TXNIP loss expands Myc-dependent transcriptional programs by increasing Myc genomic binding

Lim, Tian-Yeh; Wilde, Blake R.; Thomas, Mallory L; Murphy, Kristin; Vahrenkamp, Jeffery M.; Conway, Megan E; Varley, Katherine E.; Gertz, Jason; Ayer, Donald E.

doi:10.1371/journal.pbio.3001778

Cited by 5 publications

(4 citation statements)

References 75 publications

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“…Lim et al [ 23 ] discovered that TXNIP loss increases MYC-dependent gene expression by increasing Myc genome occupancy in several types of cells rather than by directly affecting MYC protein expression. Consistent with the findings of Lim et al [ 23 ], it was observed that knocking down Txnip in NP cells did not significantly alter the expression of MYC (Fig. 5 g; Additional file 1 : Fig.…”

Section: Resultsmentioning

confidence: 99%

“…MYC directly promotes the cellular uptake of glutamine by increasing the transcription of SLC1A5 (the main glutamine transporter) through the enhancer box (E-box, CACGTG) [ 26 ]. Intriguingly, Lim et al [ 23 ] reported that MYC-dependent genes affected by TXNIP loss are highly and significantly enriched for canonical CACGTG MYC-binding E-boxes. Our transcriptomic analysis also revealed a significant upregulation of Slc1a5 expression in response to mannose (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…In this study, focus was placed on Myc , the primary gene of interest, and found that mannose does not affect MYC protein expression but directly influences the levels of SLC1A5 and intracellular glutamine. Lim et al [ 23 ] reported that knocking down Txnip does not affect MYC protein levels but that intracellular Txnip knockdown can increase MYC genomic binding in various cell types. Therefore, it is believed that mannose upregulates the Txnip gene, which reduces MYC genomic binding, leading to the downregulation of SLC1A5 and consequently affecting intracellular glutamine levels.…”

Section: Discussionmentioning

confidence: 99%

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D-mannose alleviates intervertebral disc degeneration through glutamine metabolism

Dong,

Jiao,

Wang

et al. 2024

Military Med Res

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Background Intervertebral disc degeneration (IVDD) is a multifaceted condition characterized by heterogeneity, wherein the balance between catabolism and anabolism in the extracellular matrix of nucleus pulposus (NP) cells plays a central role. Presently, the available treatments primarily focus on relieving symptoms associated with IVDD without offering an effective cure targeting its underlying pathophysiological processes. D-mannose (referred to as mannose) has demonstrated anti-catabolic properties in various diseases. Nevertheless, its therapeutic potential in IVDD has yet to be explored. Methods The study began with optimizing the mannose concentration for restoring NP cells. Transcriptomic analyses were employed to identify the mediators influenced by mannose, with the thioredoxin-interacting protein (Txnip) gene showing the most significant differences. Subsequently, small interfering RNA (siRNA) technology was used to demonstrate that Txnip is the key gene through which mannose exerts its effects. Techniques such as colocalization analysis, molecular docking, and overexpression assays further confirmed the direct regulatory relationship between mannose and TXNIP. To elucidate the mechanism of action of mannose, metabolomics techniques were employed to pinpoint glutamine as a core metabolite affected by mannose. Next, various methods, including integrated omics data and the Gene Expression Omnibus (GEO) database, were used to validate the one-way pathway through which TXNIP regulates glutamine. Finally, the therapeutic effect of mannose on IVDD was validated, elucidating the mechanistic role of TXNIP in glutamine metabolism in both intradiscal and orally treated rats. Results In both in vivo and in vitro experiments, it was discovered that mannose has potent efficacy in alleviating IVDD by inhibiting catabolism. From a mechanistic standpoint, it was shown that mannose exerts its anti-catabolic effects by directly targeting the transcription factor max-like protein X-interacting protein (MondoA), resulting in the upregulation of TXNIP. This upregulation, in turn, inhibits glutamine metabolism, ultimately accomplishing its anti-catabolic effects by suppressing the mitogen-activated protein kinase (MAPK) pathway. More importantly, in vivo experiments have further demonstrated that compared with intradiscal injections, oral administration of mannose at safe concentrations can achieve effective therapeutic outcomes. Conclusions In summary, through integrated multiomics analysis, including both in vivo and in vitro experiments, this study demonstrated that mannose primarily exerts its anti-catabolic effects on IVDD through the TXNIP-glutamine axis. These findings provide strong evidence supporting the potential of the use of mannose in clinical applications for alleviating IVDD. Compared to existing clinically invasive or pain-relieving therapies for IVDD, the oral administration of mannose has characteristics that are more advantageous for clinical IVDD treatment.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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D-mannose alleviates intervertebral disc degeneration through glutamine metabolism

