Your search keyword '"Netropsin"' showing total 24 results

1. Disruption of nucleosomes by DNA groove binders of clinical significance and implications for chromatin remodeling.

Author

Lorch, Yahli, Kornberg, Roger D., and Maier-Davis, Barbara

Subjects

DNA, CHROMATIN, ANTINEOPLASTIC antibiotics, SMALL molecules, ANTINEOPLASTIC agents

Abstract

Small molecules that bind in the minor groove of DNA are in clinical use as antibiotics and antitumor drugs. Two members of this class of molecules, netropsin and chromomycin, are shown here to displace DNA from the nucleosome and promote transfer of the histone octamer to an acceptor protein. The effects of these groove-binding molecules are exploited to address an outstanding problem in the mechanism of the RSC chromatin remodeling complex. RSC and other remodeling complexes are DNA translocases, acting near the center of the nucleosomal DNA, but translocation is apparently impossible because DNA cannot slide across the histone surface in the nucleosome. Netropsin and chromomycin promote the release of DNA from the histone surface, enhance the formation of a RSC-nucleosome complex, and synergize with RSC in chromatin remodeling. These findings are in keeping with an involvement of bulge translocation in chromatin remodeling. [ABSTRACT FROM AUTHOR]

Published

2023

2. Oncogenic role of HMGA2 in fusion-negative rhabdomyosarcoma cells.

Author

Ouchi, Kazutaka, Miyachi, Mitsuru, Yagyu, Shigeki, Kikuchi, Ken, Kuwahara, Yasumichi, Tsuchiya, Kunihiko, Iehara, Tomoko, and Hosoi, Hajime

Subjects

SARCOMA, GENE fusion, CELL growth, CELL cycle, CELLS

Abstract

Background: Rhabdomyosarcoma (RMS) is the most common pediatric soft tissue sarcoma. There are two subtypes, fusion gene-positive RMS (FP-RMS) and fusion gene-negative RMS (FN-RMS), depending on the presence of a fusion gene, either PAX3-FOXO1 or PAX7-FOXO1. These fusion genes are thought to be oncogenic drivers of FP-RMS. By contrast, the underlying mechanism of FN-RMS has not been thoroughly investigated. It has recently been shown that HMGA2 is specifically positive in pathological tissue from FN-RMS, but the role of HMGA2 in FN-RMS remains to be clarified. Methods: In this study, we used FN-RMS cell lines to investigate the function of HMGA2. Gene expression, cell growth, cell cycle, myogenic differentiation, tumor formation in vivo, and cell viability under drug treatment were assessed. Results: We found that HMGA2 was highly expressed in FN-RMS cells compared with FP-RMS cells and that knockdown of HMGA2 in FN-RMS cells inhibited cell growth and induced G1 phase accumulation in the cell cycle and myogenic differentiation. Additionally, we showed using both gain-of-function and loss-of-function assays that HMGA2 was required for tumor formation in vivo. Consistent with these findings, the HMGA2 inhibitor netropsin inhibited the cell growth of FN-RMS. Conclusions: Our results suggest that HMGA2 has important role in the oncogenicity of FP-RMS and may be a potential therapeutic target in patients with FN-RMS. [ABSTRACT FROM AUTHOR]

Published

2020

3. СПЕКТРОФОТОМЕТРИЧЕСКОЕ ОПРЕДЕЛЕНИЕ ТЕРМОДИ- НАМИЧЕСКИХ ПАРАМЕТРОВ СВЯЗЫВАНИЯ ДОКСОРУБИ- ЦИНА И НЕТРОПСИНА С НУКЛЕИНОВЫМИ КИСЛОТАМИ

Author

АКОПЯН, С. Н., КАЗАРЯН, Р. С., ШАГИНЯН, М. А., САРКИСЯН, С. А., and БАБАЯН, Ю. С.

Abstract

Copyright of Ajastan Kensabanakan Handes is the property of National Academy of Sciences of the Republic of Armenia and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2018

4. Spectroscopic Study of the Binding of Netropsin and Hoechst 33258 to Nucleic Acids.

Author

Vardevanyan, P. O., Parsadanyan, M. A., Antonyan, A. P., and Sahakyan, V. G.

