Childhood Dementia Research Group, Flinders University, College of Medicine and Public Health, Flinders Health and Medical Research Institute, Bedford Park, South Australia, Australia.
Brain and Mind Centre, School of Medical Sciences, Faculty of Medicine & Health, University of Sydney, Camperdown, New South Wales, Australia.
J Neurochem. 2024 Sep;168(9):2791-2813. doi: 10.1111/jnc.16145. Epub 2024 Jun 7.
Sanfilippo syndrome results from inherited mutations in genes encoding lysosomal enzymes that catabolise heparan sulfate (HS), leading to early childhood-onset neurodegeneration. This study explores the therapeutic potential of photobiomodulation (PBM), which is neuroprotective and anti-inflammatory in several neurodegenerative diseases; it is also safe and PBM devices are readily available. We investigated the effects of 10-14 days transcranial PBM at 670 nm (2 or 4 J/cm/day) or 904 nm (4 J/cm/day) in young (3 weeks) and older (15 weeks) Sanfilippo or mucopolysaccharidosis type IIIA (MPS IIIA) mice. Although we found no PBM-induced changes in HS accumulation, astrocyte activation, CD206 (an anti-inflammatory marker) and BDNF expression in the brains of Sanfilippo mice, there was a near-normalisation of microglial activation in older MPS IIIA mice by 904 nm PBM, with decreased IBA1 expression and a return of their morphology towards a resting state. Immune cell immunophenotyping of peripheral blood with mass cytometry revealed increased pro-inflammatory signalling through pSTAT1 and p-p38 in NK and T cells in young but not older MPS IIIA mice (5 weeks of age), and expansion of NK, B and CD8 T cells in older affected mice (17 weeks of age), highlighting the importance of innate and adaptive lymphocytes in Sanfilippo syndrome. Notably, 670 and 904 nm PBM both reversed the Sanfilippo-induced increase in pSTAT1 and p-p38 expression in multiple leukocyte populations in young mice, while 904 nm reversed the increase in NK cells in older mice. In conclusion, this is the first study to demonstrate the beneficial effects of PBM in Sanfilippo mice. The distinct reduction in microglial activation and NK cell pro-inflammatory signalling and number suggests PBM may alleviate neuroinflammation and lymphocyte activation, encouraging further investigation of PBM as a standalone, or complementary therapy in Sanfilippo syndrome.
黏多糖贮积症 Ⅱ 型(Sanfilippo 综合征)是由于编码溶酶体酶的基因突变导致的,这些酶可以分解硫酸乙酰肝素(heparan sulfate,HS),从而导致儿童早期发病的神经退行性变。本研究探讨了光生物调节(photobiomodulation,PBM)的治疗潜力,这种方法在几种神经退行性疾病中具有神经保护和抗炎作用,并且安全,PBM 设备也很容易获得。我们研究了 670nm(2 或 4J/cm/天)或 904nm(4J/cm/天)经颅 PBM 对幼鼠(3 周龄)和老年鼠(15 周龄)Sanfilippo 或黏多糖贮积症 ⅢA 型(Mucopolysaccharidosis type IIIA,MPS IIIA)小鼠的影响,持续 10-14 天。虽然我们没有发现 PBM 诱导的 HS 积累、星形胶质细胞活化、CD206(抗炎标志物)和脑源性神经营养因子表达的变化,但在老年 MPS IIIA 小鼠中,904nm PBM 几乎使小神经胶质细胞的激活正常化,IBA1 表达减少,其形态恢复到静止状态。通过质谱流式细胞术对外周血免疫细胞的免疫表型分析显示,年轻但不是老年 MPS IIIA 小鼠(5 周龄)的自然杀伤(Natural killer,NK)和 T 细胞中 pSTAT1 和 p-p38 的促炎信号增加,并且老年受影响的小鼠(17 周龄)中 NK、B 和 CD8 T 细胞扩张,这突显了 Sanfilippo 综合征中固有和适应性淋巴细胞的重要性。值得注意的是,670nm 和 904nm PBM 均逆转了年轻小鼠中多种白细胞群体中 Sanfilippo 诱导的 pSTAT1 和 p-p38 表达增加,而 904nm PBM 逆转了老年小鼠中 NK 细胞的增加。总之,这是第一项证明 PBM 对 Sanfilippo 小鼠有益影响的研究。小神经胶质细胞激活和 NK 细胞促炎信号和数量的明显减少表明,PBM 可能减轻神经炎症和淋巴细胞激活,鼓励进一步研究 PBM 作为一种独立的或补充治疗方法在 Sanfilippo 综合征中的应用。
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