzerro, P., Bifulco, M., D'Ursi, A. M., and Rodriquez, M.

Subjects

Colorectal cancer, FPPS, N6-benzyladenosine derivatives, Adenosine, Animals, Antineoplastic Agents, Apoptosis, Cell Proliferation, Cell Survival, Colorectal Neoplasms, Computer Simulation, Drug Screening Assays, Antitumor, Geranyltranstransferase, HCT116 Cells, Humans, Mevalonic Acid, Mice, Structure-Activity Relationship, User-Computer Interface, Chemistry, Multidisciplinary, FARNESYL DIPHOSPHATE SYNTHASE, Farnesyl pyrophosphate, Pharmaceutical Science, Drug Screening Assays, Analytical Chemistry, chemistry.chemical_compound, QD241-441, colorectal cancer, Drug Discovery, CYTOKININ, chemistry.chemical_classification, ATP synthase, biology, TRANSFER DIFFERENCE NMR, APOPTOSIS, Chemistry, N6-ISOPENTENYLADENOSINE, Biochemistry, Chemistry (miscellaneous), Physical Sciences, Molecular Medicine, Life Sciences & Biomedicine, medicine.drug, Biochemistry & Molecular Biology, NUCLEOSIDES, ISOPRENOID END-PRODUCT, Article, CELL-PROLIFERATION, Prenylation, In vivo, medicine, Viability assay, BIOLOGICAL EVALUATION, Physical and Theoretical Chemistry, Science & Technology, Organic Chemistry, Antitumor, In vitro, Enzyme, chemistry, biology.protein, LIGAND

Abstract

N6-Isopentenyladenosine (i6A) is a naturally occurring modified nucleoside displaying in vitro and in vivo antiproliferative and pro-apoptotic properties. In our previous studies, including an in silico inverse virtual screening, NMR experiments and in vitro enzymatic assays, we demonstrated that i6A targeted farnesyl pyrophosphate synthase (FPPS), a key enzyme involved in the mevalonate (MVA) pathway and prenylation of downstream proteins, which are aberrant in several cancers. Following our interest in the anticancer effects of FPPS inhibition, we developed a panel of i6A derivatives bearing bulky aromatic moieties in the N6 position of adenosine. With the aim of clarifying molecular action of N6-benzyladenosine analogs on the FPPS enzyme inhibition and cellular toxicity and proliferation, herein we report the evaluation of the N6-benzyladenosine derivatives' (compounds 2a-m) effects on cell viability and proliferation on HCT116, DLD-1 (human) and MC38 (murine) colorectal cancer cells (CRC). We found that compounds 2, 2a and 2c showed a persistent antiproliferative effect on human CRC lines and compound 2f exerted a significant effect in impairing the prenylation of RAS and Rap-1A proteins, confirming that the antitumor activity of 2f was related to the ability to inhibit FPPS activity. ispartof: MOLECULES vol:26 issue:23 ispartof: location:Switzerland status: published

Published

2021

34. Structure-Activity Relationships within a Series of σ1 and σ2 Receptor Ligands: Identification of a σ2 Receptor Agonist (BS148) with Selective Toxicity against Metastatic Melanoma

Author

Paola Azzoni, Antonio Cilia, Umberto Maria Battisti, Claudia Sorbi, Cristina Magnoni, Luisa Benassi, Elena Cichero, Livio Brasili, Orazio Prezzavento, Cristina Vaschieri, Silvia Franchini, Leda Ivanova Bencheva, Simone Ronsisvalle, Annalisa Tait, Giuseppina Aricò, and Paola Fossa

Subjects

Male, 0301 basic medicine, sigma, Pharmacology, Drug Screening Assays, Ligands, Biochemistry, Mice, Piperidines, Models, Receptors, Drug Discovery, analgesia, antiproliferative activity, melanoma, sigma receptors, SK-MEL-2 cells, Analgesics, Opioid, Animals, Antineoplastic Agents, Cell Death, Cell Proliferation, Cell Survival, Cells, Cultured, Crystallography, X-Ray, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Melanoma, Models, Molecular, Molecular Structure, Receptors, sigma, Spiro Compounds, Structure-Activity Relationship, Molecular Medicine, Pharmacology, Toxicology and Pharmaceutics (all), Organic Chemistry, General Pharmacology, Toxicology and Pharmaceutics, Receptor, Analgesics, Cultured, Crystallography, Drug, Agonist, Programmed cell death, medicine.drug_class, Cells, Toxicology and Pharmaceutics (all), Opioid, Biology, Dose-Response Relationship, 03 medical and health sciences, medicine, Structure–activity relationship, Cell growth, Antagonist, Molecular, Antitumor, medicine.disease, 030104 developmental biology, Apoptosis, X-Ray

Abstract

A new series of spirocyclic σ receptor (σR) ligands were prepared and studied. Most were found to have a high affinity and selectivity for σ1 R; three compounds were shown to be σ1 R agonists, while another proved to be the only σ1 R antagonist. Only one of the σ1 R agonists (BS148) also exhibited σ2 R selectivity and was able to inhibit the growth of metastatic malignant melanoma cell lines without affecting normal human melanocytes. The antiproliferative activity of this compound suggested an σ2 R agonist profile. Further, preliminary investigations indicated that the mechanism of metastatic malignant melanoma cell death induced by BS148 is due, at least in part, to apoptosis.

