4.7 Article

Human brown adipose tissue [15O]O2 PET imaging in the presence and absence of cold stimulus

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出版社

SPRINGER
DOI: 10.1007/s00259-016-3364-y

关键词

Brown adipose tissue; cold-induced thermogenesis; oxygen consumption; [O-15]O-2 PET imaging

资金

  1. Academy of Finland [259926, 265204, 292839, 269977]
  2. Paulo Foundation
  3. Finnish Cultural Foundation Southwest Finland Regional Fund
  4. Turku University Hospital Research Funds
  5. European Union (EU FP7 project) [278373, DIABAT]
  6. Academy of Finland (AKA) [292839, 269977, 265204, 292839, 265204, 269977] Funding Source: Academy of Finland (AKA)

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Brown adipose tissue (BAT) is considered a potential target for combatting obesity, as it produces heat instead of ATP in cellular respiration due to uncoupling protein-1 (UCP-1) in mitochondria. However, BAT-specific thermogenic capacity, in comparison to whole-body thermogenesis during cold stimulus, is still controversial. In our present study, we aimed to determine human BAT oxygen consumption with [O-15]O-2 positron emission tomography (PET) imaging. Further, we explored whether BAT-specific energy expenditure (EE) is associated with BAT blood flow, non-esterified fatty acid (NEFA) uptake, and whole-body EE. Seven healthy study subjects were studied at two different scanning sessions, 1) at room temperature (RT) and 2) with acute cold exposure. Radiotracers [O-15]O-2, [O-15]H2O, and [F-18]FTHA were given for the measurements of BAT oxygen consumption, blood flow, and NEFA uptake, respectively, with PET-CT. Indirect calorimetry was performed to assess differences in whole-body EE between RT and cold. BAT-specific EE and oxygen consumption was higher during cold stimulus (approx. 50 %); similarly, whole-body EE was higher during cold stimulus (range 2-47 %). However, there was no association in BAT-specific EE and whole-body EE. BAT-specific EE was found to be a minor contributor in cold induced whole-body thermogenesis (almost 1 % of total whole-body elevation in EE). Certain deep muscles in the cervico-thoracic region made a major contribution to this cold-induced thermogenesis (CIT) without any visual signs or individual perception of shivering. Moreover, BAT-specific EE associated with BAT blood flow and NEFA uptake both at RT and during cold stimulus. Our study suggests that BAT is a minor and deep muscles are a major contributor to CIT. In BAT, both in RT and during cold, cellular respiration is linked with circulatory NEFA uptake.

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