Stoichiometric coupling of brain glucose metabolism and glutamatergic neuronal activity

Sibson, Nicola R.; Dhankhar, Ajay; Mason, Graeme F.; Rothman, Douglas L.; Behar, Kevin L.; Shulman, Robert G.

doi:10.1073/pnas.95.1.316

Cited by 800 publications

(894 citation statements)

References 28 publications

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“…This is supported by the evidence that the local field-evoked potential is attenuated by blocking glutamate release during forepaw stimulation (Kida et al, 2001(Kida et al, , 2006. This decrease in field-evoked potential is linearly related with the decrease in the evoked CMRO 2 as well as BOLD signal and CBF (Kida et al, 2001(Kida et al, , 2006, consistent with the result that the activation-dependent release of glutamate and the glutamate-glutamine cycles require a proportionate oxidative energy consumption (Sibson et al, 1998). Furthermore, a linear relationship between BOLD signals and oxygen consumption associated with cortical activation produced by either physiological perturbations or forepaw stimulation has been reported (Kida et al, 2000;Sanganahalli et al, 2009;Herman et al, 2009).…”

Section: Discussionsupporting

confidence: 59%

Comprehensive correlation between neuronal activity and spin-echo blood oxygenation level-dependent signals in the rat somatosensory cortex evoked by short electrical stimulations at various frequencies and currents

Kida

Yamamoto

2010

Brain Research

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It is essential to elucidate the relationship between blood oxygenation level-dependent (BOLD) signals and neuronal activity for the interpretation of the functional magnetic resonance imaging (fMRI) signals; this relationship has been quantitatively investigated by animal studies measuring evoked potentials as indices of neuronal activity. Although most human fMRI studies employ the event-related task design, in which the stimulus duration is short, few studies have investigated the relationship between BOLD signals and evoked potentials at short stimulus durations. The present study investigated this relationship in the somatosensory cortex of anesthetized rats by using electrical forepaw stimulation at a short duration of 4 s and comprehensively analyzed it at different frequencies (1-10 Hz) and currents (0.5-2.0 mA). Somatosensory evoked potential (SEP) responses were measured at the scalp using silver ball electrodes. The sum of the peak-to-peak amplitude (ΣSEP) and average SEP (avg. SEP) responses were calculated. BOLD signals were obtained using a spin-echo echo-planar imaging sequence at 7 T. The relationship between the avg.SEP and BOLD signals varied with frequency, whereas that between ΣSEP and BOLD signals showed a significant correlation at varying frequencies and currents. In particular, the relationship between ΣSEP and ΣBOLD, which is the sum of the BOLD signals obtained at each time point reflecting the area under the BOLD response curves, mostly converged, irrespective of the frequency. Our results suggest that ΣBOLD obtained using a spin-echo sequence reflects the neural activity as quantified by ΣSEP, which was determined at different frequencies and currents. Section: Regulatory SystemsKeywords: BOLD; fMRI; Forepaw; Neurovascular coupling; SEP Abbreviations: BOLD, blood oxygenation level-dependent; CBF, cerebral blood flow; CMRO 2 , cerebral metabolic rate of oxygen consumption; EPI, echo planar imagining; TE, echo time; fMRI, functional magnetic resonance imaging; LDF, laser Doppler flowmetry; SEP, somatosensory evoked potential; T 2 , transverse relaxation time -2 - IntroductionFunctional magnetic resonance imaging (fMRI) based on blood oxygenation level-dependent (BOLD) effect has been widely used in neuroscience and psychology to study brain function. fMRI reflects cerebral hemodynamic changes, and its signals have been interpreted by assuming a neuronal hemodynamic response (Friston et al., 1995) based on the 19 th century hypothesis of Roy and Sherrington that neuronal activity induces an increase in the regional cerebral blood flow (CBF) (Roy and Sherrington, 1890). Thus, fMRI is an indirect method for assessing neuronal activity. Therefore, it is essential to elucidate the relationship between BOLD signals and neuronal activity for interpreting the fMRI signals; this relationship has been investigated mainly by animal studies measuring evoked potentials as indices of the neuronal activity in the somatosensory cortex (Brinker et al., 1999;Van Camp et al., 2006;Goloshevsk...

