Your search keyword '"taltobulin"' showing total 19 results

1. Overcoming drug resistance of cancer cells by targeting the FGF1/FGFR1 axis with honokiol or FGF ligand trap.

Author

Szymczyk, Jakub, Sochacka, Martyna, Biadun, Martyna, Sluzalska, Katarzyna Dominika, Witkowska, Danuta, and Zakrzewska, Malgorzata

Subjects

DRUG resistance in cancer cells, DRUG resistance, CARCINOGENESIS, CANCER cells, ANTINEOPLASTIC agents, FIBROBLAST growth factors

Abstract

Background: Chemoresistance of cancer cells, resulting from various mechanisms, is a significant obstacle to the effectiveness of modern cancer therapies. Targeting fibroblast growth factors (FGFs) and their receptors (FGFRs) is becoming crucial, as their high activity significantly contributes to cancer development and progression by driving cell proliferation and activating signaling pathways that enhance drug resistance. Methods: We investigated the potential of honokiol and FGF ligand trap in blocking the FGF1/FGFR1 axis to counteract drug resistance. Using PEAQ-ITC, we verified direct interaction of honokiol with the FGFR1 kinase domain. We then demonstrated the effect of FGF1/FGFR1 inhibition on taltobulin resistance in cells expressing FGFR1. Finally, we generated drug-resistant clones by prolonged exposure of cells with negligible FGFR levels to taltobulin alone, taltobulin and honokiol, or taltobulin and FGF ligand trap. Results: We demonstrated for the first time a direct interaction of honokiol with the FGFR1 kinase domain, resulting in inhibition of downstream signaling pathways. We revealed that both honokiol and FGF ligand trap prevent FGF1- dependent protection against taltobulin in cancer cells expressing FGFR1. In addition, we showed that cells obtained by long-term exposure to taltobulin are resistant to both taltobulin and other microtubule-targeting drugs, and exhibit elevated levels of FGFR1 and cyclin D. We also found that the presence of FGFligand trap prevents the development of long-term resistance to taltobulin. Conclusion: Our results shed light on how blocking the FGF1/FGFR1 axis by honokiol and FGF ligand trap could help develop more effective cancer therapies, potentially preventing the emergence of drug-resistant relapses. [ABSTRACT FROM AUTHOR]

Published

2024

2. FGF1 Protects MCF-7 Cells against Taltobulin through Both the MEKs/ERKs and PI3K/AKT Signaling Pathway.

Author

Szymczyk, Jakub, Czyrek, Aleksandra, Otlewski, Jacek, and Zakrzewska, Malgorzata

Subjects

EXTRACELLULAR signal-regulated kinases, PI3K/AKT pathway, DRUG receptors, CELLULAR signal transduction, EPIDERMAL growth factor receptors, TUBULINS, LYMPHATIC metastasis, CANCER cell growth, ATP-binding cassette transporters

Abstract

Breast cancer is a widespread and complex disease characterized by abnormal signaling pathways that promote tumor growth and progression. Despite significant medical advances and the development of increasingly effective therapies for breast cancer, drug resistance and reduced sensitivity to prior therapies remain persistent challenges. Dysregulation of growth factors such as FGFs and EGF and their receptors is a contributing factor to reduced response to treatment, promoting cell survival and proliferation, metastasis, EMT or increased expression of ABC transporters. Our study demonstrates a protective role for FGF1 in MCF-7 breast cancer cells against taltobulin-induced cytotoxicity, mediated by activation of its receptors and compares its activity to EGF, another growth factor involved in breast cancer development and progression. The mechanisms of action of these two proteins are different: FGF1 exerts its effects through the activation of both ERKs and AKT, whereas EGF acts only through ERKs. FGF1 action in the presence of the drug promotes cell viability, reduces apoptosis and increases cell migration. Although EGF and its receptors have received more attention in breast cancer research to date, our findings highlight the key role played by FGFs and their receptors in promoting drug resistance to tubulin polymerization inhibitors in FGFR-positive tumors. [ABSTRACT FROM AUTHOR]

Published

2023

3. FGF1 protects FGFR1-overexpressing cancer cells against drugs targeting tubulin polymerization by activating AKT via two independent mechanisms.

