Your search keyword '"Benelita T. Elie"' showing total 19 results

1. Preclinical evaluation of an unconventional ruthenium‐gold‐based chemotherapeutic: RANCE‐1, in clear cell renal cell carcinoma

Author

Benelita T. Elie, Karen Hubbard, Yuriy Pechenyy, Buddhadev Layek, Swayam Prabha, and Maria Contel

Subjects

clear cell renal cell carcinoma, histopathology, kidney metastasis, mice xenograft model, pharmacokinetics, unconventional chemotherapeutics, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background There are few effective treatments for patients with advanced clear cell renal cell carcinoma (CCRCC). Recent findings indicate that ruthenium‐gold containing compounds exhibit significant antitumor efficacy against CCRCC in vitro affecting cell viability as well as angiogenesis and markers driving those 2 phenomena. However, no in vivo preclinical evaluation of this class of compounds has been reported. Methods Following the dose‐finding pharmacokinetic determination, NOD.CB17‐Prkdc SCID/J mice bearing xenograft CCRCC Caki‐1 tumors were treated in an intervention trial for 21 days at 10 mg/kg/72h of RANCE‐1. At the end of the trial, tumor samples were analyzed for histopathological and changes in protein expression levels were assessed. Results After 21 days of treatment there was no significant change in tumor size in the RANCE‐1‐treated mice as compared to the starting size (+3.87%) (P = 0.082) while the vehicle treated mice exhibited a significant tumor size increase (+138%) (P

Published

2019

2. Compensatory CSF2-driven macrophage activation promotes adaptive resistance to CSF1R inhibition in breast-to-brain metastasis

Author

Patrick N. Harter, Roy Thomas Daniel, Michael Schulz, Florian Klemm, Alexander Schaffer, Monika E. Hegi, Pia S. Zeiner, Roeltje R. Maas, Anna Salamero-Boix, Benelita T. Elie, Johanna A. Joyce, Robert L. Bowman, Katja Niesel, Lisa Sevenich, Marie Groth, Aylin Möckl, Jenny Zinke, Karl H. Plate, and Tijna Alekseeva

Subjects

Cancer Research, Cell type, Skin Neoplasms, Metastasis, Mice, Receptors, Colony-Stimulating Factor, STAT5 Transcription Factor, Tumor Microenvironment, medicine, Animals, Macrophage, Melanoma, STAT5, Neuroinflammation, biology, Microglia, Brain Neoplasms, business.industry, Granulocyte-Macrophage Colony-Stimulating Factor, Cancer, Genes, fms, Macrophage Activation, medicine.disease, medicine.anatomical_structure, Oncology, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, biology.protein, Cancer research, business, Brain metastasis

Abstract

Tumor microenvironment-targeted therapies are emerging as promising treatment options for different cancer types. Tumor-associated macrophages and microglia (TAMs) represent an abundant nonmalignant cell type in brain metastases and have been proposed to modulate metastatic colonization and outgrowth. Here we demonstrate that targeting TAMs at distinct stages of the metastatic cascade using an inhibitor of colony-stimulating factor 1 receptor (CSF1R), BLZ945, in murine breast-to-brain metastasis models leads to antitumor responses in prevention and intervention preclinical trials. However, in established brain metastases, compensatory CSF2Rb–STAT5-mediated pro-inflammatory TAM activation blunted the ultimate efficacy of CSF1R inhibition by inducing neuroinflammation gene signatures in association with wound repair responses that fostered tumor recurrence. Consequently, blockade of CSF1R combined with inhibition of STAT5 signaling via AC4-130 led to sustained tumor control, a normalization of microglial activation states and amelioration of neuronal damage. Klemm et al. show that resistance to CSF1R inhibition in breast cancer brain metastasis is driven by compensatory activation of the CSF2Rb–STAT5 axis in macrophages, which can be alleviated by combined targeting of CSF1R and STAT5.

Published

2021

3. Preclinical evaluation of an unconventional ruthenium‐gold‐based chemotherapeutic: RANCE‐1, in clear cell renal cell carcinoma

Author

Karen Hubbard, Buddhadev Layek, Yuriy Pechenyy, Benelita T. Elie, Swayam Prabha, and María Contel

Subjects

0301 basic medicine, Male, Cancer Research, Angiogenesis, unconventional chemotherapeutics, clear cell renal cell carcinoma, Fibroblast growth factor, Mice, 0302 clinical medicine, Angiogenic Proteins, Original Research, Cancer Biology, biology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Kidney Neoplasms, 3. Good health, Gene Expression Regulation, Neoplastic, Treatment Outcome, Oncology, 030220 oncology & carcinogenesis, histopathology, Female, pharmacokinetics, Platelet-derived growth factor receptor, medicine.medical_specialty, Stromal cell, Cell Survival, kidney metastasis, lcsh:RC254-282, Ruthenium, 03 medical and health sciences, In vivo, Cell Line, Tumor, medicine, Organometallic Compounds, Animals, Humans, Radiology, Nuclear Medicine and imaging, mice xenograft model, Viability assay, Carcinoma, Renal Cell, Cell Proliferation, business.industry, medicine.disease, Xenograft Model Antitumor Assays, Clear cell renal cell carcinoma, 030104 developmental biology, Cancer research, biology.protein, Histopathology, Gold, business

