Species differences in the expression of Ahi1, a protein implicated in the neurodevelopmental disorder Joubert syndrome, with preferential accumulation to stigmoid bodies

后脑 生物 伯特症候群 前脑 斑马鱼 神经科学 小脑 共济失调 脑干 中枢神经系统 基因 遗传学
作者
Jennifer Doering,Kelly Kane,Yen‐Chang Hsiao,Cong Yao,Bingxing Shi,Amber D. Slowik,Bakul Dhagat,Delisha D. Scott,Jeffrey G. Ault,Patrick Page-McCaw,Russell J. Ferland
出处
期刊:Journal of comparative neurology [Wiley]
卷期号:511 (2): 238-256 被引量:40
标识
DOI:10.1002/cne.21824
摘要

Abstract Joubert syndrome (JBTS) is an autosomal recessive disorder characterized by cerebellum and brainstem malformations. Individuals with JBTS have abnormal breathing and eye movements, ataxia, hypotonia, and cognitive difficulty, and they display mirror movements. Mutations in the Abelson‐helper integration site‐1 gene ( AHI1 ) cause JBTS in humans, suggesting that AHI1 is required for hindbrain development; however AHI1 may also be required for neuronal function. Support for this idea comes from studies demonstrating that the AHI1 locus is associated with schizophrenia. To gain further insight into the function of AHI1 in both the developing and mature central nervous system, we determined the spatial and temporal expression patterns of the gene products of AHI1 orthologs throughout development, in human, mouse, and zebrafish. Murine Ahi1 was distributed throughout the cytoplasm, dendrites, and axons of neurons, but was absent in glial cells. Ahi1 expression in the mouse brain was observed as early as embryonic day 10.5 and persisted into adulthood, with peak expression during the first postnatal week. Murine Ahi1 was observed in neurons of the hindbrain, midbrain, and ventral forebrain. Generally, the AHI1/Ahi1/ahi1 orthologs had a conserved distribution pattern in human, mouse, and zebrafish, but mouse Ahi1 was not present in the developing and mature cerebellum. Ahi1 was also observed consistently in the stigmoid body, a poorly characterized cytoplasmic organelle found in neurons. Overall, these results suggest roles for AHI1 in neurodevelopmental processes that underlie most of the neuroanatomical defects in JBTS, and perhaps in neuronal functions that contribute to schizophrenia. J. Comp. Neurol. 511:238–256, 2008. © 2008 Wiley‐Liss, Inc.
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