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5. Performance analysis of a R134a/CO2 cascade heat pump in severe cold regions of China

Author

Zhichao Wang, Shuangquan Shao, Xudong Geng, Chunqiang Si, and Hongwei Zhang

Subjects
HSPF, Mechanical Engineering, Nuclear engineering, Energy performance, Building and Construction, Coefficient of performance, Pollution, Industrial and Manufacturing Engineering, law.invention, Ambient air, General Energy, Operating temperature, Cascade, law, Air source heat pumps, Environmental science, Electrical and Electronic Engineering, Civil and Structural Engineering, Heat pump
Abstract

To achieve efficient and reliable heating in severe cold regions below −20 °C, this paper investigates a R134a/CO2 cascade air source heat pump system (ASHP). Firstly, a simulation model is constructed and used for energy performance analysis. Then experiments are carried out for model verification and performance investigation. Finally, its performance is evaluated in detail with the meteorological data of Harbin under different working conditions for energy performance forecast. Simulation results shows the heating coefficient of performance (COP) increases with higher ambient temperature and lower water supply temperature. At the same time, the modeling errors on coefficient of performance (COP) are all within ±0.2%. The experimental results show that the proposed R134a/CO2 ASHP can supply water above 50 °C with high COP up to 3.07 and 1.60 when the ambient air temperature is −5 °C and −45 °C, respectively. Furthermore, under four working conditions, the heating seasonal performance factors (HSPF) are all above 2.30 and the best is 2.39 for the −25 °C nominal operating temperature and the typical working condition of civil buildings (15 °C). Both the experimental data and the simulation results show that the proposed R134a/CO2 cascade air source heat pump system can provide efficient and reliable heating in severe cold regions.

Published
2022

6. New efficient synthesis of resorcinylic macrolides via ynolides: establishment of cyclopoparadicicol as synthetically feasible preclinical anticancer agent based on Hsp90 as the target

Author

Qiang-Zhi Yang, Xudong Geng, Solit, David, Pratilas, Christine A., Rosen, Neal, and Danishefsky, Samuel J.

Subjects
Macrolide antibiotics -- Research, Cyclopropane compounds -- Evaluation, Cyclopropane compounds -- Research, Chemistry
Abstract

An efficient synthesis to enable the full evaluation of cycloproparadicicol as a candidate for further advancement was developed. Results of these studies are in conjunction with the earlier demonstration that cycloproparadicicol binds to Hsp90 at ca. 160 nM.

Published
2004

7. Toward fully synthetic carbohydrate-based HIV antigen design: On the critical role of bivalency

Author

Dudkin, Vadim Y., Orlova, Marianna, Xudong Geng, Mandal, Mihirbaran, Olsan, William C., and Danishefsky, Samuel J.

Subjects
Peptides -- Research, Pyridine -- Chemical properties, Pyridine -- Research, Ketones -- Research, Ketones -- Structure, Chemistry
Abstract

Extensive glycosylation of HIV envelope proteins were considered to be one of the major impedients to the development of an HIV vaccine. This 'glycan shield' was perceived to confer protection from antibodies, which can recognize the peptide backbone of the gp120 trimer surface.

Published
2004

8. Design, synthesis, and biological evaluation of novel C14-C3'BzN-linked macrocyclic taxoids

Author

Liang Sun, Xudong Geng, Geney, Raphael, Yuan Li, Simmerling, Carlos, Zhong Li, Shujun Xia, Lauher, Joseph W., Horwitz, Susan B., Veith, Jean M., Pera, Paula, Bernacki, Ralph J., and Ojima, Iwao

Subjects
Benzoyl peroxide -- Chemical properties, Catalysis -- Analysis, Paclitaxel -- Chemical properties, Paclitaxel -- Structure, Ruthenium -- Chemical properties, Biological sciences, Chemistry
Abstract

The Ru-catalyzed synthesis of novel C14 position of the baccatin moiety and the ortho position of C3'N-benzoyl group (C14-C3'BzN)-linked macrocyclic taxoids (SB-T-2053) and (SB-T-2054) that mimic the 'REDOR-taxol' structure, paclitaxel is described. The results revealed that SB-T-2054 is the most active compound that exhibited similar potency and structure as that of paclitaxel.

Published
2008

9. Fully synthetic carbohydrate HIV antigens designed on the logic of the 2G12 antibody

Author

Krauss, Isaac J., Joyce, Jeseph G., Finnefrock, Adam C., Hong C. Song, Dudkin, Vadim Y., Xudong Geng, Warren, J. David, Chastain, Michael, Shiver, John W., and Danishefsky, Samuel J.

Subjects
Carbohydrates -- Structure, Carbohydrates -- Chemical properties, Chemical synthesis -- Analysis, HIV antigens -- Research, Chemistry
Abstract

The design and synthesis of multivalent glycopeptide constructs that do not contain any relation to a native gp120 peptide sequence, yet still mimic gp120's binding to 2G12, are presented. These constructs have suitable functional handles for attachment to a carrier protein, thus facilitating their use in vaccines.

