Ruthenium(II) Polypyridyl Complexes as Potential Anticancer Drugs

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Book Rating : 4.:/5 (859 download)

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Book Synopsis Ruthenium(II) Polypyridyl Complexes as Potential Anticancer Drugs by : Yanling Chen

Download or read book Ruthenium(II) Polypyridyl Complexes as Potential Anticancer Drugs written by Yanling Chen and published by . This book was released on 2013 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: Research on biological activities of ruthenium polypyridyl complexes (RPCs) continues to attract interest as these complexes have shown promising anticancer activity both in vitro and in vivo.1−3 The mononuclear RPC, [(phen)2Ru(tatpp)]2+ (MP) and related dinuclear complex [(phen)2Ru(tatpp)Ru(phen)2]4+ (P) have been shown to both intercalate with DNA and shown potentiated DNA cleavage under anaerobic and reducing conditions4−5, as well as shown good selectivity and cytotoxicity towards malignant cell lines in vitro and tumors in vivo.5 Both complexes contain the redox-active tatpp ligand which is thought to be an essential component for the observed biological activities. This thesis is focused on developing improvements to the stereoselective syntheses of the chiral complexes, [delta][delta]-P and [delta]-MP. It is also investigated the synthesis of a new analogue [(phen)2Ru(tadbp)]2+ (B) and its chiral form [delta]-B which contains a modified tatpp ligand that is only capable of binding one Ru ion. Moreover this thesis explores the ability of these large complexes to traverse the cell membranes and get into cells and cell nuclei by isolating treated cells and nuclei and determining their ruthenium content by graphite furnace atomic absorption method (GFAAS). The GFAAS data show that the two examined complexes [delta][delta]-P and [delta]-MP are able to quickly penetrate into cancer cells (H-358) and concentrate in nuclei, which is postulated due to their high binding affinity to DNA.

Redox Active Lipophilic Ruthenium Complexes as Potential Anti-cancer Drugs

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Total Pages : 126 pages
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Book Synopsis Redox Active Lipophilic Ruthenium Complexes as Potential Anti-cancer Drugs by : Nagham Alatrash

Download or read book Redox Active Lipophilic Ruthenium Complexes as Potential Anti-cancer Drugs written by Nagham Alatrash and published by . This book was released on 2015 with total page 126 pages. Available in PDF, EPUB and Kindle. Book excerpt: The dinuclear ruthenium(II) polypyridyl complexes (RPCs) [(phen)2Ru(tatpp)Ru(phen)2][PF6]4 (P4+) and the monomeric [(phen)2Ru(tatpp)]Cl2 (MP2+) are promising candidates for anti-cancer drug development in terms of the observed antitumor activity in vivo and in vitro. These complexes contain the redox-active tatpp (9,11,20,22-tetraazatetrapyrido[3,2-a:2'3'-c:3'',2''-1:2''',3''']-pentacene) ligand which seems to be the critical component for biological activity. These complexes cleave DNA when reduced in situ to a radical species. Both complexes exhibit selective cytotoxicity toward cultured malignant cell lines and showed inhibition of tumor growth in vivo. This work expands on this platform by preparing and examining more lipophilic analogues of P4+ and MP2+. Specifically, four lipophilic ruthenium(II) polypyridyl complexes, [(Ph2phen)2Ru(tatpp)Ru(Ph2phen)2][PF6]4 (PPh 4+), (Ph2phen, 4,7-diphenyl-1,10- phenanthroline), [(Me4phen)2Ru(tatpp)Ru(Me4phen)2][PF6]4 (PMe 4+), (Me4phen, 3,4,7,8- tetramethyl-1,10phenanthroline), [(Me4phen)2Ru(tatpp)][PF6]2 (MPMe 2+), and [(Ph2phen)2Ru(tatpp)][PF6]2 (MPPh 2+), have been synthesized and characterized in which 4,7-diphenyl-1,10-phenanthroline or 3,4,7,8-tetramethyl-1,10-phenanthroline ligands were used to replace the 1,10-phenanthroline ligands in P4+ and MP2+. A structure-activity examination of their partition coefficient (log P), DNA cleavage activity, cytotoxicity, and animal acute toxicity followed. Log P data revealed lipophilicity decreased in the order: MPPh 2+ > PPh 4+ > MPMe 2+ > PMe 4+ > MP2+ > P4+ as expected. We hypothesized that increasing the lipophilicity of the ruthenium complexes would increase cytotoxicity and decrease animal toxicity, yet have little effect on their DNA cleavage activity. This is because all four analogues retain the putative DNA cleaving unit (tatpp ligand) but being more lipophilic, they should more easily enter cells, increasing cytotoxicity, and on the same basis, be slower to build up in the bloodstream after IP injection in animal toxicity studies. IC50 values for all complexes were obtained for H358, CCL228, MCF-7, and against normal cell line MCF-10. The cytotoxicity of P4+, MP2+ and [Ru(phen)2dppz]2+ were also evaluated in NSCLC cell lines H358, HCC2450, H522, H1993, H2073, H322, H2122, H460 and the pancreatic cancer (PANC1) cell line using standard MTS and clonogenic assays. The lipophilic ruthenium complexes MPPh 2+, PPh 4+, MPMe 2+, and PMe 4+ showed no acute animal toxicity in a screen of the MTD in Balb/c mice with doses up to 160 mg drug/Kg mouse. Furthermore, the absorption and the distribution of drug after administration by intraperitoneal (IP) injection in male Wister Han rats were discussed. Lastly, we present the results from a NCI-60 panel prescreen of MPPh 2+ complex that was submitted through the Developmental Therapeutics Program of the National Cancer Institute. In comparison with P4+ and MP2+, these analogues generally showed similar DNA cleavage activity, enhanced cytotoxic activity in cultured malignant human cells, and reduced animal toxicity in Balb/c mice.

