Effect of metabolic disorders on reactive gliosis and glial scarring at the early subacute phase of stroke in a mouse model of diabetes and obesity

IF 2 Q3 NEUROSCIENCES

IBRO Neuroscience Reports Pub Date : 2024-12-04 DOI:10.1016/j.ibneur.2024.12.002

Julien Clain , David Couret , Matthieu Bringart , Olivier Meilhac , Christian Lefebvre d’Hellencourt , Nicolas Diotel

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Abstract

It is well recognized that type II Diabetes (T2D) and overweight/obesity are established risk factors for stroke, worsening also their consequences. However, the underlying mechanisms by which these disorders aggravate outcomes are not yet clear limiting the therapeutic opportunities. To fill this gap, we characterized, for the first time, the effects of T2D and obesity on the brain repair mechanisms occurring 7 days after stroke, notably glial scarring. In the present study, by performing a 30-minute middle cerebral artery occlusion (MCAO) on db/db (obese diabetics mice) and db/+ (controls) mice, we demonstrated that obese and diabetic mice displayed larger lesions (i.e. increased infarct volume, ischemic core, apoptotic cell number) and worsened neurological outcomes compared to their control littermates. We then investigated the formation of the glial scar in control and db/db mice 7 days post-stroke. Our observations argue in favor of a stronger and more persistent activation of astrocytes and microglia in db/db mice. Furthermore, an increased deposition of extracellular matrix (ECM) was observed in db/db vs control mice (i.e. chondroitin sulfate proteoglycan and collagen type IV). Consequently, we demonstrated for the first time that the db/db status is associated with increased astrocytic and microglial activation 7 days after stroke and resulted in higher deposition of ECM within the damaged area. Interestingly, the injury-induced neurogenesis appeared stronger in db/db as shown by the labeling of migrating neuroblast. This increase appeared correlated to the larger size of lesion. It nevertheless raises the question of the functional integration of the new neurons in db/db mice given the observed dense ECM, known to be repulsive for neuronal migration. Carefully limiting glial scar formation after stroke represents a promising area of research for reducing neuronal loss and limiting disability in diabetic/obese patients.

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代谢紊乱对糖尿病和肥胖小鼠中风早期亚急性期反应性胶质细胞形成和胶质细胞瘢痕形成的影响。

众所周知，2型糖尿病（T2D）和超重/肥胖是卒中的既定危险因素，也会恶化其后果。然而，这些疾病加重预后的潜在机制尚不清楚，限制了治疗机会。为了填补这一空白，我们首次描述了T2D和肥胖对中风后7天发生的大脑修复机制的影响，特别是神经胶质瘢痕。在本研究中，通过对db/db（肥胖糖尿病小鼠）和db/+ （对照组）小鼠进行30分钟的大脑中动脉闭塞（MCAO），我们证明，与对照组相比，肥胖和糖尿病小鼠表现出更大的病变（即梗死体积、缺血核心、凋亡细胞数量增加）和更差的神经预后。然后，我们研究了中风后7天对照组和db/db小鼠胶质瘢痕的形成。我们的观察结果支持db/db小鼠中星形胶质细胞和小胶质细胞更强、更持久的激活。此外，与对照组相比，db/db小鼠的细胞外基质（ECM）沉积增加（即硫酸软骨素蛋白聚糖和IV型胶原）。因此，我们首次证明db/db状态与中风后7天星形细胞和小胶质细胞活化增加有关，并导致受损区域内ECM沉积增加。有趣的是，根据迁移神经母细胞的标记，损伤诱导的神经发生在db/db中表现得更强。这种增加似乎与较大的病变大小有关。然而，它提出了db/db小鼠中新神经元功能整合的问题，因为观察到密集的ECM，已知对神经元迁移具有排斥作用。仔细限制中风后神经胶质疤痕的形成是减少糖尿病/肥胖患者神经元损失和限制残疾的一个有前途的研究领域。

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