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帕金森病灵长类动物模型中胚胎干细胞源性神经干细胞移植后多巴胺功能的多示踪剂评估

Multitracer assessment of dopamine function after transplantation of embryonic stem cell-derived neural stem cells in a primate model of Parkinson's disease.

作者信息

Muramatsu Shin-Ichi, Okuno Tsuyoshi, Suzuki Yutaka, Nakayama Takashi, Kakiuchi Takeharu, Takino Naomi, Iida Asako, Ono Fumiko, Terao Keiji, Inoue Nobuo, Nakano Imaharu, Kondo Yasushi, Tsukada Hideo

机构信息

Divison of Neurology, Department of Medicine, Jichi Medical University, Shimotsuke, Tochigi, Japan.

出版信息

Synapse. 2009 Jul;63(7):541-8. doi: 10.1002/syn.20634.

DOI:10.1002/syn.20634
PMID:19253400
Abstract

The ability of primate embryonic stem (ES) cells to differentiate into dopamine (DA)-synthesizing neurons has raised hopes of creating novel cell therapies for Parkinson's disease (PD). As the primary purpose of cell transplantation in PD is restoration of dopaminergic neurotransmission in the striatum, in vivo assessment of DA function after grafting is necessary to achieve better therapeutic effects. A chronic model of PD was produced in two cynomolgus monkeys (M-1 and M-2) by systemic administration of neurotoxin. Neural stem cells (NSCs) derived from cynomolgus ES cells were implanted unilaterally in the putamen. To evaluate DA-specific functions, we used multiple [(11)C]-labeled positron emission tomography (PET) tracers, including [beta-(11)C]L-3,4-dihydroxyphenylalanine (L-[beta-(11)C]DOPA, DA precursor ligand), [(11)C]-2beta-carbomethoxy-3beta-(4-fluorophenyl)tropane ([(11)C]beta-CFT, DA transporter ligand) and [(11)C]raclopride (D(2) receptor ligand). At 12 weeks after grafting NSCs, PET demonstrated significantly increased uptake of L-[beta-(11)C]DOPA (M-1:41%, M-2:61%) and [(11)C]beta-CFT (M-1:31%, M-2:36%) uptake in the grafted putamen. In addition, methamphetamine challenge in M-2 induced reduced [(11)C]raclopride binding (16%) in the transplanted putamen, suggesting release of DA. These results show that transplantation of NSCs derived from cynomolgus monkey ES cells can restore DA function in the putamen of a primate model of PD. PET with multitracers is useful for functional studies in developing cell-based therapies against PD.

摘要

灵长类胚胎干细胞分化为多巴胺(DA)合成神经元的能力,为帕金森病(PD)创造新的细胞疗法带来了希望。由于PD细胞移植的主要目的是恢复纹状体中的多巴胺能神经传递,因此移植后对DA功能进行体内评估对于获得更好的治疗效果是必要的。通过全身给予神经毒素,在两只食蟹猴(M-1和M-2)中建立了PD慢性模型。将源自食蟹猴ES细胞的神经干细胞(NSCs)单侧植入壳核。为了评估DA的特定功能,我们使用了多种[(11)C]标记的正电子发射断层扫描(PET)示踪剂,包括[β-(11)C]L-3,4-二羟基苯丙氨酸(L-[β-(11)C]多巴,DA前体配体)、[(11)C]-2β-甲氧基羰基-3β-(4-氟苯基)托烷([(11)C]β-CFT,DA转运体配体)和[(11)C]雷氯必利(D2受体配体)。在移植NSCs 12周后,PET显示移植的壳核中L-[β-(11)C]多巴摄取量显著增加(M-1:41%,M-2:61%),[(11)C]β-CFT摄取量也显著增加(M-1:31%,M-2:36%)。此外,对M-2进行甲基苯丙胺激发试验,导致移植的壳核中[(11)C]雷氯必利结合减少(16%),提示有DA释放。这些结果表明,移植源自食蟹猴ES细胞的NSCs可以恢复PD灵长类模型壳核中的DA功能。多示踪剂PET对开发针对PD的细胞疗法的功能研究很有用。

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