Your search keyword '"Nagle D."' showing total 16 results

1. Hypoxia-Inducible Factor-1 Activation by (−)-Epicatechin Gallate:  Potential Adverse Effects of Cancer Chemoprevention with High-Dose Green Tea Extracts

Author

Zhou, Y.-D., Kim, Y.-P., Li, X.-C., Baerson, S. R., Agarwal, A. K., Hodges, T. W., Ferreira, D., and Nagle, D. G.

Abstract

Hypoxia-inducible factor-1 (HIF-1) is a transcription factor that induces oxygen-regulated genes in response to reduced oxygen conditions (hypoxia). Expression of the oxygen-regulated HIF-1α subunit correlates positively with advanced disease stages and poor prognosis in cancer patients. Green tea catechins are believed to be responsible for the cancer chemopreventive activities of green tea. We found that (−)-epicatechin-3-gallate (ECG, 1), one of the major green tea catechins, strongly activates HIF-1 in T47D human breast carcinoma cells. Among the green tea catechins tested, 1 demonstrated the strongest HIF-1-inducing activity, while (−)-epigallocatechin-3-gallate (EGCG, 2) was significantly less active. However, 2 is relatively unstable in the in vitro system studied. Compound 1 also increases the expression of HIF-1 target genes including GLUT-1, VEGF, and CDKN1A. In T47D cells, 1 induces nuclear HIF-1α protein without affecting HIF-1α mRNA. Both the induction of HIF-1α protein and activation of HIF-1 by 1 can be blocked by iron and ascorbate, indicating that 1 may activate HIF-1 through the chelation of iron. These results suggest that intended cancer chemoprevention with high-dose green tea extracts may be compromised, by the ability of tea catechins to promote tumor cell survival pathways associated with HIF-1 activation.

Published

2004

2. Laurenditerpenol, a New Diterpene from the Tropical Marine Alga Laurencia intricata that Potently Inhibits HIF-1 Mediated Hypoxic Signaling in Breast Tumor Cells

Author

Mohammed, K. A., Hossain, C. F., Zhang, L., Bruick, R. K., Zhou, Y.-D., and Nagle, D. G.

Abstract

The degree of tumor hypoxia correlates with advanced disease stages and treatment resistance. The transcription factor hypoxia-inducible factor-1 (HIF-1) promotes tumor cell adaptation and survival under hypoxic conditions. Therefore, specific HIF-1 inhibitors represent an important new class of potential tumor-selective therapeutic agents. A T47D human breast tumor cell-based reporter assay was used to examine extracts of plants and marine organisms for inhibitors of HIF-1 activation. Bioassay-guided fractionation of the lipid extract of the red alga Laurencia intricata yielded a structurally novel diterpene, laurenditerpenol (1). The structure of 1 was determined spectroscopically. The relative configurations of the substituents of each ring system were assigned on the basis of NOESY correlations. The absolute configuration of position C-1 was determined by the modified Mosher ester procedure (directly in NMR tubes). Compound 1 potently inhibited hypoxia-activated HIF-1 (IC50:  0.4 μM) and hypoxia-induced VEGF (a potent angiogenic factor) in T47D cells. Compound 1 selectively inhibits HIF-1 activation by hypoxia but not iron chelator-induced activation. Further, 1 suppresses tumor cell survival under hypoxic conditions without affecting normoxic cell growth. Compound 1 inhibits HIF-1 by blocking the induction of the oxygen-regulated HIF-1α protein. Mitochondrial respiration studies revealed that 1 suppresses oxygen consumption.

Published

2004

3. Molecular-Targeted Antitumor Agents:  The Saururus cernuus Dineolignans Manassantin B and 4-O-Demethylmanassantin B Are Potent Inhibitors of Hypoxia-Activated HIF-1

Author

Hodges, T. W., Hossain, C. F., Kim, Y.-P., Zhou, Y.-D., and Nagle, D. G.