Published
2007

10. Design, Synthesis, and Biological Evaluation of New-Generation Taxoids

Author

Ilaria Zanardi, Jon Mallen-St. Clair, Iwao Ojima, Susan Band Horwitz, Shujun Xia, Xianrui Zhao, Dafna Bar-Sagi, David Gallager, Jin Chen, Tao Wang, Xudong Geng, Michael L. Miller, Ralph J. Bernacki, Larisa V. Kuznetsova, Songnian Lin, Jean M. Veith, Jennifer L. Guerriero, Chuanxing Qu, Liang Sun, Christopher P. Borella, and Paula Pera

Subjects
Male, Paclitaxel, Transplantation, Heterologous, Mice, Nude, Antineoplastic Agents, Article, Taxoid, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Biopolymers, Tubulin, In vivo, Cell Line, Tumor, Drug Discovery, Animals, Humans, Point Mutation, Structure–activity relationship, Cytotoxicity, biology, Chemistry, Discodermolide, Biochemistry, Drug Resistance, Neoplasm, Cell culture, Drug Design, biology.protein, Molecular Medicine, Female, Taxoids, Drug Screening Assays, Antitumor, Neoplasm Transplantation
Abstract

Novel second-generation taxoids with systematic modifications at the C2, C10, and C3'N positions were synthesized and their structure-activity relationships studied. A number of these taxoids exhibited exceptionally high potency against multidrug-resistant cell lines, and several taxoids exhibited virtually no difference in potency against the drug-sensitive and drug-resistant cell lines. These exceptionally potent taxoids were termed "third-generation taxoids". 19 (SB-T-1214), 14g (SB-T-121303), and 14i (SB-T-1213031) exhibited excellent activity against paclitaxel-resistant ovarian cancer cell lines with mutations in beta-tubulin as well, wherein the drug resistance is mediated by the beta-tubulin mutation. These taxoids were found to possess exceptional activity in promoting tubulin assembly, forming numerous very short microtubules similar to those formed by discodermolide. Taxoids 19 and 14g also showed excellent cytotoxicity against four pancreatic cancer cell lines, expressing three to four multidrug-resistant genes. Moreover, taxoid 19 exhibited excellent in vivo efficacy against highly drug-resistant CFPAC-1 pancreatic as well as DLD-1 human colon tumor xenografts in mice.

Published
2008

11. Design and synthesis of de novo cytotoxic alkaloids through mimicking taxoid skeleton

Author

Ralph J. Bernacki, Paula Pera, Iwao Ojima, Xudong Geng, and Raphaël Geney

Subjects
Scaffold, Stereochemistry, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Biochemistry, Chemical synthesis, Taxoid, Bridged Bicyclo Compounds, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, Alkaloids, Drug Discovery, Side chain, Tumor Cells, Cultured, Cytotoxic T cell, Humans, Cytotoxicity, Molecular Biology, chemistry.chemical_classification, Bicyclic molecule, Chemistry, Alkaloid, Molecular Mimicry, Organic Chemistry, General Medicine, Antineoplastic Agents, Phytogenic, Drug Design, Lactam, Molecular Medicine, Taxoids, Pharmacophore, Lactone
Abstract

Based on a common pharmacophore model and the hypothesis that the baccatin core of taxoids is a scaffold securing the proper orientation of the side chains, a bicyclic alkaloid scaffold was designed as a baccatin surrogate. Using this scaffold, two novel macrocyclic and open-chain ‘taxoid-mimicking’ compounds were synthesized. Two of these ‘taxoid-mimics’, 2 and 3 , were found to possess cytotoxicity with micromolar level IC 50 values against human breast cancer cell lines.

Published
2004

14. Total Synthesis of Aigialomycin D

Author

Xudong Geng and Samuel J. Danishefsky

Subjects
Cyclopropanes, Molecular Structure, Olefin metathesis, Chemistry, Stereochemistry, Organic Chemistry, Total synthesis, Stereoisomerism, Biochemistry, Lactones, Aigialomycin D, Organic chemistry, Moiety, Macrolides, Physical and Theoretical Chemistry
Abstract

[reaction: see text] The first total synthesis of resorcinylic macrolide aigialomycin D was described. The resorcinylic moiety was constructed by a highly efficient Diels-Alder reaction using a disiloxydiene and a 14-membered "ynolide" as the dienophile synthesized by ring-forming olefin metathesis.

Published
2004

15. Synthetic Development of Radicicol and Cycloproparadicicol: Highly Promising Anticancer Agents Targeting Hsp90

Author

Zhi-Qiang Yang, Xudong Geng, and Samuel J. Danishefsky

Subjects
Natural product, biology, Organic Chemistry, Total synthesis, General Medicine, Computational biology, Combinatorial chemistry, Hsp90, Radicicol, Hsp90 inhibitor, chemistry.chemical_compound, chemistry, Cycloproparadicicol, biology.protein
Abstract

Molecular chaperone Hsp90 has emerged as one of the most exciting new targets for anticancer therapy. Natural product-based modulators, such as radicicol (1), inhibit Hsp90 and induce the breakdown of its client proteins,thereby blocking multiple critical oncogenic pathways. Several total synthesis endeavors directed toward radicicol have been accomplished. Cycloproparadicicol (2), a potent Hsp90 inhibitor and highly promising pre-clinical anticancer agent, was discovered through a convergent total synthesis approach. In an effort to devise a more efficient and concise route to reach 2, a novel 'ynolide' protocol, featuring an ynolide-bissiloxydiene Diels-Alder addition, was designed and reduced to practice. This methodology was also extended to aigialomycin D.

