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小鼠外周神经损伤后性二态性免疫和神经免疫变化:性别医学的新见解

Sexually Dimorphic Immune and Neuroimmune Changes Following Peripheral Nerve Injury in Mice: Novel Insights for Gender Medicine.

作者信息

Vacca Valentina, Marinelli Sara, De Angelis Federica, Angelini Daniela F, Piras Eleonora, Battistini Luca, Pavone Flaminia, Coccurello Roberto

机构信息

CNR-National Research Council, CNR, Institute of Biochemistry and Cell Biology, Monterotondo Scalo, 00015 Rome, Italy.

IRCCS Fondazione Santa Lucia, 00143 Rome, Italy.

出版信息

Int J Mol Sci. 2021 Apr 22;22(9):4397. doi: 10.3390/ijms22094397.

Abstract

Neuropathic pain (NeP) in humans is often a life-long condition with no effective therapy available. The higher incidence of female gender in NeP onset is worldwide reported, and although the cause is generally attributed to sex hormones, the actual mechanisms and the players involved are still unclear. Glial and immune cells take part in NeP development, and orchestrate the neuroimmune and inflammatory response, releasing pro-inflammatory factors with chemoattractant properties that activate resident immune cells and recruit immune cells from circulation. The neuro-immune crosstalk is a key contributor to pain hypersensitivity following peripheral nervous system injury. Our previous works showed that in spite of the fact that female mice had an earlier analgesic response than males following nerve lesion, the recovery from NeP was never complete, suggesting that this difference could occur in the very early stages after injury. To further investigate gender differences in immune and neuroimmune responses to NeP, we studied the main immune cells and mediators elicited both in plasma and sciatic nerves by peripheral nerve lesion. After injury, we found a different pattern of distribution of immune cell populations showing either a higher infiltration of T cells in nerves from females or a higher infiltration of macrophages in nerves from males. Moreover, in comparison to male mice, the levels of cytokines and chemokines were differently up- and down-regulated in blood and nerve lysates from female mice. Our study provides some novel insights for the understanding of gender-associated differences in the generation and perseveration of NeP as well as for the isolation of specific neurodegenerative mechanisms underlying NeP. The identification of gender-associated inflammatory profiles in neuropathy is of key importance for the development of differential biomarkers and gender-specific personalized medicine.

摘要

人类的神经性疼痛(NeP)通常是一种终身疾病,目前尚无有效的治疗方法。全世界都报道了NeP发病中女性的发病率较高,尽管其原因通常归因于性激素,但实际机制和涉及的因素仍不清楚。神经胶质细胞和免疫细胞参与NeP的发展,协调神经免疫和炎症反应,释放具有化学引诱特性的促炎因子,激活驻留免疫细胞并从循环中募集免疫细胞。神经免疫串扰是外周神经系统损伤后疼痛超敏反应的关键因素。我们之前的研究表明,尽管雌性小鼠在神经损伤后比雄性小鼠有更早的镇痛反应,但从NeP中恢复从未完全,这表明这种差异可能在损伤后的非常早期阶段就出现。为了进一步研究对NeP的免疫和神经免疫反应中的性别差异,我们研究了外周神经损伤在血浆和坐骨神经中引发的主要免疫细胞和介质。损伤后,我们发现免疫细胞群体的分布模式不同,雌性小鼠神经中T细胞浸润较高,而雄性小鼠神经中巨噬细胞浸润较高。此外,与雄性小鼠相比,雌性小鼠血液和神经裂解物中细胞因子和趋化因子的水平上调和下调情况不同。我们的研究为理解NeP产生和持续存在中的性别相关差异以及分离NeP潜在的特定神经退行性机制提供了一些新的见解。确定神经病变中与性别相关的炎症特征对于开发差异生物标志物和性别特异性个性化医学至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aaeb/8122838/ac59bb4b1dfa/ijms-22-04397-g001.jpg

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