Published

2017

35. Molecular diversity of phenothiazines: design and synthesis of phenothiazine–dithiocarbamate hybrids as potential cell cycle blockers

Author

Sai-Yang Zhang, Jia-Huan Li, Li Ping, Xiaolin Zi, Qing-Qing Zhang, Bo-Wen Wu, Yan-Bing Zhang, Jia-Jia Yang, Ruo-Wang Mao, Fu Dongjun, Zhao Ruohan, Hui-Jie Cai, and Liu Hongmin

Subjects

Cell cycle checkpoint, Phenothiazine, Apoptosis, Antiproliferative activity, Chemistry Techniques, Synthetic, Drug Screening Assays, 01 natural sciences, Macromolecular and Materials Chemistry, chemistry.chemical_compound, Phenothiazines, Drug Discovery, G1 checkpoint-related protein, Cancer, chemistry.chemical_classification, Tumor, Chemistry, General Medicine, Cell cycle, Information Systems, G1 phase, Stereochemistry, Antineoplastic Agents, Article, Catalysis, Cell Line, Inorganic Chemistry, Structure-Activity Relationship, Cell Line, Tumor, Humans, Structure–activity relationship, Physical and Theoretical Chemistry, Dithiocarbamate, Molecular Biology, Cell Proliferation, 010405 organic chemistry, Cell growth, Synthetic, Organic Chemistry, Antitumor, Chemistry Techniques, Cell Cycle Checkpoints, In vitro, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Drug Design, Drug Screening Assays, Antitumor, Other Chemical Sciences

Abstract

Novel phenothiazine–dithiocarbamate analogues were designed by molecular hybridization strategy and synthesized and evaluated for their anticancer activity in vitro against three selected cancer cell lines (EC-109, MGC-803, and PC-3). The preliminary structure–activity relationship (SAR) for this phenothiazine–dithiocarbamate hybrids is explored. Among all analogues, 2-oxo-2-(10H-phenothiazin-10-yl)ethyl 4-ethylpiperazine-1-carbodithioate (8a) showed the most potent inhibitory activity with an $$\hbox {IC}_{50}$$ value of $$11.59\,\upmu \hbox {M}$$ against PC-3 cells. In addition, compound 8a could arrest the cell cycle at the G1 phase and regulate the expression of G1 checkpoint-related proteins, suggesting that phenothiazine–dithiocarbamate hybrids might be useful as cell cycle blockers.

Published

2017

36. A versatile nanoplatform for synergistic combination therapy to treat human esophageal cancer

Author

She Gan Gao, Xue zhen Ding, Yoshihiro Izumiya, Xiao Chen Hu, De Jiu Kong, Jun Qiang Yang, Li Zhang, Xiaocen Li, Xin Shuai Wang, Yuanpei Li, Tzu-yin Lin, and Kit S. Lam

Subjects

0301 basic medicine, Esophageal Neoplasms, Apoptosis, Docetaxel, Pharmacology, Drug Screening Assays, Bortezomib, 0302 clinical medicine, synergistic effect, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, Nanotechnology, Pharmacology (medical), Pharmacology & Pharmacy, Cancer, media_common, Cultured, Cell Cycle, Pharmacology and Pharmaceutical Sciences, General Medicine, Cell cycle, Esophageal cancer, Tumor Cells, 5.1 Pharmaceuticals, 6.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Taxoids, Original Article, Drug, Development of treatments and therapeutic interventions, medicine.drug, Combination therapy, Cell Survival, Drug Compounding, media_common.quotation_subject, nanoformulations, Bioengineering, Dose-Response Relationship, Structure-Activity Relationship, 03 medical and health sciences, Rare Diseases, medicine, disulfide cross-linked micelles, Humans, targeted combination therapy, Dose-Response Relationship, Drug, business.industry, Evaluation of treatments and therapeutic interventions, human esophageal cancer, Antitumor, medicine.disease, In vitro, Nanostructures, Good Health and Well Being, 030104 developmental biology, Drug Screening Assays, Antitumor, Digestive Diseases, business

Abstract

One of the major goals of precision oncology is to promote combination therapy to improve efficacy and reduce side effects of anti-cancer drugs based on their molecular mechanisms. In this study, we aimed to develop and validate new nanoformulations of docetaxel (DTX) and bortezomib (BTZ) for targeted combination therapy to treat human esophageal cancer. By leveraging our versatile disulfide cross-linked micelles (DCMs) platform, we developed nanoformulations of DTX and BTZ (named DTX-DCMs and BTZ-DCMs). Their physical properties were characterized; their anti-cancer efficacies and mechanisms of action were investigated in a human esophageal cancer cell line in vitro. Furthermore, the in vitro anti-tumor activities of combination therapies (concurrent drug treatment, sequential drug treatment, and treatment using different ratios of the drugs) were examined in comparison with the single drug treatment and free drug strategies. These drug-loaded nanoparticles were spherical in shape and relatively small in size of approximately 20-22 nm. The entrapment efficiencies of DTX and BTZ into nanoparticles were 82.4% and 84.1%, respectively. The drug release rates of DTX-DCMs and BTZ-DCMs were sustained, and greatly increased in the presence of GSH. These nanodrugs were effectively internalized by KYSE30 esophageal cancer cells, and dose-dependently induced cell apoptosis. We further revealed a strong synergistic effect between DTX-DCMs and BTZ-DCMs against KYSE30 esophageal cancer cells. Sequential combination therapy with DTX-DCMs followed by BTZ-DCMs exhibited the best anti-tumor efficacy in vitro. This study demonstrates that DTX and BTZ could be successfully nanoformulated into disulfide cross-linked micelles. The nanoformulations of DTX and BTZ demonstrate an immense potential for synergistic combination therapy to treat human esophageal cancer.