Author

Szymczyk, Jakub, Sochacka, Martyna, Chudy, Patryk, Opalinski, Lukasz, Otlewski, Jacek, and Zakrzewska, Malgorzata

Subjects

PACLITAXEL, TUBULINS, DRUG resistance in cancer cells, CANCER cells, FIBROBLAST growth factors, CYCLOSPORINE, POLYMERIZATION

Abstract

Cancer drug resistance is a common, unpredictable phenomenon that develops in many types of tumors, resulting in the poor efficacy of current anticancer therapies. One of the most common, and yet the most complex causes of drug resistance is a mechanism related to dysregulation of tumor cell signaling. Abnormal signal transduction in a cancer cell is often stimulated by growth factors and their receptors, including fibroblast growth factors (FGFs) and FGF receptors (FGFRs). Here, we investigated the effect of FGF1 and FGFR1 activity on the action of drugs that disrupt tubulin polymerization (taltobulin, paclitaxel, vincristine) in FGFR1-positive cell lines, U2OS stably transfected with FGFR1 (U2OSR1) and DMS114 cells. We observed that U2OSR1 cells exhibited reduced sensitivity to the tubulin-targeting drugs, compared to U2OS cells expressing a negligible level of FGFRs. This effect was dependent on receptor activation, as inhibition of FGFR1 by a specific small-molecule inhibitor (PD173074) increased the cells’ sensitivity to these drugs. Expression of functional FGFR1 in U2OS cells resulted in increased AKT phosphorylation, with no change in total AKT level. U2OSR1 cells also exhibited an elevated MDR1 and blocking MDR1 activity with cyclosporin A increased the toxicity of paclitaxel and vincristine, but not taltobulin. Analysis of tubulin polymerization pattern using fluorescence microscopy revealed that FGF1 in U2OSR1 cells partially reverses the drug-altered phenotype in paclitaxel- and vincrist-inetreated cells, but not in taltobulin-treated cells. Furthermore, we showed that FGF1, through activation of FGFR1, reduces caspase 3/7 activity and PARP cleavage, preventing apoptosis induced by tubulin-targeting drugs. Next, using specific kinase inhibitors, we investigated which signaling pathways are responsible for the FGF1-mediated reduction of taltobulin cytotoxicity. We found that AKT kinase is a key factor in FGF1-induced cell protection against taltobulin in U2OSR1 and DMS114 cells. Interestingly, only direct inhibition of AKT or dual-inhibition of PI3K and mTOR abolished this effect for cells treated with taltobulin. This suggests that both canonical (PI3K-dependent) and alternative (PI3K-independent) AKT-activating pathways may regulate FGF1/ FGFR1-driven cancer cell survival. Our findings may contribute to the development of more effective therapies and may facilitate the prevention of drug resistance in FGFR1-positive cancer cells. [ABSTRACT FROM AUTHOR]

Published

2022

4. FGF1 protects FGFR1-overexpressing cancer cells against drugs targeting tubulin polymerization by activating AKT via two independent mechanisms

Author

Jakub Szymczyk, Martyna Sochacka, Patryk Chudy, Lukasz Opalinski, Jacek Otlewski, and Malgorzata Zakrzewska