Published
2004

16. Synthesis of Novel C2−C3‘N-Linked Macrocyclic Taxoids by Means of Highly Regioselective Heck Macrocyclization

Author

Xudong Geng, Songnian Lin, Michael L. Miller, and Iwao Ojima

Subjects
chemistry.chemical_classification, Olefin fiber, Chemistry, Stereochemistry, Organic Chemistry, Iodide, Regioselectivity, Antineoplastic Agents, Stereoisomerism, General Medicine, Alkenes, Combinatorial chemistry, Biochemistry, Inhibitory Concentration 50, Cyclization, Cell Line, Tumor, Heck reaction, Intramolecular force, Yield (chemistry), Humans, Moiety, Taxoids, Hydrocarbons, Iodinated, Physical and Theoretical Chemistry
Abstract

[reaction: see text] Novel C2-C3'N-linked macrocyclic taxoids are synthesized using intramolecular Heck reaction in the key step. Macrocyclization proceeds with high regioselectivity in good yield. Taxoids bearing an olefin moiety at C2 and an iodide at C3'N give exo-products exclusively. However, the endo-products are formed with up to 100% regioselectivity just by switching the positions of the olefin and the iodide moieties. Some of these macrocyclic taxoids are significantly cytotoxic.

Published
2003

17. Tubulins in the primate retina: evidence that xanthophylls may be endogenous ligands for the paclitaxel-binding site††This work was presented in part at the Association for Research in Vision and Ophthalmology annual meetings May 1999 and May 2000, Fort Lauderdale, FL, USA and at the Schepens Eye Research Institute's 50th Anniversary Symposium, October 2000.‡‡The nucleotide sequences reported in this paper have been submitted to the GenBankTM with accession numbers AF141347, AF141348, AF141349, AF141923, and AF147880

Author

Alice J. Adler, Iwao Ojima, Donald V. Crabtree, and Xudong Geng

Subjects
chemistry.chemical_classification, genetic structures, biology, cDNA library, Protein subunit, Organic Chemistry, Clinical Biochemistry, Nucleic acid sequence, Pharmaceutical Science, Biochemistry, eye diseases, Amino acid, Tubulin, Macula Lutea, chemistry, Drug Discovery, Nucleic acid, biology.protein, Molecular Medicine, sense organs, Binding site, Molecular Biology
Abstract

The xanthophylls—lutein, zeaxanthin, and meso-zeaxanthin (L&Z)—are found in the central region of the primate retina, which is called the macula lutea (yellow spot). How they are anchored there and what their function is has been debated for over 50 years. Here, we present evidence that they may be bound to the paclitaxel (Taxol) binding site of the β-tubulin subunit of microtubules and that a major function may be to modulate the dynamic instability of microtubules in the macula. Also, we compare nucleic acid and amino acid sequences of tubulins that are in human brain with those we have isolated from human-retina and monkey-macula cDNA libraries. In so doing, we suggest that in primates, class I β-tubulin consists of at least two subtypes (βIa and βIb). Alignment analysis of the sequences of the genes for βIa and βIb indicates that the corresponding mRNAs may have other functions in addition to that of coding for proteins. Furthermore, we show that there are at least five different types of β-tubulin in the macula lutea of rhesus monkey.

Published
2001

18. Macrocycle Formation by Ring-Closing Metathesis. Application to the Syntheses of Novel Macrocyclic Taxoids

Author

and Xudong Geng, Tadashi Inoue, John J. Walsh, Iwao Ojima, Songnian Lin, Michael L. Miller, and Christopher P. Borella

Subjects
Colloid and Surface Chemistry, Ring-closing metathesis, Chemistry, Stereochemistry, Ic50 values, General Chemistry, Cancer cell lines, Metathesis, Biochemistry, Human breast, Combinatorial chemistry, Catalysis
Abstract

A series of novel macrocyclic taxoids 6 and 6‘ bearing 16-, 17-, and 18-membered rings connecting the substituents at the C-2 and C-3‘ positions were designed and synthesized. The syntheses of these macrocycles 6 and 6‘ were accomplished using the highly efficient ruthenium-catalyzed ring-closing metathesis (RCM) of taxoid-ω,ω‘-dienes 7 in the key step. Taxoid-ω,ω‘-dienes 7 were obtained through the ring-opening coupling of 4-alkenyl-β-lactams 9 with 2-alkenoylbaccatins 8 in good to high yields. Although various novel pentacyclic macrocycles 6 and 6‘ were successfully synthesized, there were cases in which the desired RCM did not proceed. The scope and limitation of RCM in its application to highly functionalized complex substrates are discussed. All macrocyclic taxoids 6 and 6‘ were found to be cytotoxic, with some of them exhibiting submicromolar IC50 values against a human breast cancer cell line.