Published

2017

37. Mathematical modeling of mutant transferrin-CRM107 molecular conjugates for cancer therapy

Author

Dennis J. Yoon, April A. Pan, Daniel T. Kamei, Anne B. Mason, Joseph Shiloach, André Moreni Lopes, and Kevin Y. Chen

Subjects

0301 basic medicine, Mutant, Transferrin-CRM107, Drug Screening Assays, Mathematical Sciences, 0302 clinical medicine, Theoretical, Models, Neoplasms, Site-Directed, Diphtheria Toxin, Cytotoxicity, Cancer, chemistry.chemical_classification, Applied Mathematics, Transferrin, Targeted toxin, General Medicine, Biological Sciences, Cell biology, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Modeling and Simulation, Development of treatments and therapeutic interventions, General Agricultural and Biological Sciences, Biotechnology, Statistics and Probability, Bacterial Toxins, Antineoplastic Agents, Transferrin receptor, Biology, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Information and Computing Sciences, Humans, Diphtheria toxin, Evolutionary Biology, General Immunology and Microbiology, Antitumor, Models, Theoretical, Molecular biology, In vitro, 030104 developmental biology, chemistry, Mutagenesis, Drug delivery, Mutation, Cancer cell, Mutagenesis, Site-Directed, Drug Screening Assays, Antitumor

Abstract

The transferrin (Tf) trafficking pathway is a promising mechanism for use in targeted cancer therapy due to the overexpression of transferrin receptors (TfRs) on cancerous cells. We have previously developed a mathematical model of the Tf/TfR trafficking pathway to improve the efficiency of Tf as a drug carrier. By using diphtheria toxin (DT) as a model toxin, we found that mutating the Tf protein to change its iron release rate improves cellular association and efficacy of the drug. Though this is an improvement upon using wild-type Tf as the targeting ligand, conjugated toxins like DT are unfortunately still highly cytotoxic at off-target sites. In this work, we address this hurdle in cancer research by developing a mathematical model to predict the efficacy and selectivity of Tf conjugates that use an alternative toxin. For this purpose, we have chosen to study a mutant of DT, cross-reacting material 107 (CRM107). First, we developed a mathematical model of the Tf-DT trafficking pathway by extending our Tf/TfR model to include intracellular trafficking via DT and DT receptors. Using this mathematical model, we subsequently investigated the efficacy of several conjugates in cancer cells: DT and CRM107 conjugated to wild-type Tf, as well as to our engineered mutant Tf proteins (K206E/R632A Tf and K206E/R534A Tf). We also investigated the selectivity of mutant Tf-CRM107 against non-neoplastic cells. Through the use of our mathematical model, we predicted that (i) mutant Tf-CRM107 exhibits a greater cytotoxicity than wild-type Tf-CRM107 against cancerous cells, (ii) this improvement was more drastic with CRM107 conjugates than with DT conjugates, and (iii) mutant Tf-CRM107 conjugates were selective against non-neoplastic cells. These predictions were validated with in vitro cytotoxicity experiments, demonstrating that mutant Tf-CRM107 conjugates is indeed a more suitable therapeutic agent. Validation from in vitro experiments also confirmed that such whole-cell kinetic models can be useful in cancer therapeutic design.

Published

2017

38. Metabolite profiling of ascidianStyela plicatausing LC–MS with multivariate statistical analysis and their antitumor activity

Author

Antonello Mai, Donatella Del Bufalo, Satheesh Kumar Palanisamy, Daniela Trisciuoglio, and Clemens Zwergel

Subjects

0301 basic medicine, tumor, Ascidian, Metabolite, Antineoplastic Agents, Tandem mass spectrometry, biomolecules, Mass Spectrometry, HeLa, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Metabolomics, Liquid chromatography–mass spectrometry, Cell Line, Tumor, Drug Discovery, Botany, high pressure liquid, cancer, Animals, Humans, Ascidia mentula, Urochordata, Chromatography, High Pressure Liquid, antitumor, Pharmacology, biology, Cell growth, lcsh:RM1-950, apoptosis, ascidian, metabolomics, animals, antineoplastic agents, cell line, tumor, chromatography, high pressure liquid, drug screening assays, antitumor, humans, mass spectrometry, multivariate analysis, urochordata, cell line, General Medicine, biology.organism_classification, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, Styela plicata, chemistry, Biochemistry, 030220 oncology & carcinogenesis, Multivariate Analysis, drug screening assays, chromatography, Drug Screening Assays, Antitumor, Research Article

Abstract

To identify the metabolite distribution in ascidian, we have applied an integrated liquid chromatography– tandem mass spectrometry (LC–MS) metabolomics approach to explore and identify patterns in chemical diversity of invasive ascidian Styela plicata. A total of 71 metabolites were reported among these alkaloids, fatty acids and lipids are the most dominant chemical group. Multivariate statistical analysis, principal component analysis (PCA) showed a clear separation according to chemical diversity and taxonomic groups. PCA and partial least square discriminant analysis were applied to discriminate the chemical group of S. plicata crude compounds and classify the compounds with unknown biological activities. In this study, we reported for the first time that a partially purified methanol extract prepared from the ascidian S. plicata and Ascidia mentula possess antitumor activity against four tumor cell lines with different tumor histotype, such as HeLa (cervical carcinoma), HT29 (colon carcinoma), MCF-7 (breast carcinoma) and M14 (melanoma). S. plicata fraction SP-50 showed strong inhibition of cell proliferation and induced apoptosis in HeLa and HT29 cells, thus indicating S. plicata fraction SP-50 a potential lead compound for anticancer therapy. The molecular mechanism of action and chemotherapeutic potential of these ascidian unknown biomolecules need further research.

Published

2017

39. Deep Tumor Penetration of Drug-Loaded Nanoparticles by Click Reaction-Assisted Immune Cell Targeting Strategy

Author

Kwangsoo Shin, Seung-Hae Kwon, Jonghoon Kim, Chan-Gi Pack, Giho Ko, Kang Kim, Soo Hong Lee, Nohyun Lee, Taeghwan Hyeon, and Ok Kyu Park

Subjects

Surface Properties, 010402 general chemistry, Drug Screening Assays, 01 natural sciences, Biochemistry, Catalysis, Cell Line, Mice, Cyclooctanes, Colloid and Surface Chemistry, Immune system, Antibiotics, Cell Line, Tumor, Animals, Particle Size, Cell Proliferation, Drug Carriers, Antibiotics, Antineoplastic, Tumor, CD11b Antigen, biology, Chemistry, Animal, Optical Imaging, Antitumor, General Chemistry, Silicon Dioxide, Antineoplastic, Extravasation, 0104 chemical sciences, Disease Models, Animal, Cell culture, Doxorubicin, Cancer cell, Disease Models, Chemical Sciences, Click chemistry, Cancer research, biology.protein, Nanoparticles, Click Chemistry, Drug Screening Assays, Antitumor, Bioorthogonal chemistry, Antibody, Porosity, Ex vivo

