Division of Medical Sciences, University of Victoria, Victoria, British Columbia V8P 5C2, Canada.
Department of Immunobiology, University of Arizona College of Medicine, Tucson, Arizona 85724, and.
J Neurosci. 2018 Oct 3;38(40):8707-8722. doi: 10.1523/JNEUROSCI.0734-18.2018. Epub 2018 Sep 10.
Microcirculatory damage is a common complication for those with vascular risk factors, such as diabetes. To resolve vascular insults, the brain's immune cells (microglia) must rapidly envelop the site of injury. Currently, it is unknown whether Type 1 diabetes, a condition associated with chronic immune system dysfunction, alters microglial responses to damage and what mechanisms are responsible. Using two-photon microscopy in adult male mice, we show that microglial envelopment of laser-induced cerebral microbleeds is diminished in a hyperglycemic mouse model of Type 1 diabetes, which could not be fully rescued with chronic insulin treatment. Microglia were important for vessel repair because reduced microglial accumulation in diabetic mice or near-complete depletion in healthy controls was associated with greater secondary leakage of the damaged vessel. Broadly suppressing inflammation with dexamethasone in diabetic mice but not healthy controls, significantly enhanced microglial responses to microbleeds and attenuated secondary vessel leakage. These enhancements were associated with changes in IFN-γ signaling because dexamethasone suppressed abnormally high levels of IFN-γ protein levels in brain and blood serum of diabetic mice. Further, blocking IFN-γ in diabetic mice with neutralizing antibodies restored normal microglial chemotaxic responses and purinoceptor gene expression, as well as mitigated secondary leakage. These results suggest that abnormal IFN-γ signaling disrupts microglial function in the diabetic brain, and that immunotherapies targeting IFN-γ can stimulate microglial repair of damaged vessels. Although Type 1 diabetes is an established risk factor for vascular complications, such as microbleeds, and is known to hinder wound healing in the body, no study has examined how diabetes impacts the brain's innate immune reparative response (involving cells called microglia) to vascular injury. Here we show that microglial responses to brain microbleeds were diminished in diabetic animals, which also exacerbated secondary leakage from damaged vessels. These impairments were related to abnormally high levels of the proinflammatory cytokine IFN-γ because reducing IFN-γ with immunosuppressant drugs or blocking antibodies helped restore normal microglial responses and repair of damaged vessels. These data highlight the use of IFN-γ modulating therapeutics to enhance vascular repair in at-risk populations.
微血管损伤是血管危险因素患者(如糖尿病患者)的常见并发症。为了解决血管损伤问题,大脑的免疫细胞(小胶质细胞)必须迅速包围损伤部位。目前尚不清楚 1 型糖尿病(一种与慢性免疫系统功能障碍相关的疾病)是否会改变小胶质细胞对损伤的反应,以及是什么机制负责。使用成年雄性小鼠的双光子显微镜,我们发现,在 1 型糖尿病的高血糖小鼠模型中,激光诱导的脑微出血的小胶质细胞包裹作用减弱,这种作用不能通过慢性胰岛素治疗完全挽救。小胶质细胞对血管修复很重要,因为糖尿病小鼠中小胶质细胞的积累减少或健康对照者的几乎完全耗尽与受损血管的继发性渗漏增加有关。用地塞米松广泛抑制糖尿病小鼠的炎症,但不能抑制健康对照者的炎症,这显著增强了小胶质细胞对微出血的反应,并减轻了继发性血管渗漏。这些增强作用与 IFN-γ 信号转导的变化有关,因为地塞米松抑制了糖尿病小鼠大脑和血清中异常高的 IFN-γ 蛋白水平。此外,用中和抗体阻断糖尿病小鼠中的 IFN-γ 恢复了正常的小胶质细胞趋化反应和嘌呤能受体基因表达,并减轻了继发性渗漏。这些结果表明,异常的 IFN-γ 信号转导破坏了糖尿病大脑中小胶质细胞的功能,而针对 IFN-γ 的免疫疗法可以刺激小胶质细胞修复受损的血管。尽管 1 型糖尿病是血管并发症(如微出血)的既定危险因素,并且已知会阻碍身体的伤口愈合,但尚无研究探讨糖尿病如何影响大脑先天免疫修复反应(涉及称为小胶质细胞的细胞)对血管损伤的反应。在这里,我们发现糖尿病动物中小胶质细胞对脑微出血的反应减弱,这也加剧了受损血管的继发性渗漏。这些损伤与异常高的促炎细胞因子 IFN-γ 有关,因为用免疫抑制药物或阻断抗体降低 IFN-γ 有助于恢复正常的小胶质细胞反应和受损血管的修复。这些数据突出了使用 IFN-γ 调节治疗来增强高危人群的血管修复。