Published
2000

19. Synthesis of highly potent second-generation taxoids through effective kinetic resolution coupling of racemic ?-lactams with baccatins

Author

Robert Tynebor, Chuanxing Qu, David J. Gallagher, Iwao Ojima, Elizabeth Pollina, Xudong Geng, Songnian Lin, and Jessica Rutter

Subjects
Pharmacology, Stereochemistry, Organic Chemistry, Enantioselective synthesis, chemistry.chemical_element, Catalysis, Analytical Chemistry, Kinetic resolution, chemistry.chemical_compound, Enantiopure drug, chemistry, Drug Discovery, Alkoxide, Lithium, Enantiomer, Selectivity, Chirality (chemistry), Spectroscopy
Abstract

A series of highly potent second-generation taxoids bearing a 2-methylprop-1-enyl or a 2-methylpropyl group at C-3′ with modifications at the C-2, C-10, and C-14 positions was synthesized through the coupling of racemic cis-β-lactams with properly protected/modified baccatin and 14-OH-baccatin. A high level of kinetic resolution was observed for all cases examined. The observed highly efficient enantiomer differentiation is ascribed to the markedly different chiral environment between the (+)- and (−)-β-lactams in their approach to the chiral framework of the enantiopure lithium alkoxide of a baccatin in the ring-opening coupling process. It was also observed that substantially higher selectivity was achieved when 14-OH-baccatin-1,14-carbonate was used. Analysis of the transition state models revealed that the repulsive interactions between the 3-TIPS group of a (−)-β-lactam with 1,14-carbonate group of the baccatin substantially increases the asymmetric bias in the kinetic resolution process, favoring the reaction of a (+)-β-lactam, which leads to the observed excellent selectivity. Chirality 12:431–441, 2000. © 2000 Wiley-Liss, Inc.

Published
2000

20. ChemInform Abstract: Synthesis and Structure-Activity Relationships of New Second-Generation Taxoids

Author

Iwao Ojima, Paula Pera, Christopher P. Borella, Songnian Lin, Michael L. Miller, Tao Wang, Ralph J. Bernacki, and Xudong Geng

Subjects
chemistry.chemical_compound, Paclitaxel, chemistry, Stereochemistry, General Medicine, Cancer cell lines, Human breast, Orders of magnitude (mass)
Abstract

A series of second-generation taxoids bearing a substitutent on the C-2-benzoyl group and modifications at C-3′/C-10 positions was synthesized. These taxoids exhibited 2–3 orders of magnitude higher potency than that of paclitaxel against drug-resistant human breast cancer cell lines. It is also noteworthy that three taxoids showed almost no difference in activity against drug-resistant and drug-sensitive cell lines, which are categorized as “advanced second generation taxoids“.

Published
2010

21. ChemInform Abstract: Design, Synthesis and Biological Activity of Novel C2-C3′ N-Linked Macrocyclic Taxoids

Author

Iwao Ojima, Songnian Lin, Ralph J. Bernacki, Paula Pera, and Xudong Geng

Subjects
Taxoid, Terpene, Design synthesis, Chemistry, Stereochemistry, Biological activity, General Medicine, Cancer cell lines, Cytotoxicity, Human breast
Abstract

A series of novel macrocyclic taxoids was designed and synthesized by connecting the C-2 and C-3′ N positions of the taxoid framework with various tethers. Cytotoxicity of these macrocyclic taxoids was evaluated against a human breast cancer cell line LCC6-WT, and a couple of the taxoids exhibited 0.09–0.3 μM IC 50 values.

Published
2010

22. Design, Synthesis and Biological Evaluation of Novel C14-C3’BzN–Linked Macrocyclic Taxoids¶

Author

Jean M. Veith, Raphaël Geney, Ralph J. Bernacki, Shujun Xia, Carlos Simmerling, Joseph W. Lauher, Iwao Ojima, Xudong Geng, Susan Band Horwitz, Zhong Li, Paula Pera, Yuan Li, and Liang Sun

Subjects
Models, Molecular, Ortho position, Macrocyclic Compounds, Magnetic Resonance Spectroscopy, Stereochemistry, Molecular Conformation, Metathesis, Crystallography, X-Ray, Microtubules, Article, Taxoid, Tubulin, Cell Line, Tumor, Moiety, Humans, Computational analysis, Biological evaluation, Chemistry, Organic Chemistry, Combinatorial chemistry, Antineoplastic Agents, Phytogenic, Microscopy, Electron, Design synthesis, Drug Design, Indicators and Reagents, Taxoids, Drug Screening Assays, Antitumor, Linker
Abstract