Abstract

Background There are few effective treatments for patients with advanced clear cell renal cell carcinoma (CCRCC). Recent findings indicate that ruthenium‐gold containing compounds exhibit significant antitumor efficacy against CCRCC in vitro affecting cell viability as well as angiogenesis and markers driving those 2 phenomena. However, no in vivo preclinical evaluation of this class of compounds has been reported. Methods Following the dose‐finding pharmacokinetic determination, NOD.CB17‐Prkdc SCID/J mice bearing xenograft CCRCC Caki‐1 tumors were treated in an intervention trial for 21 days at 10 mg/kg/72h of RANCE‐1. At the end of the trial, tumor samples were analyzed for histopathological and changes in protein expression levels were assessed. Results After 21 days of treatment there was no significant change in tumor size in the RANCE‐1‐treated mice as compared to the starting size (+3.87%) (P = 0.082) while the vehicle treated mice exhibited a significant tumor size increase (+138%) (P

Published

2019

4. Compensatory CSF2-driven macrophage activation promotes adaptive resistance to CSF1R inhibition in breast-to-brain metastasis

Author

Marcel H. Schulz, Tijna Alekseeva, Benelita T. Elie, A. Schaeffer, Lisa Sevenich, Johanna A. Joyce, Patrick N. Harter, Anna Salamero-Boix, Roy Thomas Daniel, Robert L. Bowman, M. Groth, Katja Niesel, Monika E. Hegi, Karl-Heinz Plate, Roeltje R. Maas, Pia S. Zeiner, Jenny Zinke, and Florian Klemm

Subjects

Cell type, biology, Microglia, business.industry, Cancer, medicine.disease, Metastasis, Blockade, Colony stimulating factor 1 receptor, medicine.anatomical_structure, biology.protein, Cancer research, Medicine, business, STAT5, Brain metastasis

Abstract

SUMMARYTumor microenvironment-targeted therapies are emerging as promising treatment options for different cancer types. Tumor-associated macrophages and microglia (TAMs) represent an abundant non-malignant cell type in brain metastases and have been proposed to modulate metastatic colonization and outgrowth. We used an inhibitor of colony stimulating factor 1 receptor (CSF1R) to target TAMs at distinct stages of the metastatic cascade in preclinical breast-to-brain metastasis models and found that CSF1R inhibition leads to anti-tumor responses in prevention and intervention trials. However, in established brain metastases, compensatory CSF2Rb-STAT5-mediated pro-inflammatory TAM activation blunted the ultimate efficacy of CSF1R inhibition by inducing neuro-inflammation gene signatures in association with wound repair responses that fostered tumor recurrence. Consequently, combined blockade of CSF1R and STAT5 signaling led to sustained tumor control, a normalization of microglial activation states and amelioration of neuronal damage.

Published

2021

5. Auranofin-Based Analogues Are Effective Against Clear Cell Renal Carcinoma In Vivo and Display No Significant Systemic Toxicity

Author

Karen Hubbard, Swayam Prabha, Won Seok Yang, Buddhadev Layek, Joe W. Ramos, Benelita T. Elie, and María Contel

Subjects

Pharmacology, medicine.medical_specialty, Auranofin, business.industry, Text mining, Systemic toxicity, Pharmacokinetics, In vivo, Clear Cell Renal Carcinoma, medicine, Cancer research, Pharmacology (medical), Histopathology, business, Cytotoxicity, medicine.drug

Abstract

[Image: see text] Effective pharmacological treatments for patients with advanced clear cell renal carcinoma (ccRCC) are limited. Bimetallic titanium–gold containing compounds exhibit significant cytotoxicity against ccRCC in vitro and in vivo and inhibit invasion and angiogenisis in vitro and markers driving these phenomena. However, in vivo preclinical evaluations of such compounds have not examined their pharmacokinetics, pathology, and hematology. Here we use NOD.CB17-Prkdc SCID/J mice bearing xenograft ccRCC Caki-1 tumors to evaluate the in vivo efficacies of two titanium–gold compounds Titanocref and Titanofin (based on auranofin analogue scaffolds) accompanied by pharmacokinetic and pathology studies. A therapeutic trial was performed over 21 days at 5 mg/kg/72h of Titanocref and 10 mg/kg/72h of Titanofin tracking changes in tumor size. We observed a significant reduction of 51% and 60%, respectively (p < 0.01) in tumor size in the Titanocref- and Titanofin-treated mice compared to the starting size, while the vehicle-treated mice exhibited a tumor size increase of 138% (p < 0.01). Importantly, no signs of pathological complication as a result of treatment were found. In addition, Titanocref and Titanofin treatment reduced angiogenesis by 38% and 54%, respectively. Microarray and qRT-PCR analysis of ccRCC Caki-1 cells treated with Titanocref revealed that the compound alters apoptosis, JNK MAP kinase, and ROS pathways within 3 h of treatment. We further show activation of apoptosis by Titanocref and Titanofin in vivo by caspase 3 assay. Titanocref is active against additional kidney cancer cells. Titanocref and Titanofin are therefore promising candidates for further evaluation toward clinical application in the treatment of ccRCC.