Subjects

cancer, FGF1, FGFR1, drug resistance, anticancer drugs, taltobulin, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Cancer drug resistance is a common, unpredictable phenomenon that develops in many types of tumors, resulting in the poor efficacy of current anticancer therapies. One of the most common, and yet the most complex causes of drug resistance is a mechanism related to dysregulation of tumor cell signaling. Abnormal signal transduction in a cancer cell is often stimulated by growth factors and their receptors, including fibroblast growth factors (FGFs) and FGF receptors (FGFRs). Here, we investigated the effect of FGF1 and FGFR1 activity on the action of drugs that disrupt tubulin polymerization (taltobulin, paclitaxel, vincristine) in FGFR1-positive cell lines, U2OS stably transfected with FGFR1 (U2OSR1) and DMS114 cells. We observed that U2OSR1 cells exhibited reduced sensitivity to the tubulin-targeting drugs, compared to U2OS cells expressing a negligible level of FGFRs. This effect was dependent on receptor activation, as inhibition of FGFR1 by a specific small-molecule inhibitor (PD173074) increased the cells’ sensitivity to these drugs. Expression of functional FGFR1 in U2OS cells resulted in increased AKT phosphorylation, with no change in total AKT level. U2OSR1 cells also exhibited an elevated MDR1 and blocking MDR1 activity with cyclosporin A increased the toxicity of paclitaxel and vincristine, but not taltobulin. Analysis of tubulin polymerization pattern using fluorescence microscopy revealed that FGF1 in U2OSR1 cells partially reverses the drug-altered phenotype in paclitaxel- and vincristine-treated cells, but not in taltobulin-treated cells. Furthermore, we showed that FGF1, through activation of FGFR1, reduces caspase 3/7 activity and PARP cleavage, preventing apoptosis induced by tubulin-targeting drugs. Next, using specific kinase inhibitors, we investigated which signaling pathways are responsible for the FGF1-mediated reduction of taltobulin cytotoxicity. We found that AKT kinase is a key factor in FGF1-induced cell protection against taltobulin in U2OSR1 and DMS114 cells. Interestingly, only direct inhibition of AKT or dual-inhibition of PI3K and mTOR abolished this effect for cells treated with taltobulin. This suggests that both canonical (PI3K-dependent) and alternative (PI3K-independent) AKT-activating pathways may regulate FGF1/FGFR1-driven cancer cell survival. Our findings may contribute to the development of more effective therapies and may facilitate the prevention of drug resistance in FGFR1-positive cancer cells.

Published

2022

5. FGF1 Protects MCF-7 Cells against Taltobulin through Both the MEKs/ERKs and PI3K/AKT Signaling Pathway

Author

Jakub Szymczyk, Aleksandra Czyrek, Jacek Otlewski, and Malgorzata Zakrzewska

Subjects

breast cancer, FGF1, EGF, drug resistance, taltobulin, ERKs, Biology (General), QH301-705.5

Abstract

Breast cancer is a widespread and complex disease characterized by abnormal signaling pathways that promote tumor growth and progression. Despite significant medical advances and the development of increasingly effective therapies for breast cancer, drug resistance and reduced sensitivity to prior therapies remain persistent challenges. Dysregulation of growth factors such as FGFs and EGF and their receptors is a contributing factor to reduced response to treatment, promoting cell survival and proliferation, metastasis, EMT or increased expression of ABC transporters. Our study demonstrates a protective role for FGF1 in MCF-7 breast cancer cells against taltobulin-induced cytotoxicity, mediated by activation of its receptors and compares its activity to EGF, another growth factor involved in breast cancer development and progression. The mechanisms of action of these two proteins are different: FGF1 exerts its effects through the activation of both ERKs and AKT, whereas EGF acts only through ERKs. FGF1 action in the presence of the drug promotes cell viability, reduces apoptosis and increases cell migration. Although EGF and its receptors have received more attention in breast cancer research to date, our findings highlight the key role played by FGFs and their receptors in promoting drug resistance to tubulin polymerization inhibitors in FGFR-positive tumors.

Published

2023

6. Conceptual DFT as a chemoinformatics tool for the study of the Taltobulin anticancer peptide

Author

Norma Flores-Holguín, Juan Frau, and Daniel Glossman-Mitnik

Subjects

Taltobulin, Conceptual DFT, Bioactivity scores, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390

Abstract

Abstract Objective A well-behaved model chemistry previously validated for the study of the chemical reactivity of peptides was considered for the calculation of the molecular properties and structure of the Taltobulin anticancer peptide. A methodology based on Conceptual Density Functional Theory (CDFT) was chosen for the determination of the reactivity descriptors. Results The molecular active sites were associated with the active regions of the molecule were associated with the nucleophilic and electrophilic Fukui functions. Finally, the bioactivity scores for the Taltobulin peptide are predicted through a homology methodology relating them with the calculated reactivity descriptors.