Investigation of Ruthenium (II) Polypyridyl Dimers as Potential Chemotherapeutic Agents

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ISBN 13 : 9780542722615
Total Pages : pages
Book Rating : 4.7/5 (226 download)

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Book Synopsis Investigation of Ruthenium (II) Polypyridyl Dimers as Potential Chemotherapeutic Agents by : Thamara K. Janaratne

Download or read book Investigation of Ruthenium (II) Polypyridyl Dimers as Potential Chemotherapeutic Agents written by Thamara K. Janaratne and published by . This book was released on 2006 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: The exploration of transition metal complexes as chemotherapeutic agents is still a relatively unexplored but promising area of research. Chapter 1 highlights the most successful anticancer drugs and potential drugs based on metal complexes, with an emphasis of platinum and ruthenium complexes. In Chapter 2, the biological activity of a series of novel ruthenium dimers is investigated with special attention given to evaluating their potential as anticancer chemotherapeutic agents. A partial list of the compound prepared includes: [Ru(bpy)(CO)2}2tpphz]4+ (74+), [Ru(bpy)(CH3CN)2}2 tpphz]4+(84+), [Ru(bpy)(C 2O4)}2tpphz] (9), [Ru(bpy)(CO)(Cl)} 2tpphz]2+ (102+), [(bpy) 2Ru(tpphz)Ru(bpy)2]4+ (11 4+), [(phen)2Ru(tpphz)Ru(phen)2] 4+ (124+), [(phen)2Ru(tatpp)Ru(phen) 2]4+ (Pp4+), [(phen) 2Ru(tatpq)Ru(phen)2]4+ (Qp 4+), [(bpy)2Ru(tatpp)Ru(bpy)2]4+ (Pb4+) and [(bpy)2Ru(tatpq)Ru(bpy) 2]4+ (Qb4+). Systematic changes in functions, such as overall charge (+4, +2, 0), the presence or absence of labile ligands, long and short bridging ligands between metal centers, and redox inactive (tpphz) and active (tatpp and tatpq) ligands allowed us to complete a structure-activity evaluation of this class of potential anticancer drugs. Most promising were the cationic dimers containing long, redox active bridging ligands, Pp4, P b4+, Qp4+ and Qb4+, which showed very high DNA binding constants (Kb = 107 to 109 M-1) and good cytotoxicity against cancer cell lines (NSCLC). Animal toxicity studies (mice) showed most cationic complexes to be acutely toxic at relatively lower doses. However, the cationic dimers containing the long tatpp or tatpq bridging ligands were well tolerated in mice with maximum tolerable doses in the range of 67-167 mg/kg for Pp 4+ and 6.7-17 mg/kg for Qp4+ as the chloride salts. These promising results led to a study of the antitumor activity of Pp4+ and Qp 4+ in vivo using a mouse melanoma model. Excitingly, complex Pp4+ seems to inhibit tumor growth in vivo although a little difference in survival times was observed. Nonetheless, the results are promising in that this was an initial screen in which numerous parameters including dosage, frequency of treatment, tumor type, etc., remains unoptimized. The ability of these complexes to damage DNA was evaluated in Chapter 3 by using a plasmid DNA assay that shows if a complex can induce single or double-strand cuts in the DNA molecule. None of the complexes causes any cleavage reactions unless an external reductant is added. However, upon addition of a common biological reductant (glutathione, dithiothritol or ascorbic acid), complex Pp4+ and Qp 4+ could be shown to induce single-strand cuts. Importantly, the DNA cleaving ability of Pp4+ is potentiated under anaerobic conditions, showing that the cleavage is not via O2 activation processes. Further studies established that complex P p4+ is doubly reduced under the assay conditions and the doubly reduced product, denoted H2Pp 4+, is the cleavage agent. As this species is oxygen sensitive and readily reoxidized to Pp4+ upon exposure to air, the [O2] 'regulates' the nuclease activity by controlling [H2Pp4+]. The ability of the ruthenium complexes to inhibit or poison topoisomerase I and II was evaluated and is reported in Chapter 4. The intercalating complexes showed the most significant topoisomerase I and II inhibition with complex Pp4+ standing out again for its potent biological activity.

