Warburg phenotype in renal cell carcinoma: High expression of glucose‐transporter 1 (GLUT‐1) correlates with low CD8<sup>+</sup> T‐cell infiltration in the tumor

Singer, Katrin; Kastenberger, Michael; Gottfried, Eva; Hammerschmied, Christine G.; Büttner, Maike; Aigner, Michael; Seliger, Barbara; Walter, Bernhard; Schlößer, Hans; Hartmann, Arndt; Andreesen, Reinhard; Mackensen, Andréas; Kreutz, Marina

doi:10.1002/ijc.25543

Cited by 137 publications

(108 citation statements)

References 44 publications

(47 reference statements)

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“…6,7 We and others have demonstrated, that lactic acid, a prominent product of glycolysis generated in increased amounts by tumor cells, is capable of modulating cellular components within the tumor stroma, including immune effector cells and antigen-presenting cells. [8][9][10][11] There is an increasingly recognized list of metabolic dysregulations linked to carcinogenesis. Various tumor entities, particularly malignant melanoma, leukemia, and hepatocellular carcinoma, can exhibit a reduced expression of 5 0 -deoxy-5 0 -methylthioadenosine phosphorylase (MTAP).…”

Section: Introductionmentioning

confidence: 99%

Suppressive effects of tumor cell-derived 5′-deoxy-5′-methylthioadenosine on human T cells

et al. 2016

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The immunosuppressive tumor microenvironment represents one of the main obstacles for immunotherapy of cancer. The tumor milieu is among others shaped by tumor metabolites such as 5 0 -deoxy-5 0 -methylthioadenosine (MTA). Increased intratumoral MTA levels result from a lack of the MTAcatabolizing enzyme methylthioadenosine phosphorylase (MTAP) in tumor cells and are found in various tumor entities. Here, we demonstrate that MTA suppresses proliferation, activation, differentiation, and effector function of antigen-specific T cells without eliciting cell death. Conversely, if MTA is added to highly activated T cells, MTA exerts cytotoxic effects on T cells. We identified the Akt pathway, a critical signal pathway for T cell activation, as a target of MTA, while, for example, p38 remained unaffected. Next, we provide evidence that MTA exerts its immunosuppressive effects by interfering with protein methylation in T cells. To confirm the relevance of the suppressive effects of exogenously added MTA on human T cells, we used an MTAP-deficient tumor cell-line that was stably transfected with the MTAPcoding sequence. We observed that T cells stimulated with MTAP-transfected tumor cells revealed a higher proliferative capacity compared to T cells stimulated with Mock-transfected cells. In conclusion, our findings reveal a novel immune evasion strategy of human tumor cells that could be of interest for therapeutic targeting.

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Section: Introductionmentioning

confidence: 99%

Suppressive effects of tumor cell-derived 5′-deoxy-5′-methylthioadenosine on human T cells

et al. 2016

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“…Világossejtes veserák (RCC) biopsziás mintáinak vizsgálata során a GLUT-1-expresszió upregulációja negatív korrelációt mutatott a CD3+, CD8+ és granzyme B+ T-sejtek jelenlétével. Továbbá az LdhA génexpressziója negatív hatást gyakorol a CD3+ T-sejtek által végbemenő daganatos szöveti infiltrációra [51]. In vitro vizsgálatok alapján a tejsav gá-tolja a T-sejtek tejsavleadását [48].…”

Section: A Tejsav Okozta Acidózis Mint Immunszuppressziót éS Daganatunclassified

A laktátdehidrogenáz (LDH) prognosztikai jelentősége az onkológiában

Deme¹,

Telekes

2017

Orvosi Hetilap

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A rosszindulatú daganatsejtek többségében fokozott a glikolízis, amely biztosítja a proliferációhoz szükséges energia legnagyobb részét. A laktátdehidrogenáz (LDH) anaerob körülmények között katalizálja a reverzibilis piruvát-tejsav átalakulást. A daganatsejtek által expresszált LDHA izoenzim hatására a tejsavképződés jelentősen fokozódik. A tejsav indukálja az oxigenizált daganatsejtek proliferációját, az angiogenezist és gátolja a veleszületett és az adaptív immunválaszt. A szérum-LDH-emelkedés rövidebb túléléssel korrelál. A szerzők áttekintik az LDH-emelkedés és a rosszindulatú daganatos betegségek prognózisa közötti összefüggést feltáró fontosabb vizsgálatokat. Orv Hetil. 2017; 158(50): 1977-1988. Kulcsszavak: laktátdehidrogenáz, rosszindulatú daganatok, prognózis Prognostic importance of lactate dehydrogenase (LDH) in oncologyGlycolysis is increased in most of the malignant cells, providing the largest proportion of energy needed for cell proliferation. Lactate dehydrogenase (LDH) catalyses the reversible process of pyruvate to lactate in anaerobic condition. LDHA isoenzyme expressed mainly by malignant cells, significantly increases lactate formation. Lactate induces the proliferation of oxygenated malignant cells, angiogenesis, and inhibits the innate and adaptive immune responses. Baseline serum LDH elevation correlates with shorter survival. The authors review the relevant studies exploring the correlation between LDH elevation and the prognosis of malignant diseases. Rövidítések A549 = (human non small cell lung cancer cell line A549) humán nem kissejtes tüdőráksejtvonal A549; acetil-CoA = (acetylcoenzyme A) acetil-koenzim A; Acr = activity-regulated cytoskeleton-associated protein; AKT = (protein kinase B) proteinkináz-B; AMP = (adenosine monophosphate) adenozin-monofoszfát; AMPK = (adenosine monophosphate-activated protein kinase) adenozin-monofoszfát aktiválta proteinkináz; ARG1 = (L-arginin metabolizing enzyme arginase-1) L-arginin-metabolizáló enzim argináz-1; ATP = (adenosine triphosphate) adenozin-trifoszfát; CAF = (cancer-associated fibroblasts) daganat asszociálta fibroblastok; CD = (cluster of differentation) differenciációs cluster; CRC = (colorectal cancer) vastag-és végbélrák; CRPC = (castration-resistant prostate cancer) kasztrációrezisztens prostatarák; CSS = (cancer specific survival) daganatspecifikus túlélés; CTL = (cytotoxic T-lymphocyte) citotoxikus T-lymphocyta; DFS = (disease-free survival) betegségmentes túlélés; EGFR = (epidermal growth factor receptor) epidermális növekedési faktor receptor; EpH4 = (nontumorigenic mammary epithelial cells) nem daganatos emlőhámsejt; ER = (estrogen receptor) ösztrogénreceptor; ErbB2 = receptor tyrosine kinase erbB-2 (HER-2/Neu); ERK-2 = (extracellular signal-regulated kinase-2) extracelluláris szignál regulálta kináz 2; FH = (fumarate hydratase) fumaráthidra-táz; c-Fos = Finkel-Biskis-Jinkins-osteosarcoma; FX11 = kis molekulájú LDHA-inhibitor; G6PDH = (glucose-6-phos- Keywords

