Tomohiko Irie
About
Tomohiko Irie is a scholar working on Cellular and Molecular Neuroscience, Molecular Biology and Sensory Systems.
According to data from OpenAlex, Tomohiko Irie has authored 22 papers receiving a total of 288 indexed citations (citations by other indexed papers that have themselves been cited), including 14 papers in Cellular and Molecular Neuroscience, 9 papers in Molecular Biology and 7 papers in Sensory Systems. Recurrent topics in Tomohiko Irie's work include Neuroscience and Neuropharmacology Research (9 papers), Hearing, Cochlea, Tinnitus, Genetics (7 papers) and Ion channel regulation and function (6 papers). Tomohiko Irie is often cited by papers focused on Neuroscience and Neuropharmacology Research (9 papers), Hearing, Cochlea, Tinnitus, Genetics (7 papers) and Ion channel regulation and function (6 papers). Tomohiko Irie collaborates with scholars based in Japan, Sri Lanka and United States. Tomohiko Irie's co-authors include Laurence O. Trussell, Hirokazu Hirai, Harunori Ohmori, Yuko Sekino, Makoto Usami, Iwao Fukui, Yasunori Matsuzaki, Norio Sakai, Ruri Kikura‐Hanajiri and Hanna Goenawan and has published in prestigious journals such as Journal of Biological Chemistry, Neuron and Journal of Neuroscience.
In The Last Decade
Tomohiko Irie
19 papers receiving 286 citations
Peers — A (Enhanced Table)
Peers by citation overlap · career bar shows stage (early→late) cites · hero ref
| Name | h | Career | Trend | Papers | Cites | |||||
|---|---|---|---|---|---|---|---|---|---|---|
| Tomohiko Irie Japan | 8 | 183 | 154 | 42 | 33 | 32 | 22 | 288 | ||
| Samuel J. Gossage United Kingdom | 5 | 178 1.0× | 192 1.2× | 89 2.1× | 25 0.8× | 52 1.6× | 8 | 375 | ||
| Jonathan P. Spencer United Kingdom | 9 | 211 1.2× | 162 1.1× | 62 1.5× | 78 2.4× | 46 1.4× | 10 | 362 | ||
| Miloslav Franěk Czechia | 11 | 220 1.2× | 187 1.2× | 41 1.0× | 30 0.9× | 22 0.7× | 22 | 431 | ||
| Yue Hao China | 11 | 253 1.4× | 154 1.0× | 36 0.9× | 67 2.0× | 44 1.4× | 19 | 468 | ||
| Flora Jow United States | 17 | 228 1.2× | 449 2.9× | 51 1.2× | 16 0.5× | 48 1.5× | 27 | 573 | ||
| Marina Bejanian United States | 13 | 121 0.7× | 120 0.8× | 12 0.3× | 25 0.8× | 20 0.6× | 28 | 474 | ||
| Ruoyuan Yin United States | 8 | 296 1.6× | 336 2.2× | 39 0.9× | 36 1.1× | 21 0.7× | 9 | 495 | ||
| Pamela Scarselli Italy | 10 | 174 1.0× | 147 1.0× | 10 0.2× | 16 0.5× | 25 0.8× | 18 | 348 | ||
| Hai-Yun Zhou China | 10 | 59 0.3× | 177 1.1× | 14 0.3× | 16 0.5× | 15 0.5× | 15 | 343 | ||
| Ryuji Yamada Japan | 9 | 164 0.9× | 158 1.0× | 76 1.8× | 41 1.2× | 33 1.0× | 21 | 326 |
Countries citing papers authored by Tomohiko Irie
Since
Specialization
Citations
This map shows the geographic impact of Tomohiko Irie's research. It shows the number of citations coming from papers published by authors working in each country. You can also color the map by specialization and compare the number of citations received by Tomohiko Irie with the expected number of citations based on a country's size and research output (numbers larger than one mean the country cites Tomohiko Irie more than expected).
Fields of papers citing papers by Tomohiko Irie
Since
Specialization
Physical SciencesHealth SciencesLife SciencesSocial Sciences
This network shows the impact of papers produced by Tomohiko Irie. Nodes represent research fields, and links connect fields that are likely to share authors. Colored nodes show fields that tend to cite the papers produced by Tomohiko Irie. The network helps show where Tomohiko Irie may publish in the future.
Co-authorship network of co-authors of Tomohiko Irie
This figure shows the co-authorship network connecting the top 25 collaborators of Tomohiko Irie. A scholar is included among the top collaborators of Tomohiko Irie based on the total number of citations received by their joint publications. Widths of edges represent the number of papers authors have co-authored together. Node borders signify the number of papers an author published with Tomohiko Irie. Tomohiko Irie is excluded from the visualization to improve readability, since they are connected to all nodes in the network.
All Works
1.
Irie, Tomohiko, et al.. (2024). The Na+ leak channel NALCN controls spontaneous activity and mediates synaptic modulation by α2-adrenergic receptors in auditory neurons. eLife. 12.
2.
Irie, Tomohiko, et al.. (2023). The Na+ leak channel NALCN controls spontaneous activity and mediates synaptic modulation by α2-adrenergic receptors in auditory neurons. eLife. 12.
3.
Irie, Tomohiko, et al.. (2022). Derivatives of methoxetamine and major methoxetamine metabolites potently block NMDA receptors. Journal of Pharmacological Sciences. 150(4). 233–243.
4.
Takahashi, Kanako, Luying Chen, Mian Wu, et al.. (2022). Leucine 434 is essential for docosahexaenoic acid–induced augmentation of L-glutamate transporter current. Journal of Biological Chemistry. 299(1). 102793–102793.
