<i>Alivin 1</i>, a Novel Neuronal Activity-Dependent Gene, Inhibits Apoptosis and Promotes Survival of Cerebellar Granule Neurons

Ono, Tsutomu; Sekino-Suzuki, Naoko; Kikkawa, Yoshiaki; Yonekawa, Hiromichi; Kawashima, Seiichi

doi:10.1523/jneurosci.23-13-05887.2003

Cited by 52 publications

(62 citation statements)

References 53 publications

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“…The expression of Amigo2 was shown to promote the survival of cerebellar granule neurons and was considered a candidate for familial Alzheimer's disease type 5 (Ono et al 2003). We found the expression of Amigo2 to be highly correlated with the granule cell number in hippocampus (r ¼ À0.76, P , Figure 2).…”

Section: Resultsmentioning

confidence: 71%

Detection, Validation, and Downstream Analysis of Allelic Variation in Gene Expression

Ciobanu

Mozhui

et al. 2010

Genetics

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Common sequence variants within a gene often generate important differences in expression of corresponding mRNAs. This high level of local (allelic) control-or cis modulation-rivals that produced by gene targeting, but expression is titrated finely over a range of levels. We are interested in exploiting this allelic variation to study gene function and downstream consequences of differences in expression dosage. We have used several bioinformatics and molecular approaches to estimate error rates in the discovery of cis modulation and to analyze some of the biological and technical confounds that contribute to the variation in gene expression profiling. Our analysis of SNPs and alternative transcripts, combined with eQTL maps and selective gene resequencing, revealed that between 17 and 25% of apparent cis modulation is caused by SNPs that overlap probes rather than by genuine quantitative differences in mRNA levels. This estimate climbs to 40-50% when qualitative differences between isoform variants are included. We have developed an analytical approach to filter differences in expression and improve the yield of genuine cis-modulated transcripts to $80%. This improvement is important because the resulting variation can be successfully used to study downstream consequences of altered expression on higherorder phenotypes. Using a systems genetics approach we show that two validated cis-modulated genes, Stk25 and Rasd2, are likely to control expression of downstream targets and affect disease susceptibility.

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Section: Resultsmentioning

confidence: 71%

Detection, Validation, and Downstream Analysis of Allelic Variation in Gene Expression

Ciobanu

Mozhui

et al. 2010

Genetics

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“…Furthermore, survival is selective for neurons that are active synchronously with other neurons (601). Activity-dependent survival of cortical neurons requires Ca 2ϩ influx via voltage-gated Ca 2ϩ channels and/or NMDA receptors (196,465,577). Brain-derived neurotrophic factor (BDNF), parathyroid hormone-related peptide, and pituitary adenylate cyclase activating polypeptide (PACAP) have each been implicated as mediators of activity-dependent survival (196,309,464,577), which also seems to involve p38-mitogen-activated protein kinase, which phosphorylates and activates the transcription factor MEF2 (365).…”

Section: Cortex: Developmental Effects Of Spontaneous Activity: Latermentioning

confidence: 99%

Ion Channel Development, Spontaneous Activity, and Activity-Dependent Development in Nerve and Muscle Cells

Moody¹,

Bosma²

2005

Physiological Reviews

345

323

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At specific stages of development, nerve and muscle cells generate spontaneous electrical activity that is required for normal maturation of intrinsic excitability and synaptic connectivity. The patterns of this spontaneous activity are not simply immature versions of the mature activity, but rather are highly specialized to initiate and control many aspects of neuronal development. The configuration of voltage- and ligand-gated ion channels that are expressed early in development regulate the timing and waveform of this activity. They also regulate Ca2+ influx during spontaneous activity, which is the first step in triggering activity-dependent developmental programs. For these reasons, the properties of voltage- and ligand-gated ion channels expressed by developing neurons and muscle cells often differ markedly from those of adult cells. When viewed from this perspective, the reasons for complex patterns of ion channel emergence and regression during development become much clearer.

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“…AMIGO-2 was independently identified by a different group using differential display screening for genes involved in depolarization and NMDA-dependent survival of cerebellar granule neurons and named alivin-1 (ali1) [9]. Over expression of alivin-1 in cerebellar granule neurons inhibited apoptosis induced by a low (5mM) KCl medium.…”

Section: Discussionmentioning

confidence: 99%

Expressions and Roles of AMIGO Gene Family in Vascular Endothelial Cells

Hossain¹,

Ahmed²,

Alam³

et al. 2012

IJBBB

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Abstract-In this study, we have developed shRNA expression vector and determined their RNAi activity. The endothelial cells (ECs) were transfected with the Amphoterin-induced gene and ORF (AMIGO-2) expression vector or AMIGO-2 shRNA expression vector using hemagglutinating virus of Japan (HVJ) Envelope Vector and then the cells were assayed for AMIGO-2 mRNA levels and its survival. In our study, here we have performed expression of AMIGO gene family in primary cultured human vascular cells, and found predominant expression on human microvascular endothelial cells (HMVEC). The expression of AMIGO-2 gene in HMVEC under hypoxia, showed AMIGO-2 gene decreased significantly, suggested that AMIGO-2 maybe involved in vascular remodeling. Based on our study of AMIGO-2 down regulation and over expression showed the down regulation appeared to cause cell death of ECs, and over expression appeared to protect EC death due to reactive oxygen species. Finally, our this study suggest that AMIGO-2 may have an important role in the vascular system as a cell survival promoting factor for vascular ECs, probably as being involved in vascular development, angiogenesis and/or vascular remodeling.

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Alivin 1, a Novel Neuronal Activity-Dependent Gene, Inhibits Apoptosis and Promotes Survival of Cerebellar Granule Neurons

Cited by 52 publications

References 53 publications

Detection, Validation, and Downstream Analysis of Allelic Variation in Gene Expression

Detection, Validation, and Downstream Analysis of Allelic Variation in Gene Expression

Ion Channel Development, Spontaneous Activity, and Activity-Dependent Development in Nerve and Muscle Cells

Expressions and Roles of AMIGO Gene Family in Vascular Endothelial Cells

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