Nuffield Department of Clinical Neurosciences, University of Oxford, Oxford, UK.
Department of Biomedical and Neuromotor Sciences, University of Bologna, Bologna, Italy.
Brain. 2019 Jul 1;142(7):2000-2012. doi: 10.1093/brain/awz119.
Serum antibodies that bind to the surface of neurons or glia are associated with a wide range of rare but treatable CNS diseases. In many, if not most instances, the serum levels are higher than CSF levels yet most of the reported attempts to reproduce the human disease in mice have used infusion of antibodies into the mouse cerebral ventricle(s) or intrathecal space. We used the intraperitoneal route and injected purified plasma IgG from either a CASPR2-antibody-positive patient (n = 10 mice) or healthy individual (n = 9 mice) daily for 8 days. Lipopolysaccharide was injected intraperitoneally on Day 3 to cause a temporary breach in the blood brain barrier. A wide range of baseline behaviours, including tests of locomotion, coordination, memory, anxiety and social interactions, were established before the injections and tested from Day 5 until Day 11. At termination, brain tissue was analysed for human IgG, CASPR2 and c-fos expression, lymphocyte infiltration, and neuronal, astrocytic and microglial markers. Mice exposed to CASPR2-IgG, compared with control-IgG injected mice, displayed reduced working memory during the continuous spontaneous alternation test with trends towards reduced short-term and long-term memories. In the open field tests, activities were not different from controls, but in the reciprocal social interaction test, CASPR2-IgG injected mice showed longer latency to start interacting, associated with more freezing behaviour and reduced non-social activities of rearing and grooming. At termination, neuropathology showed more IgG deposited in the brains of CASPR2-IgG injected mice, but a trend towards increased CASPR2 expression; these results were mirrored in short-term in vitro experiments where CASPR2-IgG binding to hippocampal neurons and to CASPR2-transfected HEK cells led to some internalization of the IgG, but with a trend towards higher surface CASPR2 expression. Despite these limited results, in the CASPR2-IgG injected mouse brains there was increased c-fos expression in the piriform-entorhinal cortex and hypothalamus, and a modest loss of Purkinje cells. There was also increased microglia density, morphological changes in both microglia and astrocytes and raised complement C3 expression on astrocytes, all consistent with glial activation. Patients with CASPR2 antibodies can present with a range of clinical features reflecting central, autonomic and peripheral dysfunction. Although the behavioural changes in mice were limited to social interactions and mild working-memory defects, the neuropathological features indicate potentially widespread effects of the antibodies on different brain regions.
与广泛的罕见但可治疗的中枢神经系统疾病相关的是结合神经元或神经胶质表面的血清抗体。在许多情况下,如果不是大多数情况下,血清水平高于脑脊液水平,但大多数报道的试图在小鼠中重现人类疾病的尝试都使用将抗体输注到小鼠脑室(或鞘内空间)中。我们使用腹腔途径,每天向 10 只 CASPR2 抗体阳性患者(n = 10 只小鼠)或健康个体(n = 9 只小鼠)的纯化血浆 IgG 注射,持续 8 天。在第 3 天,腹腔内注射脂多糖以暂时破坏血脑屏障。在注射之前建立了广泛的基线行为,包括运动、协调、记忆、焦虑和社交互动测试,并从第 5 天测试到第 11 天。在终点时,分析脑组织中人 IgG、CASPR2 和 c-fos 表达、淋巴细胞浸润以及神经元、星形胶质细胞和小胶质细胞标志物。与注射对照 IgG 的小鼠相比,暴露于 CASPR2-IgG 的小鼠在连续自发交替测试中表现出工作记忆减少,并且短期和长期记忆减少的趋势。在开阔场测试中,活动与对照无差异,但在互惠性社会互动测试中,CASPR2-IgG 注射的小鼠开始互动的潜伏期更长,与更多的冻结行为和减少的非社交活动梳理和修饰相关。在终点时,神经病理学显示在 CASPR2-IgG 注射的小鼠脑中沉积了更多的 IgG,但 CASPR2 表达呈增加趋势;这些结果在短期的体外实验中得到了反映,其中 CASPR2-IgG 与海马神经元和 CASPR2 转染的 HEK 细胞结合导致 IgG 的一些内化,但表面 CASPR2 表达呈增加趋势。尽管结果有限,但在 CASPR2-IgG 注射的小鼠脑中,梨状皮层-内嗅皮层和下丘脑的 c-fos 表达增加,浦肯野细胞轻度丢失。小胶质细胞密度增加,小胶质细胞和星形胶质细胞的形态变化以及星形胶质细胞上补体 C3 表达升高,所有这些都与神经胶质激活一致。CASPR2 抗体患者可能表现出一系列反映中枢、自主和外周功能障碍的临床特征。尽管小鼠的行为变化仅限于社交互动和轻度工作记忆缺陷,但神经病理学特征表明抗体对不同脑区可能有广泛的影响。