Abstract

The transcription factor hypoxia-inducible factor-1 (HIF-1) is a key regulator of tumor cell adaptation and survival under hypoxic conditions. Selective HIF-1 inhibitors represent an important new class of potential molecular-targeted antitumor therapeutic agents. Extracts of plants and marine organisms were evaluated using a T47D human breast tumor cell-based reporter assay for HIF-1 inhibitors. Bioassay-guided fractionation of the lipid extract of Saururus cernuus resulted in the isolation of manassantin B (1) and a new compound, 4-O-demethylmanassantin B (2). The structure of 2 was determined spectroscopically. The absolute configurations of manassantin-type dineolignans have not been previously reported. Therefore, the absolute configurations of the chiral centers in each side chain were deduced from spectroscopic analysis of the Mosher MTPA ester derivatives of 1. Both 1 and 2 are among the most potent small molecule HIF-1 inhibitors discovered, to date, with IC50 values of 3 and 30 nM, respectively. Compounds 1 and 2 selectively inhibited hypoxia-activated HIF-1 in contrast to iron chelator-activated HIF-1. Compounds 1 and 2 also inhibited hypoxic induction of the angiogenic factor VEGF. Further study revealed that 1 selectively blocked the induction of HIF-1α protein, the oxygen regulated HIF-1 subunit that determines HIF-1 activity.

Published

2004

4. Reversal of Fluconazole Resistance in Multidrug Efflux-Resistant Fungi by the Dysidea arenaria Sponge Sterol 9α,11α-Epoxycholest-7-ene-3β,5α,6α,19-tetrol 6-Acetate

Author

Jacob, M. R., Hossain, C. F., Mohammed, K. A., Smillie, T. J., Clark, A. M., Walker, L. A., and Nagle, D. G.

Abstract

The sponge sterol 9α,11α-epoxycholest-7-ene-3β,5α,6α,19-tetrol 6-acetate (ECTA) (1) is the first marine natural product to reverse fluconazole resistance mediated by a Candida albicans MDR efflux pump. The IC50 of fluconazole is decreased from 300 to 8.5 μM (35-fold enhancement) when combined with 1 (3.8 μM). A revised C-6 configuration of 1 is established.

Published

2003

5. Acetylenic Acids Inhibiting Azole-Resistant Candida albicans from Pentagonia gigantifolia

Author

Li, X.-C., Jacob, M. R., ElSohly, H. N., Nagle, D. G., Smillie, T. J., Walker, L. A., and Clark, A. M.

Abstract

Antifungal bioassay-guided isolation of the ethanol extract of the roots of Pentagonia gigantifolia yielded 6-octadecynoic acid (1) and the new 6-nonadecynoic acid (2). Compounds 1 and 2 inhibited the growth of fluconazole-susceptible and -resistant Candida albicans strains. Their antifungal potencies were comparable to those of amphotericin B and fluconazole. Of particular significance is the low cytotoxicity and specific activity of 1 and 2 against C. albicans.

Published

2003

6. Marine Natural Products as Novel Antioxidant Prototypes

Author

Takamatsu, S., Hodges, T. W., Rajbhandari, I., Gerwick, W. H., Hamann, M. T., and Nagle, D. G.

Abstract

Pure natural products isolated from marine sponges, algae, and cyanobacteria were examined for antioxidant activity using a 2,2-diphenyl-1-picrylhydrazyl radical (DPPH) solution-based chemical assay and a 2‘,7‘-dichlorodihydrofluorescein diacetate (DCFH-DA) cellular-based assay. The DCFH system detects only antioxidants that penetrate cellular membranes. Potent antioxidants were identified and the results from each system compared. The algal metabolites cymopol (1), avrainvilleol (3), and fragilamide (4), and the invertebrate constituent puupehenone (5) showed strong antioxidant activity in both systems. Several compounds were active in the DPPH assay but significantly less active in the DCFH system. The green algal metabolite 7-hydroxycymopol (2) was isolated from Cymopolia barbata and its structure determined. Compound 2 was significantly less active in the DCFH system than cymopol (1). The sponge metabolites (1S)-(+)-curcuphenol (6), aaptamine (7), isoaaptamine (8), and curcudiol (9) and the cyanobacterial pigment scytonemin (10) showed strong antioxidant activity in the DPPH assay, but were relatively inactive in the DCFH system. Thus, cellular uptake dramatically affects the potential significance of antioxidants discovered using only the DPPH assay. The apparent “proantioxidants” hormothamnione A diacetate (11) and Laurencia monomer diacetate (12) require metabolic activation for antioxidant activity. Significant advantages are achieved using both a solution- and cellular-based assay to discover new antioxidants.

