Glucose transporter GLUT1 expression and clinical outcome in solid tumors: a systematic review and meta-analysis

Ji, Wang; Ye, Chenyang; Chen, Cong; Xiong, Hanchu; Xie, Binbin; Zhou, Jichun; Chen, Yongxia; Zheng, Shu; Wang, Linbo

doi:10.18632/oncotarget.15171

Cited by 151 publications

(165 citation statements)

References 42 publications

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“…Subsequently, excessive expression of GLUT1 have been found in many types of tumours. These neoplasms with higher GLUT1 presence have usually a poorer prognosis than those with lower levels 20. A worst outcome also for patients expressing high levels of GLUT1 in SCC has been reported by the present study.…”

supporting

confidence: 64%

Early squamous cell lung carcinoma: prognostic biomarkers for the many

Pezzella

2019

Thorax

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supporting

confidence: 64%

Early squamous cell lung carcinoma: prognostic biomarkers for the many

Pezzella

2019

Thorax

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“…Analysis of a TCGA lung adenocarcinoma cohort determined an inverse correlation between expression of LIMD1 and HIF target genes SLC2A1 , GAPDH and IGF2BP2 . Overexpression of glucose transporter 1 (GLUT‐1), the uniporter protein encoded by the SLC2A1 gene, is correlated with poor survival in most solid tumours (Wang et al , ), and selective GLUT‐1 inhibition has been demonstrated to inhibit glucose uptake and reduce viability of lung adenocarcinoma and squamous cell carcinoma cell lines in vitro and in vivo (Goodwin et al , ). Correlative studies have also determined upregulation or de novo expression of the IGF2BP family of oncofetal proteins across a number of solid tumours to be associated with tumour aggressiveness, metastasis and poorer overall survival (Bell et al , ).…”

Section: Discussionmentioning

confidence: 99%

A HIF – LIMD 1 negative feedback mechanism mitigates the pro‐tumorigenic effects of hypoxia

et al. 2018

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The adaptive cellular response to low oxygen tensions is mediated by the hypoxia‐inducible factors (HIFs), a family of heterodimeric transcription factors composed of HIF‐α and HIF‐β subunits. Prolonged HIF expression is a key contributor to cellular transformation, tumorigenesis and metastasis. As such, HIF degradation under hypoxic conditions is an essential homeostatic and tumour‐suppressive mechanism. LIMD1 complexes with PHD2 and VHL in physiological oxygen levels (normoxia) to facilitate proteasomal degradation of the HIF‐α subunit. Here, we identify LIMD1 as a HIF‐1 target gene, which mediates a previously uncharacterised, negative regulatory feedback mechanism for hypoxic HIF‐α degradation by modulating PHD2‐LIMD1‐VHL complex formation. Hypoxic induction of LIMD1 expression results in increased HIF‐α protein degradation, inhibiting HIF‐1 target gene expression, tumour growth and vascularisation. Furthermore, we report that copy number variation at the LIMD1 locus occurs in 47.1% of lung adenocarcinoma patients, correlates with enhanced expression of a HIF target gene signature and is a negative prognostic indicator. Taken together, our data open a new field of research into the aetiology, diagnosis and prognosis of LIMD1‐negative lung cancers.

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“…50 What makes it especially relevant is that GLUT1 expression is upregulated by hypoxia-induced factor 1 (HIF-1) and is highly correlated with poor prognosis and survival in most solid tumors. 51,52 In summary, these results demonstrate for the first time the utility of QC-1 for multiplexed NIR FRET-MFLI imaging in living intact mice carrying tumor xenografts. 2-DG is useful for delineation of tumor margins thus eliminating the reliance on donor intensity-based ROI selection.…”

Section: Multiplexed Mfli-fret In Vivo Whole-body Imagingmentioning

confidence: 68%

Multiplexed Non-invasive in vivo Imaging to Assess Metabolism and Receptor Engagement in Tumor Xenografts

Rudkouskaya

Sinsuebphon

Ochoa

et al. 2019

Preprint

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Following an ever-increased focus on personalized medicine, there is a continuing need to develop preclinical molecular imaging modalities to guide the development and optimization of targeted therapies. To date, non-invasive quantitative imaging modalities that can comprehensively assess simultaneous cellular drug delivery efficacy and therapeutic response are lacking. In this regard, Near-Infrared (NIR) Macroscopic Fluorescence Lifetime Förster Resonance Energy Transfer (MFLI-FRET) imaging offers a unique method to robustly quantify receptor-ligand engagement in vivo and subsequent intracellular internalization, which is critical to assess the delivery efficacy of targeted therapeutics. However, implementation of multiplexing optical imaging with FRET in vivo is challenging to achieve due to spectral crowding and cross-contamination. Herein, we report on a strategy that relies on a dark quencher that enables simultaneous assessment of receptor-ligand engagement and tumor metabolism in intact live mice. First, we establish that IRDye QC-1 (QC-1) is an effective NIR dark acceptor for the FRET-induced quenching of donor Alexa Fluor 700 (AF700) using in vitro NIR FLI microscopy and in vivo wide-field MFLI imaging. Second, we report on simultaneous in vivo imaging of the metabolic probe IRDye 800CW 2-deoxyglucose (2-DG) and MFLI-FRET imaging of NIR-labeled transferrin FRET pair (Tf-AF700/Tf-QC-1) uptake in tumors. Such multiplexed imaging revealed an inverse relationship between 2-DG uptake and Tf intracellular delivery, suggesting that 2-DG signal may predict the efficacy of intracellular targeted delivery. Overall, our methodology enables for the first time simultaneous non-invasive monitoring of intracellular drug delivery and metabolic response in preclinical studies.

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Glucose transporter GLUT1 expression and clinical outcome in solid tumors: a systematic review and meta-analysis

Cited by 151 publications

References 42 publications

Early squamous cell lung carcinoma: prognostic biomarkers for the many

Early squamous cell lung carcinoma: prognostic biomarkers for the many

A HIF – LIMD 1 negative feedback mechanism mitigates the pro‐tumorigenic effects of hypoxia

Multiplexed Non-invasive in vivo Imaging to Assess Metabolism and Receptor Engagement in Tumor Xenografts

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