Published

2020

6. A heterometallic ruthenium–gold complex displays antiproliferative, antimigratory, and antiangiogenic properties and inhibits metastasis and angiogenesis-associated proteases in renal cancer

Author

Yuriy Pechenyy, Fathema Uddin, María Contel, and Benelita T. Elie

Subjects

Auranofin, Angiogenesis, Matrix metalloproteinase, 010402 general chemistry, 01 natural sciences, Biochemistry, Article, Metastasis, Inorganic Chemistry, Coordination Complexes, Cell Line, Tumor, medicine, Humans, Protease Inhibitors, Neoplasm Metastasis, Carcinoma, Renal Cell, Cell Proliferation, Neovascularization, Pathologic, 010405 organic chemistry, Chemistry, Cancer, medicine.disease, Kidney Neoplasms, In vitro, 0104 chemical sciences, Apoptosis, Cancer cell, Cancer research, Ruthenium Compounds, Gold, medicine.drug

Abstract

Heterobimetallic compounds are designed to harness chemotherapeutic traits of distinct metal species into a single molecule. The ruthenium-gold (Ru-Au) family of compounds based on Au-N-heterocyclic carbene (NHC) fragments [Cl(2)(p-cymene)Ru(μ-dppm)Au(NHC)]ClO(4) was conceived to combine the known antiproliferative and cytotoxic properties of Au-NHC-based compounds and the antimigratory, antimetastatic and antiangiogenic characteristic of specific Ru-based compounds. Following recent studies of the anticancer efficacies of these Ru–Au-NHC complexes with promising potential as chemotherapeutics against colorectal, and renal cancers in vitro, we report here on the mechanism of a selected compound, [Cl(2)(p-cymene)Ru(μ-dppm)Au(IMes)]ClO(4) (RANCE-1, 1). The studies were carried out in vitro using a human clear cell renal carcinoma cell line (Caki-1). These studies indicate that bimetallic compound RANCE-1 (1) is significantly more cytotoxic than the Ru (2) or Au (3) monometallic derivatives. RANCE-1 significantly inhibits migration, invasion and angiogenesis, which are essential for metastasis. RANCE-1 was found to disturb pericellular proteolysis by inhibiting cathepsins, and the metalloproteases MMP and ADAM which play key roles in the etiopathogenesis of cancer. RANCE-1 also inhibits the mitochondrial protein TrxR that is often overexpressed in cancer cells and facilitates apoptosis evasion. We found that while Auranofin perturbed migration and invasion to similar degrees as RANCE-1 (1) in Caki-1 renal cancer cells, RANCE-1 (1) inhibited antiangiogenic formation and VEGF expression. We found that Auranofin and RANCE-1 (1) have distinct proteolytic profiles. In summary, RANCE-1 constitutes a very promising candidate for further preclinical evaluations in renal cancer.

Published

2018

7. Bimetallic titanocene-gold phosphane complexes inhibit invasion, metastasis, and angiogenesis-associated signaling molecules in renal cancer

Author

Natalia Curado, Jacob Fernández-Gallardo, María Contel, Joe W. Ramos, Mike A. Cornejo, and Benelita T. Elie

Subjects

Auranofin, Cell Survival, Phosphines, Molecular Conformation, Angiogenesis Inhibitors, Antineoplastic Agents, Article, chemistry.chemical_compound, Structure-Activity Relationship, In vivo, Cell Movement, Coordination Complexes, Cell Line, Tumor, Drug Discovery, medicine, Organometallic Compounds, Cytotoxic T cell, Humans, Cell Proliferation, Pharmacology, Dose-Response Relationship, Drug, Neovascularization, Pathologic, Organic Chemistry, Cancer, Titanocene dichloride, General Medicine, medicine.disease, In vitro, Kidney Neoplasms, chemistry, Apoptosis, Cancer cell, Cancer research, Drug Screening Assays, Antitumor, medicine.drug

Abstract

Following promising recent in vitro and in vivo studies of the anticancer efficacies of heterometallic titanocene–gold chemotherapeutic candidates against renal cancer, we report here on the synthesis, characterization, stability studies and biological evaluation of a new titanocene complex containing a gold-triethylphosphane fragment [(η-C(5)H(5))(2)TiMe(μ-mba)Au(PEt(3))] (4) Titanofin. The compound is more stable in physiological fluid than those previously reported, and it is highly cytotoxic against a line of human clear cell renal carcinoma. We describe here preliminary mechanistic data for this compound and previously reported [(η-C(5)H(5))(2)TiMe(μ-mba)Au(PPh(3))] (2) Titanocref which displayed remarkable activity in an in vivo mouse model. Mechanistic studies were carried out in the human clear cell renal carcinoma Caki-1 line for the bimetallic compounds [(η-C(5)H(5))(2)TiMe(μ-mba)Au(PR(3))] (PR(3) = PPh(3) 2 Titanocref and PEt(3) 4 Titanofin), the two monometallic gold derivatives [Au(Hmba)(PR(3))] (PR(3) = PPh(3) 1 cref; PEt(3) 3 fin), titanocene dichloride and Auranofin as controls. These studies indicate that bimetallic compounds Titanocref (2) and Titanofin (4) are more cytotoxic than gold monometallic derivatives (1 and 3) and significantly more cytotoxic than titanocene dichloride while being quite selective. Titanocref (2) and Titanofin (4) inhibit migration, invasion, and angiogenic assembly along with molecular markers associated with these processes such as prometastatic IL(s), MMP(s), TNF-α, and proangiogenic VEGF, FGF-basic. The bimetallic compounds also strongly inhibit the mitochondrial protein TrxR often overexpressed in cancer cells evading apoptosis and also inhibit FOXC2, PECAM-1, and HIF-1α whose overexpression is linked to resistance to genotoxic chemotherapy. In summary, bimetallic titanocene-gold phosphane complexes (Titanocref 2 and Titanofin 4) are very promising candidates for further preclinical evaluations for the treatment of renal cancer.