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“…In order to counteract the deleterious effects of hypoxia, such as apoptosis and necrosis, malignant cells undergo adaptive and genetic changes. One such change is increased uptake of glucose when compared with normal cells through accelerated glycolysis -often referred to as 'glycolytic switch' or 'Warburg effect' (Warburg, 1956;Airley&Mobasheri, 2007;Singer et al, 2011). This is largely mediated by the up-regulation of GLUT especially GLUT-1 (Binder et al, 1997;Smith, 1999;Medina&Owen, 2002;Airley&Mobasheri, 2007;Ozcan et al, 2007;Suganuma et al, 2007).…”

Section: Glucose Transporter-1mentioning

confidence: 99%

“…This is largely mediated by the up-regulation of GLUT especially GLUT-1 (Binder et al, 1997;Smith, 1999;Medina&Owen, 2002;Airley&Mobasheri, 2007;Ozcan et al, 2007;Suganuma et al, 2007). It is now well established that accelerated glycolysis and increased glucose uptake mediated by GLUT-1 are the hallmarks of many malignant tumors and that these adaptive changes in glucose metabolism favor survival, proliferation and metastasis of tumor cells, even under hypoxic conditions (Airley&Mobasheri, 2007;Ozcan et al, 2007;Singer et al, 2011).…”

Section: Glucose Transporter-1mentioning

confidence: 99%

“…GLUT-1 is overexpressed in VHL-mutated mice and the GLUT-1 promoter region has an HRE (Ebert et al, 1995;Park et al, 2007;Lidgren et al, 2008). While the basal level of expression of GLUT-1 in normal PTEC is a subject of debate (Nagase et al, 1995;Ozcan et al, 2007), the overexpression of GLUT-1 in RCC has been demonstrated by many studies (Nagase et al, 1995;Miyakita et al, 2002;Ozcan et al, 2007;Suganuma et al, 2007;Lidgren et al, 2008;Singer et al, 2011). All of these studies concluded that GLUT-1 is over-expressed markedly in clear cell RCC compared with other RCC subtypes, confirming the link between VHL aberration and the subsequent HIF up-regulation.…”

Section: Glucose Transporter-1mentioning

confidence: 99%

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The VHL-HIF Signaling in Renal Cell Carcinoma: Promises and Pitfalls

Morais¹,

Johnson²,

Gobé³

2012

Emerging Research and Treatments in Renal Cell Carcinoma

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Warburg phenotype in renal cell carcinoma: High expression of glucose‐transporter 1 (GLUT‐1) correlates with low CD8⁺ T‐cell infiltration in the tumor

Cited by 137 publications

References 44 publications

Suppressive effects of tumor cell-derived 5′-deoxy-5′-methylthioadenosine on human T cells

Suppressive effects of tumor cell-derived 5′-deoxy-5′-methylthioadenosine on human T cells

A laktátdehidrogenáz (LDH) prognosztikai jelentősége az onkológiában

The VHL-HIF Signaling in Renal Cell Carcinoma: Promises and Pitfalls

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Warburg phenotype in renal cell carcinoma: High expression of glucose‐transporter 1 (GLUT‐1) correlates with low CD8+ T‐cell infiltration in the tumor

Cited by 137 publications

References 44 publications

Suppressive effects of tumor cell-derived 5′-deoxy-5′-methylthioadenosine on human T cells

Suppressive effects of tumor cell-derived 5′-deoxy-5′-methylthioadenosine on human T cells

A laktátdehidrogenáz (LDH) prognosztikai jelentősége az onkológiában

The VHL-HIF Signaling in Renal Cell Carcinoma: Promises and Pitfalls

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Warburg phenotype in renal cell carcinoma: High expression of glucose‐transporter 1 (GLUT‐1) correlates with low CD8⁺ T‐cell infiltration in the tumor