Novel macrocyclic paclitaxel congeners were designed to mimic the bioactive conformation of paclitaxel. Computational analysis of the "REDOR-Taxol" structure revealed that this structure could be rigidified by connecting the C14 position of the baccatin moiety and the ortho position of C3'N-benzoyl group (C3'BzN), which are ca. 7.5 A apart, with a short linker (4-6 atoms). 7-TES-14beta-allyloxybaccatin III and (3R,4S)-1-(2-alkenylbenzoyl)-beta-lactams were selected as key components, and the Ojima-Holton coupling afforded the corresponding paclitaxel-dienes. The Ru-catalyzed ring-closing metathesis (RCM) of paclitaxel-dienes gave the designed 15- and 16-membered macrocyclic taxoids. However, the RCM reaction to form the designed 14-membered macrocyclic taxoid did not proceed as planned. Instead, the attempted RCM reaction led to the occurrence of an unprecedented novel Ru-catalyzed diene-coupling process, giving the corresponding 15-membered macrocyclic taxoid (SB-T-2054). The biological activities of the novel macrocyclic taxoids were evaluated by tumor cell growth inhibition (i.e., cytotoxicity) and tubulin-polymerization assays. Those assays revealed high sensitivity of cytotoxicity to subtle conformational changes. Among the novel macrocyclic taxoids evaluated, SB-T-2054 is the most active compound, which possesses virtually the same potency as that of paclitaxel. The result may also indicate that SB-T-2054 structure is an excellent mimic of the bioactive conformation of paclitaxel. Computational analysis for the observed structure-activity relationships is also performed and discussed.

Published
2008

23. Fully synthetic carbohydrate HIV antigens designed on the logic of the 2G12 antibody

Author

J. David Warren, Adam C. Finnefrock, Samuel J. Danishefsky, Hong C. Song, John W. Shiver, Isaac J. Krauss, Joseph G. Joyce, Vadim Y. Dudkin, Michael Chastain, and Xudong Geng

Subjects
Glycan, HIV Antigens, Carbohydrates, Peptide, medicine.disease_cause, Biochemistry, Peptides, Cyclic, Catalysis, Epitope, Epitopes, Colloid and Surface Chemistry, medicine, Carbohydrate Conformation, chemistry.chemical_classification, AIDS Vaccines, biology, Molecular Mimicry, General Chemistry, Cyclic peptide, Glycopeptide, Molecular mimicry, chemistry, biology.protein, Carbohydrate conformation, Cysteine, Protein Binding
Abstract

Di- and trivalent glycopeptide mimics of the HIV 2G12 epitope have been synthesized and evaluated for their comparative 2G12 binding characteristics. The epitope mimics consist of a cyclic peptide scaffold (unrelated to gp120 peptide sequences) attached via aspartate linkages to two or three copies of the high-mannose glycan, Man9GlcNAc2. The synthesis has been achieved via high-yielding double and triple Lansbury aspartylations of Man9GlcNAc2-NH2 with peptides containing, respectively, two and three aspartate residues. Conjugation of such constructs with an immunogenic carrier protein, OMPC, has been accomplished through the peptide's cysteine sulfhydryl function, and Biacore assays have shown that binding affinity for 2G12 increases with increasing valency.

Published
2007

24. Synthetic Glycopeptide-Based Vaccines

Author

J. David Warren, Xudong Geng, and Samuel J. Danishefsky

Subjects
chemistry.chemical_classification, Immune system, chemistry, Antigen, Drug discovery, Glycoconjugate, Computational biology, Cancer vaccine, HIV vaccine, Glycoprotein, Glycopeptide
Abstract

This review provides an overview of our explorations into oligosaccharide and glycoconjugate construction for the creation and evaluation of glycopeptide-based vaccines. The basis for these investigations is the known tendency of both cancer cells and viruses to express selective carbohydrate motifs in the form of glycoproteins or glycolipids. Utilization of these carbohydrates in a glycopeptide-based vaccine could potentially trigger immune recognition, generating a protective response against the disease. However, obtaining large quantities of such compounds from natural sources is extremely difficult. Over the past two decades, our lab has been engaged in the total synthesis of complex oligosaccharides and glycoconjugates. With this knowledge and experience, we have begun to evaluate, in many cases at the clinical level, whether the human immune system is capable of mounting a response against such fully synthetic carbohydrate antigens in a focused and useful way. Toward this goal, we have merged the powers of both chemistry and immunology to provide insight into this problem. The synthesis and evaluation of potential vaccines for both cancer and HIV will be described.

Published
2006

25. New Efficient Synthesis of Resorcinylic Macrolides via Ynolides: Establishment of Cycloproparadicicol as Synthetically Feasible Preclinical Anticancer Agent Based on Hsp90 as the Target

Author

Christine A. Pratilas, Neal Rosen, Samuel J. Danishefsky, Xudong Geng, Zhi-Qiang Yang, and David B. Solit

Subjects
biology, Total synthesis, General Medicine, Computational biology, Key features, Hsp90, Radicicol, chemistry.chemical_compound, chemistry, Breast cancer cell line, Cycloproparadicicol, biology.protein, Salt metathesis reaction, Cytotoxicity
Abstract

A program currently ongoing in our laboratory envisions natural macrolide radicicol-based inhibitors targeting the molecular chaperone Hsp90. Such inhibitors can be potential anticancer agents due to their ability to induce the breakdown of a variety of oncogenic proteins. In this account, we first concern ourselves with a vastly important total synthesis of such an inhibitor. We accomplished this via a new approach, which we term the “ynolide method”, directed to the synthesis of resorcinylic macrolides, including cycloproparadicicol and aigialomycin D. The key features of the syntheses involve cobalt-complexation-promoted ring-closing metathesis (RCM) to generate ynolides, followed by Diels−Alder reaction with dimedone-derived bis-siloxy dienes to elaborate the benzo system. A number of interesting analogues were synthesized using this protocol. They were evaluated for their inhibitory activity against the growth of breast cancer cell line, MCF-7. The potency of their cytotoxicity was found to be consis...

