Altered metabolic landscape in
            <scp>IDH</scp>
            ‐mutant gliomas affects phospholipid, energy, and oxidative stress pathways

Fack, Fred; Tardito, Saverio; Hochart, G; Oudin, Anaïs; Zheng, Liang; Fritah, Sabrina; Golebiewska, Anna; Nazarov, Petr V.; Bernard, Amandine; Hau, Ann-Christin; Keunen, Olivier; Leenders, William P. J.; Lund‐Johansen, Morten; Stauber, Jonathan; Gottlieb, Eyal; Bjerkvig, Rolf; Niclou, Simone P.

doi:10.15252/emmm.201707729

Cited by 116 publications

(168 citation statements)

References 50 publications

(75 reference statements)

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“…Reduced serine biosynthesis may lead to increased reliance on the CBS/CTH pathway as a critical response to increased oxidative stress . In particular, high CBS expression has been shown to confer better prognosis in IDH ‐mutated 1p/19q codeleted gliomas in line with a previous study showing that decreased expression of CBS promotes glioma tumorigenesis in tumor xenografts . Correlation between higher CBS expression and survival in IDH ‐mutated 1p/19q codeleted gliomas has been confirmed also from the POLA public dataset .…”

Section: Resultssupporting

confidence: 78%

“…Correlation between higher CBS expression and survival in IDH ‐mutated 1p/19q codeleted gliomas has been confirmed also from the POLA public dataset . Fack et al have reported decreased Cyst in IDH mutant tumour xenografts compared with wild type, yet in the few samples reported in this last study, Cyst levels were roughly inversely correlated with codeletion status …”

Section: Resultssupporting

confidence: 78%

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A metabolomic data fusion approach to support gliomas grading

et al. 2019

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Magnetic resonance imaging (MRI) is the current gold standard for the diagnosis of brain tumors. However, despite the development of MRI techniques, the differential diagnosis of central nervous system (CNS) primary pathologies, such as lymphoma and glioblastoma or tumor-like brain lesions and glioma, is often challenging. MRI can be supported by in vivo magnetic resonance spectroscopy (MRS) to enhance its diagnostic power and multiproject-multicenter evaluations of classification of brain tumors have shown that an accuracy around 90% can be achieved for most of the pairwise discrimination problems. However, the survival rate for patients affected by gliomas is still low. The High-Resolution Magic-Angle-Spinning Nuclear Magnetic Resonance (HR-MAS NMR) metabolomics studies may be helpful for the discrimination of gliomas grades and the development of new strategies for clinical intervention. Here, we propose to use T 2 -filtered, diffusion-filtered and conventional waterpresaturated spectra to try to extract as much information as possible, fusing the data gathered by these different NMR experiments and applying a chemometric approach based on Multivariate Curve Resolution (MCR). Biomarkers important for glioma's discrimination were found. In particular, we focused our attention on cystathionine (Cyst) that shows promise as a biomarker for the better prognosis of glioma tumors.

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Section: Resultssupporting

confidence: 78%

Section: Resultssupporting

confidence: 78%

A metabolomic data fusion approach to support gliomas grading

et al. 2019

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“…It is, however, striking that the glycolysis route that fuels the TCA cycle is not increased (the glucose importer SLC2A3 RNA expression is even decreased). The obstructed catabolism of glucose in IDH1 mut gliomas was reported before . By metabolic flux experiments in an IDH1 R132H patient‐derived xenograft (PDX) it was shown that glucose is scarcely used as the carbon source for either α‐ketoglutarate or 2‐hydroxy‐glutarate, indicative of the use of alternative carbon sources for the production of these metabolites to fuel the TCA‐cycle .…”

Section: Discussionmentioning

confidence: 83%

Metabolic changes related to the IDH1 mutation in gliomas preserve TCA‐cycle activity: An investigation at the protein level

Dekker

Jurriëns

et al. 2020

FASEB j.