Abstract

Nanoparticles have been extensively used to deliver therapeutic drugs to tumor tissues through the extravasation of a leaky vessel via enhanced permeation and retention effect (EPR, passive targeting) or targeted interaction of tumor-specific ligands (active targeting). However, the therapeutic efficacy of drug-loaded nanoparticles is hampered by its heterogeneous distribution owing to limited penetration in tumor tissue. Inspired by the fact that cancer cells can recruit inflammatory immune cells to support their survival, we developed a click reaction-assisted immune cell targeting (CRAIT) strategy to deliver drug-loaded nanoparticles deep into the avascular regions of the tumor. Immune cell-targeting CD11b antibodies are modified with trans-cyclooctene to enable bioorthogonal click chemistry with mesoporous silica nanoparticles functionalized with tetrazines (MSNs-Tz). Sequential injection of modified antibodies and MSNs-Tz at intervals of 24 h results in targeted conjugation of the nanoparticles onto CD11b+ myeloid cells, which serve as active vectors into tumor interiors. We show that the CRAIT strategy allows the deep tumor penetration of drug-loaded nanoparticles, resulting in enhanced therapeutic efficacy in an orthotopic 4T1 breast tumor model. The CRAIT strategy does not require ex vivo manipulation of cells and can be applied to various types of cells and nanovehicles.

Published

2019

40. Identification of a new family of pyrazolo[3,4-d]pyrimidine derivatives as multitarget Fyn-Blk-Lyn inhibitors active on B- and T-lymphoma cell lines

Author

Maurizio Botta, Francesca Musumeci, Miroslava Kissova, Chiara Tarantelli, Giovanni Maga, Eugenio Gaudio, Silvia Schenone, Anna Lucia Fallacara, Filippo Spriano, Emmanuele Crespan, Francesco Bertoni, Raffaele Passannanti, Giulia Iovenitti, Chiara Greco, and Mattia Mori

Subjects

Lymphoma, Druggability, Drug Screening Assays, Proto-Oncogene Proteins c-fyn, environment and public health, 01 natural sciences, hemic and lymphatic diseases, Drug Discovery, Tumor Cells, Cultured, Src family kinase, Receptor, 0303 health sciences, Cultured, Molecular Structure, Chemistry, Cell Cycle, breakpoint cluster region, hemic and immune systems, General Medicine, Protein-Tyrosine Kinases, Tumor Cells, src-Family Kinases, Blk, Fyn, Kinase inhibitor, Lyn, pyrazolo[3,4-d]pyrimidine, Antineoplastic Agents, Cell Proliferation, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Lymphoma, T-Cell, Protein Kinase Inhibitors, Pyrazoles, Pyrimidines, Structure-Activity Relationship, Drug, biological phenomena, cell phenomena, and immunity, pyrazolo[3, Dose-Response Relationship, 03 medical and health sciences, FYN, LYN, 4-d]pyrimidine, medicine, 030304 developmental biology, Pharmacology, 010405 organic chemistry, Organic Chemistry, Antitumor, T-Cell, medicine.disease, 0104 chemical sciences, enzymes and coenzymes (carbohydrates), Cell culture, Cancer research

Abstract

Abnormal activation of B-cell receptor (BCR) signaling plays a key role in the development of lymphoid malignancies, and could be reverted by the simultaneous inhibition of Lyn, Fyn and Blk, three members of the Src family kinase (SFK). Fyn and Blk are also promising targets for the treatment of some forms of T-cell non-Hodgkin lymphoma which point to the druggability of SFKs for the treatment of these cancers. We recently identified Si308 as a potent Fyn inhibitor, while preliminary data showed that it might also inhibit Lyn and Blk. Here, molecular modelling studies were coupled with enzymatic assays to further investigate the effect of Si308 on Lyn and Blk. A small library of pyrazolo[3,4-d]pyrimidines structurally related to Si308 was synthesized and tested on human lymphoma cell lines. Compound 2h emerged as a new multitarget inhibitor of Lyn, Fyn and Blk endowed with remarkable antiproliferative effects on human B and T lymphoma cell lines. Its favorable ADME properties make the compound suitable for further developments.

Published

2019

41. Synthesis, structure-activity relationship and in vitro pharmacodynamics of A-ring modified caged xanthones in a preclinical model of inflammatory breast cancer

Author

Chantarasriwong, Oraphin, Milcarek, Andrew T, Morales, Theodore Habarth, Settle, Aspen L, Rezende, Celso O, Althufairi, Bashayer D, Theodoraki, Maria A, Alpaugh, Mary L, and Theodorakis, Emmanuel A

Subjects

Molecular Structure, Xanthones, Medicinal & Biomolecular Chemistry, Organic Chemistry, Breast Neoplasms, Antineoplastic Agents, Apoptosis, Antitumor, Pharmacology and Pharmaceutical Sciences, Drug Screening Assays, Natural product, Dose-Response Relationship, Structure-Activity Relationship, Medicinal and Biomolecular Chemistry, Rare Diseases, Breast cancer, Synthetic methods, Humans, Female, Inflammatory Breast Neoplasms, Drug, Spheroids, skin and connective tissue diseases, Cancer, Cell Proliferation

Abstract

Inflammatory breast cancer (IBC) is a highly metastatic, lethal form of breast cancer that lacks targeted therapeutic strategies. Inspired by the promising cytotoxicity of gambogic acid and related caged xanthones in spheroidsMARY-X, an invitro preclinical IBC model, we constructed a library of synthetic analogs and performed structure-activity relationship studies. The studies revealed that functionalizing the A-ring of the caged xanthone framework can significantly affect potency. Specifically, introduction of hydroxyl or fluorine groups at discrete positions of the A-ring leads to enhanced cytotoxicity at submicromolar concentrations. These compounds induce complete dissolution of spheroidsMARY-X with subsequent apoptosis of both the peripherally- and centrally-located cells, proliferative and quiescent-prone (e.g. hypoxic), respectively. These results highlight the structural flexibility and pharmacological potential of the caged xanthone motif for the design of IBC-targeting therapeutics.