Published

2018

8. Synthesis and anticancer activity of carbosilane metallodendrimers based on arene ruthenium(<scp>ii</scp>) complexes

Author

Jorge Pérez-Serrano, Marta Maroto-Díaz, Rafael Gómez, María Contel, Benelita T. Elie, Pilar Gómez-Sal, and F. Javier de la Mata

Subjects

Dendrimers, Denticity, Stereochemistry, chemistry.chemical_element, Antineoplastic Agents, Chemistry Techniques, Synthetic, Ligands, 010402 general chemistry, 01 natural sciences, Ruthenium, Article, Cathepsin B, Inorganic Chemistry, chemistry.chemical_compound, Cell Line, Tumor, Dendrimer, Pyridine, Organometallic Compounds, medicine, Humans, Molecule, Reactivity (chemistry), Cytotoxicity, Serum Albumin, Cell Death, 010405 organic chemistry, Chemistry, DNA, Silanes, Human serum albumin, Combinatorial chemistry, 0104 chemical sciences, medicine.drug

Abstract

A series of new organometallic carbosilane dendrimers (first and second generation) and the corresponding non-dendritic mononuclear based on ruthenium arene fragments are described. The metallodendrimers were prepared by reactions of the precursor [Ru(η(6)-p-cymene)Cl2]2 with carbosilane dendrimers functionalized with N-donor monodentate ligands such as NH2- and pyridine, or with N,O-, N,N-chelating imine ligands. While the dendrimer precursors are insoluble in DMSO or water, novel metallodendrimers are soluble in DMSO and some of them are even highly soluble in water. The molecular structure of the "Ru-NH2" mononuclear compound (zero generation) was determined by single-crystal X-ray crystallography. The cytotoxicity activity of these dendritic structures was evaluated in several human cancer cell lines and compared with that of the corresponding mononuclear ruthenium complexes. Most compounds display significant cytotoxic activities in the low micromolar range with the first generation ruthenium dendrimers being the most active compounds. The cell death type for selected compounds has been studied as well as their reactivity towards relevant biomolecules such as DNA, Human Serum Albumin (HSA) and Cathepsin-B. All the data point to a mode of action different from that of cisplatin for most complexes. First generation ruthenium dendrimers inhibit Cathepsin-B, which may suggest potential antimetastatic properties of these compounds.

Published

2016

9. Versatile synthesis of cationic N-heterocyclic carbene–gold(<scp>i</scp>) complexes containing a second ancillary ligand. Design of heterobimetallic ruthenium–gold anticancer agents

Author

María Contel, Benelita T. Elie, Jacob Fernández-Gallardo, and Mercedes Sanaú

Subjects

Stereochemistry, chemistry.chemical_element, Ligands, 010402 general chemistry, 01 natural sciences, Article, Ruthenium, Catalysis, chemistry.chemical_compound, Heterocyclic Compounds, Cations, Materials Chemistry, 010405 organic chemistry, Chemistry, Ligand, Second ancillary, Metals and Alloys, Cationic polymerization, General Chemistry, Combinatorial chemistry, 0104 chemical sciences, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, Ceramics and Composites, Gold, Methane, Carbene

Abstract

We describe a versatile and quick route to cationic gold(i) complexes containing N-heterocyclic carbenes and a second ancillary ligand (such as phosphanes, phosphites, arsines and amines) of interest for the synthesis of compounds with potential catalytic and medicinal applications. The general synthetic strategy has been applied in the preparation of novel cationic heterobimetallic ruthenium(ii)-gold(i) complexes that are highly cytotoxic to renal cancer Caki-1 and colon cancer HCT 116 cell lines while showing a synergistic effect and being more selective than their monometallic counterparts.

Published

2016

10. Heterometallic titanium–gold complexes inhibit renal cancer cells in vitro and in vivo

Author

Susan A. Rotenberg, Joe W. Ramos, Swayam Prabha, Jacob Fernández-Gallardo, Benelita T. Elie, Tanmoy Sadhukha, Mercedes Sanaú, and María Contel

Subjects

Biochemistry, Chemistry, Kinase, Cell culture, In vivo, Cancer cell, Cytotoxic T cell, General Chemistry, Ligand (biochemistry), Protein kinase B, In vitro, 3. Good health

Abstract

Following recent work on heterometallic titanocene-gold complexes as potential chemotherapeutics for renal cancer, we report here on the synthesis, characterization and stability studies of new titanocene complexes containing a methyl group and a carboxylate ligand (mba = S-C6H4-COO-) bound to gold(I)-phosphane fragments through a thiolate group ([(η-C5H5)2TiMe(μ-mba)Au(PR3)]. The compounds are more stable in physiological media than those previously reported and are highly cytotoxic against human cancer renal cell lines. We describe here preliminary mechanistic data involving studies on the interaction of selected compounds with plasmid (pBR322) DNA used as a model nucleic acid, and with selected protein kinases from a panel of 35 protein kinases having oncological interest. Preliminary mechanistic studies in Caki-1 renal cells indicate that the cytotoxic and anti-migration effects of the most active compound 5 ([(η-C5H5)2TiMe(μ-mba)Au(PPh3)] involve inhibition of thioredoxin reductase and loss of expression of protein kinases that drive cell migration (AKT, p90-RSK, and MAPKAPK3). The co-localization of both titanium and gold metals (1:1 ratio) in Caki-1 renal cells was demonstrated for 5 indicating the robustness of the heterometallic compound in vitro. Two compounds were selected for further in vivo studies on mice based on their selectivity in vitro against renal cancer cell lines when compared to non-tumorigenic human kidney cell lines (HEK-293T and RPTC) and the favourable preliminary toxicity profile in C57BL/6 mice. Evaluation of Caki-1 xenografts in NOD.CB17-Prkdc SCID/J mice showed an impressive tumor reduction (67%) after treatment for 28 days (3 mg/kg/every other day) with heterometallic compound 5 as compared with the previously described [(η-C5H5)2Ti{OC(O)-4-C6H4-P(Ph2)AuCI}2] 3 which was non-inhibitory. These findings indicate that structural modifications on the ligand scaffold affect the in vivo efficacy of this class of compounds.

