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Age-Related Changes in the Pattern Electroretinogram of Normal and Glatiramer Acetatea??Immunized Rats

机译:正常和Glatiramer Acetatea ??免疫大鼠的模式视网膜电图与年龄相关的变化

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Purpose.: Age-related changes in retinal ganglion cell (RGC) activity may impact results of long-term functional studies of disease progression and drug efficacy in humans and animal models. Though these changes can be evaluated using the pattern electroretinogram (PERG), longitudinal studies suffer from failure of follow-up from birth to senescence. Our aim was to perform a long-term, longitudinal study evaluating age-related changes in the rat PERG, by conducting repeated, serial recordings in the same animals. Additionally, we tested the hypothesis that neuroprotective treatment using glatiramer acetate (COP-1) immunization may delay age-related decline in function. Methods.: PERG was recorded from six untreated and seven Cop-1a??immunized Lewis rats. Recordings were conducted at 2- to 4-week intervals from age 5 to 59 weeks. Results.: PERG amplitudes significantly increased between 5 to 7 weeks of age, and decreased from age 30 weeks onward (P = 0.016 and 0.0002, respectively). Amplitudes fluctuated insignificantly in weeks 7 to 30, with peak amplitudes reached at age 18 weeks in most spatial frequencies tested. N2 implicit times were shortened, mainly during weeks 5 to 18 and 40 to 59 (P 0.001). PERG amplitudes of Cop-1a??treated rats were similar to controls (P = 0.137) but peaked later (22a??26 weeks). Conclusions.: This 14-month-long study provided accurate measurement of developmental and aging changes of rat RGC function using repeated testing of individual animals. We found functional development to extend beyond the reported period of structural changes. Cop-1a??immunized rats were not protected against age-related decline in inner retinal function, although their PERG maturation dynamics were altered.
机译:目的:视网膜神经节细胞(RGC)活性的年龄相关变化可能会影响人类和动物模型中疾病进展和药物功效的长期功能研究结果。尽管可以使用视网膜电图(PERG)评估这些变化,但纵向研究仍遭受从出生到衰老的随访失败。我们的目的是通过对同一只动物进行重复的连续记录,进行长期的纵向研究,以评估大鼠PERG中与年龄相关的变化。此外,我们测试了使用醋酸格拉替雷(COP-1)免疫进行神经保护治疗可能会延迟与年龄有关的功能下降的假说。方法:从六只未经治疗的和七只经Cop-1aβ免疫的Lewis大鼠中记录PERG。从5到59周的时间间隔为2到4周进行记录。结果:PERG振幅在5至7周龄之间显着增加,而从30周龄开始下降(分别为P = 0.016和0.0002)。在大多数测试的空间频率中,振幅在第7到30周波动不大,在18周龄时达到峰值。 N2隐式时间缩短了,主要在第5至18周和40至59周内(P <0.001)。经Cop-1aβ处理的大鼠的PERG振幅与对照组相似(P = 0.137),但后来达到峰值(22aβ26周)。结论:这项为期14个月的研究通过反复测试单个动物,提供了大鼠RGC功能发育和衰老变化的准确测量。我们发现功能开发已超出报告的结构变化时期。尽管他们的PERG成熟动态发生了改变,但接受Cop-1aβ免疫的大鼠并未受到年龄相关的内部视网膜功能下降的保护。

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