2008
DOI: 10.1074/jbc.m706494200
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Quantifying Reductive Carboxylation Flux of Glutamine to Lipid in a Brown Adipocyte Cell Line

Abstract: We previously reported that glutamine was a major source of carbon for de novo fatty acid synthesis in a brown adipocyte cell line. The pathway for fatty acid synthesis from glutamine may follow either of two distinct pathways after it enters the citric acid cycle. The glutaminolysis pathway follows the citric acid cycle, whereas the reductive carboxylation pathway travels in reverse of the citric acid cycle from ␣-ketoglutarate to citrate. To quantify fluxes in these pathways we incubated brown adipocyte cell… Show more

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Cited by 285 publications
(220 citation statements)
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“…Loss of NAD + -dependent IDH is shared with dinoflagellates, and therefore the switch to the NADP + -dependent form likely occurred early, although the reasons for this are unknown [9]. This activity is unusual because, in mammals, NADP + -dependent IDH classically operates in the reductive (or reverse) direction, allowing TCA cycle regulation [55,56], although the oxidative direction can occur when under oxidative stress [57].…”
Section: Mitochondrial Metabolism Across the Alveolatamentioning
confidence: 99%
“…Loss of NAD + -dependent IDH is shared with dinoflagellates, and therefore the switch to the NADP + -dependent form likely occurred early, although the reasons for this are unknown [9]. This activity is unusual because, in mammals, NADP + -dependent IDH classically operates in the reductive (or reverse) direction, allowing TCA cycle regulation [55,56], although the oxidative direction can occur when under oxidative stress [57].…”
Section: Mitochondrial Metabolism Across the Alveolatamentioning
confidence: 99%
“…Whereas the reductive metabolism of glutamine was known to occur in some differentiated tissues (Yoo et al 2008), recent evidence using isotope-labeled carbon tracing suggests that the reductive metabolism of glutamine can be a major pathway for lipid production when cells are hypoxic . Reductive glutamine metabolism is a minor source of lipogenic acetyl-coA when oxygen levels are high, but glutamine becomes the major source of carbon for lipid synthesis when cells are proliferating under low-oxygen conditions (Fig.…”
Section: Low Oxygen Levels or Vhl Loss Promoted Reductive Glutamine Mmentioning
confidence: 99%
“…Many proliferating cells synthesize lipids de novo (Ookhtens et al 1984;Menendez and Lupu 2007), and glucose is a major source of acetylcoA in cells (Hatzivassiliou et al 2005;Wellen et al 2009). However, glutamine can also be a source of carbon for acetyl-coA (Yoo et al 2004(Yoo et al , 2008DeBerardinis et al 2007), and it may be the principle source of this important biosynthetic precursor under some physiological conditions .…”
Section: Glutamine Carbon Can Be Used As a Precursor For Lipid Synthesismentioning
confidence: 99%
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“…Because the synthesis of fatty acids from glucose depends on flux through PDH, it is difficult to understand why a coordinated lipogenic signal by mTORC1 would include inhibition of this enzyme, which is typically stimulated by insulin. It is possible to generate fatty acids from glutamate by reductive carboxylation in the liver, adipose tissue, and some tumors by a pathway not requiring PDH (18)(19)(20), but the quantitative contribution of this pathway to normal and pathological lipid accumulation has not been defined. Interestingly, mouse livers, which have constitutive accumulation of HIF-2 by virtue of tissue-specific deletion of von Hippel-Lindau protein, develop steatosis, consistent with HIF-2 being a positive regulator of triglyceride accumulation (21).…”
mentioning
confidence: 99%