Section of Integrative Physiology and Metabolism, Research Division, Joslin Diabetes Center, Harvard Medical School, Boston, Massachusetts.
J Nucl Med. 2013 Nov;54(11):1896-901. doi: 10.2967/jnumed.113.121012. Epub 2013 Sep 26.
For brown adipose tissue (BAT) to be effective at consuming calories, its blood flow must increase enough to provide sufficient fuel to sustain energy expenditure and also transfer the heat created to avoid thermal injury. Here we used a combination of human and rodent models to assess changes in BAT blood flow and glucose utilization.
(99m)Tc-methoxyisobutylisonitrile (MIBI) SPECT (n = 7) and SPECT/CT (n = 74) scans done in adult humans for parathyroid imaging were reviewed for uptake in regions consistent with human BAT. Site-directed biopsies of subcutaneous and deep neck fat were obtained for electron microscopy and gene expression profiling. In mice, tissue perfusion was measured with (99m)Tc-MIBI (n = 16) and glucose uptake with (18)F-FDG (n = 16). Animals were kept fasting overnight, anesthetized with pentobarbital, and given intraperitoneally either the β3-adrenergic receptor agonist CL-316,243, 1 mg/kg (n = 8), or saline (n = 8) followed by radiotracer injection 5 min later. After 120 min, the mice were imaged using SPECT/CT or PET/CT. Vital signs were recorded over 30 min during the imaging. BAT, white adipose tissue (WAT), muscle, liver, and heart were resected, and tissue uptake of both (99m)Tc-MIBI and (18)F-FDG was quantified by percentage injected dose per gram of tissue and normalized to total body weight.
In 5.4% of patients (4/74), (99m)Tc-MIBI SPECT/CT showed increased retention in cervical and supraclavicular fat that displayed multilocular lipid droplets, dense capillary investment, and a high concentration of ovoid mitochondria. Expression levels of the tissue-specific uncoupling protein-1 were 180 times higher in BAT than in subcutaneous WAT (P < 0.001). In mice, BAT tissue perfusion increased by 61% (P < 0.01), with no significant changes in blood flow to WAT, muscle, heart, or liver. CL-316,243 increased glucose uptake in BAT even more, by 440% (P < 0.01).
Pharmacologic activation of BAT requires increased blood flow to deliver glucose and oxygen for thermogenesis. However, the glucose consumption far exceeds the vascular response. These findings demonstrate that activated BAT increases glucose uptake beyond what might occur by increased blood flow alone and suggest that activated BAT likely uses glucose for nonthermogenic purposes.
评估棕色脂肪组织(BAT)血流和葡萄糖利用的变化。
对接受甲状旁腺成像的成人患者进行(99m)Tc-甲氧基异丁基异腈(MIBI)单光子发射计算机断层扫描(SPECT)(n=7)和 SPECT/CT(n=74)扫描,评估其颈部和锁骨上区域的 BAT 摄取。对皮下和颈部深层脂肪进行靶向活检,进行电子显微镜和基因表达谱分析。在小鼠中,使用(99m)Tc-MIBI(n=16)测量组织灌注,使用(18)F-FDG(n=16)测量葡萄糖摄取。动物禁食过夜,用戊巴比妥麻醉,然后腹腔内给予β3-肾上腺素能受体激动剂 CL-316,243,1mg/kg(n=8)或生理盐水(n=8),5min 后注射示踪剂。120min 后,使用 SPECT/CT 或 PET/CT 进行成像。在成像过程中记录 30min 的生命体征。切除 BAT、白色脂肪组织(WAT)、肌肉、肝脏和心脏,通过组织摄取的(99m)Tc-MIBI 和(18)F-FDG 对每克组织的注入剂量百分比进行量化,并归一化为总体重。
在 5.4%的患者(4/74)中,(99m)Tc-MIBI SPECT/CT 显示颈部和锁骨上脂肪的摄取增加,这些脂肪呈现多室脂质滴、密集的毛细血管投资和高浓度的卵圆形线粒体。组织特异性解偶联蛋白-1 的表达水平在 BAT 中比皮下 WAT 高 180 倍(P<0.001)。在小鼠中,BAT 组织灌注增加 61%(P<0.01),而 WAT、肌肉、心脏或肝脏的血流无明显变化。CL-316,243 使 BAT 的葡萄糖摄取增加了 440%(P<0.01)。
BAT 的药物激活需要增加血流以输送葡萄糖和氧气用于产热。然而,葡萄糖的消耗远远超过了血管反应。这些发现表明,激活的 BAT 增加了葡萄糖摄取,超出了仅通过增加血流本身可能发生的摄取,这表明激活的 BAT 可能将葡萄糖用于非产热目的。