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Effects of Neonatal Neural Progenitor Cell Implantation on Adult Neuroanatomy and Cognition in the Ts65Dn Model of Down Syndrome

机译:新生儿神经祖细胞植入对唐氏综合症Ts65Dn模型成人神经解剖结构和认知的影响

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摘要

As much of the aberrant neural development in Down syndrome (DS) occurs postnatally, an early opportunity exists to intervene and influence life-long cognitive development. Recent success using neural progenitor cells (NPC) in models of adult neurodegeneration indicate such therapy may be a viable option in diseases such as DS. Murine NPC (mNPC, C17.2 cell line) or saline were implanted bilaterally into the dorsal hippocampus of postnatal day 2 (PND 2) Ts65Dn pups to explore the feasibility of early postnatal treatment in this mouse model of DS. Disomic littermates provided karyotype controls for trisomic pups. Pups were monitored for developmental milestone achievement, and then underwent adult behavior testing at 14 weeks of age. We found that implanted mNPC survived into adulthood and migrated beyond the implant site in both karyotypes. The implantation of mNPC resulted in a significant increase in the density of dentate granule cells. However, mNPC implantation did not elicit cognitive changes in trisomic mice either neonatally or in adulthood. To the best of our knowledge, these results constitute the first assessment of mNPC as an early intervention on cognitive ability in a DS model.
机译:由于唐氏综合症(DS)的许多异常神经发育都在出生后发生,因此存在早期干预和影响终身认知发育的机会。在成年神经退行性疾病模型中使用神经祖细胞(NPC)的最新成功表明,这种治疗可能是DS等疾病的可行选择。将鼠NPC(mNPC,C17.2细胞系)或生理盐水双边植入到出生后第2天(PND 2)Ts65Dn幼仔的海马背侧,以探索在这种DS小鼠模型中进行早期产后治疗的可行性。二体同窝幼仔为三体幼崽提供了核型控制。监测幼崽的发育里程碑成就,然后在14周龄进行成年行为测试。我们发现,植入的mNPC在两个核型中都存活到成年并迁移到植入部位之外。 mNPC的植入导致齿状颗粒细胞密度显着增加。但是,mNPC植入并没有引起新生或成年三体小鼠的认知变化。据我们所知,这些结果构成了对mNPC的首次评估,作为对DS模型中认知能力的早期干预。

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