Published

2019

7. Expeditious Total Synthesis of Hemiasterlin through a Convergent Multicomponent Strategy and Its Use in Targeted Cancer Therapeutics

Author

Jason S. Carroll, David R. Spring, Stephen J. Walsh, Jiraborrirak Charoenpattarapreeda, Charoenpattarapreeda, Jiraborrirak [0000-0002-0316-9608], Walsh, Stephen J [0000-0002-3164-1519], Carroll, Jason S [0000-0003-3643-0080], Spring, David R [0000-0001-7355-2824], and Apollo - University of Cambridge Repository

Subjects

Cell Survival, Receptor, ErbB-2, Taltobulin, Molecular Conformation, antibody-drug conjugates, Antineoplastic Agents, 010402 general chemistry, 01 natural sciences, Hemiasterlin, Catalysis, chemistry.chemical_compound, Rare Diseases, Cell Line, Tumor, Breast Cancer, medicine, Humans, Cytotoxicity, 5 Development of treatments and therapeutic interventions, total synthesis, targeted therapeutics, Cancer, Cell Proliferation, hemiasterlin, Natural product, 34 Chemical Sciences, 010405 organic chemistry, Chemistry, Antibody–Drug Conjugates, multicomponent reactions, Communication, Total synthesis, 3405 Organic Chemistry, General Chemistry, General Medicine, medicine.disease, Combinatorial chemistry, Communications, 0104 chemical sciences, Orphan Drug, 5.1 Pharmaceuticals, Cancer cell, Ugi reaction, Generic health relevance, Drug Screening Assays, Antitumor, Oligopeptides, Biotechnology

Abstract

Hemiasterlin is an antimitotic marine natural product with reported sub‐nanomolar potency against several cancer cell lines. Herein, we describe an expeditious total synthesis of hemiasterlin featuring a four‐component Ugi reaction (Ugi‐4CR) as the key step. The convergent synthetic strategy enabled rapid access to taltobulin (HTI‐286), a similarly potent synthetic analogue. This short synthetic sequence enabled investigation of both hemiasterlin and taltobulin as cytotoxic payloads in antibody–drug conjugates (ADCs). These novel ADCs displayed sub‐nanomolar cytotoxicity against HER2‐expressing cancer cells, while showing no activity against antigen‐negative cells. This study demonstrates an improved synthetic route to a highly valuable natural product, facilitating further investigation of hemiasterlin and its analogues as potential payloads in targeted therapeutics., Hemiasterlin, a highly cytotoxic marine natural product (see structure), was synthesised by a multicomponent approach with a longest linear sequence of 10 steps. Its use in a targeted therapeutic was demonstrated by incorporation as a payload in an antibody–drug conjugate (ADC), which showed mid‐picomolar cytotoxicity against HER2‐expressing cancer cell lines.

Published

2020

8. Versatile synthesis of new cytotoxic agents structurally related to hemiasterlins

Author

Simoni, Daniele, Lee, Ray M., Durrant, David E., Chi, Nai-Wen, Baruchello, Riccardo, Rondanin, Riccardo, Rullo, Cinzia, and Marchetti, Paolo

Subjects

*ANTINEOPLASTIC agents, *ANTIMITOTIC agents, *ORGANIC synthesis, *STEREOCHEMISTRY, *DRUG derivatives, *CELL lines, *POLYMERIZATION, *NUCLEOPHILIC reactions, *DRUG development

Abstract

Abstract: A representative series of structural analogues of the antimitotic tripeptides hemiasterlins have been synthesized. The key-step of this synthetic strategy consists of an Ag2O-promoted nucleophilic substitution on a common precursor, a chiral non-racemic 2-bromoacyl derivative. Simple variation of nucleophile substituents allows a rapid and stereocontrolled development of new series of derivatives. Some reported compounds showed potent biological activity as growth inhibitors of cancer cell lines and tubulin polymerization inhibitors. [Copyright &y& Elsevier]

Published

2010

9. Mapping the bound conformation and protein interactions of microtubule destabilizing peptides by STD–NMR spectroscopy

Author

Milton, Mark J., Thomas Williamson, R., and Koehn, Frank E.

