Horst Flotow
Indiana University Bloomington
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Publication
Featured researches published by Horst Flotow.
Phytochemistry | 2002
Simon P. B. Ovenden; Shugeng Cao; Chungyan Leong; Horst Flotow; Mahabir P. Gupta; Antony D. Buss; Mark S. Butler
Crude MeOH extracts from the stem bark and leaves of a Panamanian specimen of Albizia adinocephala (Leguminosae) were found to inhibit the malarial enzyme plasmepsin II. Bioassay guided fractionation led to the isolation of two new bioactive spermine alkaloids, budmunchiamines L4 and L5.
Journal of Biomolecular Screening | 2002
Horst Flotow; Chungyan Leong; Antony D. Buss
Despite decades of research, malaria remains the worlds most deadly parasitic disease. New treatments with novel mechanisms of action are urgently needed. Plasmepsin II is an aspartyl protease that has been validated as an antimalarial therapeutic target enzyme. Although natural products form the basis of most modern antimalarial drugs, no systematic high-throughput screening has been reported against this target. We have designed an effective strategy for carrying out high-throughput screening of an extensive library of natural products that uses a fluorescence resonance energy transfer primary screening assay in tandem with a fluorescence polarization assay. This strategy allows rapid screening of the library coupled with effective discrimination and elimination of false-positive samples and selection of true hits for chemical isolation of inhibitors of plasmepsin II.
The Journal of Antibiotics | 2013
Brinda Somanadhan; Santosh R. Kotturi; Chung Yan Leong; Robert P. Glover; Yicun Huang; Horst Flotow; Antony D. Buss; Martin J. Lear; Mark S. Butler
A 384-well microtitre plate fluorescence cleavage assay was developed to identify inhibitors of the cysteine protease falcipain-2, an important antimalarial drug target. Bioassay-guided isolation of a MeOH extract from a myxobacterium Chitinophaga sp. Y23 isolated from soil collected in Singapore, led to the identification of a new acyltetrapeptide, falcitidin (1), which displayed an IC50 value of 6 μM against falcipain-2. The planar structure of 1 was secured by NMR and MS/MS analysis. Attempts to isolate further material for biological testing were hampered by inconsistent production and by a low yield (<100 μg l−1). The absolute configuration of 1 was determined by Marfey’s analysis and the structure was confirmed through total synthesis as isovaleric acid-D-His-L-Ile-L-Val-L-Pro-NH2. Falcitidin (1) is the first member of a new class of falcipain-2 inhibitors and, unlike other peptide-based inhibitors, does not contain reactive groups that irreversibly bind to active cysteine sites.
Journal of Biological Chemistry | 1990
Horst Flotow; Paul R. Graves; Aiqun Wang; Carol J. Fiol; Roger W. Roeske; Peter J. Roach
Journal of Biological Chemistry | 2003
Shing-Leng Chan; Mei Chin Lee; Kuan Onn Tan; Lay-Kien Yang; Alex S. Y. Lee; Horst Flotow; Nai Yang Fu; Mark S. Butler; D. Doel Soejarto; Antony D. Buss; Victor C. Yu
Journal of Biological Chemistry | 1991
Horst Flotow; Peter J. Roach
Journal of Biological Chemistry | 1989
Horst Flotow; Peter J. Roach
Journal of Natural Products | 2002
Jin-Feng Hu; John A. Schetz; Michelle Kelly; Jiangnan Peng; Kenny K. H. Ang; Horst Flotow; Chung Yan Leong; Siew Bee Ng; Antony D. Buss; Scott P. Wilkins; Mark T. Hamann
Journal of Natural Products | 2002
Shugeng Cao; Alex S. Y. Lee; Yicun Huang; Horst Flotow; Siewbee Ng; Mark S. Butler; Antony D. Buss
Archive | 2006
Antony D. Buss; Mark S. Butler; Horst Flotow; Yogonathan Kanagasundaram; Bernard Mach; Krzysztof Masternak; Chee Wee Phoon; Mui Mui Sim; Peter Traxler; Stephen R. Whitton; Guo Xuming