5.
Irie, Tomohiko. (2021). Essential Role of Somatic Kv2 Channels in High-Frequency Firing in Cartwheel Cells of the Dorsal Cochlear Nucleus. eNeuro. 8(3). ENEURO.0515–20.2021.
6.
Irie, Tomohiko, Takehito Suzuki, Yoko Miyazaki, et al.. (2021). Valproic acid promotes differentiation of adipose tissue-derived stem cells to neuronal cells selectively expressing functional N-type voltage-gated Ca2+ channels. Biochemical and Biophysical Research Communications. 589. 55–62.
7.
Irie, Tomohiko, Daiju Yamazaki, & Ruri Kikura‐Hanajiri. (2021). A potential of methoxpropamine to be a widespread recreational drug: it blocks NMDA receptors and inhibits NMDA receptor-mediated synaptic transmission in a brain preparation of mice. Forensic Toxicology. 39(2). 474–480.
8.
Irie, Tomohiko, Daiju Yamazaki, & Ruri Kikura‐Hanajiri. (2020). F-phenibut (β-(4-Fluorophenyl)-GABA), a potent GABAB receptor agonist, activates an outward-rectifying K+ current and suppresses the generation of action potentials in mouse cerebellar Purkinje cells. European Journal of Pharmacology. 884. 173437–173437.
9.
Miyajima, Atsuko, Makoto Usami, Katsuyoshi Mitsunaga, et al.. (2020). Inhibitory and inductive effects of 4- or 5-methyl-2-mercaptobenzimidazole, thyrotoxic and hepatotoxic rubber antioxidants, on several forms of cytochrome P450 in primary cultured rat and human hepatocytes. Toxicology Reports. 7. 979–985.
10.
Irie, Tomohiko & Laurence O. Trussell. (2017). Double-Nanodomain Coupling of Calcium Channels, Ryanodine Receptors, and BK Channels Controls the Generation of Burst Firing. Neuron. 96(4). 856–870.e4.
11.
Miyajima, Atsuko, Makoto Usami, Katsuyoshi Mitsunaga, et al.. (2017). Thyrotoxic rubber antioxidants, 2-mercaptobenzimidazole and its methyl derivatives, cause both inhibition and induction of drug-metabolizing activity in rat liver microsomes after repeated oral administration. Biochemical and Biophysical Research Communications. 492(1). 116–120.
12.
Irie, Tomohiko, Tsuyoshi Kawakami, Kaoru Sato, & Makoto Usami. (2017). Sub-toxic concentrations of nano-ZnO and nano-TiO<sub>2</sub> suppress neurite outgrowth in differentiated PC12 cells. The Journal of Toxicological Sciences. 42(6). 723–729.
13.
Irie, Tomohiko, Ruri Kikura‐Hanajiri, Makoto Usami, et al.. (2015). MAM-2201, a synthetic cannabinoid drug of abuse, suppresses the synaptic input to cerebellar Purkinje cells via activation of presynaptic CB1 receptors. Neuropharmacology. 95. 479–491.
14.
Usami, Makoto, Katsuyoshi Mitsunaga, Atsuko Miyajima, et al.. (2015). Effects of 13 developmentally toxic chemicals on the migration of rat cephalic neural crest cells in vitro. Congenital Anomalies. 56(2). 52–59.
15.
Usami, Makoto, Katsuyoshi Mitsunaga, Tomohiko Irie, Atsuko Miyajima, & Osamu Doi. (2014). Proteomic analysis of ethanol-induced embryotoxicity in cultured post-implantation rat embryos. The Journal of Toxicological Sciences. 39(2). 285–292.
16.
Usami, Makoto, Katsuyoshi Mitsunaga, Tomohiko Irie, Atsuko Miyajima, & Osamu Doi. (2014). Simplein vitromigration assay for neural crest cells and the opposite effects of all‐trans‐retinoic acid on cephalic‐ and trunk‐derived cells. Congenital Anomalies. 54(3). 184–188.
17.
Irie, Tomohiko, Yasunori Matsuzaki, Yuko Sekino, & Hirokazu Hirai. (2013). Kv3.3 channels harbouring a mutation of spinocerebellar ataxia type 13 alter excitability and induce cell death in cultured cerebellar Purkinje cells. The Journal of Physiology. 592(1). 229–247.
18.
Shuvaev, Аnton N., Hajime Horiuchi, Takahiro Seki, et al.. (2011). Mutant PKCγ in Spinocerebellar Ataxia Type 14 Disrupts Synapse Elimination and Long-Term Depression in Purkinje CellsIn Vivo. Journal of Neuroscience. 31(40). 14324–14334.
19.
Irie, Tomohiko & Harunori Ohmori. (2008). Presynaptic GABAB receptors modulate synaptic facilitation and depression at distinct synapses in fusiform cells of mouse dorsal cochlear nucleus. Biochemical and Biophysical Research Communications. 367(2). 503–508.
20.
Irie, Tomohiko, Iwao Fukui, & Harunori Ohmori. (2006). Activation of GIRK Channels by Muscarinic Receptors and Group II Metabotropic Glutamate Receptors Suppresses Golgi Cell Activity in the Cochlear Nucleus of Mice. Journal of Neurophysiology. 96(5). 2633–2644.
Rankless uses publication and citation data sourced from OpenAlex, an open and comprehensive bibliographic database. While OpenAlex provides broad and valuable coverage of the global research landscape, it—like all bibliographic datasets—has inherent limitations. These include incomplete records, variations in author disambiguation, differences in journal indexing, and delays in data updates. As a result, some metrics and network relationships displayed in Rankless may not fully capture the entirety of a scholar's output or impact.
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