Subjects

*TUBULINS, *NUCLEAR magnetic resonance spectroscopy, *SPECTRUM analysis, *ORGANIC compounds

Abstract

Abstract: Using the hemiasterlin analogs taltobulin (I, HTI-286), II, and III as model compounds, we demonstrate that relaxation-compensated STD–NMR can be used as an effective tool to efficiently provide a qualitative epitope map for microtubule destabilizing peptides. Due to the disparate relaxation behavior of the protons in these model compounds, it was essential to collect STD with very short saturation times to render an accurate picture of the binding interaction. The conformation of HTI-286 (I) in complex with the protein was determined from TRNOESY/ROESY experiments and is similar to the X-ray crystal structure conformation observed for hemiasterlin methyl ester in the absence of protein. [Copyright &y& Elsevier]

Published

2006

10. Structural Insights into the Pharmacophore of Vinca Domain Inhibitors of Microtubules

Author

Yangping Wu, Frederick W. Benz, Xiangzheng Chen, Yunfeng Chen, Huiyan Li, Qisheng Wang, Yonghui Zhang, Jinliang Yang, Rundong Zhang, and Yuxi Wang

Subjects

0301 basic medicine, Vinca, Swine, Stereochemistry, Molecular Conformation, Taltobulin, Microtubules, Protein Structure, Secondary, 03 medical and health sciences, Protein structure, X-Ray Diffraction, Microtubule, Animals, Pharmacology, biology, Chemistry, Tubulin Modulators, Rational design, biology.organism_classification, Protein Structure, Tertiary, 030104 developmental biology, Tubulin, biology.protein, Molecular Medicine, Pharmacophore, Protein Binding

Abstract

Antibody-drug conjugates (ADCs) have achieved great success in cancer therapy in recent years. Some peptidyl microtubule inhibitors consisting of natural and unnatural amino acids, such as monomethyl auristatin E (MMAE) and F (MMAF), are extremely cytotoxic and have been used as a payload in ADCs. However, their precise molecular interaction with tubulin and microtubules remains unclear. We determined the crystal structures of tubulin in complex with three ultra-potent peptidyl microtubule inhibitors [MMAE, taltobulin (HTI- 286), and tubulysin M] at 2.5 Å. Our data showed that the three peptides bound to the vinca domain and shared a common and key pharmacophore containing two consecutive hydrophobic groups (Val, Ile-like side chain). These groups protruded in opposite directions into hydrophobic pockets on the tubulin β and α subunits. Nitrogen and oxygen atoms from the same backbone formed hydrogen bonds with Asn329 from the α subunit and Asp179 from the β subunit in a direction normal to the surface formed by the aforementioned hydrophobic groups. In addition, our crystal structure data indicated that tubulysin M bound to the β subunit alone, providing a structural explanation for its higher affinity. We also compared the conformations of two representative structurally different vinca domain compounds, ustiloxin D and vinblastine, with those of the aforementioned peptidyl ligands, and found that they shared a similar pharmacophore. Our findings lay a foundation for the rational design of novel vinca domain ligands and may facilitate the development of microtubule inhibitors with high specificity, affinity, and efficiency as payloads for ADCs in cancer therapy.

Published

2015

11. Absolute configurations of tubulin inhibitors taltobulin (HTI-286) and HTI-042 characterized by X-ray diffraction analysis and NMR studies

Author

Chuansheng, Niu, Douglas M, Ho, Robert Thomas, Williamson, Arie, Zask, and Semiramis, Ayral-Kaloustian

Subjects

Diffraction, Magnetic Resonance Spectroscopy, Chemistry, Organic Chemistry, Clinical Biochemistry, Molecular Conformation, Absolute configuration, Taltobulin, Pharmaceutical Science, Stereoisomerism, Crystallography, X-Ray, Biochemistry, Tubulin Modulators, Structure-Activity Relationship, Crystallography, Tubulin Inhibitors, Tubulin, Drug Discovery, X-ray crystallography, Molecular Medicine, Oligopeptides, Molecular Biology, Single crystal

Abstract

The stereochemistry of the tubulin inhibitors taltobulin HTI-286 (2) and HTI-042 (3) was determined by utilizing the DPFGSE 1D NOE experiment. Single crystal X-ray diffraction analysis further confirmed the absolute configuration of these two compounds, which carry the (S,S,S)-configuration necessary for biological activity.