Published
2004

26. Toward fully synthetic carbohydrate-based HIV antigen design: on the critical role of bivalency

Author

William C. Olson, Samuel J. Danishefsky, Marianna Orlova, Xudong Geng, Mihirbaran Mandal, and Vadim Y. Dudkin

Subjects
Glycan, HIV Antigens, Dimer, Molecular Sequence Data, Carbohydrates, HIV Envelope Protein gp120, Biochemistry, Catalysis, Epitope, law.invention, chemistry.chemical_compound, Colloid and Surface Chemistry, Antigen, law, Surface plasmon resonance, chemistry.chemical_classification, biology, Glycopeptides, General Chemistry, Glycopeptide, Peptide Fragments, chemistry, Carbohydrate Sequence, Recombinant DNA, biology.protein, Glycoprotein, Mannose
Abstract

Synthetic gp120331-335 glycopeptide fragments carrying hybrid and high-mannose type N-linked glycans were evaluated for binding to broadly neutralizing antibody 2G12 using surface plasmon resonance technology. None of the hybrid-type constructs demonstrated binding to 2G12. In the high-mannose series, the “Cys dimer” construct, presenting two undecasaccharide glycans, showed significantly higher binding than the Cys-protected monomer. The binding of the dimeric structure was further investigated in competition with recombinant gp120. The data suggest that gp120 and its designed synthetic epitope construct bind to the same site on 2G12.

Published
2004

28. New efficient synthesis of resorcinylic macrolides via ynolides: establishment of cycloproparadicicol as synthetically feasible preclinical anticancer agent based on Hsp90 as the target

Author

Neal Rosen, Samuel J. Danishefsky, Christine A. Pratilas, David B. Solit, Zhi-Qiang Yang, and Xudong Geng

Subjects
Cyclopropanes, Antineoplastic Agents, Breast Neoplasms, Computational biology, Biochemistry, Catalysis, chemistry.chemical_compound, Inhibitory Concentration 50, Lactones, Colloid and Surface Chemistry, Breast cancer cell line, Cell Line, Tumor, Humans, HSP90 Heat-Shock Proteins, Cytotoxicity, biology, Molecular Structure, Total synthesis, Biological activity, General Chemistry, Cobalt, Resorcinols, Key features, Hsp90, Radicicol, chemistry, Cycloproparadicicol, biology.protein, Macrolides, Molecular Chaperones
Abstract

A program currently ongoing in our laboratory envisions natural macrolide radicicol-based inhibitors targeting the molecular chaperone Hsp90. Such inhibitors can be potential anticancer agents due to their ability to induce the breakdown of a variety of oncogenic proteins. In this account, we first concern ourselves with a vastly important total synthesis of such an inhibitor. We accomplished this via a new approach, which we term the "ynolide method", directed to the synthesis of resorcinylic macrolides, including cycloproparadicicol and aigialomycin D. The key features of the syntheses involve cobalt-complexation-promoted ring-closing metathesis (RCM) to generate ynolides, followed by Diels-Alder reaction with dimedone-derived bis-siloxy dienes to elaborate the benzo system. A number of interesting analogues were synthesized using this protocol. They were evaluated for their inhibitory activity against the growth of breast cancer cell line, MCF-7. The potency of their cytotoxicity was found to be consistent with their ability to degrade the oncogenic protein, Her2. From these assays, cycloproparadicicol was identified as a most promising candidate for further development.

Published
2004

29. Total Synthesis of Aigialomycin D

Author

Samuel J. Danishefsky and Xudong Geng

Subjects
Aigialomycin D, Olefin metathesis, Chemistry, Stereochemistry, Moiety, Total synthesis, General Medicine
Abstract

The first total synthesis of resorcinylic macrolide aigialomycin D was described. The resorcinylic moiety was constructed by a highly efficient Diels−Alder reaction using a disiloxydiene and a 14-membered “ynolide” as the dienophile synthesized by ring-forming olefin metathesis.

