侏儒小鼠中神经内分泌对葡萄糖生成的抑制作用及抗癌抗性
Neuroendocrine inhibition of glucose production and resistance to cancer in dwarf mice.
作者信息
Alderman J McKee, Flurkey Kevin, Brooks Natasha L, Naik Sneha B, Gutierrez Jonathan M, Srinivas Urmila, Ziara Kristen B, Jing Linhong, Boysen Gunnar, Bronson Rod, Klebanov Simon, Chen Xian, Swenberg James A, Stridsberg Mats, Parker Carol E, Harrison David E, Combs Terry P
机构信息
University of North Carolina, Chapel Hill, NC 27599, USA.
出版信息
Exp Gerontol. 2009 Jan-Feb;44(1-2):26-33. doi: 10.1016/j.exger.2008.05.014. Epub 2008 Jun 7.
Pit1 null (Snell dwarf) and Proph1 null (Ames dwarf) mutant mice lack GH, PRL and TSH. Snell and Ames dwarf mice also exhibit reduced IGF-I, resistance to cancer and a longer lifespan than control mice. Endogenous glucose production during fasting is reduced in Snell dwarf mice compared to fasting control mice. In view of cancer cell dependence on glucose for energy, low endogenous glucose production may provide Snell dwarf mice with resistance to cancer. We investigated whether endogenous glucose production is lower in Snell dwarf mice during feeding. Inhibition of endogenous glucose production by glucose injection was enhanced in 12 to 14 month-old female Snell dwarf mice. Thus, we hypothesize that lower endogenous glucose production during feeding and fasting reduces cancer cell glucose utilization providing Snell dwarf mice with resistance to cancer. The elevation of circulating adiponectin, a hormone produced by adipose tissue, may contribute to the suppression of endogenous glucose production in 12 to 14 month-old Snell dwarf mice. We compared the incidence of cancer at time of death between old Snell dwarf and control mice. Only 18% of old Snell dwarf mice had malignant lesions at the time of death compared to 82% of control mice. The median ages at death for old Snell dwarf and control mice were 33 and 26 months, respectively. By contrast, previous studies showed a high incidence of cancer in old Ames dwarf mice at the time of death. Hence, resistance to cancer in old Snell dwarf mice may be mediated by neuroendocrine factors that reduce glucose utilization besides elevated adiponectin, reduced IGF-I and a lack of GH, PRL and TSH, seen in both Snell and Ames dwarf mice. Proteomics analysis of pituitary secretions from Snell dwarf mice confirmed the absence of GH and PRL, the secretion of ACTH and elevated secretion of Chromogranin B and Secretogranin II. Radioimmune assays confirmed that circulating Chromogranin B and Secretogranin II were elevated in 12 to 14 month-old Snell dwarf mice. In summary, our results in Snell dwarf mice suggest that the pituitary gland and adipose tissue are part of a neuroendocrine loop that lowers the risk of cancer during aging by reducing the availability of glucose.
Pit1基因敲除(Snell侏儒)和Proph1基因敲除(Ames侏儒)突变小鼠缺乏生长激素(GH)、催乳素(PRL)和促甲状腺激素(TSH)。Snell和Ames侏儒小鼠的胰岛素样生长因子-I(IGF-I)水平也降低,对癌症具有抗性,并且寿命比对照小鼠更长。与禁食对照小鼠相比,Snell侏儒小鼠在禁食期间的内源性葡萄糖生成减少。鉴于癌细胞依赖葡萄糖获取能量,较低的内源性葡萄糖生成可能赋予Snell侏儒小鼠抗癌能力。我们研究了在进食期间Snell侏儒小鼠的内源性葡萄糖生成是否更低。在12至14月龄的雌性Snell侏儒小鼠中,通过注射葡萄糖对内源性葡萄糖生成的抑制作用增强。因此,我们推测,进食和禁食期间较低的内源性葡萄糖生成会减少癌细胞对葡萄糖的利用,从而赋予Snell侏儒小鼠抗癌能力。循环脂联素(一种由脂肪组织产生的激素)水平升高,可能有助于抑制12至14月龄Snell侏儒小鼠的内源性葡萄糖生成。我们比较了老年Snell侏儒小鼠和对照小鼠死亡时的癌症发病率。死亡时,只有18%的老年Snell侏儒小鼠有恶性病变,而对照小鼠的这一比例为82%。老年Snell侏儒小鼠和对照小鼠的中位死亡年龄分别为33个月和26个月。相比之下,先前的研究表明老年Ames侏儒小鼠死亡时癌症发病率很高。因此,老年Snell侏儒小鼠的抗癌能力可能是由神经内分泌因子介导的,这些因子除了脂联素升高、IGF-I降低以及缺乏GH、PRL和TSH(Snell和Ames侏儒小鼠均有这些情况)外,还会减少葡萄糖的利用。对Snell侏儒小鼠垂体分泌物的蛋白质组学分析证实缺乏GH和PRL,促肾上腺皮质激素(ACTH)分泌以及嗜铬粒蛋白B和分泌粒蛋白II分泌增加。放射免疫分析证实,12至14月龄的Snell侏儒小鼠循环中的嗜铬粒蛋白B和分泌粒蛋白II升高。总之,我们在Snell侏儒小鼠中的研究结果表明,垂体和脂肪组织是神经内分泌环路的一部分,该环路通过减少葡萄糖的可利用性来降低衰老过程中患癌风险。
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