Selective neuronal expression of progranulin is sufficient to provide neuroprotective and anti-inflammatory effects after traumatic brain injury.

IF 9.3 1区医学 Q1 IMMUNOLOGY Journal of Neuroinflammation Pub Date : 2024-10-10 DOI:10.1186/s12974-024-03249-7

Sudena Wang, Marc-Philipp Weyer, Regina Hummel, Annett Wilken-Schmitz, Irmgard Tegeder, Michael K E Schäfer

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Abstract

Progranulin (PGRN), which is produced in neurons and microglia, is a neurotrophic and anti-inflammatory glycoprotein. Human loss-of-function mutations cause frontotemporal dementia, and PGRN knockout (KO) mice are a model for dementia. In addition, PGRN KO mice exhibit severe phenotypes in models of traumatic or ischemic central nervous system (CNS) disorders, including traumatic brain injury (TBI). It is unknown whether restoration of progranulin expression in neurons (and not in microglia) might be sufficient to prevent excessive TBI-evoked brain damage. To address this question, we generated mice with Nestin-Cre-driven murine PGRN expression in a PGRN KO line (PGRN-KO^NestinGrn) to rescue PGRN in neurons. PGRN expression analysis in primary CNS cell cultures from naïve mice and in (non-) injured brain tissue from PGRN-KO^NestinGrn revealed expression of PGRN in neurons but not in microglia. After experimental TBI, examination of the structural brain damage at 5 days post-injury (dpi) showed that the TBI-induced loss of brain tissue and hippocampal neurons was exacerbated in PGRN-KO^Grnflfl mice (PGRN knockout with the mGrn fl-STOP-fl allele, Cre-negative), as expected, whereas the tissue damage in PGRN-KO^NestinGrn mice was similar to that in PGRN-WT mice. Analysis of CD68⁺ immunofluorescent microglia and Cd68 mRNA expression showed that excessive microglial activation was rescued in PGRN-KO^NestinGrn mice, and the correlation of brain injury with Cd68 expression suggested that Cd68 was a surrogate marker for excessive brain injury caused by PGRN deficiency. The results show that restoring neuronal PGRN expression was sufficient to rescue the exacerbated neuropathology of TBI caused by PGRN deficiency, even in the absence of microglial PGRN. Hence, endogenous microglial PGRN expression was not essential for the neuroprotective or anti-inflammatory effects of PGRN after TBI in this study.

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选择性神经元表达原粒细胞蛋白足以在脑外伤后提供神经保护和抗炎作用。

Progranulin（PGRN）产生于神经元和小胶质细胞，是一种神经营养和抗炎糖蛋白。人类功能缺失突变会导致额颞叶痴呆症，PGRN 基因敲除（KO）小鼠是痴呆症的模型。此外，PGRN KO 小鼠在创伤性或缺血性中枢神经系统（CNS）疾病（包括创伤性脑损伤（TBI））模型中表现出严重的表型。恢复神经元（而非小胶质细胞）中原粒蛋白的表达是否足以防止创伤性脑损伤诱发的过度脑损伤，目前尚不清楚。为了解决这个问题，我们在 PGRN KO 株系（PGRN-KONestinGrn）中产生了 Nestin-Cre 驱动的小鼠 PGRN 表达，以挽救神经元中的 PGRN。在来自天真小鼠的初级中枢神经系统细胞培养物和来自 PGRN-KONestinGrn 的（非）损伤脑组织中的 PGRN 表达分析显示，神经元中有 PGRN 的表达，但小胶质细胞中没有。实验性创伤性脑损伤后，在损伤后 5 天（dpi）对脑组织结构损伤的检查显示，创伤性脑损伤引起的脑组织和海马神经元的损失在 PGRN-KOGrnflfl 小鼠（PGRN 基因敲除 mGrn fl-STOP-fl 等位基因，Cre 阴性）中如预期的那样加剧，而 PGRN-KONestinGrn 小鼠的组织损伤与 PGRN-WT 小鼠相似。对CD68+免疫荧光小胶质细胞和Cd68 mRNA表达的分析表明，PGRN-KONestinGrn小鼠过度的小胶质细胞活化得到了挽救，脑损伤与Cd68表达的相关性表明，Cd68是PGRN缺乏导致过度脑损伤的替代标记物。结果表明，恢复神经元 PGRN 的表达足以挽救因 PGRN 缺乏而加重的创伤性脑损伤神经病理学，即使在缺乏小胶质细胞 PGRN 的情况下也是如此。因此，在本研究中，内源性小胶质细胞 PGRN 的表达对于 PGRN 在创伤性脑损伤后的神经保护或抗炎作用并不是必不可少的。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Neuroinflammation 医学-神经科学

CiteScore

15.90

自引率

3.20%

发文量

276

审稿时长

1 months

期刊介绍： The Journal of Neuroinflammation is a peer-reviewed, open access publication that emphasizes the interaction between the immune system, particularly the innate immune system, and the nervous system. It covers various aspects, including the involvement of CNS immune mediators like microglia and astrocytes, the cytokines and chemokines they produce, and the influence of peripheral neuro-immune interactions, T cells, monocytes, complement proteins, acute phase proteins, oxidative injury, and related molecular processes. Neuroinflammation is a rapidly expanding field that has significantly enhanced our knowledge of chronic neurological diseases. It attracts researchers from diverse disciplines such as pathology, biochemistry, molecular biology, genetics, clinical medicine, and epidemiology. Substantial contributions to this field have been made through studies involving populations, patients, postmortem tissues, animal models, and in vitro systems. The Journal of Neuroinflammation consolidates research that centers around common pathogenic processes. It serves as a platform for integrative reviews and commentaries in this field.