Subjects

NETROPSIN, HOECHST 33258, NUCLEIC acids spectra, POLYAMIDES, DOUBLE-strand DNA breaks

Abstract

The interaction of groove binding compounds — peptide antibiotic (polyamide) netropsin and fluorescent dye (bisbenzimidazole) Hoechst 33258 — with the double-stranded DNA and synthetic double-stranded polynucleotide poly(rA)-poly(rU) has been studied by spectrophotometry. Absorption spectra of these ligand complexes with nucleic acids have been obtained. Spectral changes at the complexation of individual ligands with the mentioned nucleic acids reveal the similarity of binding of each of these ligands with both DNA and RNA. Based on the spectroscopic measurements, the binding parameters of netropsin and Hoechst 33258 binding to DNA and poly(rA)-poly(rU) - K and n, as well as the thermodynamic parameters ΔS, ΔG, and ΔH have been determined. It was found that the binding of Hoechst 33258 to both nucleic acids is accompanied by a positive change in enthalpy, while in the case of netropsin the change in enthalpy is negative. Moreover, the contribution of entropy to the formation of the complexes is more pronounced in the case of Hoechst 33258. [ABSTRACT FROM AUTHOR]

Published

2018

5. Accurate Estimation of the Standard Binding Free Energy of Netropsin with DNA.

Author

Zhang, Hong, Gattuso, Hugo, Dumont, Elise, Cai, Wensheng, Monari, Antonio, Chipot, Christophe, and Dehez, François

Subjects

DNA structure, BASE pairs, DOUBLE helix structure, MOLECULAR dynamics, NETROPSIN

Abstract

DNA is the target of chemical compounds (drugs, pollutants, photosensitizers, etc.), which bind through non-covalent interactions. Depending on their structure and their chemical properties, DNA binders can associate to the minor or to the major groove of double-stranded DNA. They can also intercalate between two adjacent base pairs, or even replace one or two base pairs within the DNA double helix. The subsequent biological effects are strongly dependent on the architecture of the binding motif. Discriminating between the different binding patterns is of paramount importance to predict and rationalize the effect of a given compound on DNA. The structural characterization of DNA complexes remains, however, cumbersome at the experimental level. In this contribution, we employed all-atom molecular dynamics simulations to determine the standard binding free energy of DNA with netropsin, a well-characterized antiviral and antimicrobial drug, which associates to the minor groove of double-stranded DNA. To overcome the sampling limitations of classical molecular dynamics simulations, which cannot capture the large change in configurational entropy that accompanies binding, we resort to a series of potentials of mean force calculations involving a set of geometrical restraints acting on collective variables. [ABSTRACT FROM AUTHOR]

Published

2018

6. EFFECT OF NON-THERMAL MILLIMETER ELECTROMAGNETIC RADIATION ON THERMODYNAMIC PARAMETERS OF THE BINDING OF LIGANDS WITH NUCLEIC ACIDS.

Author

Hakobyan, S. N., Kalantaryan, V. P., and Babayan, Y. S.

Subjects

ELECTROMAGNETIC radiation, THERMODYNAMIC functions, NUCLEIC acid synthesis, LIGANDS (Biochemistry), NUCLEOTIDE analysis

Abstract

Copyright of Ajastan Kensabanakan Handes is the property of National Academy of Sciences of the Republic of Armenia and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2018

7. Interaction of Netropsin with Double-Stranded Nucleic Acids Irradiated with Nonionizing Athermal Millimeter Electromagnetic Waves.

Author

Babayan, Yu. S., Kalantaryan, V. P., Hakobyan, S. H., and Ghazaryan, R. S.

Subjects

NETROPSIN, NUCLEIC acids, ANTINEOPLASTIC agents

Abstract

The binding of antitumor drug netropsin with natural and synthetic double-stranded nucleic acids was investigated. Nucleic acids were irradiated by non-thermal millimeter coherent electromagnetic waves with resonant (64.5 and 50.3 GHz) and nonresonant (48.3 GHz) frequencies of water structures. Studies demonstrate that absorption curves of the complexes and the character of change during titration process are the same for irradiated and non-irradiated DNAs. The results show that binding constant (K) of netropsin with irradiated DNAs changes: almost by one order for B-form DNA (extracted from calf thymus) and is tripled in case of A-form DNA (poly(A)poly(U)). The changes of enthalpy (ΔH) and entropy (ΔS) for binding process were calculated by Van't Hoff analysis from the dependence of K on the temperature. As a result of irradiation with resonant frequencies, increase in absolute values of ΔH and ΔS takes place, while in case of nonresonant irradiation these values practically remain constant. [ABSTRACT FROM AUTHOR]

Published

2016

8. Effect of dimeric netropsin analogue 15Lys-bis-Nt and acyclovir on the reproduction of herpes simplex virus type 1. The search for variants of herpes virus with drug resistance to 15Lys-bis-Nt and acyclovir.

