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在阿尔茨海默病和帕金森病中,蓝斑核的神经元损失比基底核和黑质更严重。

Neuronal loss is greater in the locus coeruleus than nucleus basalis and substantia nigra in Alzheimer and Parkinson diseases.

作者信息

Zarow Chris, Lyness Scott A, Mortimer James A, Chui Helena C

机构信息

Department of Neurology, University of Southern California, Los Angeles, CA, USA.

出版信息

Arch Neurol. 2003 Mar;60(3):337-41. doi: 10.1001/archneur.60.3.337.

Abstract

CONTEXT

Alzheimer disease (AD) and Parkinson disease (PD) are associated with neuronal degeneration in major subcortical nuclei, but few studies have examined the neuronal degeneration in these nuclei concurrently.

OBJECTIVE

To identify clinical and pathological correlates of neuronal loss in the nucleus basalis (NB), locus coeruleus (LC), and substantia nigra pars compacta (SN) in AD and PD.

DESIGN

The study sample comprised 86 cases with pathologically confirmed AD, 19 cases with PD, and 13 healthy elderly control subjects. The number of nucleolated neurons was counted in representative sections of the NB, LC, and SN. Effect sizes (ES) were computed to determine the standardized difference in cell counts relative to healthy controls.

RESULTS

Cases of AD showed the greatest neuronal loss in the LC (ES = 3.16) followed by the NB (ES = 1.10), but variable loss in the SN (ES = 0.16). Cases of PD also showed the greatest neuronal loss in the LC (ES = 6.47), followed by the SN (ES = 2.58) and the NB (ES = 0.85). Significant correlations were found between the number of neurons in the NB and LC in PD (r = 0.54, P<.05), as well as AD (r = 0.24, P<.05). The duration of illness correlated with greater neuronal loss in the LC and NB in AD, and greater neuronal loss in the SN in PD.

CONCLUSIONS

For both AD and PD the greatest neuronal loss was found in the LC. In AD, neuronal loss was most severe and best correlated with the duration of illness in the LC, rather than in NB as traditionally expected. Correlations between neuronal loss in the LC and NB (but not SN) in both PD and AD suggest that the former 2 nuclei may share common pathogenetic susceptibilities. Given the prominent loss of neurons in the LC, detection and treatment of noradrenergic deficiencies warrant attention in both AD and PD.

摘要

背景

阿尔茨海默病(AD)和帕金森病(PD)与主要皮质下核团的神经元变性有关,但很少有研究同时检测这些核团中的神经元变性情况。

目的

确定AD和PD中基底核(NB)、蓝斑(LC)和黑质致密部(SN)神经元丢失的临床和病理相关性。

设计

研究样本包括86例经病理证实的AD患者、19例PD患者和13名健康老年对照者。在NB、LC和SN的代表性切片中计数有核仁神经元的数量。计算效应大小(ES)以确定相对于健康对照者细胞计数的标准化差异。

结果

AD患者中,LC的神经元丢失最为严重(ES = 3.16),其次是NB(ES = 1.10),而SN的神经元丢失情况不一(ES = 0.16)。PD患者同样是LC的神经元丢失最为严重(ES = 6.47),其次是SN(ES = 2.58)和NB(ES = 0.85)。在PD(r = 0.54,P<0.05)以及AD(r = 0.24,P<0.05)中,NB和LC中的神经元数量之间存在显著相关性。疾病持续时间与AD中LC和NB中更严重的神经元丢失以及PD中SN中更严重的神经元丢失相关。

结论

AD和PD中,LC的神经元丢失最为严重。在AD中,神经元丢失最为严重且与LC而非传统预期的NB中的疾病持续时间最相关。PD和AD中LC和NB(而非SN)的神经元丢失之间的相关性表明,前两个核团可能具有共同的致病易感性。鉴于LC中神经元的显著丢失,去甲肾上腺素能缺乏的检测和治疗在AD和PD中均值得关注。

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