Chung Chee Yeun, Koprich James B, Endo Shogo, Isacson Ole
Neuroregeneration Laboratories, Harvard Medical School, McLean Hospital, Belmont, Massachusetts 02478, USA.
J Neurosci. 2007 Aug 1;27(31):8314-23. doi: 10.1523/JNEUROSCI.1972-07.2007.
Relative neuronal vulnerability is a universal yet poorly understood feature of neurodegenerative diseases. In Parkinson's disease, dopaminergic (DA) neurons in the substantia nigra (SN) (A9) are particularly vulnerable, whereas adjacent DA neurons within the ventral tegmental area (A10) are essentially spared. Our previous laser capture microdissection and microarray study (Chung et al., 2005) demonstrated that molecular differences between these DA neurons may underlie their differential vulnerability. Here we show that G-substrate, an endogenous inhibitor of Ser/Thr protein phosphatases, exhibits higher expression in A10 compared with A9 DA neurons in both rodent and human midbrain. Overexpression of G-substrate protected dopaminergic BE(2)-M17 cells against toxins, including 6-OHDA and MG-132 (carbobenzoxy-L-leucyl- L-leucyl-L-leucinal), whereas RNA interference (RNAi)-mediated knockdown of endogenous G-substrate increased their vulnerability to these toxins. G-substrate reduced 6-OHDA-mediated protein phosphatase 2A (PP2A) activation in vitro and increased phosphorylated levels of PP2A targets including Akt, glycogen synthase kinase 3beta, and extracellular signal-regulated kinase 2 but not p38. RNAi to Akt diminished the protective effect of G-substrate against 6-OHDA. In vivo, lentiviral delivery of G-substrate to the rat SN increased baseline levels of phosphorylated Akt and protected A9 DA neurons from 6-OHDA-induced toxicity. These results suggest that inherent differences in the levels of G-substrate contribute to the differential vulnerability of DA neurons and that enhancing G-substrate levels may be a neuroprotective strategy for the vulnerable A9 (SN) DA neurons in Parkinson's disease.
相对神经元易损性是神经退行性疾病的一个普遍但却知之甚少的特征。在帕金森病中,黑质(SN)(A9)中的多巴胺能(DA)神经元特别易损,而腹侧被盖区(A10)内相邻的DA神经元基本未受影响。我们之前的激光捕获显微切割和微阵列研究(Chung等人,2005年)表明,这些DA神经元之间的分子差异可能是它们不同易损性的基础。在此我们表明,G底物,一种丝氨酸/苏氨酸蛋白磷酸酶的内源性抑制剂,在啮齿动物和人类中脑中,与A9 DA神经元相比,在A10中表达更高。G底物的过表达保护多巴胺能BE(2)-M17细胞免受毒素影响,包括6-羟基多巴胺(6-OHDA)和MG-132(苄氧羰基-L-亮氨酰-L-亮氨酰-L-亮氨酸醛),而RNA干扰(RNAi)介导的内源性G底物敲低增加了它们对这些毒素的易损性。G底物在体外降低了6-OHDA介导的蛋白磷酸酶2A(PP2A)激活,并增加了PP2A靶点的磷酸化水平,包括Akt、糖原合酶激酶3β和细胞外信号调节激酶2,但不包括p38。对Akt进行RNAi减弱了G底物对6-OHDA的保护作用。在体内,将G底物通过慢病毒递送至大鼠黑质增加了磷酸化Akt的基线水平,并保护A9 DA神经元免受6-OHDA诱导的毒性。这些结果表明,G底物水平的内在差异导致了DA神经元的不同易损性,并且提高G底物水平可能是帕金森病中易损的A9(SN)DA神经元的一种神经保护策略。