Pyrazine ring-based Na+/H+ exchanger (NHE) inhibitors potently inhibit cancer cell growth in 3D culture, independent of NHE1

Rolver, Michala G; Elingaard-Larsen, Line O; Andersen, Anne Poder; Counillon, Laurent; Pedersen, Stine Falsig

doi:10.1038/s41598-020-62430-z

Cited by 44 publications

(26 citation statements)

References 55 publications

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“…One such pathway is paraptosis, in which ER and mitochondria dilate in absence of classical features of apoptosis and necrosis [ 187 ]. The process is induced by a number of natural compounds and anticancer drugs [ 188 ], including compounds previously considered specific NHE1 inhibitors [ 189 ] and is of interest in the treatment of cancer cells, which have downregulated apoptotic machinery. Notably, while the mechanisms involved in paraptosis are still incompletely understood, substantial evidence links it to Ca 2+ dysregulation, and also BK channel dysfunction and disturbed K + homeostasis has been suggested [ 188 ].…”

Section: Cancer Cell Functions Driven By Changes In Mitochondrial Architecturementioning

confidence: 99%

The Interplay between Dysregulated Ion Transport and Mitochondrial Architecture as a Dangerous Liaison in Cancer

Pedersen

Flinck

Pardo

2021

IJMS

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Transport of ions and nutrients is a core mitochondrial function, without which there would be no mitochondrial metabolism and ATP production. Both ion homeostasis and mitochondrial phenotype undergo pervasive changes during cancer development, and both play key roles in driving the malignancy. However, the link between these events has been largely ignored. This review comprehensively summarizes and critically discusses the role of the reciprocal relationship between ion transport and mitochondria in crucial cellular functions, including metabolism, signaling, and cell fate decisions. We focus on Ca2+, H+, and K+, which play essential and highly interconnected roles in mitochondrial function and are profoundly dysregulated in cancer. We describe the transport and roles of these ions in normal mitochondria, summarize the changes occurring during cancer development, and discuss how they might impact tumorigenesis.

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Section: Cancer Cell Functions Driven By Changes In Mitochondrial Architecturementioning

confidence: 99%

The Interplay between Dysregulated Ion Transport and Mitochondrial Architecture as a Dangerous Liaison in Cancer

Pedersen

Flinck

Pardo

2021

IJMS

Self Cite

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“…11 Furthermore, the use of ion transport inhibitors is very common 12,13 but recent studies have reported significant off-target effects of various pHi-lowering drugs. 14,15 Micropipette pHi manipulation techniques are highly specific and adaptable to single-cell analysis. 16 However, micropipette pHi manipulation is technically challenging, has poor temporal control, is damaging to the cell, and is low-throughput.…”

Section: Introductionmentioning

confidence: 99%

An optogenetic tool to raise intracellular pH in single cells and drive localized membrane dynamics

Donahue

Siroky

White

2021

Preprint

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Intracellular pH (pHi) dynamics are critical for regulating normal cell physiology. For example, transient increases in pHi (7.2-7.6) regulate cell behaviors like cell polarization, actin cytoskeleton remodeling, and cell migration. Most studies on pH-dependent cell behaviors have been performed at the population level and use non-specific methods to manipulate pHi. The lack of tools to specifically manipulate pHi at the single-cell level has hindered investigation of the role of pHi dynamics in driving single cell behaviors. In this work, we show that Archaerhodopsin (ArchT), a light-driven outward proton pump, can be used to elicit robust and physiological pHi increases over the minutes timescale. We show that activation of ArchT is repeatable, enabling the maintenance of high pHi in single cells for approximately 45 minutes. We apply this spatiotemporal pHi manipulation tool to determine whether increased pHi is a sufficient driver of membrane ruffling in single cells. Using the ArchT tool, we show that increased pHi in single cells can drive localized membrane ruffling responses within seconds and 2 increased membrane dynamics (both protrusion and retraction events) compared to control cells. Overall, this tool allows us to directly investigate the relationship between increased pHi and cell behaviors such as membrane ruffling. This tool will be transformative in facilitating the experiments required to determine if increased pHi is a driver of these cell behaviors at the single-cell level.

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“…The work described above suggests that the cell biological and biochemical effects of increased pHi in cancer correlate with and perhaps reinforce transcriptional and proteostatic changes associated with cancer. However, several recent papers that note off-target effects of key pHi manipulating drugs [ 130 , 131 ] have begun to call into question the previous causative role of cytosolic pH in driving tumorigenic phenotypes at the population level. Indeed, the work in this field so far has been crippled by the lack of tools to spatiotemporally manipulate and measure pHi across multiple cancer model systems (cell lines, organoids, and in vivo models) to determine the roles of pHi dynamics across biological scales.…”

Section: Discussionmentioning

confidence: 99%

Cancer and pH Dynamics: Transcriptional Regulation, Proteostasis, and the Need for New Molecular Tools

Czowski

Romero-Moreno

Trull

et al. 2020

Cancers

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An emerging hallmark of cancer cells is dysregulated pH dynamics. Recent work has suggested that dysregulated intracellular pH (pHi) dynamics enable diverse cancer cellular behaviors at the population level, including cell proliferation, cell migration and metastasis, evasion of apoptosis, and metabolic adaptation. However, the molecular mechanisms driving pH-dependent cancer-associated cell behaviors are largely unknown. In this review article, we explore recent literature suggesting pHi dynamics may play a causative role in regulating or reinforcing tumorigenic transcriptional and proteostatic changes at the molecular level, and discuss outcomes on tumorigenesis and tumor heterogeneity. Most of the data we discuss are population-level analyses; lack of single-cell data is driven by a lack of tools to experimentally change pHi with spatiotemporal control. Data is also sparse on how pHi dynamics play out in complex in vivo microenvironments. To address this need, at the end of this review, we cover recent advances for live-cell pHi measurement at single-cell resolution. We also discuss the essential role for tool development in revealing mechanisms by which pHi dynamics drive tumor initiation, progression, and metastasis.

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Pyrazine ring-based Na+/H+ exchanger (NHE) inhibitors potently inhibit cancer cell growth in 3D culture, independent of NHE1

Cited by 44 publications

References 55 publications

The Interplay between Dysregulated Ion Transport and Mitochondrial Architecture as a Dangerous Liaison in Cancer

The Interplay between Dysregulated Ion Transport and Mitochondrial Architecture as a Dangerous Liaison in Cancer

An optogenetic tool to raise intracellular pH in single cells and drive localized membrane dynamics

Cancer and pH Dynamics: Transcriptional Regulation, Proteostasis, and the Need for New Molecular Tools

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