Author

Andronova, V., Grokhovsky, S., Surovaya, A., Gursky, G., and Galegov, G.

Subjects

NETROPSIN, ANTIVIRAL agents, HERPES genitalis treatment, HERPES simplex prevention, ACYCLOVIR, THERAPEUTICS

Abstract

The article presents a study which examines the antiviral activity of dimeric netropsin derivative 15Lys-bis-Nt used in combination with herpes infection treatment drug acyclovir (ACV). The study used a multiciplity of infection (MOI) and demonstration of the international guidelines on ACV as treatment and prevention of recurrences of genital herpes. The study conclude the use of 15Lys-bis-Nt did not yield a drug-resistant with HSV-1 variant.

Published

2015

9. Sequence-Specific DNA Alkylation by Tandem Py-Im Polyamide Conjugates.

Author

Taylor, Rhys Dylan, Kawamoto, Yusuke, Hashiya, Kaori, Bando, Toshikazu, and Sugiyama, Hiroshi

Subjects

DNA alkylation, POLYAMIDES, GEL electrophoresis, DISTAMYCIN, NETROPSIN, HAIRPIN (Genetics), TELOMERES

Abstract

Tandem N-methylpyrrole-N-methylimidazole (Py-Im) polyamides with good sequence-specific DNA-alkylating activities have been designed and synthesized. Three alkylating tandem Py-Im polyamides with different linkers, which each contained the same moiety for the recognition of a 10 bp DNA sequence, were evaluated for their reactivity and selectivity by DNA alkylation, using high-resolution denaturing gel electrophoresis. All three conjugates displayed high reactivities for the target sequence. In particular, polyamide 1, which contained a β lanine linker, displayed the most-selective sequence-specific alkylation towards the target 10 bp DNA sequence. The tandem Py-Im polyamide conjugates displayed greater sequence-specific DNA alkylation than conventional hairpin Py-Im polyamide conjugates (4 and 5). For further research, the design of tandem Py-Im polyamide conjugates could play an important role in targeting specific gene sequences. [ABSTRACT FROM AUTHOR]

Published

2014

10. Semi-Automatic Synthesis, Antiproliferative Activity and DNA-Binding Properties of New Netropsin and bis-Netropsin Analogues.

Author

Szerszenowicz, Jakub and Drozdowska, Danuta

Subjects

COMBINATORIAL chemistry, NETROPSIN, DNA-binding proteins, BREAST cancer, CANCER cells

Abstract

A general route for the semi-automatic synthesis of some new potential minor groove binders was established. Six four-numbered sub-libraries of new netropsin and bis-netropsin analogues have been synthesized using a Syncore Reactor. The structures of the all new substances prepared in this investigation were fully characterized by NMR (¹H, 13C), HPLC and LC-MS. The antiproliferative activity of the obtained compounds was tested on MCF-7 breast cancer cells. The ethidium displacement assay using pBR322 confirmed the DNA-binding properties of the new analogues of netropsin and bis-netropsin. [ABSTRACT FROM AUTHOR]

Published

2014

11. Differential Activation of Diverse Glutathione Transferases of Clonorchis sinensis in Response to the Host Bile and Oxidative Stressors

Author

Bae, Young-An, Ahn, Do-Whan, Lee, Eung-Goo, Kim, Seon-Hee, Cai, Guo-Bin, Kang, Insug, Sohn, Woon-Mok, and Kong, Yoon

Subjects

TRANSFERASES, ENZYMES, OLIGOPEPTIDES, GLUTATHIONE, 3-Deoxy-D-manno-octulosonate 8-phosphate synthase, NETROPSIN