Published

2019

42. Chemically stable inhibitors of 14-3-3 protein-protein interactions derived from BV02

Author

Mattia Mori, Lorenzo Franci, Daniela Valensin, Letizia Clementi, Leire Iralde-Lorente, Adriano Angelucci, Maurizio Botta, Mario Chiariello, Ylenia Cau, and G. Tassone

Subjects

14-3-3, 4-aminoantipyrine, c-Abl, leukaemia, protein–protein interaction, 14-3-3 Proteins, Antineoplastic Agents, Benzamides, Cell Proliferation, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, HeLa Cells, Humans, K562 Cells, Molecular Structure, Protein Binding, Pyrazoles, Structure-Activity Relationship, Pharmacology, Drug Discovery3003 Pharmaceutical Science, Plasma protein binding, Drug Screening Assays, 01 natural sciences, law.invention, Protein–protein interaction, Dose-Response Relationship, law, Drug Discovery, Structure–activity relationship, 14-3-3 protein, 010405 organic chemistry, Chemistry, Cell growth, lcsh:RM1-950, Antitumor, General Medicine, Nuclear magnetic resonance spectroscopy, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, lcsh:Therapeutics. Pharmacology, Biochemistry, Recombinant DNA, Drug, K562 cells

Abstract

14-3-3 are regulatory proteins that through protein–protein interactions (PPI) with numerous binding partners could be involved in several human diseases, including cancer, neurodegenerative disorders, and pathogens infections. Following our research interest in the development of 14-3-3 PPI inhibitors, here we exploited the privileged 4-aminoantipyrine scaffold in the design and synthesis of some derivatives endowed with antiproliferative activity against K-562 cells, and capable of binding to recombinant 14-3-3σ as evidenced by NMR spectroscopy. The binding mode was further explored by molecular modelling, while coupling confocal microscopy with intensitometric analysis showed that compound 1 was able to promote the nuclear translocation of c-Abl at low micromolar concentrations. Overall, 1 is chemically stable compared to parent 14-3-3 PPI inhibitors, and thus emerged as a confirmed hit for further development.

Published

2019

43. Epigenetic drug screen identifies the histone deacetylase inhibitor NSC3852 as a potential novel drug for the treatment of pediatric acute myeloid leukemia

Author

Marije Bartels, Edwin Sonneveld, Paul J. Coffer, Daphne Lelieveld, David A. Egan, Anita M.A.P. Govers, C. Michel Zwaan, Caroline R.M. Wiggers, Pediatrics, and Ophthalmology

Subjects

Myeloid, Apoptosis, epigenetic treatment, Drug Screening Assays, Leukemia, Megakaryoblastic, Acute/drug therapy, Pediatrics, Epigenesis, Genetic, Acute megakaryoblastic leukemia, 0302 clinical medicine, Immunophenotyping, Neutrophil differentiation, Leukemia, Megakaryoblastic, Acute, hemic and lymphatic diseases, Tumor Cells, Cultured, Non-U.S. Gov't, Leukemoid Reaction/drug therapy, Child, Leukemia, Cultured, Hematology, Research Support, Non-U.S. Gov't, HDACi, Histone deacetylase inhibitor, Myeloid leukemia, Prognosis, Perinatology, Tumor Cells, and Child Health, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Down Syndrome/drug therapy, Oncology, 030220 oncology & carcinogenesis, Hydroxyquinolines, Nitroso Compounds, Megakaryoblastic, medicine.medical_specialty, Down syndrome, Histone Deacetylases/chemistry, medicine.drug_class, Leukemia, Myeloid, Acute/drug therapy, Antitumor/methods, Drug Screening Assays, Antitumor/methods, Research Support, Histone Deacetylases, Leukemoid Reaction, 03 medical and health sciences, Genetic, NSC3852, Internal medicine, DS-AMKL, Journal Article, medicine, Acute/drug therapy, Humans, Pediatrics, Perinatology, and Child Health, pediatric AML, Cell Proliferation, business.industry, Hydroxyquinolines/pharmacology, medicine.disease, High-Throughput Screening Assays, Histone Deacetylase Inhibitors, Pediatrics, Perinatology and Child Health, Cancer research, Nitroso Compounds/pharmacology, Down Syndrome, Drug Screening Assays, Antitumor, business, Histone Deacetylase Inhibitors/pharmacology, Epigenesis, 030215 immunology

Abstract

Background Acute myeloid leukemia (AML) is a heterogeneous disease regarding morphology, immunophenotyping, genetic abnormalities, and clinical behavior. The overall survival rate of pediatric AML is 60% to 70%, and has not significantly improved over the past two decades. Children with Down syndrome (DS) are at risk of developing acute megakaryoblastic leukemia (AMKL), which can be preceded by a transient myeloproliferative disorder during the neonatal period. Intensification of current treatment protocols is not feasible due to already high treatment‐related morbidity and mortality. Instead, more targeted therapies with less severe side effects are highly needed. Procedure To identify potential novel therapeutic targets for myeloid disorders in children, including DS‐AMKL and non‐DS‐AML, we performed an unbiased compound screen of 80 small molecules targeting epigenetic regulators in three pediatric AML cell lines that are representative for different subtypes of pediatric AML. Three candidate compounds were validated and further evaluated in normal myeloid precursor cells during neutrophil differentiation and in (pre‐)leukemic pediatric patient cells. Results Candidate drugs LMK235, NSC3852, and bromosporine were effective in all tested pediatric AML cell lines with antiproliferative, proapoptotic, and differentiation effects. Out of these three compounds, the pan‐histone deacetylase inhibitor NSC3852 specifically induced growth arrest and apoptosis in pediatric AML cells, without disrupting normal neutrophil differentiation. Conclusion NSC3852 is a potential candidate drug for further preclinical testing in pediatric AML and DS‐AMKL.