Published

2003

7. A New 2D-TLC Bioautography Method for the Discovery of Novel Antifungal Agents To Control Plant Pathogens

Author

Wedge, D. E. and Nagle, D. G.

Abstract

A new bioassay has been developed combining the simplicity of direct bioautography with the improved chromatographic resolution of 2D-TLC. Mixtures of structurally diverse antifungal agents were tested to establish the validity and utility of this method in the discovery of new natural products with activity against agriculturally important fungal pathogens.

Published

2000

8. Symplostatin 2:  A Dolastatin 13 Analogue from the Marine Cyanobacterium Symploca hydnoides

Author

Harrigan, G. G., Luesch, H., Yoshida, W. Y., Moore, R. E., Nagle, D. G., and Paul, V. J.

Abstract

An analogue of dolastatin 13 (2) has been isolated from a marine cyanobacterium, Symploca hydnoides, collected near Guam. This new cyclic depsipeptide contains a l-methionine sulfoxide residue; however, the sulfoxide exists as both R- and S-forms, resulting in the doubling of several signals in the ¹H and ¹³C NMR spectra. Structure elucidation required extensive application of 2-D NMR techniques such as COSY, HMQC, HMBC, and ROESY. The trivial name symplostatin 2 (1) has been assigned to the new metabolite and its isolation from S. hydnoides further supports the proposal that many compounds originally isolated from the sea hare Dolabella auricularia are most probably of cyanobacterial origin.

Published

1999

9. Tumonoic Acids, Novel Metabolites from a Cyanobacterial Assemblage of Lyngbya majuscula and Schizothrix calcicola

Author

Harrigan, G. G., Luesch, H., Yoshida, W. Y., Moore, R. E., Nagle, D. G., Biggs, J., Park, P. U., and Paul, V. J.

Abstract

Five new metabolites have been isolated from a lyngbyastatin 1- and dolastatin 12-producing assemblage of Lyngbya majuscula and Schizothrix calcicola collected at Tumon Bay, Guam. Structure elucidation employed 2D NMR techniques and chemical derivatization. These compounds have been assigned the trivial names tumonoic acids A (2), B (1), and C (5); methyl tumonoate A (3), and methyl tumonoate B (4). Compounds 1 and 4 were also found in a lyngbyastatin 1-producing strain of L. majuscula from Guam.

Published

1999

10. Isolation, Structure Determination, and Biological Activity of Dolastatin 12 and Lyngbyastatin 1 from Lyngbya majuscula/Schizothrix calcicola Cyanobacterial Assemblages

Author

Harrigan, G. G., Yoshida, W. Y., Moore, R. E., Nagle, D. G., Park, P. U., Biggs, J., Paul, V. J., Mooberry, S. L., Corbett, T. H., and Valeriote, F. A.

Abstract

Lyngbyastatin 1 (1a), a new cytotoxic analogue of dolastatins 12 (2a) and 11 (4), was isolated as an inseparable mixture with its C-15 epimer (1b) from extracts of a Lyngbya majuscula/Schizothrix calcicola assemblage and a L. majuscula strain collected near Guam. Dolastatin 12 (2a) was also encountered as an inseparable mixture with its C-15 epimer (2b) in L. majuscula/S. calcicola assemblages. At least one of the compounds in each mixture appeared to exist in solution as a mixture of slowly interconverting conformers resulting in broadened signals in ¹H NMR spectra. Structure elucidation therefore relied principally on mass spectroscopy and chemical degradation studies. Both 1ab and 2ab proved toxic with only marginal or no antitumor activity when tested against colon adenocarcinoma #38 or mammary adenocarcinoma #16/C. Both 1ab and 2ab were shown to be potent disrupters of cellular microfilament networks.

Published

1998

11. Genipatriol, a New Cycloartane Triterpene from Genipa spruceana

Author

Hossain, C. F., Jacob, M. R., Clark, A. M., Walker, L. A., and Nagle, D. G.

Abstract

Genipatriol (1), a new 2α,3β-dihydroxylated cycloartane triterpene, was isolated from the aerial parts of Genipa spruceana. The structure of genipatriol was determined by a combination of spectroscopic methods.