Abstract

Background: Clonorchis sinensis causes chronic cumulative infections in the human hepatobiliary tract and is intimately associated with cholangiocarcinoma. Approximately 35 million people are infected and 600 million people are at risk of infections worldwide. C. sinensis excretory-secretory products (ESP) constitute the first-line effector system affecting the host-parasite interrelationship by interacting with bile fluids and ductal epithelium. However, the secretory behavior of C. sinensis in an environment close to natural host conditions is unclear. C. sinensis differs from Fasciola hepatica in migration to, and maturation in, the hepatic bile duct, implying that protein profile of the ESP of these two trematodes might be different from each other. Methodology/Principal Findings: We conducted systemic approaches to analyze the C. sinensis ESP proteome and the biological reactivity of C. sinensis glutathione transferases (GSTs), such as global expression patterns and induction profiles under oxidative stress and host bile. When we observed ex host excretion behavior of C. sinensis in the presence of 10% host bile, the global proteome pattern was not significantly altered, but the amount of secretory proteins was increased by approximately 3.5-fold. Bioactive molecules secreted by C. sinensis revealed universal/unique features in relation to its intraluminal hydrophobic residing niche. A total of 38 protein spots identified abundantly included enzymes involved in glucose metabolism (11 spots, 28.9%) and diverse-classes of glutathione transferases (GSTs; 10 spots, 26.3%). Cathepsin L/F (four spots, 10.5%) and transporter molecules (three spots, 7.9%) were also recognized. The universal secretory proteins found in other parasites, such as several enzymes involved in glucose metabolism and oxygen transporters, were commonly detected. C. sinensis secreted less cysteine proteases and fatty acid binding proteins compared to other tissue-invading or intravascular trematodes. Interestingly, secretion of a 28 kDa σ-class GST (Cs28σGST3) was significantly affected by the host bile, involving reduced secretion of the 28 kDa species and augmented secretion of Cs28σGST3-related high-molecular-weight 85 kDa protein. Oxidative stressors induced upregulated secretion of 28 kDa Cs28σGST3, but not an 85 kDa species. A secretory 26 kDa μ-class GST (Cs26μGST2) was increased upon treatment with oxidative stressors and bile juice, while another 28 kDa σ-class GST (Cs28σGST1) showed negligible responses. Conclusions/Significance: Our results represent the first analysis of the genuine nature of the C. sinensis ESP proteome in the presence of host bile mimicking the natural host environments. The behavioral patterns of migration and maturation of C. sinensis in the bile ducts might contribute to the secretion of copious amounts of diverse GSTs, but a smaller quantity and fewer kinds of cysteine proteases. The Cs28σGST1 and its paralog(s) detoxify endogenous oxidative molecules, while Cs28σGST3 and Cs26μGST2 conjugate xenobiotics/hydrophobic substances in the extracellular environments, which imply that diverse C. sinensis GSTs might have evolved for each of the multiple specialized functions. [ABSTRACT FROM AUTHOR]

Published

2013

12. Overexpression of HMGA1 deregulates tumor growth via cdc25A and alters migration/invasion through a cdc25A-independent pathway in medulloblastoma.

Author

Lau, Kin-Mang, Chan, Queeny, Pang, Jesse, Ma, Fanny, Li, Kay, Yeung, Walter, Cheng, Alfred, Feng, Hai, Chung, Nellie, Li, Hiu-Ming, Zhou, Liangfu, Wang, Yin, Mao, Ying, and Ng, Ho-Keung

Subjects

HIGH mobility group proteins, TUMOR growth, MEDULLOBLASTOMA, CEREBELLAR tumors, APOPTOSIS, NETROPSIN, DIAGNOSIS, PHYSIOLOGY

Abstract

Overexpression of high mobility group AT-hook 1 (HMGA1) is common in human cancers. Little is known about the mechanisms underlying its deregulation and downstream targets, and information about its clinical and biological significance in medulloblastoma (MB) is lacking. Here, we demonstrated frequent genomic gain at 6p21.33-6p21.31 with copy number increase leading to overexpression of HMGA1 in MB. The overexpression correlated with a high proliferation index and poor prognosis. Moreover, we found that hsa-miR-124a targeted 3′UTR of HMGA1 and negatively modulated the expression in MB cells, indicating that loss/downregulation of hsa-miR-124a reported in our previous study could contribute to the overexpression. Regarding the biological significance of HMGA1, siRNA knockdown and ectopic expression studies revealed the crucial roles of HMGA1 in controlling MB cell growth and migration/invasion through modulation of apoptosis and formation of filopodia and stress fibers, respectively. Furthermore, we identified cdc25A as a target of HMGA1 and showed that physical interaction between HMGA1 and the cdc25A promoter is required for transcriptional upregulation. In clinical samples, HMGA1 and cdc25A were concordantly overexpressed. Functionally, cdc25A is involved in the HMGA1-mediated control of MB cell growth. Finally, netropsin, which competes with HMGA1 in DNA binding, reduced the expression of cdc25A by suppression of its promoter activity and inhibited in vitro and in vivo intracranial MB cell growth. In conclusion, our results delineate the mechanisms underlying the deregulation and reveal the functional significance of HMGA1 in controlling MB cell growth and migration/invasion. Importantly, the results highlight the therapeutic potential of targeting HMGA1 in MB patients. [ABSTRACT FROM AUTHOR]

Published

2012

13. Assessment of enveloping distribution sampling to calculate relative free enthalpies of binding for eight netropsin-DNA duplex complexes in aqueous solution.