Published

2015

11. In Vitro and in Vivo Evaluation of Water-Soluble Iminophosphorane Ruthenium(II) Compounds. A Potential Chemotherapeutic Agent for Triple Negative Breast Cancer

Author

Isabel Marzo, Oscar Gonzalo, Joe W. Ramos, Tanmoy Sadhukha, Daniel Ramírez de Mingo, Swayam Prabha, Malgorzata Frik, Benelita T. Elie, Mercedes Sanaú, Alberto Martínez, Roberto A. Sánchez-Delgado, and María Contel

Subjects

Programmed cell death, Stereochemistry, Phosphoranes, Antineoplastic Agents, Triple Negative Breast Neoplasms, Mice, SCID, Pharmacology, In Vitro Techniques, Article, Ruthenium, In vivo, Coordination Complexes, Mice, Inbred NOD, Drug Discovery, medicine, Organometallic Compounds, Cytotoxic T cell, Animals, Humans, Cathepsin, Cisplatin, Chemistry, Water, In vitro, 3. Good health, HEK293 Cells, Solubility, Cell culture, Apoptosis, Molecular Medicine, Female, medicine.drug

Abstract

A series of organometallic ruthenium(II) complexes containing iminophosphorane ligands have been synthesized and characterized. Cationic compounds with chloride as counterion are soluble in water (70–100 mg/mL). Most compounds (especially highly water-soluble 2) are more cytotoxic to a number of human cancer cell lines than cisplatin. Initial mechanistic studies indicate that the cell death type for these compounds is mainly through canonical or caspase-dependent apoptosis, nondependent on p53, and that the compounds do not interact with DNA or inhibit protease cathepsin B. In vivo experiments of 2 on MDA-MB-231 xenografts in NOD.CB17-Prkdc SCID/J mice showed an impressive tumor reduction (shrinkage) of 56% after 28 days of treatment (14 doses of 5 mg/kg every other day) with low systemic toxicity. Pharmacokinetic studies showed a quick absorption of 2 in plasma with preferential accumulation in the breast tumor tissues when compared to kidney and liver, which may explain its high efficacy in vivo.

Published

2014

12. Organometallic Titanocene–Gold Compounds as Potential Chemotherapeutics in Renal Cancer. Study of their Protein Kinase Inhibitory Properties

Author

Jacob Fernández-Gallardo, Benelita T. Elie, Florian J. Sulzmaier, Joe W. Ramos, María Contel, and Mercedes Sanaú

Subjects

Cisplatin, 010405 organic chemistry, Kinase, Chemistry, Stereochemistry, Organic Chemistry, Cancer, Titanocene dichloride, Nanotechnology, 010402 general chemistry, medicine.disease, 01 natural sciences, Article, In vitro, 0104 chemical sciences, 3. Good health, Inorganic Chemistry, chemistry.chemical_compound, Gold Compounds, medicine, Physical and Theoretical Chemistry, Protein kinase A, Protein kinase B, medicine.drug

Abstract

Early–late transition metal TiAu2 compounds [(η-C5H5)2Ti{OC(O)CH2PPh2AuCl}2] (3) and new [(η-C5H5)2Ti{OC(O)-4-C6H4PPh2AuCl}2] (5) were evaluated as potential anticancer agents in vitro against renal and prostate cancer cell lines. The compounds were significantly more effective than monometallic titanocene dichloride and gold(I) [{HOC(O)RPPh2}AuCl] (R = −CH2– 6, −4-C6H4– 7) derivatives in renal cancer cell lines, indicating a synergistic effect of the resulting heterometallic species. The activity on renal cancer cell lines (for 5 in the nanomolar range) was considerably higher than that of cisplatin and highly active titanocene Y. Initial mechanistic studies in Caki-1 cells in vitro coupled with studies of their inhibitory properties on a panel of 35 kinases of oncological interest indicate that these compounds inhibit protein kinases of the AKT and MAPKAPK families with a higher selectivity toward MAPKAPK3 (IC503 = 91 nM, IC505 = 117 nM). The selectivity of the compounds in vitro against renal cancer cell lines when compared to a nontumorigenic human embryonic kidney cell line (HEK-293T) and the favorable preliminary toxicity profile on C57black6 mice indicate that these compounds (especially 5) are excellent candidates for further development as potential renal cancer chemotherapeutics.

