Lee Kevin, Jung Yewon, Vyas Yukti, Skelton Imogen, Abraham Wickliffe C, Hsueh Yi-Ping, Montgomery Johanna M
Department of Physiology and Centre for Brain Research, Faculty of Medical and Health Sciences, University of Auckland, 85 Park Road, Grafton, Auckland, 1023, New Zealand.
INSERM, Neurocentre Magendie, U1215, Bordeaux, France.
Mol Autism. 2022 Mar 18;13(1):13. doi: 10.1186/s13229-022-00494-6.
Autism spectrum disorder (ASD) is a neurodevelopmental disorder characterised by a dyad of behavioural symptoms-social and communication deficits and repetitive behaviours. Multiple aetiological genetic and environmental factors have been identified as causing or increasing the likelihood of ASD, including serum zinc deficiency. Our previous studies revealed that dietary zinc supplementation can normalise impaired social behaviours, excessive grooming, and heightened anxiety in a Shank3 mouse model of ASD, as well as the amelioration of synapse dysfunction. Here, we have examined the efficacy and breadth of dietary zinc supplementation as an effective therapeutic strategy utilising a non-Shank-related mouse model of ASD-mice with Tbr1 haploinsufficiency.
We performed behavioural assays, amygdalar slice whole-cell patch-clamp electrophysiology, and immunohistochemistry to characterise the synaptic mechanisms underlying the ASD-associated behavioural deficits observed in Tbr1 mice and the therapeutic potential of dietary zinc supplementation. Two-way analysis of variance (ANOVA) with Šídák's post hoc test and one-way ANOVA with Tukey's post hoc multiple comparisons were performed for statistical analysis.
Our data show that dietary zinc supplementation prevents impairments in auditory fear memory and social interaction, but not social novelty, in the Tbr1 mice. Tbr1 haploinsufficiency did not induce excessive grooming nor elevate anxiety in mice. At the synaptic level, dietary zinc supplementation reversed α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor (AMPAR) and N-methyl-D-aspartate receptor (NMDAR) hypofunction and normalised presynaptic function at thalamic-lateral amygdala (LA) synapses that are crucial for auditory fear memory. In addition, the zinc supplemented diet significantly restored the synaptic puncta density of the GluN1 subunit essential for functional NMDARs as well as SHANK3 expression in both the basal and lateral amygdala (BLA) of Tbr1 mice.
The therapeutic effect of dietary zinc supplementation observed in rodent models may not reproduce the same effects in human patients. The effect of dietary zinc supplementation on synaptic function in other brain structures affected by Tbr1 haploinsufficiency including olfactory bulb and anterior commissure will also need to be examined.
Our data further the understanding of the molecular mechanisms underlying the effect of dietary zinc supplementation and verify the efficacy and breadth of its application as a potential treatment strategy for ASD.
自闭症谱系障碍(ASD)是一种神经发育障碍,其特征为社交和沟通缺陷以及重复行为这一双重行为症状。多种病因,包括血清锌缺乏,已被确定为导致ASD或增加其发病可能性的因素。我们之前的研究表明,在ASD的Shank3小鼠模型中,饮食中补充锌可以使受损的社交行为、过度梳理毛发和焦虑加剧恢复正常,还能改善突触功能障碍。在此,我们利用一种与Shank无关的ASD小鼠模型——Tbr1单倍体不足小鼠,研究了饮食中补充锌作为一种有效治疗策略的疗效和适用范围。
我们进行了行为分析、杏仁核切片全细胞膜片钳电生理学和免疫组织化学实验,以确定Tbr1小鼠中观察到的与ASD相关的行为缺陷背后的突触机制以及饮食中补充锌的治疗潜力。采用双向方差分析(ANOVA)和Šídák事后检验以及单向ANOVA和Tukey事后多重比较进行统计分析。
我们的数据表明,饮食中补充锌可预防Tbr1小鼠听觉恐惧记忆和社交互动方面的损伤,但不能预防社交新奇性方面的损伤。Tbr1单倍体不足并未导致小鼠过度梳理毛发或焦虑加剧。在突触水平上,饮食中补充锌可逆转丘脑 - 外侧杏仁核(LA)突触处的α - 氨基 - 3 - 羟基 - 5 - 甲基 - 4 - 异恶唑丙酸受体(AMPAR)和N - 甲基 - D - 天冬氨酸受体(NMDAR)功能减退,并使对听觉恐惧记忆至关重要的突触前功能恢复正常。此外,补充锌的饮食显著恢复了功能性NMDAR所必需的GluN1亚基的突触小体密度以及Tbr1小鼠基底杏仁核和外侧杏仁核(BLA)中SHANK3的表达。
在啮齿动物模型中观察到的饮食中补充锌的治疗效果可能无法在人类患者中重现相同的效果。饮食中补充锌对受Tbr1单倍体不足影响的其他脑结构(包括嗅球和前连合)突触功能的影响也需要进一步研究。
我们的数据进一步加深了对饮食中补充锌作用的分子机制的理解,并验证了其作为ASD潜在治疗策略的疗效和适用范围。
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