CNS, Central nervous system

CNS,中枢神经系统
  • 文章类型: Journal Article
    精神障碍(MD)是非常普遍的,并且可能使人衰弱的复杂疾病,其原因仍然难以捉摸。研究这些疾病的病因或病理生理学的更深层次方面将是非常有益的,作为稀缺的知识在机械和分子途径肯定代表了一个重要的限制。MD和炎症/神经炎症之间的关联已被许多人广泛讨论和接受,据报道,在几个MD的患者中,有高水平的促炎细胞因子,如精神分裂症(SCZ),双相情感障碍(BD)和重度抑郁障碍(MDD),在其他人中。还报道了促炎标志物与症状强度的相关性。然而,在MD中观察到的炎症功能障碍的潜在机制尚未完全了解。在这种情况下,小胶质细胞功能障碍最近已经成为一个可能的关键因素,在神经炎症反应期间,小胶质细胞可以被过度激活,和过度产生促炎细胞因子,可以改变犬尿氨酸和谷氨酸信号,据报道。此外,小胶质细胞激活也导致增加的星形胶质细胞活性和随之而来的谷氨酸释放,它们都对中枢神经系统(CNS)有毒。此外,由于MD中的小胶质细胞活化增加,犬尿氨酸途径的产物显示出变化,然后影响多巴胺能,血清素能,和谷氨酸能信号通路。因此,在本次审查中,我们的目的是讨论神经炎症如何影响谷氨酸和犬尿氨酸信号通路,以及它们如何影响单胺能信号。随后还讨论了与MD主要症状的关联。因此,这项工作旨在通过提供对这些替代途径的见解,并通过揭示可能改善药物干预和/或治疗方案的策略以对抗MD的主要药理学上不匹配的症状的潜在靶标,从而为该领域做出贡献。作为SCZ。
    Mental disorders (MDs) are highly prevalent and potentially debilitating complex disorders which causes remain elusive. Looking into deeper aspects of etiology or pathophysiology underlying these diseases would be highly beneficial, as the scarce knowledge in mechanistic and molecular pathways certainly represents an important limitation. Association between MDs and inflammation/neuroinflammation has been widely discussed and accepted by many, as high levels of pro-inflammatory cytokines were reported in patients with several MDs, such as schizophrenia (SCZ), bipolar disorder (BD) and major depression disorder (MDD), among others. Correlation of pro-inflammatory markers with symptoms intensity was also reported. However, the mechanisms underlying the inflammatory dysfunctions observed in MDs are not fully understood yet. In this context, microglial dysfunction has recently emerged as a possible pivotal player, as during the neuroinflammatory response, microglia can be over-activated, and excessive production of pro-inflammatory cytokines, which can modify the kynurenine and glutamate signaling, is reported. Moreover, microglial activation also results in increased astrocyte activity and consequent glutamate release, which are both toxic to the Central Nervous System (CNS). Also, as a result of increased microglial activation in MDs, products of the kynurenine pathway were shown to be changed, influencing then the dopaminergic, serotonergic, and glutamatergic signaling pathways. Therefore, in the present review, we aim to discuss how neuroinflammation impacts on glutamate and kynurenine signaling pathways, and how they can consequently influence the monoaminergic signaling. The consequent association with MDs main symptoms is also discussed. As such, this work aims to contribute to the field by providing insights into these alternative pathways and by shedding light on potential targets that could improve the strategies for pharmacological intervention and/or treatment protocols to combat the main pharmacologically unmatched symptoms of MDs, as the SCZ.
