Graduate Interdisciplinary Program in Neuroscience, University of Arizona, Tucson, AZ, 85721, USA.
Department of Neurology, University of Arizona Health Sciences, 1501 N. Campbell Ave, Tucson, AZ, 85724-5023, USA.
Neural Dev. 2023 Oct 7;18(1):6. doi: 10.1186/s13064-023-00174-y.
CASK-related neurodevelopmental disorders are untreatable. Affected children show variable severity, with microcephaly, intellectual disability (ID), and short stature as common features. X-linked human CASK shows dosage sensitivity with haploinsufficiency in females. CASK protein has multiple domains, binding partners, and proposed functions at synapses and in the nucleus. Human and Drosophila CASK show high amino-acid-sequence similarity in all functional domains. Flies homozygous for a hypomorphic CASK mutation (∆18) have motor and cognitive deficits. A Drosophila genetic model of CASK-related disorders could have great scientific and translational value.
We assessed the effects of CASK loss of function on morphological phenotypes in Drosophila using established genetic, histological, and primary neuronal culture approaches. NeuronMetrics software was used to quantify neurite-arbor morphology. Standard nonparametric statistics methods were supplemented by linear mixed effects modeling in some cases. Microfluidic devices of varied dimensions were fabricated and numerous fluid-flow parameters were used to induce oscillatory stress fields on CNS tissue. Dissociation into viable neurons and neurite outgrowth in vitro were assessed.
We demonstrated that ∆18 homozygous flies have small brains, small heads, and short bodies. When neurons from developing CASK-mutant CNS were cultured in vitro, they grew small neurite arbors with a distinctive, quantifiable "bushy" morphology that was significantly rescued by transgenic CASK. As in humans, the bushy phenotype showed dosage-sensitive severity. To overcome the limitations of manual tissue trituration for neuronal culture, we optimized the design and operation of a microfluidic system for standardized, automated dissociation of CNS tissue into individual viable neurons. Neurons from CASK-mutant CNS dissociated in the microfluidic system recapitulate the bushy morphology. Moreover, for any given genotype, device-dissociated neurons grew larger arbors than did manually dissociated neurons. This automated dissociation method is also effective for rodent CNS.
These biological and engineering advances set the stage for drug discovery using the Drosophila model of CASK-related disorders. The bushy phenotype provides a cell-based assay for compound screening. Nearly a dozen genes encoding CASK-binding proteins or transcriptional targets also have brain-development mutant phenotypes, including ID. Hence, drugs that improve CASK phenotypes might also benefit children with disorders due to mutant CASK partners.
CASK 相关的神经发育障碍是无法治疗的。受影响的儿童表现出不同程度的严重程度,其特征包括小头畸形、智力障碍(ID)和身材矮小。X 连锁的人类 CASK 表现出剂量敏感性,杂合子女性表现为功能不全。CASK 蛋白具有多个结构域、结合伴侣,并在突触和核内提出了功能。人类和果蝇 CASK 在所有功能结构域都具有很高的氨基酸序列相似性。果蝇 CASK 功能缺失突变(∆18)纯合子表现出运动和认知缺陷。CASK 相关疾病的果蝇遗传模型可能具有巨大的科学和转化价值。
我们使用已建立的遗传、组织学和原代神经元培养方法,评估 CASK 功能丧失对果蝇形态表型的影响。使用 NeuronMetrics 软件对神经突树突形态进行定量分析。在某些情况下,标准的非参数统计方法辅以线性混合效应模型。我们还制造了不同尺寸的微流控装置,并使用多种流体流动参数在中枢神经系统组织上诱导振荡应激场。评估体外分离的神经元的存活和神经突的生长。
我们证明,∆18 纯合子果蝇的大脑、头部和身体都较小。当来自发育中的 CASK 突变中枢神经系统的神经元在体外培养时,它们的神经突树突生长较小,具有独特的、可量化的“丛生”形态,通过转基因 CASK 显著挽救。与人类一样,丛生表型显示出剂量敏感的严重程度。为了克服手动组织匀浆进行神经元培养的局限性,我们优化了微流控系统的设计和操作,以标准化、自动分离中枢神经系统组织为单个存活神经元。从 CASK 突变中枢神经系统中分离出来的神经元在微流控系统中再现了丛生形态。此外,对于任何给定的基因型,与手动分离的神经元相比,设备分离的神经元生长出更大的树突。这种自动化分离方法对啮齿动物中枢神经系统也有效。
这些生物学和工程学的进展为使用果蝇 CASK 相关疾病模型进行药物发现奠定了基础。丛生表型为化合物筛选提供了一种基于细胞的检测方法。近十几个编码 CASK 结合蛋白或转录靶标的基因也具有脑发育突变表型,包括智力障碍。因此,改善 CASK 表型的药物也可能使患有 CASK 突变伴侣疾病的儿童受益。
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