Abstract

Natural products have immense structural diversity and interact with a wide range of proteins in diverse organisms and, due to structural homology, also in humans. This proposal seeks to develop a toolbox of reagents and reactions that will enable simultaneous arming and structure- activity studies (SAR) of natural products (NPs). The SAR studies may identify potential new activities of the NP derivatives and will also ensure that initial biological activity has not been lost. While not a Specific Aim of this grant given the scope of this RFA, the arming aspect leads to NP derivatives that are equipped for subsequent conjugation to various tags via Sharpless-Huisgen cycloadditions, enabling biological studies such as mechanism of action (MOA) studies (including off-targets) and provide useful probes for basic cell biology. The long-term objective is to develop a more systemized approach to mine the rich potential of NPs as activators/inactivators of cellular pathways contributing to chemical genetics. The team includes a synthetic organic chemist (D. Romo), an analytical chemist (G. Vigh), a bioorganic/biosynthetic chemist (C. Watanabe), and a biochemist/molecular biologist (J. Liu, Johns Hopkins). We propose to further develop a set of chemo- and site selective reactions employing bifunctional reagents to obtain NP derivatives that are also useful cellular probes. These studies will contribute to a fundamental understanding of the chemo- and site selectivity of various reactions in the context of complex NPs. We have established collaborations with synthetic, biosynthetic, and isolation chemists and they have provided or agreed to provide ~25 bioactive NPs for the proposed studies. Primary reactions to be studied are Rh(II)-promoted O-H insertion reactions, C-H aminations and alkene aziridinations with metal nitrenoids, and mild aryl halogenations. After an initial site non-selective step, we will employ robust/versatile NP derivative purification methods, re- assay the resulting pure derivatives (SAR studies), and determine the most appropriate site for tag attachment, i.e. find the derivatives that retain the greatest bioactivity. We will also screen for potential novel bioactivities of the NP derivatives in various cellular assays and make quantities available to the Molecular Libraries Small Molecule Repository. The subsequent development of both chemo and site-selective versions of the initial reactions will rely on screening various chiral metal complexes, and robust methods for reaction monitoring (LC-MSn) and semi-preparative HPLC purification, to modulate site-selectivity via a type of """"""""double asymmetric synthesis."""""""" ? ?

Public Health Relevance

The long-term objective of this project is the development of a more systematized approach to mine the rich potential of natural products as activators and inactivators of cellular pathways. Natural products have a rich history as tools for identification of novel therapeutic targets for human disease and as lead structures for drug development. Results from these studies will be directly relevant to human disease including diabetes, inflammation, and cancer since novel methods are proposed for derivatization of natural products (this proposal) pertinent to these disease. Subsequent SAR studies (this proposal) will be pursued to identify potential new bioactivities and suitable sites for probe attachment enabling subsequent mode of action studies (not in this proposal) relevant to these diseases. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM086307-01
Application #
7559825
Study Section
Special Emphasis Panel (ZRG1-BCMB-H (50))
Program Officer
Schwab, John M
Project Start
2008-09-12
Project End
2011-06-30
Budget Start
2008-09-12
Budget End
2009-06-30
Support Year
1
Fiscal Year
2008
Total Cost
$377,447
Indirect Cost

  Institution

Name
Texas A&M University
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
078592789
City
College Station
State
TX
Country
United States
Zip Code
77845

  Publications

Mori, Shogo; Williams, Howard; Cagle, Davey et al. (2015) Macrolactone Nuiapolide, Isolated from a Hawaiian Marine Cyanobacterium, Exhibits Anti-Chemotactic Activity. Mar Drugs 13:6274-90
Robles, Omar; Romo, Daniel (2014) Chemo- and site-selective derivatizations of natural products enabling biological studies. Nat Prod Rep 31:318-34
Li, Jing; Cisar, Justin S; Zhou, Cong-Ying et al. (2013) Simultaneous structure-activity studies and arming of natural products by C-H amination reveal cellular targets of eupalmerin acetate. Nat Chem 5:510-7
Robles, Omar; Serna-Saldívar, Sergio O; Gutiérrez-Uribe, Janet A et al. (2012) Cyclopropanations of olefin-containing natural products for simultaneous arming and structure activity studies. Org Lett 14:1394-7
Chamni, Supakarn; He, Qing-Li; Dang, Yongjun et al. (2011) Diazo reagents with small steric footprints for simultaneous arming/SAR studies of alcohol-containing natural products via O-H insertion. ACS Chem Biol 6:1175-81
Agunanne, Enoch; Horvat, Darijana; Harrison, Recherael et al. (2011) Marinobufagenin levels in preeclamptic patients: a preliminary report. Am J Perinatol 28:509-14
Abi-Ghanem, Daad; Lai, Xinzhong; Berghman, Luc R et al. (2011) A chemifluorescent immunoassay for the determination of marinobufagenin in body fluids. J Immunoassay Immunochem 32:31-46
Zhou, Cong-Ying; Li, Jing; Peddibhotla, Satyamaheshwar et al. (2010) Mild arming and derivatization of natural products via an In(OTf)3-catalyzed arene iodination. Org Lett 12:2104-7