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  • 文章类型: Journal Article
    长时间输注高剂量的犬尿烯酸(KYNA)可降低大鼠脊髓中的髓磷脂含量,同时保留轴突完整性,并且不会引起炎症反应。我们假设硬膜下输注高浓度的KYNA可以诱导鸡视神经(ON)的髓磷脂损失。然而,现有的将代理递送到ON的方法效率低下,非局部暴露,仅提供急性暴露。因此,我们开发了一种将KYNA持续递送至鸡ON的手术方法。简而言之,新颖的外科技术,这不包括眼外肌的切除,涉及切开皮肤和下面的筋膜鞘以进入肌肉锥内的视神经,在视神经硬膜植入导管,另一端在皮肤下退出轨道。导管在外侧can附近的皮肤下延伸,从耳朵到脖子后面,其中进行第二切口以植入渗透泵并将导管附接到渗透泵。印度墨水用于确认对视神经和交叉的长期持续给药。该手术模型用于研究KYNA对ON中髓磷脂损失的影响。将7天大的鸡的ON用50mMKYNA或磷酸盐缓冲盐水(PBS)输注7天。对KYNA输注的对侧ONg比率和蛋白质水平的分析表明髓鞘减少。这些发现证明了我们的手术方法用于将KYNA持续递送到ON的实用性,并暗示了KYNA在调节CNS髓鞘形成中的作用。
    Prolonged infusion of a high dose of kynurenic acid (KYNA) reduces the myelin content in the rat spinal cord with preservation of the axonal integrity and without inducing an inflammatory response. We hypothesized that subdural infusion of a high concentration of KYNA can induce myelin loss in the optic nerves (ONs) of chickens. However, existing methods to deliver agents to the ON are inefficient, unlocalized and provide only acute exposure. Thus, we developed a surgical approach for sustained delivery of KYNA to the chicken ON. In brief, the novel surgical technique, which does not include excision of the extraocular muscles, involves incision of the skin and underlying fascial sheath to access the optic nerve within the muscle cone, implantation of a catheter in the dura of the optic nerve, the other end of which exits the orbit under the skin. The catheter runs under the skin near the lateral canthus, over the ears to the back of the neck, where a second incision is made to both implant the osmotic pump and to attach the catheter to the osmotic pump. India ink was used to confirm prolonged sustained administration to the optic nerves and across the chiasm. This surgical model was used to investigate KYNA\'s effect(s) on myelin loss in the ON. ONs of 7-day old chickens were infused with 50 mM KYNA or phosphate buffered saline (PBS) for seven days. Analysis of KYNA-infused contralateral ON g-ratios and protein levels indicated a reduction in myelin. These findings demonstrate the utility of our surgical approach for sustained delivery of KYNA into the ON and suggest a role for KYNA in modulating CNS myelination.
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  • 文章类型: Journal Article
    IIIB型粘多糖贮积症(MPSIIIB)是一种超级病,没有批准治疗的致命儿科疾病。它是由溶酶体酶α-N-乙酰氨基葡萄糖苷酶(NAGLU)编码基因中的突变引起的。Tralesinidasealfa(TA)是一种融合蛋白,由重组NAGLU和修饰的人胰岛素样生长因子2组成,正在开发作为MPSIIIB的酶替代疗法。由于MPSIIIB是儿科疾病的安全性/毒性,在幼年非人灵长类动物中评估了TA的药代动力学和生物分布,这些灵长类动物每周进行5次侧脑室(ICV)或单次静脉(IV)输注TA。由ICV慢速管理的TA,ICV等体积推注或静脉输注耐受性良好,在临床观察中没有观察到影响,心电图或眼科参数,或呼吸频率。观察到的药物相关变化仅限于ICV施用后CSF中和沿ICV导管轨道的细胞浸润增加。这些发现与功能变化无关,与ICV导管的使用有关。CSFPK谱在所有测试条件下是一致的,并且在ICV施用后TA广泛分布在CNS中。观察到抗药物抗体,但似乎并未显着影响对TA的暴露。血浆中TA浓度与直接与大池接触的大脑区域之间的相关性表明,淋巴引流可能是CNS中TA清除的原因。数据支持通过等体积推注ICV输注向患有MPSIIIB的儿科患者施用TA。
    Mucopolysaccharidosis Type IIIB (MPS IIIB) is an ultrarare, fatal pediatric disease with no approved therapy. It is caused by mutations in the gene encoding for lysosomal enzyme alpha-N-acetylglucosaminidase (NAGLU). Tralesinidase alfa (TA) is a fusion protein comprised of recombinant NAGLU and a modified human insulin-like growth factor 2 that is being developed as an enzyme replacement therapy for MPS IIIB. Since MPS IIIB is a pediatric disease the safety/toxicity, pharmacokinetics and biodistribution of TA were evaluated in juvenile non-human primates that were administered up to 5 weekly intracerebroventricular (ICV) or single intravenous (IV) infusions of TA. TA administered by ICV slow-, ICV isovolumetric bolus- or IV-infusion was well-tolerated, and no effects were observed on clinical observations, electrocardiographic or ophthalmologic parameters, or respiratory rates. The drug-related changes observed were limited to increased cell infiltrates in the CSF and along the ICV catheter track after ICV administration. These findings were not associated with functional changes and are associated with the use of ICV catheters. The CSF PK profiles were consistent across all conditions tested and TA distributed widely in the CNS after ICV administration. Anti-drug antibodies were observed but did not appear to significantly affect the exposure to TA. Correlations between TA concentrations in plasma and brain regions in direct contact with the cisterna magna suggest glymphatic drainage may be responsible for clearance of TA from the CNS. The data support the administration of TA by isovolumetric bolus ICV infusion to pediatric patients with MPS IIIB.