Author

Hansen, Niels, Dolenc, Jožica, Knecht, Matthias, Riniker, Sereina, and van Gunsteren, Wilfred F.

Subjects

GIBBS' free energy, NETROPSIN, AQUEOUS solutions, ESTIMATION theory, DNA-binding proteins, THERMODYNAMICS

Abstract

The performance of enveloping distribution sampling (EDS) simulations to estimate free enthalpy differences associated with seven alchemical transformations of A-T into G-C base pairs at the netropsin binding site in the minor groove of a 13-base pair DNA duplex in aqueous solution is evaluated. It is demonstrated that sufficient sampling can be achieved with a two-state EDS Hamiltonian even for large perturbations such as the simultaneous transformation of up to three A-T into three G-C base pairs. The two parameters required to define the EDS reference state Hamiltonian are obtained automatically using a modified version of a scheme presented in earlier work. The sensitivity of the configurational sampling to a variation of these parameters is investigated in detail. Although for relatively small perturbations, that is, one base pair, the free enthalpy estimate depends only weakly on the EDS parameters, the sensitivity is stronger for the largest perturbation. Yet, EDS offers various convenient measures to evaluate the degree of sampling and thus the reliability of the free enthalpy estimate and appears to be an efficient alternative to the conventional thermodynamic integration methodology to obtain free energy differences for molecular systems. © 2012 Wiley Periodicals, Inc. J Comput Chem, 2012 [ABSTRACT FROM AUTHOR]

Published

2012

14. Atomic force microscopy study of DNA conformation in the presence of drugs.

Author

Cassina, Valeria, Seruggia, Davide, Beretta, Giovanni, Salerno, Domenico, Brogioli, Doriano, Manzini, Stefano, Zunino, Franco, and Mantegazza, Francesco

Subjects

ATOMIC force microscopy, DNA, CONFORMATIONAL analysis, DRUG-DNA interactions, ILEX vomitoria, DOXORUBICIN, LIGANDS (Chemistry)

Abstract

Binding of ligands to DNA gives rise to several relevant biological and biomedical effects. Here, through the use of atomic force microscopy (AFM), we studied the consequences of drug binding on the morphology of single DNA molecules. In particular, we quantitatively analyzed the effects of three different DNA-binding molecules (doxorubicin, ethidium bromide, and netropsin) that exert various pharmacologic and therapeutic effects. The results of this study show the consequences of intercalation and groove molecular binding on DNA conformation. These single-molecule measurements demonstrate morphological features that reflect the specific modes of drug-DNA interaction. This experimental approach may have implications in the design of therapeutically effective agents. [ABSTRACT FROM AUTHOR]

Published

2011

15. Carbocyclic potential DNA minor groove binders and their biological evaluation.

Author

Drozdowska, Danuta, Bruzgo, Irena, and Midura-Nowaczek, Krystyna

Subjects

CARBOCYCLIC acids, BINDING agents, ANTINEOPLASTIC agents, BREAST cancer, BACTERIOPHAGE T4, CANCER cells

Abstract

The biological evaluation of carbocyclic minor groove binders 1–6 is described. The cytotoxicity of the obtained compounds was tested on MDA-MB-231 breast cancer cells. The mechanism of action of compounds 1–6 was studied employing the topoisomerase I/II inhibition assay and ethidium displacement assay using pBR322. Determination of association constants was done using calf thymus DNA, T4 coliphage DNA, poly(dA-dT)2, and poly(dG-dC)2. The effect of compounds 1–6 on the amidolytic activity of plasmin, trypsin, thrombin, and urokinase was also examined. [ABSTRACT FROM AUTHOR]

Published

2010

16. Netropsin binding in five duplex-dimer DNA constructs as a function of size and distance between binding sites: circular dichroism and absorption spectroscopy.

Author

Premvardhan, Lavanya and Maurizot, Jean-Claude

Subjects

DRUG-DNA interactions, DNA-ligand interactions, DICHROISM, ELECTROSTATICS, BIOPHYSICS

