PrP基因的剂量决定了痒病病理中病变的时间,而不是最终的强度或分布。

J C Manson, A R Clarke, P A McBride, I McConnell, J Hope
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摘要

我们已经生产出了一种针对具有非活性PrP基因的小鼠系的基因。在这种突变杂合的动物中,与野生型小鼠相比,PrP mRNA在整个大脑中减少了约50%。与野生型小鼠相比,杂合子中PrPc的稳态水平也显著降低。在突变纯合的小鼠大脑中未检测到PrP mRNA和蛋白。我们用野生型小鼠、杂合型小鼠和纯合型小鼠感染了ME7突变。基因剂量效应可以在疾病发病时间和疾病症状发展期间看到。杂合子在220天左右发病,到280天达到终末期。在野生型小鼠中,疾病在130天左右发病,在160天左右进入终末期。PrP-/-小鼠对疾病的抵抗力长达475天。杂合小鼠的PrP沉积开始于与野生型小鼠相同的脑区,早在50天就可以检测到。杂合子大脑中PrP沉积的模式与野生型小鼠相同,在疾病末期沉积的数量与野生型小鼠相当。在野生型和杂合型小鼠中,液泡形成的时间晚于PrP沉积的时间,其在疾病终末期的分布和程度相似。这些结果表明,疾病的迹象,液泡化和PrP沉积依赖于PrPc的速率依赖方式。
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PrP gene dosage determines the timing but not the final intensity or distribution of lesions in scrapie pathology.

We have produced by gene targeting a mouse line with an inactive PrP gene. In animals heterozygous for this mutation, PrP mRNA is reduced by approximately 50% throughout the brain compared with wild type mice. The steady-state level of PrPc is also significantly reduced in heterozygotes compared to wild type mice. PrP mRNA and protein are not detected in brains of mice homozygous for the mutation. We have infected wild type mice and mice heterozygous and homozygous for the mutation with the ME7 strain of scrapie. A gene dosage effect can be seen in time of disease onset and period over which the disease symptoms develop. In heterozygotes disease onset occurs around 220 days and terminal stages are reached by 280 days. In wild type mice disease onset occurs around 130 days and the terminal stages by 160 days. The PrP-/- mice are resistant to disease up to 475 days. PrP deposition in heterozygous mice starts in the same brain area as wild type mice and can be detected as early as 50 days. The pattern of PrP deposition in the brain of heterozygotes follows an identical course to that observed in wild type mice and by terminal stages of disease the amount deposited is equivalent to wild type mice. Vacuolation is detected later than PrP deposition and distribution and degree in the terminal stages of disease is similar in wild type and heterozygous mice. These results show that signs of disease, vacuolation and PrP deposition are dependent upon PrPc in a rate dependent manner.

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