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  • 文章类型: Case Reports
    原发性家族性脑钙化(PFBC)是一种特发性病理,其特征是在幕上区域,如端脑和间脑,以更广泛的形式,在小脑.脑膜瘤是最常见的中枢神经系统(CNS)肿瘤之一,通常与良好的预后有关。脑内或轴外肿瘤和PFBC的同时存在代表非常罕见的发生。一名72岁的女性患者因失眼危象和全身性癫痫发作而入院。她进行了脑部CT扫描,显示室旁幕上区域广泛的高密度,基底神经节和双侧小脑齿状核水平,PFBC的特点。合并的左额叶和较小的右颞叶轴外病变被发现,然后在脑MRI中被证实。患者接受了病变的显微外科手术切除,随后的组织学检查报告了脑膜上皮脑膜瘤(WHOI级)。根据我们的文献综述,这是第一篇报道颅内脑膜瘤和PFBC共存的论文。迄今为止,不可能提供发病机制和遗传机制之间的确切相关性。
    Primary familial brain calcification (PFBC) is an idiopathic pathology characterized by the development of calcific deposits in the supratentorial region such as telencephalon and diencephalon but also, in more extensive forms, in the cerebellum. Meningiomas are among the most common central nervous system (CNS) tumors generally related to a good prognosis. The simultaneous presence of intracerebral or extra-axial tumors and PFBC represents an exceedingly rare occurrence. A 72-year-old female patient was admitted to our department because of anoculogyric crisis followed by generalized seizures. She performed a brain CT scan which showed widespread hyperdensities in the paraventricular supratentorial region, basal ganglia and at the level of bilateral cerebellar dentate nuclei, characteristics of PFBC. Concomitant left frontal and smaller right temporal extra-axial lesions were identified and then confirmed in a brain MRI. The patient underwent a microsurgical resection of the lesion and subsequent histological examination reported a meningothelial meningioma (WHO Grade I). According to our literature review, this is the first paper that reports the coexistence of both intracranial meningiomas and PFBC. To date, it is not possible to provide an exact correlation between pathogenesis and genetic mechanism underlying this association.
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  • 文章类型: Journal Article
    微生理系统(MPS),一种用于体外测试平台的新技术,被认为是药物开发的有力工具。在中枢神经系统(CNS),血脑屏障(BBB)限制了循环物质从血管到大脑的渗透,从而保护CNS免受循环的异生物化合物的影响。同时,BBB通过在各个阶段引入挑战来阻碍药物开发,如药代动力学/药效学(PK/PD),安全评估,和疗效评估。为了解决这些问题,正在努力开发BBBMPS,特别是人性化类型。在这项研究中,我们建议最少的基本基准项目来建立BBBMPS的BBB相似度;这些标准支持最终用户确定候选BBBMPS的适当应用范围.此外,我们在二维(2D)人源化三细胞静态transwellBBBMPS中检查了这些基准项目,最常规的人细胞系BBBMPS设计。在基准项目中,P-gp和BCRP的外排率在两个独立的设施中显示出高重现性,而通过Glut1或TfR冥想的定向运输未得到证实。我们已经将上述实验的方案组织为标准操作程序(SOP)。我们在这里为SOP提供流程图,包括整个过程以及如何应用每个SOP。我们的研究是BBBMPS走向社会接受的重要发展步骤,它使最终用户能够检查和比较BBBMPS的性能。
    Microphysiological system (MPS), a new technology for in vitro testing platforms, have been acknowledged as a strong tool for drug development. In the central nervous system (CNS), the blood‒brain barrier (BBB) limits the permeation of circulating substances from the blood vessels to the brain, thereby protecting the CNS from circulating xenobiotic compounds. At the same time, the BBB hinders drug development by introducing challenges at various stages, such as pharmacokinetics/pharmacodynamics (PK/PD), safety assessment, and efficacy assessment. To solve these problems, efforts are being made to develop a BBB MPS, particularly of a humanized type. In this study, we suggested minimal essential benchmark items to establish the BBB-likeness of a BBB MPS; these criteria support end users in determining the appropriate range of applications for a candidate BBB MPS. Furthermore, we examined these benchmark items in a two-dimensional (2D) humanized tricellular static transwell BBB MPS, the most conventional design of BBB MPS with human cell lines. Among the benchmark items, the efflux ratios of P-gp and BCRP showed high reproducibility in two independent facilities, while the directional transports meditated through Glut1 or TfR were not confirmed. We have organized the protocols of the experiments described above as standard operating procedures (SOPs). We here provide the SOPs with the flow chart including entire procedure and how to apply each SOP. Our study is important developmental step of BBB MPS towards the social acceptance, which enable end users to check and compare the performance the BBB MPSs.