Published

2019

44. A Plug-and-Play, Drug-on-Pillar Platform for Combination Drug Screening Implemented by Microfluidic Adaptive Printing

Author

Tingrui Pan, Wenwu Xiao, Gerald Quon, Jiannan Li, Yuanpei Li, Randy P. Carney, Kit S. Lam, Yousif Ajena, Yongfan Men, and Wen Tan

Subjects

0301 basic medicine, Drug Evaluation, Preclinical, Triple Negative Breast Neoplasms, 02 engineering and technology, Drug Screening Assays, Analytical Chemistry, Drug dispensing, Tumor Cells, Cultured, media_common, Cancer, Cultured, Chemistry, Pillar, Microfluidic Analytical Techniques, 021001 nanoscience & nanotechnology, Preclinical, Tumor Cells, Drug Combinations, Printing, Three-Dimensional, Printing, Drug, 0210 nano-technology, Combination drug, Plug and play, Cell Survival, media_common.quotation_subject, Microfluidics, Antineoplastic Agents, Article, Dose-Response Relationship, 03 medical and health sciences, Structure-Activity Relationship, Breast Cancer, Humans, Cell Proliferation, Dose-Response Relationship, Drug, Extramural, business.industry, Antitumor, 030104 developmental biology, Doxorubicin, Embedded system, Three-Dimensional, Drug Evaluation, Drug Screening Assays, Antitumor, Drug Storage, business, Other Chemical Sciences

Abstract

Traditional high-throughput drug combination screening requires automatic pipetting of drugs into high-density microtiter plates. Here, a drug-on-pillar platform is proposed for efficient combination drug screening. Using the proposed approach, combination drug screening can be carried out in a plug-and-play manner, allowing for high-throughput screening of large permutations of drug combinations at various concentrations, such that drug dispensing and cell-based screening can be temporally separated and therefore can potentially be performed at distant laboratories. The dispensing is implemented using our recently developed microfluidic pneumatic printing platform, which features a low-cost disposable cartridge that minimizes cross contamination. Moreover, our previously developed drug nanoformulation method with amphiphilic telodendrimers has been utilized to maintain drug stability in a dry form, allowing for convenient drug storage, shipping, and subsequent rehydration. Combining the features described above, we have implemented a 1260-spot drug combination array to study the effect of paired drugs against MDA-MB-231 triple negative human breast cancer cells. This study supports the feasibility of the drug-on-pillar platform for combination drug screening and has provided valuable insight into drug combination efficacy against breast cancer.

Published

2018

45. Self-Assembled Aptamer-Grafted Hyperbranched Polymer Nanocarrier for Targeted and Photoresponsive Drug Delivery

Author

Yang, Lu, Sun, Hao, Liu, Yuan, Hou, Weijia, Yang, Yu, Cai, Ren, Cui, Cheng, Zhang, Penghui, Pan, Xiaoshu, Li, Xiaowei, Li, Long, Sumerlin, Brent S, and Tan, Weihong

Subjects

Polymers, Ultraviolet Rays, aptamers, Bioengineering, Drug Screening Assays, Fluorescence, Cell Line, Drug Delivery Systems, Antibiotics, Humans, Nanotechnology, Cell Proliferation, Cancer, Drug Carriers, Tumor, Spectrometry, Organic Chemistry, Antitumor, self-assembly, Photochemical Processes, Antineoplastic, hyperbranched polymers, Doxorubicin, 5.1 Pharmaceuticals, drug delivery, photoresponsive systems, Chemical Sciences, Nanoparticles, Development of treatments and therapeutic interventions, Nucleotide, Biotechnology

Abstract

Photoresponsive materials are emerging as ideal carriers for precisely controlled drug delivery owing to their high spatiotemporal selectivity. However, drawbacks such as slow release kinetics, inherent toxicity, and lack of targeting ability hinder their translation into clinical use. We constructed a new DNA aptamer-grafted photoresponsive hyperbranched polymer, which can self-assemble into nanoparticles, thereby achieving biocompatibility and target specificity, as well as light-controllable release behavior. Upon UV-irradiation, rapid release induced by disassembly was observed for Nile Red-loaded nanoparticles. Further in vitro cell studies confirmed this delivery system's specific binding and internalization performance arising from the DNA aptamer corona. The DOX-loaded nanoassembly exhibited selective phototriggered cytotoxicity towards cancer cells, indicating its promising therapeutic effect as a smart drug delivery system.

Published

2018

46. Rapid Discovery of Functional Small Molecule Ligands against Proteomic Targets through Library-Against-Library Screening

Author

Brittany Weems, Carolina F. Reis, Hsing Jien Kung, Brianna Ribeiro, Xiaobing Wang, Don Hong Wang, Chao Yu Chen, Daniel H. Enter, Sara Ahadi, Seth Dixon, Liping Meng, Laura M. Ramirez, Leonardo J. Leon, Jason Kato, Yoshiko Maeda, Kit S. Lam, and Chun Yi Wu