Structure-activity Relationships of Ruthenium(II) Polypyridyl Complexes with Redox-active Intercalating Ligands

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Total Pages : 124 pages
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Book Synopsis Structure-activity Relationships of Ruthenium(II) Polypyridyl Complexes with Redox-active Intercalating Ligands by : Eugenia Soyo Narh

Download or read book Structure-activity Relationships of Ruthenium(II) Polypyridyl Complexes with Redox-active Intercalating Ligands written by Eugenia Soyo Narh and published by . This book was released on 2016 with total page 124 pages. Available in PDF, EPUB and Kindle. Book excerpt: The investigation and development of transition metal complexes as cancer chemotherapeutics has gained a lot of interest in the past few decades and has become a promising area of research. Metal complexes of platinum and ruthenium in particular that have demonstrated success as anticancer drugs or are under exploration currently for clinical use are highlighted in Chapter 1. Chapter 2 describes studies undertaken to understand the neurotoxicity of ruthenium(II) polypyridyl complexes (RPCs), including toxicity in mice and inhibition of the enzyme acetylcholinesterase (AChE), as previous work by Dwyer demonstrated that RPCs could be acutely toxic in mice, presumably due to their inhibition of AChE. Several ruthenium complexes were screened for their enzyme inhibitory potency which was correlated to their structural properties including size, charge, and lipophilicity. In addition, the inhibitory activity of the compounds was correlated to their animal toxicity data so as to understand the potential mode of action of the RPCs in vivo. Chapter 3 describes the synthesis of a series of novel ruthenium(II) polypyridyl complexes and their characterization. These complexes were prepared in an effort to tune the reduction potential of the redox-active intercalating ligand (RAIL) to potentials slightly above and below those observed for the Ru-tatpp complexes. The redox activity of ruthenium-tatpp complexes appears to be responsible for their DNA cleavage activity and these analogues, with slightly different reduction potentials, should give us additional insight into the activity of this class of RPCs. In Chapter 4, the electrochemical properties of the RPCs were measured and correlated with their ability to cause DNA cleavage under reducing conditions with GSH. Complexes with reduction potentials less (more positive) than the redox couple of GSH/GSSG were shown to efficiently cleave DNA. However complexes with higher reduction potentials than the biological reducing agent were not observed to cleave DNA under the same conditions. Cytotoxicity screening of these complexes in human non-small cell lung carcinoma cell lines (NSCLC -- H358 and HOP-62) and breast adenocarcinoma cell line (MCF-7), as well as the non-malignant cell line (MCF-10) was performed and described in Chapter 4.