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Section: Discussionsupporting

confidence: 59%

Comprehensive correlation between neuronal activity and spin-echo blood oxygenation level-dependent signals in the rat somatosensory cortex evoked by short electrical stimulations at various frequencies and currents

Kida

Yamamoto

2010

Brain Research

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“…4 But recent experimental studies in rodents and theoretical modeling have converged on the conclusion that majority of the resting energy consumption supports glutamatergic signaling and the energy demand changes linearly with pyramidal neuron firing rates and glutamate neurotransmitter release and reuptake. [5][6][7][8][9] Therefore in rodent models it is possible, to a first order, to show that the resting energy is primarily dedicated to total glutamatergic signaling, and the changes in neuronal signaling relative to a well-defined resting activity level can be used to calibrate changes in energy consumption during functional magnetic resonance imaging (fMRI) experiments. 10,11 In the awake human brain, however, the fraction of resting energy usage devoted to glutamatergic signaling is less well understood.…”

Section: Introductionmentioning

confidence: 99%

“…The magnitude of neuronal signaling in the human brain, and by inference the commensurate energy demand, underscores the functional relevance of resting activity and has profound implications for interpreting fMRI experiments in humans. [12][13][14] Given the rapidly increasing use of resting-state fMRI in mapping networks-defined as a subset of cortical and subcortical gray-matter regions that function together 15,16 -it is important to quantitatively establish if in the resting human the metabolic demand for neuronal signaling is high, as has been established for the rodent, 5,[7][8][9] and to what extent metabolic demand varies across gray-matter regions. 13 C magnetic resonance spectroscopy (MRS) of 13 C-labeled substrates (e.g., glucose and acetate) can measure rates of 13 C label incorporation into cell-specific pools (e.g., glutamate and gamino butyric acid (GABA) are predominantly neuronal and glutamine is predominantly glial) thereby estimating metabolic fluxes 17 of neuronal glucose oxidation (CMR glc(ox),N ) and of total glutamate neurotransmitter cycling (V cyc(tot) ).…”

Section: Introductionmentioning

confidence: 99%

Glutamatergic Function in the Resting Awake Human Brain is Supported by Uniformly High Oxidative Energy

Hyder

Fulbright

Shulman

et al. 2013

J Cereb Blood Flow Metab

109

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Rodent 13 C magnetic resonance spectroscopy studies show that glutamatergic signaling requires high oxidative energy in the awake resting state and allowed calibration of functional magnetic resonance imaging (fMRI) signal in terms of energy relative to the resting energy. Here, we derived energy used for glutamatergic signaling in the awake resting human. We analyzed human data of electroencephalography (EEG), positron emission tomography (PET) maps of oxygen (CMR O2 ) and glucose (CMR glc ) utilization, and calibrated fMRI from a variety of experimental conditions. CMR glc and EEG in the visual cortex were tightly coupled over several conditions, showing that the oxidative demand for signaling was four times greater than the demand for nonsignaling events in the awake state. Variations of CMR O2 and CMR glc from gray-matter regions and networks were within ±10% of means, suggesting that most areas required similar energy for ubiquitously high resting activity. Human calibrated fMRI results suggest that changes of fMRI signal in cognitive studies contribute at most ± 10% CMR O2 changes from rest. The PET data of sleep, vegetative state, and anesthesia show metabolic reductions from rest, uniformly 420% across, indicating no region is selectively reduced when consciousness is lost. Future clinical investigations will benefit from using quantitative metabolic measures. Keywords: astrocytes; baseline; field potentials; glutamate; multiunit activity; resting state INTRODUCTIONThe human brain consumes 20% of the body's energy at rest despite being only 2% of total body mass. 1 Normally glucose oxidation is the source of energy production supporting brain function 2 in which gray-matter signaling (i.e., events associated with neuronal firing) is dominated by glutamatergic neurons. 3 Estimates of the fraction of resting brain energy devoted to signaling were originally quite low. 4 But recent experimental studies in rodents and theoretical modeling have converged on the conclusion that majority of the resting energy consumption supports glutamatergic signaling and the energy demand changes linearly with pyramidal neuron firing rates and glutamate neurotransmitter release and reuptake. [5][6][7][8][9] Therefore in rodent models it is possible, to a first order, to show that the resting energy is primarily dedicated to total glutamatergic signaling, and the changes in neuronal signaling relative to a well-defined resting activity level can be used to calibrate changes in energy consumption during functional magnetic resonance imaging (fMRI) experiments. 10,11 In the awake human brain, however, the fraction of resting energy usage devoted to glutamatergic signaling is less well understood. The magnitude of neuronal signaling in the human brain, and by inference the commensurate energy demand, underscores the functional relevance of resting activity and has profound implications for interpreting fMRI experiments in humans. [12][13][14] Given the rapidly increasing use of resting-state fMRI in mapping networks-defined as a...

