长期消瘦和肥胖重症患者脂肪组织的增殖与分化
Proliferation and differentiation of adipose tissue in prolonged lean and obese critically ill patients.
作者信息
Goossens Chloë, Vander Perre Sarah, Van den Berghe Greet, Langouche Lies
机构信息
Clinical Division and Laboratory of Intensive Care Medicine, Department of Cellular and Molecular Medicine, KU Leuven, 3000, Leuven, Belgium.
出版信息
Intensive Care Med Exp. 2017 Dec;5(1):16. doi: 10.1186/s40635-017-0128-3. Epub 2017 Mar 16.
BACKGROUND
In prolonged non-obese critically ill patients, preservation of adipose tissue is prioritized over that of the skeletal muscle and coincides with increased adipogenesis. However, we recently demonstrated that in obese critically ill mice, this priority was switched. In the obese, the use of abundantly available adipose tissue-derived energy substrates was preferred and counteracted muscle wasting. These observations suggest that different processes are ongoing in adipose tissue of lean vs. overweight/obese critically ill patients.
METHODS
We hypothesize that to preserve adipose tissue mass during critical illness, adipogenesis is increased in prolonged lean critically ill patients, but not in overweight/obese critically ill patients, who enter the ICU with excess adipose tissue. To test this, we studied markers of adipogenesis in subcutaneous and visceral biopsies of matched lean (n = 24) and overweight/obese (n = 24) prolonged critically ill patients. Secondly, to further unravel the underlying mechanism of critical illness-induced adipogenesis, local production of eicosanoid PPARγ agonists was explored, as well as the adipogenic potential of serum from matched lean (n = 20) and overweight/obese (n = 20) critically ill patients.
RESULTS
The number of small adipocytes, PPARγ protein, and CEBPB expression were equally upregulated (p ≤ 0.05) in subcutaneous and visceral adipose tissue biopsies of lean and overweight/obese prolonged critically ill patients. Gene expression of key enzymes involved in eicosanoid production was reduced (COX1, HPGDS, LPGDS, ALOX15, all p ≤ 0.05) or unaltered (COX2, ALOX5) during critical illness, irrespective of obesity. Gene expression of PLA2G2A and ALOX15B was upregulated in lean and overweight/obese patients (p ≤ 0.05), whereas their end products, the PPARγ-activating metabolites 15s-HETE and 9-HODE, were not increased in the adipose tissue. In vitro, serum of lean and overweight/obese prolonged critically ill patients equally stimulated adipocyte proliferation (p ≤ 0.05) and differentiation (lipid accumulation, DLK1, and CEBPB expression, p ≤ 0.05).
CONCLUSIONS
Contrary to what was hypothesized, adipogenesis increased independently of initial BMI in prolonged critically ill patients. Not the production of local eicosanoid PPARγ agonists but circulating adipogenic factors seem to be involved in critical illness-induced adipogenesis. Importantly, our findings suggest that abundantly available energy substrates from the adipose tissue, rather than excess adipocytes, can play a beneficial role during critical illness.
背景
在长期患病的非肥胖重症患者中,脂肪组织的保存优先于骨骼肌,且与脂肪生成增加相一致。然而,我们最近证明,在肥胖重症小鼠中,这种优先顺序发生了改变。在肥胖患者中,优先使用大量可得的脂肪组织衍生能量底物,这抵消了肌肉萎缩。这些观察结果表明,瘦与超重/肥胖重症患者的脂肪组织中正在发生不同的过程。
方法
我们假设,为了在危重病期间维持脂肪组织质量,长期患病的瘦重症患者脂肪生成增加,但超重/肥胖重症患者脂肪生成不增加,因为他们进入重症监护病房时脂肪组织过多。为了验证这一点,我们研究了匹配的瘦(n = 24)和超重/肥胖(n = 24)长期重症患者皮下和内脏活检组织中的脂肪生成标志物。其次,为了进一步阐明危重病诱导脂肪生成的潜在机制,我们探索了类花生酸PPARγ激动剂的局部产生,以及匹配的瘦(n = 20)和超重/肥胖(n = 20)重症患者血清的脂肪生成潜力。
结果
瘦和超重/肥胖长期重症患者的皮下和内脏脂肪组织活检中,小脂肪细胞数量、PPARγ蛋白和CEBPB表达均同样上调(p≤0.05)。无论肥胖与否,在危重病期间,参与类花生酸生成的关键酶的基因表达降低(COX1、HPGDS、LPGDS、ALOX15,均p≤0.05)或未改变(COX2、ALOX5)。PLA2G2A和ALOX15B的基因表达在瘦和超重/肥胖患者中上调(p≤0.05),而它们的终产物,即PPARγ激活代谢物15s - HETE和9 - HODE,在脂肪组织中并未增加。在体外,瘦和超重/肥胖长期重症患者的血清同样刺激脂肪细胞增殖(p≤0.05)和分化(脂质积累、DLK1和CEBPB表达,p≤0.05)。
结论
与假设相反,长期重症患者的脂肪生成增加与初始体重指数无关。参与危重病诱导脂肪生成的似乎是循环中的脂肪生成因子,而非局部类花生酸PPARγ激动剂的产生。重要的是,我们的研究结果表明,脂肪组织中大量可得的能量底物,而非过多的脂肪细胞,在危重病期间可能发挥有益作用。
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