Ruthenium(II) Polypyridyl Complexes as Mitochondria-targeted Two-photon Photodynamic Anticancer Agents

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ISBN 13 :
Total Pages : pages
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Book Synopsis Ruthenium(II) Polypyridyl Complexes as Mitochondria-targeted Two-photon Photodynamic Anticancer Agents by :

Download or read book Ruthenium(II) Polypyridyl Complexes as Mitochondria-targeted Two-photon Photodynamic Anticancer Agents written by and published by . This book was released on 2015 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt:

Study of the Mechanism of Action for Ru(II) Polypyridyl Complexes as Potential Anticancer Agents

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ISBN 13 :
Total Pages : 175 pages
Book Rating : 4.:/5 (15 download)

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Book Synopsis Study of the Mechanism of Action for Ru(II) Polypyridyl Complexes as Potential Anticancer Agents by : Yang Sun

Download or read book Study of the Mechanism of Action for Ru(II) Polypyridyl Complexes as Potential Anticancer Agents written by Yang Sun and published by . This book was released on 2018 with total page 175 pages. Available in PDF, EPUB and Kindle. Book excerpt:

The Effects of the Stereochemistry of Ruthenium (II) Polypyridyl Complexes on Microtubules as Targets for Chemotherapy

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ISBN 13 :
Total Pages : 74 pages
Book Rating : 4.:/5 (132 download)

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Book Synopsis The Effects of the Stereochemistry of Ruthenium (II) Polypyridyl Complexes on Microtubules as Targets for Chemotherapy by : Radhiyah Himawan

Download or read book The Effects of the Stereochemistry of Ruthenium (II) Polypyridyl Complexes on Microtubules as Targets for Chemotherapy written by Radhiyah Himawan and published by . This book was released on 2020 with total page 74 pages. Available in PDF, EPUB and Kindle. Book excerpt: Ruthenium polypyridyl complexes (RPCs) are promising anticancer agents due to their robustness and tunability of their polypyridyl ligands. Their axial chirality generally allows for more selective binding to biological molecules. The ruthenium complexes [Ru(phen)3]Cl2 (RPC 1),[Ru(DIP)3]Cl2 (RPC 2), [(phen)2Ru(tatpp)]Cl2 (RPC 3), [(phen)2Ru(tatpp)Ru(phen)2]Cl4 (RPC 4), and [(phen)2Ru(dppz)]Cl2 (RPC 5) have all been investigated, and RPCs 2, 3, and 4 have shown lower micromolar cytotoxicity against malignant cell lines without irradiation. Here in we show that microtubules (MTs) may be the target of some RPCs in cells and all these RPCs 1-5 promote tubulin polymerization in vitro. How they interact with MTs is still yet to be discovered. We examined how the different enantiomers of RPC 2 and 3 affected the cytotoxicity, the cellular uptake, and the MT polymerization. Chapter 1 of this thesis reviews prior literature and discusses other metal complexes as well as RPCs that have anticancer potential for their cellular target and correlation to their structures. Chapters 2 and 3 presents how the stereochemistry of the RPCs in their chloride salt affects their ability to stabilize MTs in addition to entering the cell in the first place. Chapter 2 also presents evidence that MT stabilization by RPCs may not be simple due to electrostatic interactions. MT stabilization is done by comparing the in vitro polymerization of free tubulin with and without the presence of the microtubule stabilizing agent (MSA) as a factor of increased light scattering at 340 nm. Cellular uptake is done in the non-small cell lung carcinoma cell line, H358. The amount of ruthenium was analyzed using ICP-MS and the protein concentration using a bicinchoninic acid assay and UV-Vis spectrometry. Although there were no significant chiral differences in MT stabilization, there was a difference in cellular uptake of enantiopure RPC 2. Chapter 4 outlines the resolution of the RPCs by use of Na2[As2(+ or -)tartrate2] and Na2[Sb2(+ or -)tartrate2], as well discussing the optimization of the syntheses of Na2[Sb2(+ or -)tartrate2] and K2[Sb2(+ or -)tartrate2].

Mono- and Bi-functional Chelated Ruthenium(II) Arene Complexes as Potential Anticancer Agents

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ISBN 13 :
Total Pages : 250 pages
Book Rating : 4.:/5 (66 download)

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Book Synopsis Mono- and Bi-functional Chelated Ruthenium(II) Arene Complexes as Potential Anticancer Agents by : Michael Melchart

Download or read book Mono- and Bi-functional Chelated Ruthenium(II) Arene Complexes as Potential Anticancer Agents written by Michael Melchart and published by . This book was released on 2006 with total page 250 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Synthesis and Characterization of Hybrid Drugs Based on Ruthenium Complex Moiety and Biologically Active Organic Compounds

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ISBN 13 :
Total Pages : 0 pages
Book Rating : 4.:/5 (11 download)