Published

2014

13. Titanocene–gold complexes containing N-heterocyclic carbene ligands inhibit growth of prostate, renal, and colon cancers in vitro

Author

Jacob Fernández-Gallardo, Oscar Navarro, Ahmed Gubran, Yiu Fung Mui, Benelita T. Elie, Mercedes Sanaú, Irene Maluenda, and María Contel

Subjects

010405 organic chemistry, Ligand, Stereochemistry, Organic Chemistry, 010402 general chemistry, medicine.disease, 01 natural sciences, Article, In vitro, 3. Good health, 0104 chemical sciences, Inorganic Chemistry, chemistry.chemical_compound, Prostate cancer, medicine.anatomical_structure, chemistry, Prostate, medicine, Carboxylate, Physical and Theoretical Chemistry, QD0146, Selectivity, Carbene, Methyl group

Abstract

We report on the synthesis, characterization, and stability studies of new titanocene complexes containing a methyl group and a carboxylate ligand (mba = −OC(O)-p-C6H4-S−) bound to gold(I)−N-heterocyclic carbene fragments through the thiolate group: [(η5 -C5H5)2TiMe(μ-mba)Au(NHC)]. The cytotoxicities of the heterometallic compounds along with those of novel monometallic gold−N-heterocyclic carbene precursors [(NHC)Au(mbaH)] have been evaluated against renal, prostate, colon, and breast cancer cell lines. The highest activity and selectivity and a synergistic effect of the resulting heterometallic species was found for the prostate and colon cancer cell lines. The colocalization of both titanium and gold metals (1:1 ratio) in PC3 prostate cancer cells was demonstrated for the selected compound 5a, indicating the robustness of the heterometallic compound in vitro. We describe here preliminary mechanistic data involving studies on the interaction of selected mono- and bimetallic compounds with plasmid (pBR322) used as a model nucleic acid and the inhibition of thioredoxin reductase in PC3 prostate cancer cells. The heterometallic compounds, which are highly apoptotic, exhibit strong antimigratory effects on the prostate cancer cell line PC3.

Published

2016

14. Water‐Soluble (Phosphane)gold(I) Complexes – Applications as Recyclable Catalysts in a Three‐Component Coupling Reaction and as Antimicrobial and Anticancer Agents

Author

Rafael Ovalle, Renato J. Aguilera, Armando Varela-Ramirez, Benelita T. Elie, Chaya Levine, Iban Ubarretxena-Belandia, and María Contel

Subjects

chemistry.chemical_classification, Chemistry, Biological activity, Antimicrobial, Combinatorial chemistry, Article, Coupling reaction, Catalysis, Inorganic Chemistry, chemistry.chemical_compound, Lipophilicity, Organic chemistry, Antibacterial activity, TPPTS, Alkyl

Abstract

Water-soluble compounds of the type [AuCl(PR3)] with alkyl-bis-(m-sulfonated-phenyl)-(mC6H4SO3Na)2 and dialkyl-(m-sulfonated-phenyl)-(mC6H4SO3Na) (R = nBu, Cp) phosphanes have been prepared. Dialkyl-phosphane compounds generate water-soluble nanoparticles of 10-15 nm radius when dissolved in water. These air-stable complexes have been evaluated as catalysts in the synthesis of propargylamines via a three-component coupling reaction of aldehydes, amines and alkynes in water. The antimicrobial activity of the new complexes against Gram-positive and Gram-negative bacteria and yeast has been evaluated. The new compounds display moderate to high antibacterial activity. The more lipophilic compounds are also potent against fungi. Their cytotoxic properties have been analyzed in vitro utilizing human Jurkat T-cell acute lymphoblastic leukemia cells. Compounds with dialkyl-(m-sulfonated-phenyl)-(mC6H4SO3Na) phosphanes displayed moderate to high cytotoxicity on this cell line. Death cell mechanism occurs mainly by early apoptosis. The catalytic/biological activity of the previously described compound with commercial m-trisulfonated-triphenylphosphine [AuCl(TPPTS)] (6) has been also evaluated to compare the effects of the higher basicity and lipophilicity of the alkyl- and di-alkyl-(m-sulfonated-phenyl) phosphanes on these new compounds.

Published

2009

15. Analysis of tumour- and stroma-supplied proteolytic networks reveals a brain-metastasis-promoting role for cathepsin S

Author

Franck Rapaport, Johanna A. Joyce, Lisa Sevenich, William C. Hahn, Benelita T. Elie, Robert L. Bowman, Steven D. Mason, Christina S. Leslie, Edi Brogi, Joan Massagué, Priscilla K. Brastianos, Daniela F. Quail, and Leslie J. Holsinger

Subjects

Lung Neoplasms, Mice, Nude, Antineoplastic Agents, Bone Neoplasms, Breast Neoplasms, Kaplan-Meier Estimate, Mice, SCID, Biology, Blood–brain barrier, Disease-Free Survival, Article, Metastasis, Mice, Stroma, Cell Movement, Mice, Inbred NOD, Cell Line, Tumor, medicine, Biomarkers, Tumor, Tumor Microenvironment, Animals, Humans, Protease Inhibitors, Serpins, Cathepsin S, Cathepsin, Mice, Knockout, Tumor microenvironment, Tight Junction Proteins, Brain Neoplasms, Cancer, Cell Biology, medicine.disease, Cathepsins, Cystatins, Xenograft Model Antitumor Assays, 3. Good health, Cell biology, medicine.anatomical_structure, Blood-Brain Barrier, Organ Specificity, Immunology, Proteolysis, Cancer research, Female, Brain metastasis

Abstract

Metastasis remains the most common cause of death in most cancers, with limited therapies for combating disseminated disease. While the primary tumour microenvironment is an important regulator of cancer progression, it is less well understood how different tissue environments influence metastasis. We analysed tumour-stroma interactions that modulate organ tropism of brain, bone and lung metastasis in xenograft models. We identified a number of potential modulators of site-specific metastasis, including cathepsin S as a regulator of breast-to-brain metastasis. High cathepsin S expression at the primary site correlated with decreased brain metastasis-free survival in breast cancer patients. Both macrophages and tumour cells produce cathepsin S, and only the combined depletion significantly reduced brain metastasis in vivo. Cathepsin S specifically mediates blood-brain barrier transmigration through proteolytic processing of the junctional adhesion molecule, JAM-B. Pharmacological inhibition of cathepsin S significantly reduced experimental brain metastasis, supporting its consideration as a therapeutic target for this disease.