Published
2004

30. In pursuit of carbohydrate-based HIV vaccines, part 1: The total synthesis of hybrid-type gp120 fragments

Author

Samuel J. Danishefsky, Mihirbaran Mandal, Xudong Geng, and Vadim Y. Dudkin

Subjects
AIDS Vaccines, Oligosaccharides, Branched-Chain, Molecular Structure, Chemistry, HIV Antigens, Hybrid type, Human immunodeficiency virus (HIV), Glycopeptides, Total synthesis, Oligosaccharides, General Chemistry, Carbohydrate, HIV Envelope Protein gp120, medicine.disease_cause, Catalysis, Biochemistry, medicine, Humans, Glycoconjugates
Published
2004

31. Tumor-specific novel taxoid-monoclonal antibody conjugates

Author

Iwao Ojima, Laura M Bartle, Christopher P. Borella, Sharon D. Wilhelm, Xinyuan Wu, Chuanxing Qu, Xudong Geng, Ravi V J Chari, Barbara A. Leece, Victor S. Goldmacher, and Hongsheng Xie

Subjects
Immunoconjugates, Paclitaxel, medicine.drug_class, Antineoplastic Agents, Mice, SCID, Monoclonal antibody, Taxoid, Mice, Structure-Activity Relationship, Immune system, In vivo, Drug Discovery, medicine, Animals, Humans, Prodrugs, Epidermal growth factor receptor, Cytotoxicity, biology, Chemistry, Antibodies, Monoclonal, Xenograft Model Antitumor Assays, ErbB Receptors, Epidermoid carcinoma, Biochemistry, biology.protein, Cancer research, Molecular Medicine, Antibody
Abstract

Taxoids bearing methyldisulfanyl(alkanoyl) groups for taxoid-antibody immunoconjugates were designed, synthesized and their activities evaluated. A highly cytotoxic C-10 methyldisulfanylpropanoyl taxoid was conjugated to monoclonal antibodies recognizing the epidermal growth factor receptor (EGFR) expressed in human squamous cancers. These conjugates were shown to possess remarkable target-specific antitumor activity in vivo against EGFR-expressing A431 tumor xenografts in severe combined immune deficiency mice, resulting in complete inhibition of tumor growth in all the treated mice.

Published
2002

32. Design, synthesis and biological activity of novel C2-C3' N-Linked macrocyclic taxoids

Author

Paula Pera, Iwao Ojima, Ralph J. Bernacki, Songnian Lin, and Xudong Geng

Subjects
Paclitaxel, Stereochemistry, Cell Survival, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Breast Neoplasms, Crystallography, X-Ray, Biochemistry, Chemical synthesis, Taxoid, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Tumor Cells, Cultured, Humans, Cytotoxicity, Molecular Biology, chemistry.chemical_classification, Organic Chemistry, Biological activity, Stereoisomerism, Antineoplastic Agents, Phytogenic, chemistry, Design synthesis, Drug Design, Lactam, Molecular Medicine, Female, Indicators and Reagents, Diterpene, Drug Screening Assays, Antitumor, Lactone
Abstract

A series of novel macrocyclic taxoids was designed and synthesized by connecting the C-2 and C-3′ N positions of the taxoid framework with various tethers. Cytotoxicity of these macrocyclic taxoids was evaluated against a human breast cancer cell line LCC6-WT, and a couple of the taxoids exhibited 0.09–0.3 μM IC 50 values.

Published
2002

33. New Generation Taxoids and Hybrids of Microtuble-Stabilizing Anticancer Agents

Author

Iwao Ojima, Scott D. Kuduk, Subrata Chakravarty, Songnian Lin, Tao Wang, Xudong Geng, Michael L. Miller, Pierre-Yves Bounaud, Evelyne Michaud, Young Hoon Park, Chung-Ming Sun, John C. Slater, Tadashi Inoue, Christopher P. Borella, John J. Walsh, Ralph J. Bernacki, Paula Pera, Jean M. Veith, Ezio Bombardelli, Antonella Riva, Srinivasa Rao, Lifeng He, George A. Orr, Susan B. Horwitz, Samuel J. Danishefsky, Giovanni Scambia, and Cristiano Ferlini

Published
2001

35. Design, Synthesis, and Biological Evaluation of New-Generation Taxoids.

Author

Iwao Ojima, Jin Chen, Liang Sun, Christopher P. Borella, Tao Wang, Michael L. Miller, Songnian Lin, Xudong Geng, Larisa Kuznetsova, Chuanxing Qu, David Gallager, Xianrui Zhao, Ilaria Zanardi, Shujun Xia, Susan B. Horwitz, Jon Mallen-St. Clair, Jennifer L. Guerriero, Dafna Bar-Sagi, Jean M. Veith, and Paula Pera

Published
2008
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36. New Efficient Synthesis of Resorcinylic Macrolides via Ynolides: Establishment of Cycloproparadicicol as Synthetically Feasible Preclinical Anticancer Agent Based on Hsp90 as the Target.

Author

Zhi-Qiang Yang, Xudong Geng, Solit, David, Pratilas, Christine A., Rosen, Neal, and Danishefsky, Samuel J.