Subjects

Proteomics, 0301 basic medicine, Phage display, Druggability, Ligands, Drug Screening Assays, 01 natural sciences, Jurkat Cells, Methionine, Complementary, Drug Discovery, Combinatorial Chemistry Techniques, Cancer, Drug discovery, Chemistry, Cell Cycle, General Medicine, Small molecule, Drug development, 5.1 Pharmaceuticals, Target protein, Development of treatments and therapeutic interventions, Research Article, Biotechnology, DNA, Complementary, small molecule compound beads, Antineoplastic Agents, Computational biology, Cell Line, Small Molecule Libraries, Medicinal and Biomolecular Chemistry, 03 medical and health sciences, phage display cDNA expression proteome library, Peptide Library, Humans, Peptide library, one-bead-one-compound combinatorial library, library-against-library screening, 010405 organic chemistry, Organic Chemistry, DNA, Antitumor, General Chemistry, Combinatorial chemistry, High-Throughput Screening Assays, 0104 chemical sciences, 030104 developmental biology, Benzimidazoles, Drug Screening Assays, Antitumor, molecular interactions

Abstract

Identifying "druggable" targets and their corresponding therapeutic agents are two fundamental challenges in drug discovery research. The one-bead-one-compound (OBOC) combinatorial library method has been developed to discover peptides or small molecules that bind to a specific target protein or elicit a specific cellular response. The phage display cDNA expression proteome library method has been employed to identify target proteins that interact with specific compounds. Here, we combined these two high-throughput approaches, efficiently interrogated approximately 10(13) possible molecular interactions, and identified 91 small molecule compound beads that interacted strongly with the phage library. Of 19 compounds resynthesized, 4 were cytotoxic against cancer cells; one of these compounds was found to interact with EIF5B and inhibit protein translation. As more binding pairs are confirmed and evaluated, the "library-against-library" screening approach and the resulting small molecule-protein domain interaction database may serve as a valuable tool for basic research and drug development.

Published

2016

47. Discovery of Highly Potent Inhibitors Targeting the Predominant Drug-Resistant S31N Mutant of the Influenza A Virus M2 Proton Channel

Author

Chunlong Ma, Fang Li, William F. DeGrado, and Jun Wang

Subjects

Models, Molecular, 0301 basic medicine, Drug Resistance, Drug resistance, Pharmacology, Drug Screening Assays, medicine.disease_cause, 01 natural sciences, Models, Drug Discovery, Influenza A virus, Viral, media_common, Molecular Structure, Drug discovery, Pharmacology and Pharmaceutical Sciences, Infectious Diseases, 5.1 Pharmaceuticals, Pneumonia & Influenza, Molecular Medicine, Drug, Development of treatments and therapeutic interventions, Infection, Medicinal & Biomolecular Chemistry, media_common.quotation_subject, Biology, 010402 general chemistry, Antiviral Agents, Article, Dose-Response Relationship, Vaccine Related, Viral Matrix Proteins, Medicinal and Biomolecular Chemistry, Structure-Activity Relationship, 03 medical and health sciences, Biodefense, Drug Resistance, Viral, medicine, Structure–activity relationship, Viral matrix protein, Dose-Response Relationship, Drug, Prevention, Organic Chemistry, Molecular, Proton Pump Inhibitors, Antitumor, Virology, Influenza, Influenza A virus subtype H5N1, 0104 chemical sciences, Emerging Infectious Diseases, Good Health and Well Being, 030104 developmental biology, M2 proton channel, biology.protein, Drug Screening Assays, Antitumor

Abstract

With the emergence of highly pathogenic avian influenza (HPAI) H7N9 and H5N1 strains, there is a pressing need to develop direct-acting antivirals (DAAs) to combat such deadly viruses. The M2-S31N proton channel of the influenza A virus (A/M2) is one of the validated and most conserved proteins encoded by the current circulating influenza A viruses; thus, it represents a high-profile drug target for therapeutic intervention. We recently discovered a series of S31N inhibitors with the general structure of adamantyl-1-NH2(+)CH2-aryl, but they generally had poor physical properties and some showed toxicity in vitro. In this study, we sought to optimize both the adamantyl as well as the aryl/heteroaryl group. Several compounds from this study exhibited submicromolar EC50 values against S31N-containing A/WSN/33 influenza viruses in antiviral plaque reduction assays with a selectivity index greater than 100, indicating that these compounds are promising candidates for in-depth preclinical pharmacology.

Published

2016

48. Predicting Drug Response and Synergy Using a Deep Learning Model of Human Cancer Cells

Author

Trey Ideker, John Lee, Kyle S. Sanchez, Brent M. Kuenzi, Jianzhu Ma, Jisoo Park, Samson Fong, and Jason F. Kreisberg

Subjects

Patient-Specific Modeling, 0301 basic medicine, Cancer Research, drug synergy, Databases, Factual, Computer science, Drug Screening Assays, 0302 clinical medicine, Neoplasms, Drug response, CRISPR, Interpretability, media_common, network modeling, Tumor, Drug Synergism, machine learning, Oncology, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Development of treatments and therapeutic interventions, Biotechnology, Drug, Genotype, precision medicine, media_common.quotation_subject, Oncology and Carcinogenesis, Antineoplastic Agents, Computational biology, Cell Line, Predictive medicine, Databases, 03 medical and health sciences, Deep Learning, Cell Line, Tumor, Humans, cancer, interpretable deep learning, Oncology & Carcinogenesis, Factual, business.industry, Deep learning, Neurosciences, Computational Biology, Antitumor, Clinical trial, Good Health and Well Being, 030104 developmental biology, Generic health relevance, Artificial intelligence, Drug Screening Assays, Antitumor, business, Human cancer

Abstract

Summary Most drugs entering clinical trials fail, often related to an incomplete understanding of the mechanisms governing drug response. Machine learning techniques hold immense promise for better drug response predictions, but most have not reached clinical practice due to their lack of interpretability and their focus on monotherapies. We address these challenges by developing DrugCell, an interpretable deep learning model of human cancer cells trained on the responses of 1,235 tumor cell lines to 684 drugs. Tumor genotypes induce states in cellular subsystems that are integrated with drug structure to predict response to therapy and, simultaneously, learn biological mechanisms underlying the drug response. DrugCell predictions are accurate in cell lines and also stratify clinical outcomes. Analysis of DrugCell mechanisms leads directly to the design of synergistic drug combinations, which we validate systematically by combinatorial CRISPR, drug-drug screening in vitro, and patient-derived xenografts. DrugCell provides a blueprint for constructing interpretable models for predictive medicine.

