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Literature DB >> 32616180

Yohimbine as a Starting Point to Access Diverse Natural Product-Like Agents with Re-programmed Activities against Cancer-Relevant GPCR Targets.

Nicholas G Paciaroni¹, Verrill M Norwood¹, Ranjala Ratnayake¹, Hendrik Luesch², Robert W Huigens³.

Abstract

G protein-coupled receptors (GPCRs) constitute the largest protein superfamily in the human genome. GPCRs play key roles in mediating a wide variety of physiological events including proliferation and cancer metastasis. Given the major roles that GPCRs play in mediating cancer growth, they present promising targets for small molecule therapeutics. One of the principal goals of our lab is to identify complex natural products (NPs) suitable for ring distortion, or the dramatic altering of the inherently complex architectures of NPs, to rapidly generate an array of compounds with diverse molecular skeletal systems. The overarching goal of our ring distortion approach is to re-program the biological activity of select natural products and identify new compounds of importance to the treatment of disease, such as cancer. Described herein are the results from biological screens of diverse small molecules derived from the indole alkaloid yohimbine against a panel of GPCRs involved in various diseases. Several analogues displayed highly differential antagonistic activities across the GPCRs tested. We highlight the re-programmed profile of one analogue, Y7g, which exhibited selective antagonistic activities against AVPR2 (IC50 = 459 nM) and OXTR (IC50 = 1.16 µM). The activity profile of Y7g could correlate its HIF-dependent anti-cancer activity to its GPCR antagonism since these receptors are known to be upregulated in hypoxic cellular environments. Our findings demonstrate that the ring distortion of yohimbine can lead to the identification of new compounds capable of interacting with distinct cancer-relevant targets.

Entities: CellLine Chemical Disease Gene Species

Keywords: Cancer; Drug discovery; GPCR drug targets; Indole alkaloids; Ring distortion; Yohimbine

Mesh：

Substances：

Year: 2020 PMID： 32616180 PMCID： PMC7392148 DOI： 10.1016/j.bmc.2020.115546

Source DB: PubMed Journal: Bioorg Med Chem ISSN： 0968-0896 Impact factor: 3.641

52 in total

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Yohimbine as a Starting Point to Access Diverse Natural Product-Like Agents with Re-programmed Activities against Cancer-Relevant GPCR Targets.

Review 1. Natural products and their biological targets: proteomic and metabolomic labeling strategies.

2. Follicle-Stimulating Hormone Receptor Is Expressed by Most Ovarian Cancer Subtypes and Is a Safe and Effective Immunotherapeutic Target.

Review 3. How were new medicines discovered?

4. Discovery of Amantamide, a Selective CXCR7 Agonist from Marine Cyanobacteria.

5. Biology-oriented synthesis: harnessing the power of evolution.

6. Agonist and antagonist actions of yohimbine as compared to fluparoxan at alpha(2)-adrenergic receptors (AR)s, serotonin (5-HT)(1A), 5-HT(1B), 5-HT(1D) and dopamine D(2) and D(3) receptors. Significance for the modulation of frontocortical monoaminergic transmission and depressive states.

7. A Tryptoline Ring-Distortion Strategy Leads to Complex and Diverse Biologically Active Molecules from the Indole Alkaloid Yohimbine.

Review 8. Principles of early drug discovery.

9. Diversity-oriented synthesis yields novel multistage antimalarial inhibitors.

10. Chromopynones are pseudo natural product glucose uptake inhibitors targeting glucose transporters GLUT-1 and -3.

1. Re-engineering natural products to engage new biological targets.

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3. Limonin as a Starting Point for the Construction of Compounds with High Scaffold Diversity.

4. Synthesis of Conformationally Liberated Yohimbine Analogues and Evaluation of Cytotoxic Activity.

Review 5. An Insight into GPCR and G-Proteins as Cancer Drivers.