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The discovery of the IDH1 R132H (IDH1 mut) mutation in low‐grade glioma and the associated change in function of the IDH1 enzyme has increased the interest in glioma metabolism. In an earlier study, we found that changes in expression of genes involved in the aerobic glycolysis and the TCA cycle are associated with IDH1 mut. Here, we apply proteomics to FFPE samples of diffuse gliomas with or without IDH1 mutations, to map changes in protein levels associated with this mutation. We observed significant changes in the enzyme abundance associated with aerobic glycolysis, glutamate metabolism, and the TCA cycle in IDH1 mut gliomas. Specifically, the enzymes involved in the metabolism of glutamate, lactate, and enzymes involved in the conversion of α‐ketoglutarate were increased in IDH1 mut gliomas. In addition, the bicarbonate transporter (SLC4A4) was increased in IDH1 mut gliomas, supporting the idea that a mechanism preventing intracellular acidification is active. We also found that enzymes that convert proline, valine, leucine, and isoleucine into glutamate were increased in IDH1 mut glioma. We conclude that in IDH1 mut glioma metabolism is rewired (increased input of lactate and glutamate) to preserve TCA‐cycle activity in IDH1 mut gliomas.

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“…Additionally, our observations suggested that cystathionine increase is associated with enhanced cystathionine beta‐synthase activity likely due to a compensatory mechanism induced by oxidative stress, and that this process may be exacerbated in the presence of 1p/19q codeletion due to reduced activity of cystathionine gamma‐lyase (located on chromosome 1p) . Notably, high cystathionine beta‐synthase expression was suggested to confer better prognosis in IDH ‐mutated gliomas with 1p/19q codeletion . Further investigations are needed to evaluate the possible role of cystathionine as a marker of antioxidative activity in brain tumors and, eventually, its prognostic value.…”

Section: Discussionmentioning

confidence: 83%

In vivo ¹H MRS detection of cystathionine in human brain tumors

Branzoli

Deelchand

Sanson

et al. 2019

Magnetic Resonance in Med

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Purpose To report the technical aspects of noninvasive detection of cystathionine in human brain glioma with edited MRS, and to investigate possible further acquisition improvements for robust quantification of this metabolite. Methods In vivo 1H MR spectra were acquired at 3 T in 15 participants with an isocitrate dehydrogenase‐mutated glioma using a MEGA‐PRESS (MEscher GArwood point resolved spectroscopy) sequence previously employed for 2‐hydroxyglutarate detection (TR = 2 s, TE = 68 ms). The editing pulse was applied at 1.9 ppm for the edit‐on condition and at 7.5 ppm for the edit‐off condition. To evaluate the editing efficiency, spectra were acquired in 1 participant by placing the editing pulse for the edit‐on condition at 1.9, 2.03, and 2.16 ppm. Cystathionine concentration was quantified using LCModel and a simulated basis set. To confirm chemical shifts and J‐coupling values of cystathionine, the 1H NMR cystathionine spectrum was measured using a high‐resolution 500 MHz spectrometer. Results In 12 gliomas, cystathionine was observed in the in vivo edited MR spectra at 2.72 and 3.85 ppm and quantified. The signal intensity of the cystathionine resonance at 2.72 ppm increased 1.7 and 2.13 times when the editing pulse was moved to 2.03 and 2.16 ppm, respectively. Cystathionine was not detectable in normal brain tissue. Conclusion Cystathionine can be detected in vivo by edited MRS using the same protocol as for 2‐hydroxyglutarate detection. This finding may enable a more accurate, noninvasive investigation of cellular metabolism in glioma.

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Altered metabolic landscape in IDH ‐mutant gliomas affects phospholipid, energy, and oxidative stress pathways

Cited by 116 publications

References 50 publications

A metabolomic data fusion approach to support gliomas grading

A metabolomic data fusion approach to support gliomas grading

Metabolic changes related to the IDH1 mutation in gliomas preserve TCA‐cycle activity: An investigation at the protein level

In vivo ¹H MRS detection of cystathionine in human brain tumors

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Altered metabolic landscape in IDH ‐mutant gliomas affects phospholipid, energy, and oxidative stress pathways

Cited by 116 publications

References 50 publications

A metabolomic data fusion approach to support gliomas grading

A metabolomic data fusion approach to support gliomas grading

Metabolic changes related to the IDH1 mutation in gliomas preserve TCA‐cycle activity: An investigation at the protein level

In vivo 1H MRS detection of cystathionine in human brain tumors

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In vivo ¹H MRS detection of cystathionine in human brain tumors