Published

2013

16. Macrophages and cathepsin proteases blunt chemotherapeutic response in breast cancer

Author

Jemila C. Kester, Emily C. Zabor, Tanaya Shree, Kenishana Simpson, Benelita T. Elie, Oakley C. Olson, Katherine M. Bell-McGuinn, Johanna A. Joyce, Alfred L. Garfall, and Edi Brogi

Subjects

Proteases, Lung Neoplasms, Paclitaxel, medicine.medical_treatment, Antineoplastic Agents, Mammary Neoplasms, Animal, Mice, Inbred Strains, Pharmacology, Biology, Metastasis, chemistry.chemical_compound, Mice, Cell Line, Tumor, Genetics, medicine, Neoplasm, Animals, Doxorubicin, Drug Interactions, Neoplasm Invasiveness, Etoposide, Cathepsin, Chemotherapy, Macrophages, medicine.disease, Cathepsins, Mice, Inbred C57BL, chemistry, Tumor progression, Drug Resistance, Neoplasm, Female, Research Paper, Developmental Biology, medicine.drug

Abstract

The microenvironment is known to critically modulate tumor progression, yet its role in regulating treatment response is poorly understood. Here we found increased macrophage infiltration and cathepsin protease levels in mammary tumors following paclitaxel (Taxol) chemotherapy. Cathepsin-expressing macrophages protected against Taxol-induced tumor cell death in coculture, an effect fully reversed by cathepsin inhibition and mediated partially by cathepsins B and S. Macrophages were also found to protect against tumor cell death induced by additional chemotherapeutics, specifically etoposide and doxorubicin. Combining Taxol with cathepsin inhibition in vivo significantly enhanced efficacy against primary and metastatic tumors, supporting the therapeutic relevance of this effect. Additionally incorporating continuous low-dose cyclophosphamide dramatically impaired tumor growth and metastasis and improved survival. This study highlights the importance of integrated targeting of the tumor and its microenvironment and implicates macrophages and cathepsins in blunting chemotherapeutic response.

Published

2011

17. Identification and pre-clinical testing of a reversible cathepsin protease inhibitor reveals anti-tumor efficacy in a pancreatic cancer model

Author

Vasilena Gocheva, Leslie J. Holsinger, Benelita T. Elie, Tanaya Shree, Stacie A. Dalrymple, and Johanna A. Joyce

Subjects

Cyclopropanes, Hydrocarbons, Fluorinated, medicine.medical_treatment, Drug Evaluation, Preclinical, Biological Availability, Antineoplastic Agents, Apoptosis, Biology, Biochemistry, Article, Metastasis, chemistry.chemical_compound, Mice, Leucine, Pancreatic cancer, medicine, Animals, Humans, Neoplasm Invasiveness, Protease Inhibitors, Sulfones, Cell Proliferation, Cathepsin, geography, Protease, geography.geographical_feature_category, Neovascularization, Pathologic, Cancer, General Medicine, medicine.disease, Islet, Cathepsins, Protease inhibitor (biology), Tumor Burden, Pancreatic Neoplasms, Papain, Disease Models, Animal, chemistry, Drug Design, Immunology, Cancer research, medicine.drug

Abstract

Proteolytic activity is required for several key processes in cancer development and progression, including tumor growth, invasion and metastasis. Accordingly, high levels of protease expression and activity have been found to correlate with malignant progression and poor patient prognosis in a wide variety of human cancers. Members of the papain family of cysteine cathepsins are among the protease classes that have been functionally implicated in cancer. Therefore, the discovery of effective cathepsin inhibitors has considerable potential for anti-cancer therapy. In this study we describe the identification of a novel, reversible cathepsin inhibitor, VBY-825, which has high potency against cathepsins B, L, S and V. VBY-825 was tested in a pre-clinical model of pancreatic islet cancer and found to significantly decrease tumor burden and tumor number. Thus, the identification of VBY-825 as a new and effective anti-tumor drug encourages the therapeutic application of cathepsin inhibitors in cancer.