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“…In line with 'a', the Glu-neurotransmitter cycling would also be expected to be reduced Figure 7 In the parietal cortex, the metabolomic analysis revealed a significant separation between the isoflurane-and propofolanesthetized animals, which was observed in the score plot (A -each blue diamond in the score plot represents a propofolanesthetized rat; and each of the black squares represents an isoflurane-anesthetized rat) with a cumulative Q 2 value of 0.70 on the combined first and second components, indicating an excellent fit of the data according to the classification and a model of high predictive power. (Sibson et al, 1998), and the observation that [glu] and [glc] were negatively correlated in the parietal cortex suggesting that higher Glu levels were present in animals with lower Glc content is in opposition to this notion (cf. Figure 4).…”

Section: Discussionmentioning

confidence: 99%

The metabolomic profile during isoflurane anesthesia differs from propofol anesthesia in the live rodent brain

Makaryus

Lee

et al. 2011

J Cereb Blood Flow Metab

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Development of noninvasive techniques to discover new biomarkers in the live brain is important to further understand the underlying metabolic pathways of significance for processes such as anesthesia-induced apoptosis and cognitive dysfunction observed in the undeveloped brain. We used in vivo proton magnetic resonance spectroscopy and two different signal processing approaches to test the hypothesis that volatile (isoflurane) and intravenous (propofol) anesthetics at equipotent doses produce distinct metabolomic profiles in the hippocampus and parietal cortex of the live rodent. For both brain regions, prolonged isoflurane anesthesia was characterized by higher levels of lactate (Lac) and glutamate compared with long-lasting propofol. In contrast, propofol anesthesia was characterized by very low concentrations of Lac ([lac]) as well as glucose. Quantitative analysis revealed that the [lac] was fivefold higher with isoflurane compared with propofol anesthesia and independent of [lac] in blood. The metabolomic profiling further demonstrated that for both brain regions, Lac was the most important metabolite for the observed differences, suggesting activation of distinct metabolic pathways that may impact mechanisms of action, background cellular functions, and possible agent-specific neurotoxicity.

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Stoichiometric coupling of brain glucose metabolism and glutamatergic neuronal activity

Cited by 800 publications

References 28 publications

Comprehensive correlation between neuronal activity and spin-echo blood oxygenation level-dependent signals in the rat somatosensory cortex evoked by short electrical stimulations at various frequencies and currents

Comprehensive correlation between neuronal activity and spin-echo blood oxygenation level-dependent signals in the rat somatosensory cortex evoked by short electrical stimulations at various frequencies and currents

Glutamatergic Function in the Resting Awake Human Brain is Supported by Uniformly High Oxidative Energy

The metabolomic profile during isoflurane anesthesia differs from propofol anesthesia in the live rodent brain

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