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  • 文章类型: Journal Article
    转移性脊柱黑色素瘤是一种罕见的侵袭性疾病,预后不良。我们回顾了转移性脊柱黑色素瘤的文献,专注于其流行病学,管理,和治疗结果。转移性脊柱黑色素瘤的人口统计学特征与皮肤黑色素瘤相似,皮肤原发性肿瘤往往是最常见的。传统上,减压手术干预和放疗被认为是治疗的支柱。立体定向放射外科已成为转移性脊柱黑色素瘤手术治疗的一种有前途的方法。虽然转移性脊柱黑色素瘤的生存结果仍然很差,近年来随着免疫检查点抑制的出现,它们有所改善,与手术和放疗结合使用。新的治疗方案仍在调查中,特别是对于免疫疗法难以治疗的患者。我们还探索了其中几个有希望的未来方向。然而,进一步调查治疗结果,理想情况下,结合来自随机对照试验的高质量前瞻性数据,需要确定转移性脊柱黑色素瘤的最佳管理。
    Metastatic spinal melanoma is a rare and aggressive disease process with poor prognosis. We review the literature on metastatic spinal melanoma, focusing on its epidemiology, management, and treatment outcomes. Demographics of metastatic spinal melanoma are similar to those for cutaneous melanoma, and cutaneous primary tumors tend to be most common. Decompressive surgical intervention and radiotherapy have traditionally been considered mainstays of treatment, and stereotactic radiosurgery has emerged as a promising approach in the operative management of metastatic spinal melanoma. While survival outcomes for metastatic spinal melanoma remain poor, they have improved in recent years with the advent of immune checkpoint inhibition, used in conjunction with surgery and radiotherapy. New treatment options remain under investigation, especially for patients with disease refractory to immunotherapy. We additionally explore several of these promising future directions. Nevertheless, further investigation of treatment outcomes, ideally incorporating high-quality prospective data from randomized controlled trials, is needed to identify optimal management of metastatic spinal melanoma.