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Book Synopsis Synthesis and Characterization of Hybrid Drugs Based on Ruthenium Complex Moiety and Biologically Active Organic Compounds by : Michał Pawel Łomzik

Download or read book Synthesis and Characterization of Hybrid Drugs Based on Ruthenium Complex Moiety and Biologically Active Organic Compounds written by Michał Pawel Łomzik and published by . This book was released on 2016 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: The main goal of this thesis was synthesis and preliminary characterization of novel ruthenium(II) polypyridyl complexes bearing biologically active molecules as potential theranostic agents. Luminescence for the diagnostic applications, and cytotoxicity for the anticancer, therapeutic applications are considered as the theranostic properties. Four new ligands containing biologically active moieties - 5-(4-4'-methyl-[2,2'-bipyridine]-4-ylbut-1-yn-1-yl)pyridine-2-carbaldehyde semicarbazone (L1), 3-(5-4'-methyl-[2,2'-bipyridine]-4-ylpentyl)imidazolidine-2,4-dione (L2), 5,5-dimethyl-3-(5-4'-methyl-[2,2'-bipyridine]-4-ylpentyl)imidazolidine-2,4-dione (L3) and [1-(5-4'-methyl-[2,2'-bipyridine]-4-ylpentyl)-2,5-dioxoimidazolidin-4-yl]urea (L4) were synthesized and characterized. The ligands were used to obtain nine novel ruthenium(II) polypyridyl complexes. Six complexes were synthesized with ligand L1 ([Ru(bpy)2(L1)]2+, [Ru(Mebpy)2(L1)]2+, [Ru(tBubpy)2(L1)]2+, [Ru(Phbpy)2(L1)]2+, [Ru(dip)2(L1)]2+, [Ru(SO3dip)2(L1)]2-) and three with ligands L2, L3 and L4 ([Ru(bpy)2(L2)]2+, [Ru(bpy)2(L3)]2+, [Ru(bpy)2(L4)]2+) (bpy = 2,2'-bipyridine, Mebpy = 4,4'-dimethyl-2,2-bipyridine, tBubpy = 4,4'-tert-butyl-2,2'-bipyridine, Phbpy = 4,4'-diphenyl-2,2-bipyridine, dip = 4,7-diphenyl-1,10-phenantroline and SO3dip = 4,7-di-(4-sulfonatophenyl)-1,10-phenantroline). The spectroscopic and photophysical properties of those complexes were determined. The presence of ligands L1-L4 in the structure of the complex decreased luminescence quantum yield and luminescence lifetime in comparison with unmodified [Ru(bpy)3]2+ complex. The theoretical calculations have shown that ligands L1-L4 do not have influence on ruthenium core geometry. However, they increased the energy of the HOMO that resulted in a shorter band gap. The simulated electronic absorption spectra were in a good agreement with the experimental data. The interactions between the studied ruthenium complexes and human serum albumin (HSA) were investigated. All studied Ru(II) complexes exhibited strong affinity to HSA with the association constant 105 M-1s-1, which suggests formation of Ru complex-HSA adducts. It was also determined that ruthenium complexes most likely bind to the hydrophobic pocket of protein, located in Sudlow's site I in the subdomain II A. Preliminary cytotoxicity evaluation for the studied ruthenium complexes showed their cytotoxic activity towards cancer cell lines. Those results, together with good luminescence properties of the studied ruthenium complexes (luminescence lifetimes and luminescence quantum yield) make them interesting candidates for potential theranostic applications.

Advances in Metallodrugs

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Publisher : John Wiley & Sons
ISBN 13 : 1119640423
Total Pages : 432 pages
Book Rating : 4.1/5 (196 download)

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Book Synopsis Advances in Metallodrugs by : Shahid Ul-Islam

Download or read book Advances in Metallodrugs written by Shahid Ul-Islam and published by John Wiley & Sons. This book was released on 2020-07-08 with total page 432 pages. Available in PDF, EPUB and Kindle. Book excerpt: This book is organized into 12 important chapters that focus on the progress made by metal-based drugs as anticancer, antibacterial, antiviral, anti-inflammatory, and anti-neurodegenerative agents, as well as highlights the application areas of newly discovered metallodrugs. It can prove beneficial for researchers, investigators and scientists whose work involves inorganic and coordination chemistry, medical science, pharmacy, biotechnology and biomedical engineering.

