Cellular Molecular Medicine, School of Medicine, University of Ottawa, Ottawa, Ontario K1H 8M5, Canada.
J Neurosci. 2013 Mar 27;33(13):5773-84. doi: 10.1523/JNEUROSCI.4247-12.2013.
Ubiquitous classical (typical) calpains, calpain-1 and calpain-2, are Ca(+2)-dependent cysteine proteases, which have been associated with numerous physiological and pathological cellular functions. However, a clear understanding of the role of calpains in the CNS has been hampered by the lack of appropriate deletion paradigms in the brain. In this study, we describe a unique model of conditional deletion of both calpain-1 and calpain-2 activities in mouse brain, which more definitively assesses the role of these ubiquitous proteases in brain development/function and pathology. Surprisingly, we show that these calpains are not critical for gross CNS development. However, calpain-1/calpain-2 loss leads to reduced dendritic branching complexity and spine density deficits associated with major deterioration in hippocampal long-term potentiation and spatial memory. Moreover, calpain-1/calpain-2-deficient neurons were significantly resistant to injury induced by excitotoxic stress or mitochondrial toxicity. Examination of downstream target showed that the conversion of the Cdk5 activator, p35, to pathogenic p25 form, occurred only in the presence of calpain and that it played a major role in calpain-mediated neuronal death. These findings unequivocally establish two central roles of calpain-1/calpain-2 in CNS function in plasticity and neuronal death.
普遍存在的经典(典型)钙蛋白酶,钙蛋白酶-1 和钙蛋白酶-2,是依赖 Ca(+2)的半胱氨酸蛋白酶,与许多生理和病理细胞功能有关。然而,由于大脑中缺乏适当的缺失范例,钙蛋白酶在中枢神经系统中的作用仍不清楚。在这项研究中,我们描述了一种在小鼠大脑中特异性缺失钙蛋白酶-1 和钙蛋白酶-2 活性的独特模型,该模型更明确地评估了这些普遍存在的蛋白酶在大脑发育/功能和病理学中的作用。令人惊讶的是,我们发现这些钙蛋白酶对于中枢神经系统的大体发育并不是必需的。然而,钙蛋白酶-1/钙蛋白酶-2 的缺失导致树突分支复杂性降低和棘突密度不足,与海马长时程增强和空间记忆的严重恶化有关。此外,钙蛋白酶-1/钙蛋白酶-2 缺陷神经元对兴奋性毒性应激或线粒体毒性诱导的损伤具有显著的抗性。对下游靶标的检查表明,Cdk5 激活剂 p35 向致病性 p25 形式的转化仅在钙蛋白酶存在的情况下发生,并且它在钙蛋白酶介导的神经元死亡中起主要作用。这些发现明确确立了钙蛋白酶-1/钙蛋白酶-2 在中枢神经系统功能中的两个核心作用:可塑性和神经元死亡。