Published

2010

12. A novel hybrid drug between two potent anti-tubulin agents as a potential prolonged anticancer approach

Author

Carlo Mischiati, Alessandro Dalpiaz, Lih-Ching Hsu, Giordana Feriotto, Barbara Pavan, Ray M. Lee, Riccardo Rondanin, Riccardo Baruchello, Daniele Simoni, Luca Ferraro, and Paolo Marchetti

Subjects

0301 basic medicine, Male, ATP Binding Cassette Transporter, Subfamily B, NCM460 cells, Stereochemistry, Taltobulin, Hybrid drug, Pharmaceutical Science, Socio-culturale, Antineoplastic Agents, Hemiasterlin, Cell Line, 03 medical and health sciences, Hydrolysis, 0302 clinical medicine, Drug Stability, Cell Line, Tumor, Stilbenes, Animals, Humans, Rats, Wistar, Permeation, Stilbene, 3003, chemistry.chemical_classification, biology, Chemistry, Cell growth, Cell Cycle, Tubulin Modulators, Amino acid, 030104 developmental biology, Tubulin, Liver, Solubility, 030220 oncology & carcinogenesis, biology.protein, Efflux, Multidrug Resistance-Associated Proteins, Linker, Oligopeptides, Conjugate

Abstract

We report the design, synthesis and biological characterisation of a novel hybrid drug by conjugation of two tubulin inhibitors, a hemiasterlin derivative A (H-Mpa-Tle-Aha-OH), obtained by condensation of three non-natural amino acids, and cis -3,4′,5-trimethoxy-3′aminostilbene ( B ). As we have previously demonstrated synergy between A and B , we used a monocarbonyl derivative of triethylene glycol as linker ( L ) to synthesise compounds A-L and A-L-B ; via HPLC we analysed the release of its potential hydrolysis products A , A-L , B and B-L in physiological fluids: the hybrid A-L-B undergo hydrolysis in rat whole blood of the ester bond between A and L (half-life = 118.2 ± 9.5 min) but not the carbamate bond between B and L ; the hydrolysis product B-L was further hydrolyzed, but with a slower rate (half-life = 288 ± 12 min). The compound A-L was the faster hydrolyzed conjugate (half-life = 25.4 ± 1.1 min). The inhibitory activity of the compounds against SKOV3 ovarian cancer cell growth was analysed. The IC 50 values were 7.48 ± 1.27 nM for A , 40.3 ± 6.28 nM for B , 738 ± 38.5 nM for A-L and 37.9 ± 2.11 nM for A-L-B . The anticancer effect of A-L-B was evidenced to be obtained via microtubule dynamics suppression. Finally, we stated the expression of the active efflux transporters P-gp (ABCB1) and MRP1 (ABCC1) in the human normal colon epithelial NCM460 cell line by reverse-transcription PCR. Via permeation studies across NCM460 monolayers we demonstrate the poor aptitude of A to interact with active efflux transporters (AET): indeed, the ratio between its permeability coefficients for the basolateral (B) → apical (A) and B → A transport was 1.5 ± 0.1, near to the ratio of taltobulin (1.12 ± 0.06), an hemiasterlin derivative able to elude AETs, and significantly different form the ratio of celiprolol (3.4 ± 0.2), an AET substrate.

Published

2016

13. Conceptual DFT as a chemoinformatics tool for the study of the Taltobulin anticancer peptide.

Author

Flores-Holguín, Norma, Frau, Juan, and Glossman-Mitnik, Daniel

Subjects

DENSITY functional theory, CHEMICAL models, MOLECULAR structure

Abstract

Objective: A well-behaved model chemistry previously validated for the study of the chemical reactivity of peptides was considered for the calculation of the molecular properties and structure of the Taltobulin anticancer peptide. A methodology based on Conceptual Density Functional Theory (CDFT) was chosen for the determination of the reactivity descriptors. Results: The molecular active sites were associated with the active regions of the molecule were associated with the nucleophilic and electrophilic Fukui functions. Finally, the bioactivity scores for the Taltobulin peptide are predicted through a homology methodology relating them with the calculated reactivity descriptors. [ABSTRACT FROM AUTHOR]