Abstract

The optical activity induced on binding the drug netrospin (NET) in the minor groove of DNA is studied in five oligonucleotides (OGNs) as a function of (1) the size of the binding site in (5′-(GC)2AATT(GC)2-3′)2 (OGN 1a) versus (5′-(GC)2AAATTT(GC)2-3′)2 (OGN 1b) and (2) the distance between two AATT binding sites in (5′-(GC)2AATT(GC) xAATT(GC)2-3′)2, with x = 1, 2, or 3 (OGNs 2a, b, c, respectively). NET binding is monitored via the induced circular dichroism (CD) at ~315 nm, where the nucleic acids are optically inactive. The CD titrations, fit to a tight binding model, yield lower limits for the binding constant, Ka, ≥8 × 107 M−1 for OGN 1a and ≥2 × 108 M−1 for OGNs 2a, b, c in 1 mM buffer. In 100 mM buffer, tight binding occurs in all five OGNs with Ka ≥ 8 × 107 M−1 for OGN 1a and ≥1 × 108 M−1 for OGNs 1b and 2a, b, c. In contrast, the elongated AAATTT binding site of OGN 1b results in weak binding of NET in 1 mM buffer, where competing electrostatic interactions with the solvent environment are lower. In the constructs with two binding sites, the increase in flexibility introduced by intervening GC base pairs does not induce co-operative binding, although differences in the number of binding sites, n (2.05–2.65), indicate that there may be differences in the way NET is bound in OGNs 2a, b, c. In addition, the large shifts in the absorption spectra induced in bound versus free NET, and effects on the CD spectral bands at higher energy, are discussed in terms of electrostatic and excitonic interactions. [ABSTRACT FROM AUTHOR]

Published

2010

17. Netropsin interactions in the minor groove of d(GGCCAATTGG) studied by a combination of resolution enhancement and ab initio calculations.

Author

Van Hecke, Kristof, Pham Cam Nam, Minh Tho Nguyen, and Van Meervelt, Luc

Subjects

DRUGS, HYDROGEN bonding, AMIDES, NITROGEN, QUANTUM chemistry, PHYSICAL & theoretical chemistry

Abstract

The structure of the complex between the minor groove binder netropsin and d(GGCCAATTGG) was determined via single-crystal X-ray techniques. The structure was refined to completion using refmac5.1.24, resulting in a residual R-factor of 20.0% (including 68 water molecules). Using crystal engineering and cryocooling techniques, the resolution could be enhanced to 1.75 Å, resulting in an unambiguous determination of the drug conformation and orientation. As previously noticed, bifurcated hydrogen bonds are formed between the amide nitrogen atoms of the drug and the N3 and O2 atoms of A and T base pairs, respectively, clearly cataloging the structure to class I. As the bulky NH2 group on guanine was believed to prevent binding of the drug in the minor groove, the detailed nature of several of the amidinium and guanidinium end contacts were further investigated by ab initio quantum chemical methods. [ABSTRACT FROM AUTHOR]

Published

2005

18. Quantitative Methods of Analysis of Footprinting Diagrams for the Complexes Formed by a Ligand with a DNA Fragment of Known Sequence.

Author

NECHIPURENKO, YURII D., JOVANOVIĆ, BOŠKO, RIABOKON, VADIM F., and GURSKY, GEORGII V.

Subjects

GENE expression, GENETIC regulation, FOOTPRINTS, DNA, RADIOLIGAND assay

Abstract

The regulation of gene expression is based on the interaction of DNA with different ligands. A model of adsorption was considered that can be applied to the quantitative analysis of footprinting diagrams for the complexes formed by a ligand with a DNA fragment of known structure. This model allows the probabilities of ligand binding to DNA sites with a known sequence to be calculated and the variance of probabilities of ligand binding with a specified binding site to be estimated. The model was used for quantitative analysis of diagrams of DNAse footprinting for the complexes of the dimeric analogue of the antitumor antibiotic netropsin. Experimental and theoretically calculated profiles of distribution of netropsin bound on DNA are in good agreement with one another. [ABSTRACT FROM AUTHOR]

Published

2005

19. DNA Sequence-Specific Ligands: XI.* The Synthesis and Binding to DNA of bis-Netropsins with the C-Ends of Their Netropsin Fragments Tethered by Tetra- or Pentamethylene Linkers.

Author

Grokhovsky, S., Nikolaev, V., Gottikh, B., and Zhuze, A.

Abstract

Bis-Netropsins with the C-ends of their netropsin fragments tethered via tetra- or pentamethylene linkers and with Gly or L-Lys-Gly residues on their N-ends were synthesized. The footprinting technique was used to study the specificity of bis-netropsin binding to the specially constructed DNA fragments containing various clusters of A · T pairs. It was found that the linker length affects the binding of bis-netropsins, with the tetramethylene linker providing better protection than the pentamethylene linker. It was shown that the newly synthesized bis-netropsins bind tighter to the 5"- A4 T4-3" sequence, whereas the bis-netropsin with a linker between the netropsin N-ends binds better to 5"- T4 A4-3" sequences. [ABSTRACT FROM AUTHOR]

Published

2002

20. A novel synthetic DNA minor groove binder, MS-247: antitumor activity and cytotoxic mechanism.

Author

Matsuba, Y., Edatsugi, H., Mita, I., Matsunaga, A., and Nakanishi, O.

