创伤性脑损伤后抗氧化酶纳米颗粒作用的性别差异。
Sex-based differences of antioxidant enzyme nanoparticle effects following traumatic brain injury.
机构信息
Department of Biological Systems Engineering, University of Nebraska - Lincoln, 262 Morrison Center, Lincoln, NE 68583, USA.
Department of Biological Systems Engineering, University of Nebraska - Lincoln, 262 Morrison Center, Lincoln, NE 68583, USA; ProTransit Nanotherapy, 16514L St., Omaha, NE 68135, USA.
出版信息
J Control Release. 2023 Mar;355:149-159. doi: 10.1016/j.jconrel.2023.01.065. Epub 2023 Feb 6.
Following traumatic brain injury (TBI), reactive oxygen species (ROS) are released in excess, causing oxidative stress, carbonyl stress, and cell death, which induce the additional release of ROS. The limited accumulation and retention of small molecule antioxidants commonly used in clinical trials likely limit the target engagement and therapeutic effect in reducing secondary injury. Small molecule drugs also need to be administered every several hours to maintain bioavailability in the brain. Therefore, there is a need for a burst and sustained release system with high accumulation and retention in the injured brain. Here, we utilized Pro-NP™ with a size of 200 nm, which was designed to have a burst and sustained release of encapsulated antioxidants, Cu/Zn superoxide dismutase (SOD1) and catalase (CAT), to scavenge ROS for >24 h post-injection. Here, we utilized a controlled cortical impact (CCI) mouse model of TBI and found the accumulation of Pro-NP™ in the brain lesion was highest when injected immediately after injury, with a reduction in the accumulation with delayed administration of 1 h or more post-injury. Pro-NP™ treatment with 9000 U/kg SOD1 and 9800 U/kg CAT gave the highest reduction in ROS in both male and female mice. We found that Pro-NP™ treatment was effective in reducing carbonyl stress and necrosis at 1 d post-injury in the contralateral hemisphere in male mice, which showed a similar trend to untreated female mice. Although we found that male and female mice similarly benefit from Pro-NP™ treatment in reducing ROS levels 4 h post-injury, Pro-NP™ treatment did not significantly affect markers of post-traumatic oxidative stress in female CCI mice as compared to male CCI mice. These findings of protection by Pro-NP™ in male mice did not extend to 7 d post-injury, which suggests subsequent treatments with Pro-NP™ may be needed to afford protection into the chronic phase of injury. Overall, these different treatment effects of Pro-NP™ between male and female mice suggest important sex-based differences in response to antioxidant nanoparticle delivery and that there may exist a maximal benefit from local antioxidant activity in injured brain.
颅脑创伤(TBI)后,活性氧(ROS)过度释放,导致氧化应激、羰基应激和细胞死亡,进而引起 ROS 的额外释放。临床试验中常用的小分子抗氧化剂的积累和保留有限,可能限制了其作为减少继发性损伤的靶点结合和治疗效果。小分子药物也需要每隔几个小时给药一次,以维持大脑中的生物利用度。因此,需要一种具有高积累和保留能力的爆发式和持续释放系统,用于受损大脑。在这里,我们利用 Pro-NP™,其尺寸为 200nm,设计用于爆发式和持续释放封装的抗氧化剂,Cu/Zn 超氧化物歧化酶(SOD1)和过氧化氢酶(CAT),以清除注射后超过 24 小时的 ROS。在这里,我们利用 TBI 的控制性皮质撞击(CCI)小鼠模型,发现 Pro-NP™在受伤后立即注射时在大脑损伤中的积累最高,随着受伤后 1 小时或更长时间的延迟给药,积累减少。9000U/kg SOD1 和 9800U/kg CAT 的 Pro-NP™治疗使雄性和雌性小鼠的 ROS 减少最多。我们发现,Pro-NP™治疗可有效降低雄性小鼠伤后 1 天对侧大脑的羰基应激和坏死,这与未治疗的雌性小鼠表现出相似的趋势。尽管我们发现雄性和雌性小鼠在伤后 4 小时接受 Pro-NP™治疗同样可以降低 ROS 水平,但与雄性 CCI 小鼠相比,Pro-NP™治疗对雌性 CCI 小鼠的创伤后氧化应激标志物没有显著影响。雄性小鼠中 Pro-NP™的保护作用并没有延伸到伤后 7 天,这表明可能需要后续的 Pro-NP™治疗来提供对损伤慢性期的保护。总之,Pro-NP™在雄性和雌性小鼠中的不同治疗效果表明,抗氧化纳米颗粒递送的反应存在重要的性别差异,而受伤大脑中局部抗氧化活性可能存在最大的益处。
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