4.8 Article

Intracellular Generation of a Diterpene-Peptide Conjugate that Inhibits 14-3-3-Mediated Interactions

Journal

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY
Volume 137, Issue 50, Pages 15624-15627

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/jacs.5b09817

Keywords

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Funding

  1. JSPS [25.3344, 25288076, 26102727, 26220206, 23510277]
  2. Cooperative Research Program, Network Joint Research Center for Materials and Devices, Osaka University [2015349]
  3. World Premier International Research Center Initiative (WPI), MEXT, Japan
  4. Grants-in-Aid for Scientific Research [26102728, 23510277, 25288076, 13F03344, 26102727, 26220206, 26440005, 26560445] Funding Source: KAKEN

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Synthetic agents that disrupt intracellular protein protein interactions (PPIs) are highly desirable for elucidating signaling networks and developing new therapeutics. However, designing cell-penetrating large molecules equipped with the many functional groups necessary for binding to large interfaces remains challenging. Here, we describe a rational strategy for the intracellular oxime ligation-mediated generation of an amphipathic bivalent inhibitor composed of a peptide and diterpene natural product, fusicoccin, which binds 14-3-3 protein with submicromolar affinity. Our results demonstrate that co-treatment of cells with small module molecules, the aldehyde-containing fusicoccin 1 and the aminooxy-containing peptide 2, generates the corresponding conjugate 3 in cells, resulting in significant cytotoxicity. In contrast chemically synthesized 3 is not cytotoxic, likely due to its inability to penetrate cells. compound 3, but not 1 or 2, disrupts endogenous 14-3,3/cRaf intetactions, suggesting that cell death is caused by inhibition a 14-3-3 activity. These results suggest that intracellular generation of large-sized molecules may serve as a new approach for modulating PPIs.

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