Subjects

DNA, ANTINEOPLASTIC agents, DOXORUBICIN, CISPLATIN, PACLITAXEL, CELL-mediated cytotoxicity, LEUKEMIA, CANCER chemotherapy, DNA metabolism, ANIMAL experimentation, CELL physiology, COLON tumors, COMPARATIVE studies, HETEROCYCLIC compounds, RESEARCH methodology, MEDICAL cooperation, MELANOMA, MICE, MOLECULAR structure, RADIATION-sensitizing agents, RESEARCH, EVALUATION research, FLUORESCENT dyes, PHARMACODYNAMICS

Abstract

Purpose: MS-247 is a novel synthetic compound possessing a DNA-binding moiety and a DNA-alkylating residue, chlorambucil. In this study, we evaluated the antitumor activity of MS-247 against murine tumor cell lines and its effects on DNA molecules in both cell-free and cellular systems.Methods: The in vitro cytotoxic activity of MS-247 was evaluated against four murine tumor cell lines, P388, L1210, Colon26 and B16, and its in vivo antitumor activity was also tested in comparison with Adriamycin (ADM), cisplatin (CDDP) and paclitaxel. The ability of MS-247 to associate with the DNA minor groove was assessed by measuring quenching of Hoechst 33342 fluorescence. DNA-DNA interstrand crosslinks (ICL) were detected by an alkaline elution assay for cellular DNA and a band-shift assay using the plasmid pBR322. The effects of MS-247 on macromolecule synthesis (DNA, RNA and proteins) were examined by measuring incorporation of the radiolabeled precursors.Results: MS-247 exhibited in vitro cytotoxicity with IC(50) values ranging 11 to 500 nM, and MS-247 given i.v. showed strong in vivo antitumor activity against i.p.-implanted L1210 leukemia cells and s.c.-implanted Colon26 carcinoma cells, and moderate activity against i.p.-implanted P388 leukemia cells but no apparent activity against s.c.-implanted B16 melanoma cells. MS-247 reversibly displaced Hoechst 33342 bound to DNA within a few minutes, and irreversibly formed ICL within 1-6 h in both the cell-free system and the cellular system. These results suggest that an association of MS-247 with the DNA minor groove occurred more quickly than ICL formation. The inhibition of DNA synthesis was more prominent than the inhibition of RNA and protein synthesis in L1210 cells exposed to MS-247, and a 6-h incubation with MS-247, which formed apparent ICL in the cellular system, strongly inhibited DNA synthesis. This result suggests that impairment of DNA replication preceded the inhibition of RNA and protein synthesis and that ICL formation greatly contributed to the inhibition of macromolecule synthesis.Conclusion: The results of this study suggest that MS-247 exerts its cytotoxic effect through impairment of DNA function by getting into the minor groove of DNA and subsequently forming ICL. MS-247 has potent antitumor activity with a different spectrum from the activity of clinically proven antitumor agents such as paclitaxel, ADM and CDDP against several murine tumor cell lines. This result suggests that MS-247 may be useful for the treatment of human cancers. [ABSTRACT FROM AUTHOR]

Published

2000

21. Examining the Effects of Netropsin on the Curvature of DNA A-Tracts Using Electrophoresis.

Author

Miller, Jillian and Peters, Justin P.

Subjects

MOLECULAR shapes, DNA, ELECTROPHORESIS, CURVATURE, SMALL molecules, ADENINE

Abstract

A-tracts are sequences of repeated adenine bases that, under the proper conditions, are capable of mediating DNA curvature. A-tracts occur naturally in the regulatory regions of many organisms, yet their biological functions are not fully understood. Orienting multiple A-tracts together constructively or destructively in a phase has the potential to create different shapes in the DNA helix axis. One means of detecting these molecular shape differences is from altered DNA mobilities measured using electrophoresis. The small molecule netropsin binds the minor groove of DNA, particularly at AT-rich sequences including A-tracts. Here, we systematically test the hypothesis that netropsin binding eliminates the curvature of A-tracts by measuring the electrophoretic mobilities of seven 98-base pair DNA samples containing different numbers and arrangements of centrally located A-tracts under varying conditions with netropsin. We find that netropsin binding eliminates the mobility difference between the DNA fragments with different A-tract arrangements in a concentration-dependent manner. This work provides evidence for the straightening of A-tracts upon netropsin binding and illustrates an artificial approach to re-sculpt DNA shape. [ABSTRACT FROM AUTHOR]

