C. Warren Olanow, Raymond T. Bartus, Tiffany L. Baumann, Stewart Factor, Nicholas Boulis, Mark Stacy, Dennis A. Turner, William Marks, Paul Larson

首页> 外文期刊>Annals of neurology >C. Warren Olanow, Raymond T. Bartus, Tiffany L. Baumann, Stewart Factor, Nicholas Boulis, Mark Stacy, Dennis A. Turner, William Marks, Paul Larson

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C. Warren Olanow, Raymond T. Bartus, Tiffany L. Baumann, Stewart Factor, Nicholas Boulis, Mark Stacy, Dennis A. Turner, William Marks, Paul Larson

机译：C. Warren Olanow，Raymond T. Bartus，Tiffany L. BAUMANN，Stewart因子，尼古拉斯伯利，Mark Stacy，Dennis A. Turner，William Marks，Paul Larson

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Objective: A 12-month double-blind sham-surgery-controlled trial assessing adeno-associated virus type 2 (AAV2)-neurturin injected into the putamen bilaterally failed to meet its primary endpoint, but showed positive results for the primary endpoint in the subgroup of subjects followed for 18 months and for several secondary endpoints. Analysis of postmortem tissue suggested impaired axonal transport of neurturin from putamen to substantia nigra. In the present study, we tested the safety and efficacy of AAV2-neurturin delivered to putamen and substantia nigra. Methods: We performed a 15- to 24-month, multicenter, double-blind trial in patients with advanced Parkinson disease (PD) who were randomly assigned to receive bilateral AAV2-neurturin injected bilaterally into the substantia nigra (2.0 × 10~(11) vector genomes) and putamen (1.0 × 10~(12) vector genomes) or sham surgery. The primary endpoint was change from baseline to final visit performed at the time the last enrolled subject completed the 15-month evaluation in the motor subscore of the Unified Parkinson's Disease Rating Scale in the practically defined off state. Results: Fifty-one patients were enrolled in the trial. There was no significant difference between groups in the primary endpoint (change from baseline: AAV2-neurturin, -7.0 ±9.92; sham, -5.2 ± 10.01; p = 0.515) or in most secondary endpoints. Two subjects had cerebral hemorrhages with transient symptoms. No clinically meaningful adverse events were attributed to AAV2-neurturin.

机译：目的：12个月的双盲假手术控制试验评估腺相关病毒型2（AAV2）-NEURTURIN注入腐烂中，双侧未能满足其主要终点，但为亚组中的主要终点显示阳性结果受试者随访18个月和几个辅助端点。后期组织的分析表明，从腐败到基础NIGRA的神经素轴突运输受损。在本研究中，我们测试了Aav2-Neurururin的安全性和功效送给腐凝和体积NIGRA。方法：进行15至24个月，多中心，双盲试验，患有先进的帕金森病（Pd），被随机分配接受双侧注射的双侧AAV2-Neururin（2.0×10〜（11 ）载体基因组）和腐烂（1.0×10〜（12）载体基因组）或假手术。主要终点是在上次注册主题完成统一帕金森病评级规模的电机子科学中的15个月评估时，从基线改变到最终访问。结果：在试验中注册了五十一名患者。初级终点中的组之间没有显着差异（从基线的变化：Aav2-neurturin，-7.0±9.92; sham，-5.2±10.01; p = 0.515）或大多数次级端点。两个受试者具有脑出血，瞬态症状。没有临床有意义的不良事件归因于AAV2-Neurturin。

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《Annals of neurology》 |2015年第2期|共10页
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1. C. Warren Olanow, Raymond T. Bartus, Tiffany L. Baumann, Stewart Factor, Nicholas Boulis, Mark Stacy, Dennis A. Turner, William Marks, Paul Larson [J] . Annals of neurology . 2015,第2期

机译：C. Warren Olanow，Raymond T. Bartus，Tiffany L. BAUMANN，Stewart因子，尼古拉斯伯利，Mark Stacy，Dennis A. Turner，William Marks，Paul Larson
2. Erratum for the Research Article: “Loci associated with skin pigmentation identified in African populations” by Nicholas G. Crawford, D. E. Kelly, M. E. B. Hansen, M. H. Beltrame, S. Fan, S. L. Bowman, E. Jewett, A. Ranciaro, S. Thompson, Y. Lo, S. P. Pfeifer, J. D. Jensen, M. C. Campbell, W. Beggs, F. Hormozdiari, S. W. Mpoloka, G. G. Mokone, T. Nyambo, D. Wolde Meskel, G. Belay, J. Haut, NISC Comparative Sequencing Program, H. Rothschild, L. Zon, Y. Zhou, M. A. Kovacs, M. Xu, T. Zhang, K. Bishop, J. Sinclair, C. Rivas, E. Elliot, J. Choi, S. A. Li, B. Hicks, S. Burgess, C. Abnet, D. E. Watkins-Chow, E. Oceana, Y. S. Song, E. Eskin, K. M. Brown, M. S. Marks, S. K. Loftus, W. J. Pavan, M. Yeager, S. Chanock, S. A. Tishkoff [O] . 2020

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C. Warren Olanow, Raymond T. Bartus, Tiffany L. Baumann, Stewart Factor, Nicholas Boulis, Mark Stacy, Dennis A. Turner, William Marks, Paul Larson

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