Published

2003

12. A New Dehydrogeranylgeraniol Antioxidant from Saururus cernuus that Inhibits Intracellular Reactive Oxygen Species (ROS)-Catalyzed Oxidation within HL-60 Cells

Author

Rajbhandari, I., Takamatsu, S., and Nagle, D. G.

Abstract

A new triene, 12,13-dehydrogeranylgeraniol (1), was isolated from the aquatic plant Saururus cernuus and its structure determined spectroscopically. Compound 1 inhibits PMA-induced peroxide-catalyzed oxidation of 2‘,7‘-dichlorodihydrofluorescein dye (DCFH) by reactive oxygen species (ROS) within human promyelocyctic HL-60 cells.

Published

2001

13. A New Indanone from the Marine Cyanobacterium Lyngbya majuscula That Inhibits Hypoxia-Induced Activation of the VEGF Promoter in Hep3B Cells

Author

Nagle, D. G., Zhou, Y.-D., Park, P. U., Paul, V. J., Rajbhandari, I., Duncan, C. J. G., and Pasco, D. S.

Abstract

A new indanone (1) has been isolated from the filamentous marine cyanobacterium Lyngbya majuscula, and its structure determined spectroscopically. Vascular endothelial growth factor (VEGF) is an important regulator of tumor angiogenesis. Compound 1 inhibits hypoxia-induced activation of the VEGF gene promoter in Hep3B human liver tumor cells, in vitro.

Published

2000

14. Symplostatin 1:  A Dolastatin 10 Analogue from the Marine Cyanobacterium Symploca hydnoides

Author

Harrigan, G. G., Luesch, H., Yoshida, W. Y., Moore, R. E., Nagle, D. G., Paul, V. J., Mooberry, S. L., Corbett, T. H., and Valeriote, F. A.

Abstract

A new solid tumor selective cytotoxic analogue of dolastatin 10 (1) has been isolated from the marine cyanobacterium Symploca hydnoides, collected near Guam. This metabolite has been assigned the trivial name symplostatin 1 (2). This discovery supports the proposal that many compounds isolated from the seahare Dolabella auricularia, the original source of the dolastatins, are of dietary origin.

Published

1998

15. Malyngamide H, an ichthyotoxic amide possessing a new carbon skeleton from the Caribbean cyanobacterium Lyngbya majuscula.

Author

Orjala J, Nagle D, and Gerwick WH

Subjects

Animals, Chromatography, Ion Exchange, Circular Dichroism, Cyclohexanones isolation & purification, Cyclohexanones toxicity, Fatty Acids, Monounsaturated isolation & purification, Fatty Acids, Monounsaturated toxicity, Goldfish, Magnetic Resonance Spectroscopy, Stereoisomerism, Toxins, Biological isolation & purification, Toxins, Biological toxicity, Cyanobacteria chemistry, Cyclohexanones chemistry, Fatty Acids, Monounsaturated chemistry, Toxins, Biological chemistry

Abstract

Guided by ichthyotoxic activity against goldfish, a new lipopeptide, malyngamide H [1], and its corresponding free acid, 7-methoxytetradec-4(E)-enoic acid [2], have been isolated from the tropical marine cyanobacterium Lyngbya majuscula. The structure of the new carbon skeleton borne by malyngamide H was elucidated on the basis of spectroscopic analysis, mainly 2D nmr. The absolute stereochemistry of the cyclohexenone moiety of malyngamide H [1] was deduced by a combination of 2D NOESY and exciton chirality circular dichroism spectroscopy.

Published

1995

16. New glycosphingolipids from the marine sponge Halichondria panicea.

Author

Nagle DG, McClatchey WC, and Gerwick WH

Subjects

Animals, Glycosphingolipids chemistry, Molecular Conformation, Molecular Structure, Optical Rotation, Glycosphingolipids isolation & purification, Porifera chemistry

Abstract

A novel sphingolipid containing an iso-fatty acid, (4E,8E)-N-13'-methyltetradecanoyl-1-O-beta-D-glucopyra nosyl-4-sphingadiene, was isolated from the Oregon marine sponge Halichondria panicea and its structure determined using a combination of spectroscopic and chemical degradation techniques. A second galactosyl-ceramide, which contained an unusually long chain fatty acid amide component, was also isolated from H. panicea.

Published

1992