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  • 文章类型: Journal Article
    活化的小胶质细胞分为促炎和抗炎功能状态。在抗炎状态下,活化的小胶质细胞有助于吞噬作用,神经修复和抗炎。Nrf2作为脑出血(ICH)后血肿清除的主要内源性调节因子备受关注。本研究旨在探讨Nrf2介导的小胶质细胞表型和吞噬作用在脑出血后血肿清除中的作用机制。体外实验,将BV-2细胞分为正常组和给药组(Nrf2-siRNA,Nrf2激动剂Monascin和血脂康)。体内实验,将小鼠分为5组:假手术,ICH+车辆,ICH+Nrf2-/-,ICH+Monascin和ICH+血脂康。在体外和体内,Monascin和血脂康给药后72小时,Nrf2、炎症相关因子Trem1、TNF-α和CD80的表达,通过Westernblot方法分析神经修复和吞噬相关因子如Trem2,CD206和BDNF。体外,BV-2细胞摄取荧光乳胶珠或红细胞,以研究小胶质细胞的吞噬能力。在体内,血红蛋白水平反映血肿体积。在这项研究中,Nrf2激动剂(Monascin和血脂康)在体内和体外均上调Trem2,CD206和BDNF的表达,而在体内和体外均降低Trem1,TNF-α和CD80的表达。同时,经过Monascin和血脂康治疗,小胶质细胞的吞噬能力在体外增加,体内神经功能缺损改善,血肿体积减少。这些结果在Nrf2-siRNA或Nrf2-/-小鼠中逆转。所有这些结果表明Nrf2增强血肿清除和神经修复,通过增强小胶质细胞吞噬作用和减轻神经炎症改善神经系统预后。
    Activated microglia are divided into pro-inflammatory and anti-inflammatory functional states. In anti-inflammatory state, activated microglia contribute to phagocytosis, neural repair and anti-inflammation. Nrf2 as a major endogenous regulator in hematoma clearance after intracerebral hemorrhage (ICH) has received much attention. This study aims to investigate the mechanism underlying Nrf2-mediated regulation of microglial phenotype and phagocytosis in hematoma clearance after ICH. In vitro experiments, BV-2 cells were assigned to normal group and administration group (Nrf2-siRNA, Nrf2 agonists Monascin and Xuezhikang). In vivo experiments, mice were divided into 5 groups: sham, ICH + vehicle, ICH + Nrf2-/-, ICH + Monascin and ICH + Xuezhikang. In vitro and in vivo, 72 h after administration of Monascin and Xuezhikang, the expression of Nrf2, inflammatory-associated factors such as Trem1, TNF-α and CD80, anti-inflammatory, neural repair and phagocytic associated factors such as Trem2, CD206 and BDNF were analyzed by the Western blot method. In vitro, fluorescent latex beads or erythrocytes were uptaken by BV-2 cells in order to study microglial phagocytic ability. In vivo, hemoglobin levels reflect the hematoma volume. In this study, Nrf2 agonists (Monascin and Xuezhikang) upregulated the expression of Trem2, CD206 and BDNF while decreased the expression of Trem1, TNF-α and CD80 both in vivo and in vitro. At the same time, after Monascin and Xuezhikang treatment, the phagocytic capacity of microglia increased in vitro, neurological deficits improved and hematoma volume lessened in vivo. These results were reversed in the Nrf2-siRNA or the Nrf2-/- mice. All these results indicated that Nrf2 enhanced hematoma clearance and neural repair, improved neurological outcomes through enhancing microglial phagocytosis and alleviating neuroinflammation.
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  • 文章类型: Case Reports
    抗髓磷脂少突胶质细胞糖蛋白(MOG)-免疫球蛋白G(IgG)相关疾病(MOGAD)是一种免疫介导的中枢神经系统(CNS)炎性脱髓鞘疾病,近年来已被广泛认可。它不同于多发性硬化症(MS)和视神经脊髓炎谱系障碍(NMOSD),它们是独立的疾病谱。在这里,我们报道了一个5岁男孩因发烧入院3天的案例,头痛,和呕吐。磁共振成像显示左丘脑异常高强度和肺炎支原体血清IgM阳性。阿奇霉素治疗后,头痛逐渐消失,但在入院后第6天出现瘫痪和尿潴留。MRI复检显示左丘脑原始异常信号明显减弱,但是大脑和脑脊髓出现了新的异常信号,血清MOG-IgG阳性。治疗后,孩子已经完全康复,仍在接受后续护理。我们认为,这是一例MOGAD的儿童,具有继发于肺炎支原体感染的双相ADEM表型,这对阐明MOGAD的病理生理学具有潜在价值。
    Anti-myelin oligodendrocyte glycoprotein (MOG)-immunoglobulin G (IgG) associated disorder (MOGAD) is an immune-mediated central nervous system (CNS) inflammatory demyelinating disorder that has been widely recognized in recent years. It is distinct from multiple sclerosis (MS) and neuromyelitis optica spectrum disorder (NMOSD), which are separate disease spectrums. Here we report the case of a 5-year-old boy who was admitted for 3 days with fever, headache, and vomiting. Magnetic resonance imaging revealed abnormal hyperintensity in the left thalamus and positive serum IgM for M. pneumoniae. After treatment with azithromycin, the headache gradually disappeared, but paralysis and urinary retention occurred on the 6th day after admission. MRI re-examination showed that the original abnormal signal in the left thalamus was significantly weakened, but new abnormal signals appeared in the brain and cerebrospinal cord, and the serum MOG-IgG was positive. After treatment, the child has fully recovered and is still receiving follow-up care. We believe that this is a case of MOGAD in a child with a biphasic ADEM phenotype secondary to M. pneumoniae infection, which has potential value in elucidating the pathophysiology of MOGAD.
