Differential gene expression profiles in the hippocampus of senescence-accelerated mouse

Tipo de material: Texto

TextoSeries ; NeuroBiology of Aging, 28(4), p.497-506, 2007Trabajos contenidos:

Cheng, X
Zhou, W
Zhang, Y
Zhou, D
Yang, R
Chen, L

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Resumen: The senescence-accelerated mouse (SAM)is an animal model for studying senescence and age-associated disorders due to its inherited aging phenotype. The SAM/prone8 (SAMP8)is a useful animal model to investigate the fundamental mechanisms involved in age-related learning and memory deficits that may have relevance to age-associated AD, while SAM/resistant1 (SAMR1)shows normal. To identify genes rendering the cognitive deterioration with aging, the subtractive cDNA libraries containing 1924 clones with the positive ratio of 96.18

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The senescence-accelerated mouse (SAM)is an animal model for studying senescence and age-associated disorders due to its inherited aging phenotype. The SAM/prone8 (SAMP8)is a useful animal model to investigate the fundamental mechanisms involved in age-related learning and memory deficits that may have relevance to age-associated AD, while SAM/resistant1 (SAMR1)shows normal. To identify genes rendering the cognitive deterioration with aging, the subtractive cDNA libraries containing 1924 clones with the positive ratio of 96.18

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