Ruthenium and Gold Complexes as Potential Anticancer Drugs Targeting Selectively Integrin Receptors

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ISBN 13 :
Total Pages : 0 pages
Book Rating : 4.:/5 (962 download)

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Book Synopsis Ruthenium and Gold Complexes as Potential Anticancer Drugs Targeting Selectively Integrin Receptors by : Eva Maria Hahn

Download or read book Ruthenium and Gold Complexes as Potential Anticancer Drugs Targeting Selectively Integrin Receptors written by Eva Maria Hahn and published by . This book was released on 2016 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Syntheses, Characterization, and Preliminary Evaluation of Potential Ruthenium Anticancer Complexes Containing Schiff Base Ligands

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ISBN 13 : 9781687926043
Total Pages : 104 pages
Book Rating : 4.9/5 (26 download)

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Book Synopsis Syntheses, Characterization, and Preliminary Evaluation of Potential Ruthenium Anticancer Complexes Containing Schiff Base Ligands by : Stephen Mensah

Download or read book Syntheses, Characterization, and Preliminary Evaluation of Potential Ruthenium Anticancer Complexes Containing Schiff Base Ligands written by Stephen Mensah and published by . This book was released on 2019 with total page 104 pages. Available in PDF, EPUB and Kindle. Book excerpt: Platinum-based drugs have over the years been administered in the treatment of tumours.Unfortunately, platinum resistance and the severe side effects associated with the treatments has necessitated the research for new anti-cancer drugs. Ruthenium(II) and Ruthenium(III) complexes have shown promise as useful alternative anticancer agents. The lead candidates include the Ru(II) complex RAPTA-C, a ruthenium(II)-arene complex [Ru(Îʺ6-p-cymene)Cl2(1,3,5-triaza-7-phosphaadamantane)] and the Ru(III) complex NAMI-A [imidazoleH][trans-Ru(imidazole) (dimethyl sulfoxide)Cl4]. Both compounds have shown potent cytotoxic activity in several primary human tumor models. Unfortunately, NAMI-A could not advance in clinical evaluations due to limited efficacy in vivo, while the clinical evaluation of RAPTA-C is unknown. Therefore, there is a need for novel cancer therapeutics that have high biological activity, are relatively easy to synthesize, and can readily be modified. This work focuses on the use of 2-acetylpyridine and 2-pyridinecarboxaldehyde for the synthesis, characterization, and preliminary evaluation of derivatives of both the RAPTA-C and NAMI-A anticancer complexes containing Schiff base ligands. Here, the results of the synthesis of these compounds and their subsequent characterization using 1H NMR, MS, fluorescence and UV-Vis spectroscopies are presented.

Metal-based Anticancer Agents

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Publisher : Royal Society of Chemistry
ISBN 13 : 1788017676
Total Pages : 370 pages
Book Rating : 4.7/5 (88 download)

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Book Synopsis Metal-based Anticancer Agents by : Angela Casini

Download or read book Metal-based Anticancer Agents written by Angela Casini and published by Royal Society of Chemistry. This book was released on 2019-04-05 with total page 370 pages. Available in PDF, EPUB and Kindle. Book excerpt: Metal-based anticancer drugs are among the most successful therapeutic agents, as evidenced by the frequent prescription of selected platinum and arsenic compounds to patients. Metal-based Anticancer Agents covers the interdisciplinary world of inorganic drug discovery and development by introducing the most prominent compound classes based on different transition metals, discussing emerging concepts and enabling methods, as well as presenting key pre-clinical and clinical aspects. Recent progress on the unique features of next-generation targeted metal-based anticancer agents, including supramolecular coordination complexes used for both therapy and drug delivery, promise a bright future beyond the benefits of pure cytotoxic activity. With contributions from global leaders in the field, this book will serve as a useful reference to established researchers as well as a practical guide to those new to metallodrugs, and postgraduate students of medicinal chemistry and metallobiology.