Published

2020

49. In vitro and in vivo anticancer activity of tridentate thiosemicarbazone copper complexes: Unravelling an unexplored pharmacological target

Author

Marika Salvalaio, Dominga Rogolino, Matteo Tegoni, Mauro Carcelli, Cristina Marzano, Jennifer Bartoli, Valentina Gandin, and Giorgio Pelosi

Subjects

Models, Molecular, Drug Screening Assays, Inbred C57BL, Crystallography, X-Ray, 01 natural sciences, Mice, Models, Neoplasms, Drug Discovery, Tumor Cells, Cultured, Protein disulfide-isomerase, Protein disulfide isomerase inhibitors, 0303 health sciences, Crystallography, Cultured, Molecular Structure, Chemistry, General Medicine, Tumor Cells, Nanomolar activity, Anticancer compounds, Drug, medicine.symptom, medicine.drug, Thiosemicarbazones, Cell Survival, Copper complexes, X-ray structure, Animals, Antineoplastic Agents, Cell Proliferation, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Mice, Inbred C57BL, Neoplasms, Experimental, Organometallic Compounds, Structure-Activity Relationship, Dose-Response Relationship, Experimental, 03 medical and health sciences, In vivo, medicine, 030304 developmental biology, Pharmacology, Cisplatin, 010405 organic chemistry, Organic Chemistry, HEK 293 cells, Molecular, Cancer, Antitumor, medicine.disease, In vitro, 0104 chemical sciences, Mechanism of action, Cancer cell, X-Ray, Cancer research

Abstract

Certain metal complexes can have a great antitumor activity, as the use of cisplatin in therapy has been demonstrating for the past fifty years. Copper complexes, in particular, have attracted much attention as an example of anticancer compounds based on an endogenous metal. In this paper we present the synthesis and the activity of a series of copper(II) complexes with variously substituted salicylaldehyde thiosemicarbazone ligands. The in vitro activity of both ligands and copper complexes was assessed on a panel of cell lines (HCT-15, LoVo and LoVo oxaliplatin resistant colon carcinoma, A375 melanoma, BxPC3 and PSN1 pancreatic adenocarcinoma, BCPAP thyroid carcinoma, 2008 ovarian carcinoma, HEK293 non-transformed embryonic kidney), highlighting remarkable activity of the metal complexes, in some cases in the low nanomolar range. The copper(II) complexes were also screened, with good results, against 3D spheroids of colon (HCT-15) and pancreatic (PSN1) cancer cells. Detailed investigations on the mechanism of action of the copper(II) complexes are also reported: they are able to potently inhibit Protein Disulfide Isomerase, a copper-binding protein, that is recently emerging as a new therapeutic target for cancer treatment. Good preliminary results obtained in C57BL mice indicate that this series of metal-based compounds could be a very promising weapon in the fight against cancer.

Published

2020

50. Harnessing the Anti-Cancer Natural Product Nimbolide for Targeted Protein Degradation

Author

Jessica N. Spradlin, Carl C. Ward, Daniel K. Nomura, Dirksen E. Bussiere, Lisha Ou, Thomas J. Maimone, Andrew Proudfoot, James A. Olzmann, Jason R. Thomas, Mikias Woldegiorgis, Markus Schirle, Xirui Hu, John A. Tallarico, Jeffrey Mckenna, Michael D. Jones, Elizabeth Ornelas, Scott M. Brittain, and Milton To

Subjects

Druggability, Drug Screening Assays, 01 natural sciences, law.invention, chemistry.chemical_compound, Ubiquitin, law, Phytogenic, ZNF313, Cancer, 0303 health sciences, RNF114, biology, 030302 biochemistry & molecular biology, Cell biology, Ubiquitin ligase, 5.1 Pharmaceuticals, Female, Development of treatments and therapeutic interventions, Limonins, Biochemistry & Molecular Biology, Ubiquitin-Protein Ligases, Cancer therapy, Antineoplastic Agents, Breast Neoplasms, Protein degradation, Article, Medicinal and Biomolecular Chemistry, 03 medical and health sciences, Breast Cancer, medicine, Humans, ABPP, Molecular Biology, activity-based protein profiling, Cell Proliferation, 030304 developmental biology, Biological Products, Natural product, 010405 organic chemistry, Antitumor, Cell Biology, medicine.disease, chemoproteomics, Antineoplastic Agents, Phytogenic, 0104 chemical sciences, Protein profiling, nimbolide, chemistry, Proteolysis, biology.protein, Suppressor, Biochemistry and Cell Biology, degraders, Drug Screening Assays, Antitumor, Carrier Proteins, targeted protein degradation

Abstract

Nimbolide, a terpenoid natural product derived from the Neem tree, impairs cancer pathogenicity across many types of human cancers; however, the direct targets and mechanisms by which nimbolide exerts its effects are poorly understood. Here, we used activity-based protein profiling (ABPP) chemoproteomic platforms to discover that nimbolide reacts with a novel functional cysteine crucial for substrate recognition in the E3 ubiquitin ligase RNF114. Nimbolide impairs breast cancer cell proliferation in-part by disrupting RNF114 substrate recognition, leading to inhibition of ubiquitination and degradation of the tumor-suppressors such as p21, resulting in their rapid stabilization. We further demonstrate that nimbolide can be harnessed to recruit RNF114 as an E3 ligase in targeted protein degradation applications and show that synthetically simpler scaffolds are also capable of accessing this unique reactive site. Our study highlights the utility of ABPP platforms in uncovering unique druggable modalities accessed by natural products for cancer therapy and targeted protein degradation applications.

Published

2018