Subjects
*MACROLIDE antibiotics, *COBALT, *TRANSITION metals, *ONCOGENES, *VIRAL genetics, *CELL lines
Abstract

A program currently ongoing in our laboratory envisions natural macrolide radicicol-based inhibitors targeting the molecular chaperone Hsp90. Such inhibitors can be potential anticancer agents due to their ability to induce the breakdown of a variety of oncogenic proteins. In this account, we first concern ourselves with a vastly important total synthesis of such an inhibitor. We accomplished this via a new approach, which we term the "ynolide method", directed to the synthesis of resorcinylic macrolides, including cycloproparadicicol and aigialomycin D. The key features of the syntheses involve cobalt-complexation- promoted ring-closing metathesis (ACM) to generate ynolides, followed by Diels-Alder reaction with dimedone-derived bis-siloxy dienes to elaborate the benzo system. A number of interesting analogues were synthesized using this protocol. They were evaluated for their inhibitory activity against the growth of breast cancer cell line, MCF-7. The potency of their cytotoxicity was found to be consistent with their ability to degrade the oncogenic protein, Her2. From these assays, cycloproparadicicol was identified as a most promising candidate for further development. [ABSTRACT FROM AUTHOR]

Published
2004
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37. In Pursuit of Carbohydrate-Based HIV Vaccines, Part 2: The Total Synthesis of High-Mannose-Type gp120 Fragments—Evaluation of Strategies Directed to Maximal Convergence ( This work was supported by the National Institutes of Health (CA-28824). US Army Breast Cancer Foundation postdoctoral fellowship support is gratefully acknowledged by X.G. (BC022120) and V.D. (BC020513). We thank Ms. Anna Dudkina and Ms. Sylvi Rusli (NMR Core Facility, CA-02848) for mass spectrometric analyses, Dr. George Sukenic for NMR spectroscopic analyses, and Dr. J. David Warren for help in the preparation of starting materials. We also thank Dr. Justin S. Miller, Dr. Tom Muir, Mr. Michael Hahn, and Mr. Matthew Sekedat for their generous help in the preparation of the peptides. )

Author

Xudong Geng, Vadim Y. Dudkin, Mihirbaran Mandal, and Samuel J. Danishefsky

Published
2004
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38. Anticancer Agents

Author

Iwao Ojima, Gregory D. Vite, Karl-Heinz Altmann, E. A. Sausville, J. I. Johnson, G. M. Cragg, S. Decker, George R. Pettit, John F. Kadow, Thomas Alstadt, Shu-Hui Chen, Pierre Dextraze, Karen Du, Craig Fairchild, Jerzy Golik, Steven Hansel, Kathy A. Johnston, Robert A. Kramer, David R. Langley, Frank Lee, Byron Long, Harold Mastalerz, Carl Ouellet, Robert Perrone, William C. Rose, Paul Scola, Gene Schulze, Andrew Staab, Quifen May Xue, Michael Walker, Jen-Mei Wei, Mark Wittman, J. J. Kim Wright, Mary Zoeckler, Dolatrai M. Vyas, Scott D. Kuduk, Subrata Chakravarty, Songnian Lin, Tao Wang, Xudong Geng, Michael L. Miller, Pierre-Yves Bounaud, Evelyne Michaud, Young Hoon Park, Chung-Ming Sun, John C. Slater, Tadashi Inoue, Christopher P. Borella, John J. Walsh, Ralph J. Bernacki, Paula Pera, Jean M. Veith, Ezio Bombardelli, Antonella Riva, Srinivasa Rao, Lifeng He, George A. Orr, Susan B. Horwitz, Samuel J. Danishefsky, Giovanni Scambia, Cristiano Ferlini, Susan Band Horwitz, Laura A. Martello, Chia-Ping H. Yang, Amos B. Smith, Hayley M. McDaid, Robert M., Iwao Ojima, Gregory D. Vite, Karl-Heinz Altmann, E. A. Sausville, J. I. Johnson, G. M. Cragg, S. Decker, George R. Pettit, John F. Kadow, Thomas Alstadt, Shu-Hui Chen, Pierre Dextraze, Karen Du, Craig Fairchild, Jerzy Golik, Steven Hansel, Kathy A. Johnston, Robert A. Kramer, David R. Langley, Frank Lee, Byron Long, Harold Mastalerz, Carl Ouellet, Robert Perrone, William C. Rose, Paul Scola, Gene Schulze, Andrew Staab, Quifen May Xue, Michael Walker, Jen-Mei Wei, Mark Wittman, J. J. Kim Wright, Mary Zoeckler, Dolatrai M. Vyas, Scott D. Kuduk, Subrata Chakravarty, Songnian Lin, Tao Wang, Xudong Geng, Michael L. Miller, Pierre-Yves Bounaud, Evelyne Michaud, Young Hoon Park, Chung-Ming Sun, John C. Slater, Tadashi Inoue, Christopher P. Borella, John J. Walsh, Ralph J. Bernacki, Paula Pera, Jean M. Veith, Ezio Bombardelli, Antonella Riva, Srinivasa Rao, Lifeng He, George A. Orr, Susan B. Horwitz, Samuel J. Danishefsky, Giovanni Scambia, Cristiano Ferlini, Susan Band Horwitz, Laura A. Martello, Chia-Ping H. Yang, Amos B. Smith, Hayley M. McDaid, and Robert M.

Published
2001

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