Published

2021

22. Conditional Cooperativity in DNA Minor-Groove Recognition by Oligopeptides.

Author

Lah, Jurij and Hadži, San

Subjects

DNA sequencing, CARRIER proteins, DNA, PHASE diagrams, OLIGOPEPTIDES

Abstract

The recognition of specific DNA sequences in processes such as transcription is associated with a cooperative binding of proteins. Some transcription regulation mechanisms involve additional proteins that can influence the binding cooperativity by acting as corepressors or coactivators. In a conditional cooperativity mechanism, the same protein can induce binding cooperativity at one concentration and inhibit it at another. Here, we use calorimetric (ITC) and spectroscopic (UV, CD) experiments to show that such conditional cooperativity can also be achieved by the small DNA-directed oligopeptides distamycin and netropsin. Using a global thermodynamic analysis of the observed binding and (un)folding processes, we calculate the phase diagrams for this system, which show that distamycin binding cooperativity is more pronounced at lower temperatures and can be first induced and then reduced by increasing the netropsin or/and Na+ ion concentration. A molecular interpretation of this phenomenon is suggested. [ABSTRACT FROM AUTHOR]

Published

2021

23. Synthesis, Biological Activity, and Molecular Dynamics Study of Novel Series of a Trimethoprim Analogs as Multi-Targeted Compounds: Dihydrofolate Reductase (DHFR) Inhibitors and DNA-Binding Agents.

Author

Wróbel, Agnieszka, Baradyn, Maciej, Ratkiewicz, Artur, Drozdowska, Danuta, and Gómez-Puertas, Paulino

Subjects

TETRAHYDROFOLATE dehydrogenase, MOLECULAR dynamics, TRIMETHOPRIM, BACTERIOPHAGE T4, BINDING agents, DNA synthesis

Abstract

Eighteen previously undescribed trimethoprim (TMP) analogs containing amide bonds (1–18) were synthesized and compared with TMP, methotrexate (MTX), and netropsin (NT). These compounds were designed as potential minor groove binding agents (MGBAs) and inhibitors of human dihydrofolate reductase (hDHFR). The all-new derivatives were obtained via solid phase synthesis using 4-nitrophenyl Wang resin. Data from the ethidium displacement test confirmed their DNA-binding capacity. Compounds 13–14 (49.89% and 43.85%) and 17–18 (41.68% and 42.99%) showed a higher binding affinity to pBR322 plasmid than NT. The possibility of binding in a minor groove as well as determination of association constants were performed using calf thymus DNA, T4 coliphage DNA, poly (dA-dT)2, and poly (dG-dC)2. With the exception of compounds 9 (IC50 = 56.05 µM) and 11 (IC50 = 55.32 µM), all of the compounds showed better inhibitory properties against hDHFR than standard, which confirms that the addition of the amide bond into the TMP structures increases affinity towards hDHFR. Derivatives 2, 6, 13, 14, and 16 were found to be the most potent hDHFR inhibitors. This molecular modelling study shows that they interact strongly with a catalytically important residue Glu-30. [ABSTRACT FROM AUTHOR]

Published

2021

24. Sustained Release of Minor-Groove-Binding Antibiotic Netropsin from Calcium-Coated Groove-Rich DNA Particles.

Author

Jeon, Hyunsu, Nam, Hyangsu, and Lee, Jong Bum

Subjects

DNA, DRUG delivery systems, CHEMICAL systems, NANOPARTICLES, DRUG development

Abstract

Control of the release properties of drugs has been considered a key factor in the development of drug delivery systems (DDSs). However, drug delivery has limitations including cytotoxicity, low loading efficiency, and burst release. To overcome these challenges, nano or micro-particles have been suggested as carrier systems to deliver chemical drugs. Herein, nano-sized DNA particles (DNAp) were manufactured to deliver netropsin, which is known to bind to DNA minor grooves. The rationally designed particles with exposed rich minor grooves were prepared by DNAp synthesis via rolling circle amplification (RCA). DNAp could load large quantities of netropsin in its minor grooves. An analytical method was also developed for the quantification of netropsin binding to DNAp by UV–visible spectrometry. Moreover, controlled release of netropsin was achieved by forming a layer of Ca2+ on the DNAp (CaDNAp). As a proof of concept, the sustained release of netropsin by CaDNAp highlights the potential of the DNAp-based delivery approach. [ABSTRACT FROM AUTHOR]

Published

2019