4.6 Article

Development of a High-throughput NanoBRET Screening Platform to Identify Modulators of the RAS/RAF Interaction

MOLECULAR CANCER THERAPEUTICS (2021)

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Journal

MOLECULAR CANCER THERAPEUTICS
Volume 20, Issue 9, Pages 1743-1754

Publisher

AMER ASSOC CANCER RESEARCH
DOI: 10.1158/1535-7163.MCT-21-0175

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Categories

Oncology

Funding

  1. NCI, NIH [HHSN261200800001E]
  2. Intramural Research Program of the NIH, NCI, Center for Cancer Research [ZIA BC010329, ZIA BC 011469]

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This study utilized a NanoBRET screening platform to identify compounds that inhibit the binding between activated KRAS and CRAF kinase, leading to suppression of RAS-driven ERK activation. However, some compounds were found to enhance the interaction and upregulate pathway signaling.
Activating mutations in RAS are found in approximately 30% of human cancers, resulting in the delivery of a persistent signal to critical downstream effectors that drive tumorigenesis. RAS-driven malignancies respond poorly to conventional cancer treatments and inhibitors that target RAS directly are limited; therefore, the identification of new strategies and/or drugs to disrupt RAS signaling in tumor cells remains a pressing therapeutic need. Taking advantage of the live-cell bioluminescence resonance energy transfer (BRET) methodology, we describe the development of a NanoBRET screening platform to identify compounds that modulate binding between activated KRAS and the CRAF kinase, an essential effector of RAS that initiates ERK cascade signaling. Using this strategy, libraries containing synthetic compounds, targeted inhibitors, purified natural products, and natural product extracts were evaluated. These efforts resulted in the identification of compounds that inhibit RAS/RAF binding and in turn suppress RAS-driven ERK activation, but also compounds that have the deleterious effect of enhancing the interaction to upregulate pathway signaling. Among the inhibitor hits identified, the majority were compounds derived from natural products, including ones reported to alter KRAS nanoclustering (ophiobolin A), to impact RAF function (HSP90 inhibitors and ROS inducers) as well as some with unknown targets and activities. These findings demonstrate the potential for this screening platform in natural product drug discovery and in the development of new therapeutic agents to target dysregulated RAS signaling in human disease states such as cancer.

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