Published

2019

14. Hybrids of the Hemiasterlin Analogue Taltobulin and the Dolastatins Are Potent Antimicrotubule Agents

Author

Arie Zask, Joshua Kaplan, Sylvia Musto, and Frank Loganzo

Subjects

Models, Molecular, Vinca, Protein Conformation, Stereochemistry, Taltobulin, Antineoplastic Agents, Tripeptide, Biochemistry, KB Cells, Catalysis, Tubulin binding, Structure-Activity Relationship, Colloid and Surface Chemistry, Microtubule, Cell Line, Tumor, Depsipeptides, Humans, Binding site, biology, Chemistry, Transporter, General Chemistry, biology.organism_classification, Tubulin Modulators, Tubulin, biology.protein, Thermodynamics, Drug Screening Assays, Antitumor, Oligopeptides

Abstract

The targeting of microtubules is an important mechanism for cancer chemotherapy. However, there is still a need for improved antimicrotubule agents. A number of seemingly structurally disparate peptidic natural products inhibit tubulin polymerization by binding to a region of the tubulin heterodimer close to the vinca binding site. An analogue of the naturally occurring tripeptide hemiasterlin, taltobulin (HTI-286, 3), has advanced to clinical trials. Structure-activity relationship studies of 3 have revealed critical structural elements necessary for antimicrotubule activity that correspond to comparable groups in the amino terminus tripeptide region of the dolastatins. To investigate the structural relationship between the hemiasterlins and the more complex dolastatins, hybrid compounds composed of 3 and the carboxy terminus dipeptides of dolastatin 10, or the dolastatin 15 analogue cemadotin, were synthesized. The resulting hybrid compounds were potent antimicrotubule agents, thus establishing a structural relationship between the hemiasterlins and the dolastatins. This relationship may be useful in the design of analogues having improved activity in resistant cell lines expressing the P-glycoprotein transporter, for establishing structural relationships with other classes of peptidic antimicrotubule agents, or for modeling studies of the tubulin binding site of these agents.

Published

2005

15. HTI-286 (Taltobulin), A Synthetic Analog of the Antimitotic Natural Product Hemiasterlin

Author

Gordon M. Cragg, David J. Newman, and David G. I. Kingston

Subjects

chemistry.chemical_compound, Natural product, chemistry, Stereochemistry, Computer science, Taltobulin, Hemiasterlin

Published

2011

16. Versatile Synthesis of New Cytotoxic Agents Structurally Related to Emiasterlins

Author

Ray M. Lee, Riccardo Rondanin, Daniele Simoni, David Durrant, Nai-Wen Chi, Paolo Marchetti, Riccardo Baruchello, and Cinzia Rullo

Subjects

Stereochemistry, Clinical Biochemistry, Taltobulin, Pharmaceutical Science, Antineoplastic Agents, Peptide, Tripeptide, Hemiasterlin, Biochemistry, Chemical synthesis, Anticancer drugs, Ag2O, Nucleophile, Cell Line, Tumor, Drug Discovery, Nucleophilic substitution, Animals, Humans, Cytotoxicity, Molecular Biology, chemistry.chemical_classification, Molecular Structure, Chemistry, Organic Chemistry, Biological activity, Combinatorial chemistry, Rats, Molecular Medicine, Oligopeptides

Abstract

A representative series of structural analogues of the antimitotic tripeptides hemiasterlins have been synthesized. The key-step of this synthetic strategy consists of an Ag2O-promoted nucleophilic substitution on a common precursor, a chiral non-racemic 2-bromoacyl derivative. Simple variation of nucleophile substituents allows a rapid and stereocontrolled development of new series of derivatives. Some reported compounds showed potent biological activity as growth inhibitors of cancer cell lines and tubulin polymerization inhibitors.

