Bastien Dominic, Bellver Landete Victor, Lessard Martine, Vallières Nicolas, Champagne Mathieu, Takashima Akira, Tremblay Marie-Ève, Doyon Yannick, Lacroix Steve
Centre de Recherche du Centre Hospitalier Universitaire (CHU) de Québec-CHUL et Département de Médecine Moléculaire de l'Université Laval, Québec, Québec G1V 4G2, Canada, and.
Department of Medical Microbiology and Immunology, University of Toledo College of Medicine, Toledo, Ohio 43614-5806.
J Neurosci. 2015 Jul 29;35(30):10715-30. doi: 10.1523/JNEUROSCI.0498-15.2015.
Spinal cord injury (SCI) causes the release of danger signals by stressed and dying cells, a process that leads to neuroinflammation. Evidence suggests that inflammation plays a role in both the damage and repair of injured neural tissue. We show that microglia at sites of SCI rapidly express the alarmin interleukin (IL)-1α, and that infiltrating neutrophils and macrophages subsequently produce IL-1β. Infiltration of these cells is dramatically reduced in both IL-1α(-/-) and IL-1β(-/-) mice, but only IL-1α(-/-) mice showed rapid (at day 1) and persistent improvements in locomotion associated with reduced lesion volume. Similarly, intrathecal administration of the IL-1 receptor antagonist anakinra restored locomotor function post-SCI. Transcriptome analysis of SCI tissue at day 1 identified the survival factor Tox3 as being differentially regulated exclusively in IL-1α(-/-) mice compared with IL-1β(-/-) and wild-type mice. Accordingly, IL-1α(-/-) mice have markedly increased Tox3 levels in their oligodendrocytes, beginning at postnatal day 10 (P10) and persisting through adulthood. At P10, the spinal cord of IL-1α(-/-) mice showed a transient increase in mature oligodendrocyte numbers, coinciding with increased IL-1α expression in wild-type animals. In adult mice, IL-1α deletion is accompanied by increased oligodendrocyte survival after SCI. TOX3 overexpression in human oligodendrocytes reduced cellular death under conditions mimicking SCI. These results suggest that IL-1α-mediated Tox3 suppression during the early phase of CNS insult plays a crucial role in secondary degeneration.
The mechanisms underlying bystander degeneration of neurons and oligodendrocytes after CNS injury are ill defined. We show that microglia at sites of spinal cord injury (SCI) rapidly produce the danger signal interleukin (IL)-1α, which triggers neuroinflammation and locomotor defects. We uncovered that IL-1α(-/-) mice have markedly increased levels of the survival factor Tox3 in their oligodendrocytes, which correlates with the protection of this cell population, and reduced lesion volume, resulting in unprecedented speed, level, and persistence of functional recovery after SCI. Our data suggest that central inhibition of IL-1α or Tox3 overexpression during the acute phase of a CNS insult may be an effective means for preventing the loss of neurological function in SCI, or other acute injuries such as ischemia and traumatic brain injuries.
脊髓损伤(SCI)会导致应激和濒死细胞释放危险信号,这一过程会引发神经炎症。有证据表明,炎症在受损神经组织的损伤和修复过程中均发挥作用。我们发现,SCI部位的小胶质细胞会迅速表达警报素白细胞介素(IL)-1α,随后浸润的中性粒细胞和巨噬细胞会产生IL-1β。在IL-1α(-/-)和IL-1β(-/-)小鼠中,这些细胞的浸润均显著减少,但只有IL-1α(-/-)小鼠在损伤后第1天就迅速且持续地改善了运动能力,同时损伤体积减小。同样,鞘内注射IL-1受体拮抗剂阿那白滞素可恢复SCI后的运动功能。对损伤后第1天的SCI组织进行转录组分析发现,与IL-1β(-/-)和野生型小鼠相比,存活因子Tox3仅在IL-1α(-/-)小鼠中受到差异调节。因此,从出生后第10天(P10)开始,IL-1α(-/-)小鼠少突胶质细胞中的Tox3水平显著升高,并持续至成年期。在P10时,IL-1α(-/-)小鼠脊髓中成熟少突胶质细胞数量短暂增加,这与野生型动物中IL-1α表达增加相一致。在成年小鼠中,SCI后IL-1α缺失伴随着少突胶质细胞存活率增加。在模拟SCI的条件下,人少突胶质细胞中TOX3过表达可减少细胞死亡。这些结果表明,中枢神经系统损伤早期IL-1α介导的Tox3抑制在继发性变性中起关键作用。
中枢神经系统损伤后神经元和少突胶质细胞旁观者变性的潜在机制尚不明确。我们发现,脊髓损伤(SCI)部位的小胶质细胞会迅速产生危险信号白细胞介素(IL)-1α,它会引发神经炎症和运动缺陷。我们发现,IL-1α(-/-)小鼠少突胶质细胞中存活因子Tox3水平显著升高,这与该细胞群体的保护以及损伤体积减小相关,从而导致SCI后功能恢复前所未有的速度、程度和持续性。我们的数据表明,在中枢神经系统损伤急性期对IL-1α进行中枢抑制或过表达Tox3可能是预防SCI或其他急性损伤(如缺血和创伤性脑损伤)中神经功能丧失的有效手段。
