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帕金森病和亨廷顿病患者的猪异种移植:初步结果。

Porcine xenografts in Parkinson's disease and Huntington's disease patients: preliminary results.

作者信息

Fink J S, Schumacher J M, Ellias S L, Palmer E P, Saint-Hilaire M, Shannon K, Penn R, Starr P, VanHorne C, Kott H S, Dempsey P K, Fischman A J, Raineri R, Manhart C, Dinsmore J, Isacson O

机构信息

Genzyme Corporation, Cambridge, MA 02139, USA.

出版信息

Cell Transplant. 2000 Mar-Apr;9(2):273-8. doi: 10.1177/096368970000900212.

Abstract

The observation that fetal neurons are able to survive and function when transplanted into the adult brain fostered the development of cellular therapy as a promising approach to achieve neuronal replacement for treatment of diseases of the adult central nervous system. This approach has been demonstrated to be efficacious in patients with Parkinson's disease after transplantation of human fetal neurons. The use of human fetal tissue is limited by ethical, infectious, regulatory, and practical concerns. Other mammalian fetal neural tissue could serve as an alternative cell source. Pigs are a reasonable source of fetal neuronal tissue because of their brain size, large litters, and the extensive experience in rearing them in captivity under controlled conditions. In Phase I studies porcine fetal neural cells grafted unilaterally into Parkinson's disease (PD) and Huntington's disease (HD) patients are being evaluated for safety and efficacy. Clinical improvement of 19% has been observed in the Unified Parkinson's Disease Rating Scale "off" state scores in 10 PD patients assessed 12 months after unilateral striatal transplantation of 12 million fetal porcine ventral mesencephalic (VM) cells. Several patients have improved more than 30%. In a single autopsied PD patient some porcine fetal VM cells were observed to survive 7 months after transplantation. Twelve HD patients have shown a favorable safety profile and no change in total functional capacity score 1 year after unilateral striatal placement of up to 24 million fetal porcine striatal cells. Xenotransplantation of fetal porcine neurons is a promising approach to delivery of healthy neurons to the CNS. The major challenges to the successful use of xenogeneic fetal neuronal cells in neurodegenerative diseases appear to be minimizing immune-mediated rejection, management of the risk of xenotic (cross-species) infections, and the accurate assessment of clinical outcome of diseases that are slowly progressive.

摘要

胎儿神经元移植到成人大脑后能够存活并发挥功能,这一发现推动了细胞疗法的发展,使其成为一种有前景的方法,有望实现神经元替代,用于治疗成人中枢神经系统疾病。在移植人类胎儿神经元后,这种方法已被证明对帕金森病患者有效。人类胎儿组织的使用受到伦理、感染、监管和实际问题的限制。其他哺乳动物的胎儿神经组织可作为替代细胞来源。猪是胎儿神经元组织的合理来源,因为它们的脑大小合适、产仔多,且在可控条件下圈养繁殖的经验丰富。在I期研究中,正在评估将猪胎儿神经细胞单侧移植到帕金森病(PD)和亨廷顿病(HD)患者体内的安全性和有效性。在10名PD患者中,单侧纹状体移植1200万个胎儿猪腹侧中脑(VM)细胞12个月后进行评估,统一帕金森病评定量表“关”状态评分的临床改善率为19%。几名患者的改善率超过了30%。在一名接受尸检的PD患者中,观察到一些猪胎儿VM细胞在移植后存活了7个月。12名HD患者在单侧纹状体植入多达2400万个胎儿猪纹状体细胞1年后,显示出良好的安全性,总功能能力评分无变化。胎儿猪神经元异种移植是一种将健康神经元输送到中枢神经系统的有前景的方法。在神经退行性疾病中成功使用异种胎儿神经元细胞的主要挑战似乎是尽量减少免疫介导的排斥反应、管理异种(跨物种)感染风险,以及准确评估缓慢进展性疾病的临床结果。

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