Published

2010

17. Inhibition of hepatic tumor cell proliferation in vitro and tumor growth in vivo by taltobulin, a synthetic analogue of the tripeptide hemiasterlin

Author

Claudio A Redaelli, Christoforos Stoupis, Celine Tiffon, and Yogesh K. Vashist

Subjects

Liver Cancer, Carcinoma, Hepatocellular, Taltobulin, Biology, Pharmacology, Microtubules, In vivo, Cell Line, Tumor, Animals, Humans, IC50, Cell Proliferation, Dose-Response Relationship, Drug, Cell growth, Antimicrotubule agent, Cell Cycle, Liver Neoplasms, Gastroenterology, General Medicine, Cell cycle, Xenograft Model Antitumor Assays, In vitro, Tubulin Modulators, Rats, Cell culture, Female, Oligopeptides

Abstract

AIM: To investigate the inhibitory effects of taltobulin (HTI-286), a synthetic analogue of natural hemiasterlin derived from marine sponges, on hepatic tumor growth in vitro and in vivo. METHODS: The potential anti-proliferative effects of HTI-286 on different hepatic tumor cell lines in vitro and in vivo were examined. RESULTS: HTI-286 significantly inhibited proliferation of all three hepatic tumor cell lines (mean IC50 = 2 nmol/L ± 1 nmol/L) in vitro. Interestingly, no decrease in viable primary human hepatocytes (PHH) was detected under HTI-286 exposure. Moreover, intravenous administration of HTI-286 significantly inhibited tumor growth in vivo (rat allograft model). CONCLUSION: HTI-286 might be considered a potent promising drug in treatment of liver malignancies. HTI-286 is currently undergoing clinical evaluation in cancer patients.

Published

2006

18. Mapping the bound conformation and protein interactions of microtubule destabilizing peptides by STD-NMR spectroscopy

Author

Mark J. Milton, Frank E. Koehn, and R. Thomas Williamson

Subjects

Models, Molecular, Magnetic Resonance Spectroscopy, Stereochemistry, Protein Conformation, Chemistry, Pharmaceutical, Clinical Biochemistry, Taltobulin, Molecular Conformation, Pharmaceutical Science, Peptide, Crystallography, X-Ray, Biochemistry, Microtubules, Tubulin binding, Protein–protein interaction, chemistry.chemical_compound, Microtubule, Drug Discovery, Molecular Biology, chemistry.chemical_classification, Dipeptide, biology, Organic Chemistry, Esters, Nuclear magnetic resonance spectroscopy, Tubulin, chemistry, Models, Chemical, Spectrophotometry, Drug Design, biology.protein, Molecular Medicine, Microtubule-Associated Proteins, Protein Binding

Abstract

Using the hemiasterlin analogs taltobulin (I, HTI-286), II, and III as model compounds, we demonstrate that relaxation-compensated STD-NMR can be used as an effective tool to efficiently provide a qualitative epitope map for microtubule destabilizing peptides. Due to the disparate relaxation behavior of the protons in these model compounds, it was essential to collect STD with very short saturation times to render an accurate picture of the binding interaction. The conformation of HTI-286 (I) in complex with the protein was determined from TRNOESY/ROESY experiments and is similar to the X-ray crystal structure conformation observed for hemiasterlin methyl ester in the absence of protein.

Published

2006

19. Corrigendum to 'Absolute configurations of tubulin inhibitors taltobulin (HTI-286) and HTI-042 characterized by X-ray diffraction analysis and NMR studies' [Bioorg. Med. Chem. Lett. 20 (2010) 1535–1538]

Author

Chuansheng Niu, Arie Zask, Semiramis Ayral-Kaloustian, Robert Williamson, and Douglas M. Ho

Subjects

Tubulin Inhibitors, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, X-ray crystallography, Taltobulin, Pharmaceutical Science, Molecular Medicine, Molecular Biology, Biochemistry

Abstract

Corrigendum Corrigendum to ‘‘Absolute configurations of tubulin inhibitors taltobulin (HTI-286) and HTI-042 characterized by X-ray diffraction analysis and NMR studies’’ [Bioorg. Med. Chem. Lett. 20 (2010) 1535–1538] Chuansheng Niu a,⇑, Douglas M. Ho , Robert Thomas Williamson , Arie Zask , Semiramis Ayral-Kaloustian a Wyeth Research, Pearl River, NY 10965, USA Department of Chemistry, Princeton University, Princeton, NJ 08544, USA

Published

2012