Inorganic Chemical Biology

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Publisher : John Wiley & Sons
ISBN 13 : 111851002X
Total Pages : 437 pages
Book Rating : 4.1/5 (185 download)

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Book Synopsis Inorganic Chemical Biology by : Gilles Gasser

Download or read book Inorganic Chemical Biology written by Gilles Gasser and published by John Wiley & Sons. This book was released on 2014-06-23 with total page 437 pages. Available in PDF, EPUB and Kindle. Book excerpt: Understanding, identifying and influencing the biological systems are the primary objectives of chemical biology. From this perspective, metal complexes have always been of great assistance to chemical biologists, for example, in structural identification and purification of essential biomolecules, for visualizing cellular organelles or to inhibit specific enzymes. This inorganic side of chemical biology, which continues to receive considerable attention, is referred to as inorganic chemical biology. Inorganic Chemical Biology: Principles, Techniques and Applications provides a comprehensive overview of the current and emerging role of metal complexes in chemical biology. Throughout all of the chapters there is a strong emphasis on fundamental theoretical chemistry and experiments that have been carried out in living cells or organisms. Outlooks for the future applications of metal complexes in chemical biology are also discussed. Topics covered include: • Metal complexes as tools for structural biology • IMAC, AAS, XRF and MS as detection techniques for metals in chemical biology • Cell and organism imaging and probing DNA using metal and metal carbonyl complexes • Detection of metal ions, anions and small molecules using metal complexes • Photo-release of metal ions in living cells • Metal complexes as enzyme inhibitors and catalysts in living cells Written by a team of international experts, Inorganic Chemical Biology: Principles, Techniques and Applications is a must-have for bioinorganic, bioorganometallic and medicinal chemists as well as chemical biologists working in both academia and industry.

Ruthenium Complexes

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Publisher : John Wiley & Sons
ISBN 13 : 3527695206
Total Pages : 347 pages
Book Rating : 4.5/5 (276 download)

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Book Synopsis Ruthenium Complexes by : Alvin A. Holder

Download or read book Ruthenium Complexes written by Alvin A. Holder and published by John Wiley & Sons. This book was released on 2017-10-27 with total page 347 pages. Available in PDF, EPUB and Kindle. Book excerpt: Edited by a team of highly respected researchers combining their expertise in chemistry, physics, and medicine, this book focuses on the use of rutheniumcontaining complexes in artificial photosynthesis and medicine. Following a brief introduction to the basic coordination chemistry of ruthenium complexes and their synthesis in section one, as well as their photophysical and photochemical properties, the authors discuss in detail the major concepts of artificial photosynthesis and mechanisms of hydrogen production and water oxidation with ruthenium in section two. The third section of the text covers biological properties and important medical applications of ruthenium complexes as therapeutic agents or in diagnostic imaging. Aimed at stimulating research in this active field, this is an invaluable information source for researchers in academia, health research institutes and governmental departments working in the field of organometallic chemistry, green and sustainable chemistry as well as medicine/drug discovery, while equally serving as a useful reference also for scientists in industry.

Radiotherapy in Prostate Cancer

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Publisher : Springer
ISBN 13 : 3642370993
Total Pages : 288 pages
Book Rating : 4.6/5 (423 download)

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Book Synopsis Radiotherapy in Prostate Cancer by : Hans Geinitz

Download or read book Radiotherapy in Prostate Cancer written by Hans Geinitz and published by Springer. This book was released on 2014-11-18 with total page 288 pages. Available in PDF, EPUB and Kindle. Book excerpt: Today, the arsenal of “high-precision” or “targeted” radiotherapy includes a variety of techniques and approaches that, like the pieces of a puzzle, need to be put together to provide the prostate cancer patient with high-level optimized radiation treatment. This book examines in detail the role of these innovative radiation techniques in the management of prostate cancer. In addition, a variety of current controversies regarding treatment are carefully explored, including whether prophylactic treatment of the pelvic lymphatics is essential, the magnitude of the effect of dose escalation, whether a benefit accrues from hypofractionation, and what evidence exists for the superiority of protons or heavy ions. Radiotherapy in Prostate Cancer: Innovative Techniques and Current Controversies is intended for both radiation oncologists and urologists with an interest in the up-to-date capabilities of modern radiation oncology for the treatment of prostate cancer.

Metal Poly-pyridyl Complexes as Quadruplex DNA Binders and Potential Anticancer Agents

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ISBN 13 :
Total Pages : pages
Book Rating : 4.:/5 (812 download)

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Book Synopsis Metal Poly-pyridyl Complexes as Quadruplex DNA Binders and Potential Anticancer Agents by : Kogularamanan Suntharalingham

Download or read book Metal Poly-pyridyl Complexes as Quadruplex DNA Binders and Potential Anticancer Agents written by Kogularamanan Suntharalingham and published by . This book was released on 2012 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: