Targeting non-canonical pathways as a strategy to modulate the sodium iodide symporter

Martin Read; Katie Brookes; Caitlin Thornton; Alice Fletcher; Hannah Nieto; Mohammed Alshahrani; Rashida Khan; Patricia Borges de Souza; Ling Zha; Jamie Webster; Luke Alderwick; Moray Campbell; Kristien Boelaert; Vicki Smith; Christopher McCabe

doi:10.1016/j.chembiol.2021.07.016

Targeting non-canonical pathways as a strategy to modulate the sodium iodide symporter

Martin Read, Katie Brookes, Caitlin Thornton, Alice Fletcher, Hannah Nieto, Mohammed Alshahrani, Rashida Khan, Patricia Borges de Souza, Ling Zha, Jamie Webster, Luke Alderwick, Moray Campbell, Kristien Boelaert, Vicki Smith, Christopher McCabe

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Abstract

The sodium iodide symporter (NIS) functions to transport iodide and is critical for successful radioiodide ablation of cancer cells. Approaches to bolster NIS function and diminish recurrence post-radioiodide therapy are impeded by oncogenic pathways that suppress NIS, as well as the inherent complexity of NIS regulation. Here, we utilize NIS in high-throughput drug screening and undertake rigorous evaluation of lead compounds to identify and target key processes underpinning NIS function. We find that multiple proteostasis pathways, including proteasomal degradation and autophagy, are central to the cellular processing of NIS. Utilizing inhibitors targeting distinct molecular processes, we pinpoint combinatorial drug strategies giving robust >5-fold increases in radioiodide uptake. We also reveal significant dysregulation of core proteostasis genes in human tumors, identifying a 13-gene riskscore classifier as an independent predictor of recurrence in radioiodide-treated patients. We thus propose and discuss a model for targetable steps of intracellular processing of NIS function.

Original language	English
Pages (from-to)	1-23
Number of pages	23
Journal	Cell Chemical Biology
Volume	2021
DOIs	https://doi.org/10.1016/j.chembiol.2021.07.016
Publication status	Published - 13 Sept 2021

Keywords

NIS
VCP
autophagy
drug screening
proteasome
protein homeostasis
radioiodide
recurrence
risk score
thyroid cancer

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.chembiol.2021.07.016Licence: Creative Commons: Attribution (CC BY)

ReadM2021Targeting
Read et al., Targeting non-canonical pathways as a strategy to modulate the sodium iodide symporter, Cell Chemical Biology (2021), https://doi.org/10.1016/j.chembiol.2021.07.016
Final published version, 6.2 MBLicence: Creative Commons: Attribution (CC BY)

Re-Engineering Radioiodine Therapy for the 21st Century
Smith, V., McCabe, C. & Boelaert, K.
Medical Research Council
1/12/16 → 30/09/21
Project: Research Councils

Cite this

Read, M., Brookes, K., Thornton, C., Fletcher, A., Nieto, H., Alshahrani, M., Khan, R., Borges de Souza, P., Zha, L., Webster, J., Alderwick, L., Campbell, M., Boelaert, K., Smith, V., & McCabe, C. (2021). Targeting non-canonical pathways as a strategy to modulate the sodium iodide symporter. Cell Chemical Biology, 2021, 1-23. https://doi.org/10.1016/j.chembiol.2021.07.016

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abstract = "The sodium iodide symporter (NIS) functions to transport iodide and is critical for successful radioiodide ablation of cancer cells. Approaches to bolster NIS function and diminish recurrence post-radioiodide therapy are impeded by oncogenic pathways that suppress NIS, as well as the inherent complexity of NIS regulation. Here, we utilize NIS in high-throughput drug screening and undertake rigorous evaluation of lead compounds to identify and target key processes underpinning NIS function. We find that multiple proteostasis pathways, including proteasomal degradation and autophagy, are central to the cellular processing of NIS. Utilizing inhibitors targeting distinct molecular processes, we pinpoint combinatorial drug strategies giving robust >5-fold increases in radioiodide uptake. We also reveal significant dysregulation of core proteostasis genes in human tumors, identifying a 13-gene riskscore classifier as an independent predictor of recurrence in radioiodide-treated patients. We thus propose and discuss a model for targetable steps of intracellular processing of NIS function.",

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author = "Martin Read and Katie Brookes and Caitlin Thornton and Alice Fletcher and Hannah Nieto and Mohammed Alshahrani and Rashida Khan and {Borges de Souza}, Patricia and Ling Zha and Jamie Webster and Luke Alderwick and Moray Campbell and Kristien Boelaert and Vicki Smith and Christopher McCabe",

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AU - Khan, Rashida

AU - Borges de Souza, Patricia

AU - Zha, Ling

AU - Webster, Jamie

AU - Alderwick, Luke

AU - Campbell, Moray

AU - Boelaert, Kristien

AU - Smith, Vicki

AU - McCabe, Christopher

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AB - The sodium iodide symporter (NIS) functions to transport iodide and is critical for successful radioiodide ablation of cancer cells. Approaches to bolster NIS function and diminish recurrence post-radioiodide therapy are impeded by oncogenic pathways that suppress NIS, as well as the inherent complexity of NIS regulation. Here, we utilize NIS in high-throughput drug screening and undertake rigorous evaluation of lead compounds to identify and target key processes underpinning NIS function. We find that multiple proteostasis pathways, including proteasomal degradation and autophagy, are central to the cellular processing of NIS. Utilizing inhibitors targeting distinct molecular processes, we pinpoint combinatorial drug strategies giving robust >5-fold increases in radioiodide uptake. We also reveal significant dysregulation of core proteostasis genes in human tumors, identifying a 13-gene riskscore classifier as an independent predictor of recurrence in radioiodide-treated patients. We thus propose and discuss a model for targetable steps of intracellular processing of NIS function.

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KW - drug screening

KW - proteasome

KW - protein homeostasis

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KW - recurrence

KW - risk score

KW - thyroid cancer

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SP - 1

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JO - Cell Chemical Biology

JF - Cell Chemical Biology

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Targeting non-canonical pathways as a strategy to modulate the sodium iodide symporter

Abstract

Keywords

UN SDGs

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Projects

Re-Engineering Radioiodine Therapy for the 21st Century

Cite this