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  • 文章类型: Journal Article
    未经证实:尽管心血管系统的稳态是由大脑皮层通过自主神经系统调节的,脑功能连接(FC)网络异常在心功能不全患者中的作用尚不清楚.这里,我们报道了以丘脑为基础的FC改变及其与冠心病(CHD)患者临床特征的关系.
    UNASSIGNED:我们采用静息态功能磁共振成像(rs-fMRI)采集26例冠心病患者和16例健康对照(HCs)的影像学数据。接下来,我们进行了基于丘脑的FC分析,分析了全脑的异常FC模式.随后,FC分析中存活的脑区的平均时间序列用于确定CHD患者与临床参数的相关性.
    UNASSIGNED:我们发现CHD和HCs患者的人口统计学和临床数据没有统计学上的显著差异。CHD患者在双侧丘脑和左半球之间表现出减少的FC模式,包括辅助电机区域,额上回,顶叶上回,顶下回,中扣带皮质,舌回和钙背沟。
    UNASSIGNED:这些发现不仅对阐明脑功能失衡与心血管系统之间的关系有意义,而且还提供了有价值的见解,以指导未来通过脑-心轴进行心脏自主神经调节的评估和管理。
    UNASSIGNED: Although homeostasis of the cardiovascular system is regulated by the cerebral cortex via the autonomic nervous system, the role of abnormal brain functional connectivity (FC) networks in patients with cardiac dysfunction remains unclear. Here, we report thalamus-based FC alterations and their relationship with clinical characteristics in patients with coronary heart disease (CHD).
    UNASSIGNED: We employed resting-state functional magnetic resonance imaging (rs-fMRI) to acquire imaging data in twenty-six patients with CHD alongside sixteen healthy controls (HCs). Next, we performed a thalamus-based FC analysis to profile abnormal FC patterns in the whole brain. Subsequently, the mean time series of the brain regions that survived in the FC analysis were used to determine correlations with clinical parameters in patients with CHD.
    UNASSIGNED: We found no statistically significant differences in demographic and clinical data between patients with CHD and HCs. Patients with CHD showed decreased FC patterns between bilateral thalami and left hemisphere, encompassing supplementary motor area, superior frontal gyrus, superior parietal gyrus, inferior parietal gyrus, middle cingulate cortex, lingual gyrus and calcarine sulcus.
    UNASSIGNED: These findings not only have implications in clarifying the relationship between cerebral functional imbalance and cardiovascular system, but also provide valuable insights to guide future evaluation and management of cardiac autonomic regulation via the brain-heart axis.
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  • 文章类型: Case Reports
    虽然在目前的文献中有很好的描述,当医生面对时,神经囊虫病[NCC]仍然是一个谜。这部分是由于中枢神经系统[CNS]上的寄生虫感染的偶然性。这些包括感染的单个或多个解剖部位,寄生虫病阶段,以及由此产生的炎症反应。因此,NCC可以呈现复杂的症状表现,使治疗方案高度个性化。尽管干预,由于感染的性质,治疗后可能会出现其他障碍。我们介绍了一个快速进展的症状性NCC的病例,最初成功治疗,然而,最终会屈服于脑室炎的并发症。
    Although well described in the current literature, Neurocysticercosis [NCC] remains an enigma when confronted by practitioners. This is in part due to the haphazard nature of the parasitic infection on the central nervous system [CNS]. These include single or multiple anatomic sites of infection, stage of parasitosis, and the resultant inflammatory response. As a result, NCC can present with a complex constellation of symptomatic presentations, making therapeutic regiments highly individualized. Despite intervention, other impediments may arise post-therapy due to the nature of the infection. We present a case of rapidly progressive symptomatic NCC that initially was successfully treated, however would eventually succumb to complications of ventriculitis.
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