Dong,

Jiao,

Wang

et al. 2024

Military Med Res

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“…At the same time, metabolic stress activates metabolic sensors, such as MondoA, which is able to reduce glucose uptake and aerobic glycolysis via induction of thioredoxin-interacting protein (TXNIP) [ 135 , 136 ]. TXNIP activation decreases the genome occupancy of MYC, thereby inhibiting its transactivating function [ 137 ]. However, the functional relationship between MYC and MondoA is tumor type-specific and influenced by altered MYC levels.…”

Section: Conclusion and Potential Therapeutic Aspectsmentioning

confidence: 99%

Rewired Metabolism Caused by the Oncogenic Deregulation of MYC as an Attractive Therapeutic Target in Cancers

Vízkeleti

Spisák

2023

Cells

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MYC is one of the most deregulated oncogenes on multiple levels in cancer. As a node transcription factor, MYC plays a diverse regulatory role in many cellular processes, including cell cycle and metabolism, both in physiological and pathological conditions. The relentless growth and proliferation of tumor cells lead to an insatiable demand for energy and nutrients, which requires the rewiring of cellular metabolism. As MYC can orchestrate all aspects of cellular metabolism, its altered regulation plays a central role in these processes, such as the Warburg effect, and is a well-established hallmark of cancer development. However, our current knowledge of MYC suggests that its spatial- and concentration-dependent contribution to tumorigenesis depends more on changes in the global or relative expression of target genes. As the direct targeting of MYC is proven to be challenging due to its relatively high toxicity, understanding its underlying regulatory mechanisms is essential for the development of tumor-selective targeted therapies. The aim of this review is to comprehensively summarize the diverse forms of MYC oncogenic deregulation, including DNA-, transcriptional- and post-translational level alterations, and their consequences for cellular metabolism. Furthermore, we also review the currently available and potentially attractive therapeutic options that exploit the vulnerability arising from the metabolic rearrangement of MYC-driven tumors.

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Amino acid deprivation induces TXNIP expression by NRF2 downregulation

Ahn,

Jang,

Kim

et al. 2023

IUBMB Life

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Thioredoxin‐interacting protein (TXNIP) is sensitive to oxidative stress and is involved in the pathogenesis of various metabolic, cardiovascular, and neurodegenerative disorders. Therefore, several studies have suggested that TXNIP is a promising therapeutic target for several diseases, particularly cancer and diabetes. However, the regulation of TXNIP expression under amino acid (AA)‐restricted conditions is not well understood. In the present study, we demonstrated that TXNIP expression was promoted by the deprivation of AAs, especially arginine, glutamine, lysine, and methionine, in non‐small cell lung cancer (NSCLC) cells. Interestingly, we determined that increased TXNIP expression induced by AA deprivation was associated with nuclear factor erythroid 2‐related factor 2 (NRF2) downregulation, but not with activating transcription factor 4 (ATF4) activation. Furthermore, N‐acetyl‐l‐cysteine (NAC), a scavenger of reactive oxygen species (ROS), suppressed TXNIP expression in NSCLC cells deprived of AA. Collectively, the induction of TXNIP expression by AA deprivation was mediated by ROS production, potentially through NRF2 downregulation. Our findings suggest that TXNIP expression may be associated with the redox homeostasis of AA metabolism and provide a possible rationale for a therapeutic strategy to treat cancer with AA restriction.

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TXNIP loss expands Myc-dependent transcriptional programs by increasing Myc genomic binding

Cited by 5 publications

References 75 publications

D-mannose alleviates intervertebral disc degeneration through glutamine metabolism

D-mannose alleviates intervertebral disc degeneration through glutamine metabolism

Rewired Metabolism Caused by the Oncogenic Deregulation of MYC as an Attractive Therapeutic Target in Cancers

Amino acid deprivation induces TXNIP expression by NRF2 downregulation

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