Published

2010

18. Abstract IA18: A brain metastasis-promoting role for cathepsin S identified from analysis of tumor- and stroma-supplied proteolytic networks

Author

Priscilla K. Brastianos, Daniela F. Quail, Leslie J. Holsinger, Robert L. Bowman, Franck Rapaport, Edi Brogi, Joan Massagué, Lisa Sevenich, William C. Hahn, Johanna A. Joyce, Benelita T. Elie, Steven D. Mason, and Christina S. Leslie

Subjects

Cathepsin, Cancer Research, Tumor microenvironment, Pathology, medicine.medical_specialty, Stromal cell, Cancer, Biology, medicine.disease, Primary tumor, Metastasis, Oncology, Cancer cell, Cancer research, medicine, Cathepsin S

Abstract

Cancer cells in an aggressive primary tumor are adept at exploiting their local tissue microenvironment. In contrast, when metastatic cells leave these favorable surroundings, they must possess or acquire traits that will allow them to survive and colonize foreign, potentially hostile tissue environments. The obstacles that metastasizing tumor cells encounter vary from organ to organ, and are highly influenced by non-cancerous stromal cells of the tumor microenvironment. For example, the blood-brain barrier, composed of endothelial cells, astrocytes and pericytes, presents a far more formidable structure for tumor cells to penetrate, compared to the fenestrated capillaries in the bone marrow. While the primary tumor microenvironment has emerged as an important regulator of cancer progression, it is less well understood how different tissue environments influence metastatic processes. We used a dual species-specific microarray platform to uncover tumor-stroma interactions that modulate organ tropism of brain, bone and lung metastasis in animal models of cancer. Among the differentially regulated tumor- and stroma-specific genes, we identified cathepsin S as a novel regulator of breast-to-brain metastasis. In breast cancer patients, high cathepsin S expression at the primary site correlated with decreased brain metastasis-free survival. Both macrophages and tumor cells produce cathepsin S, and only the combined depletion significantly reduced brain metastasis in experimental models in vivo. We show that cathepsin S specifically mediates blood-brain barrier transmigration via proteolytic processing of the junctional adhesion molecule (JAM)-B. Pharmacological inhibition of cathepsin S significantly reduced experimental brain metastasis, supporting its consideration as a therapeutic target for this disease. Citation Format: Lisa Sevenich, Robert Bowman, Steve Mason, Daniela Quail, Franck Rapaport, Benelita Elie, Edi Brogi, Priscilla Brastianos, William Hahn, Leslie Holsinger, Joan Massagué, Christina Leslie, Johanna A. Joyce. A brain metastasis-promoting role for cathepsin S identified from analysis of tumor- and stroma-supplied proteolytic networks. [abstract]. In: Abstracts: AACR Special Conference on Cellular Heterogeneity in the Tumor Microenvironment; 2014 Feb 26-Mar 1; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2015;75(1 Suppl):Abstract nr IA18. doi:10.1158/1538-7445.CHTME14-IA18

Published

2015

19. Abstract 549: Sensitization to chemotherapy by inhibition of cathepsin proteases in a mouse model of metastatic breast cancer

Author

Kenisha Simpson, Katherine M. Bell-McGuinn, Edi Brogi, Johanna A. Joyce, Tanaya Shree, Emily C. Zabor, Benelita T. Elie, Alfred L. Garfall, and Oakley C. Olson

Subjects

Cathepsin, Cancer Research, Mammary tumor, Tumor microenvironment, Angiogenesis, business.industry, Cancer, medicine.disease, Metastatic breast cancer, Metastasis, Oncology, Tumor progression, Immunology, Cancer research, medicine, business

Abstract

A growing body of evidence supports the role of the tumor microenvironment in promoting malignant progression and modulating the response to anti-cancer therapy. Tumor associated macrophages (TAMs) have been established as an important component of the tumor microenvironment, contributing to angiogenesis, matrix remodeling, invasion and metastasis. We and others have identified cysteine cathepsin proteases as key effectors of these pro-tumorigenic functions of TAMs. These same processes, which are integral to tumor progression, may also aid tumors in recovering from cytotoxic insults, thereby blunting our therapeutic efforts. There is thus a strong rationale for combinatorial targeting of both the tumor and the supporting stroma. We have uncovered such a phenomenon in a mouse model of metastatic mammary carcinogenesis (MMTV-PyMT). Following maximum tolerated dose paclitaxel treatment (TaxMTD), we observed an elevation in levels of circulating cathepsin-activity+ myeloid cells and a subsequent increase in macrophages and cathepsin activity levels in the tumor. In co-cultures, cathepsin-activity+ macrophages reduced paclitaxel-induced tumor cell death. Furthermore, the use of primary macrophages from various cathepsin null genetic backgrounds identified cathepsins B and S as mediators of this effect. To determine whether cathepsin inhibition could therefore enhance the effects of chemotherapy, we treated MMTV-PyMT mice with both TaxMTD and a pan-cathepsin inhibitor, JPM. While JPM alone had no effect on mammary tumor burden, it significantly impaired tumor growth when combined with TaxMTD, demonstrating that the TaxMTD-induced elevation in tumor cathepsin activity is functionally relevant. To further our goal of simultaneous targeting of tumor and stroma, we added a low-dose cyclophosphamide regimen, which has been shown to have both anti-angiogenic and immune-stimulatory properties. This triple combination treatment was substantially more effective than any double or single drug combination. Importantly, metastatic burden was also significantly reduced in triple-treated mice as compared to controls, and long-term survival was improved. These studies suggest cathepsin+ macrophages are recruited to the tumor after TaxMTD treatment to promote tumor survival and recovery. The efficacy of combining cathepsin inhibition with paclitaxel highlights both the importance of integrated therapeutic targeting of tumor and stroma, as well as the role of TAMs in modulating resistance to chemotherapy. The addition of cysteine cathepsin inhibition to chemotherapeutic regimens thus holds considerable promise for clinical translation. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 102nd Annual Meeting of the American Association for Cancer Research; 2011 Apr 2-6; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2011;71(8 Suppl):Abstract nr 549. doi:10.1158/1538-7445.AM2011-549

Published

2011