Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in mice

Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in mice

Recent studies have shown that mutation at Ser522 causes inhibition of collapsin response mediator protein 2 (CRMP2) phosphorylation and induces axon elongation and partial recovery of the lost sensorimotor function after spinal cord injury (SCI). We aimed to reveal the intracellular mechanism in ax...

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Main Authors: Ayaka Sugeno, Wenhui Piao, Miki Yamazaki, Kiyofumi Takahashi, Koji Arikawa, Hiroko Matsunaga, Masahito Hosokawa, Daisuke Tominaga, Yoshio Goshima, Haruko Takeyama, Toshio Ohshima
Format: Article
Language:English
Published: Wolters Kluwer Medknow Publications 2021-01-01
Series:Neural Regeneration Research
Subjects:
cns regeneration; cortex; crmp2; hemoglobin; metabolic pathway; spinal cord injury; spine; transcriptome
Online Access:http://www.nrronline.org/article.asp?issn=1673-5374;year=2021;volume=16;issue=7;spage=1258;epage=1265;aulast=Sugeno
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spelling doaj-2158abf1a82d4b4da29f7e642ff2d2322021-01-08T04:40:09ZengWolters Kluwer Medknow PublicationsNeural Regeneration Research1673-53742021-01-011671258126510.4103/1673-5374.301035Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in miceAyaka SugenoWenhui PiaoMiki YamazakiKiyofumi TakahashiKoji ArikawaHiroko MatsunagaMasahito HosokawaDaisuke TominagaYoshio GoshimaHaruko TakeyamaToshio OhshimaRecent studies have shown that mutation at Ser522 causes inhibition of collapsin response mediator protein 2 (CRMP2) phosphorylation and induces axon elongation and partial recovery of the lost sensorimotor function after spinal cord injury (SCI). We aimed to reveal the intracellular mechanism in axotomized neurons in the CRMP2 knock-in (CRMP2KI) mouse model by performing transcriptome analysis in mouse sensorimotor cortex using micro-dissection punching system. Prior to that, we analyzed the structural pathophysiology in axotomized or neighboring neurons after SCI and found that somatic atrophy and dendritic spine reduction in sensorimotor cortex were suppressed in CRMP2KI mice. Further analysis of the transcriptome has aided in the identification of four hemoglobin genes Hba-a1, Hba-a2, Hbb-bs, and Hbb-bt that are significantly upregulated in wild-type mice with concomitant upregulation of genes involved in the oxidative phosphorylation and ribosomal pathways after SCI. However, we observed substantial upregulation in channel activity genes and downregulation of genes regulating vesicles, synaptic function, glial cell differentiation in CRMP2KI mice. Moreover, the transcriptome profile of CRMP2KI mice has been discussed wherein energy metabolism and neuronal pathways were found to be differentially regulated. Our results showed that CRMP2KI mice displayed improved SCI pathophysiology not only via microtubule stabilization in neurons, but also possibly via the whole metabolic system in the central nervous system, response changes in glial cells, and synapses. Taken together, we reveal new insights on SCI pathophysiology and the regenerative mechanism of central nervous system by the inhibition of CRMP2 phosphorylation at Ser522. All these experiments were performed in accordance with the guidelines of the Institutional Animal Care and Use Committee at Waseda University, Japan (2017-A027 approved on March 21, 2017; 2018-A003 approved on March 25, 2018; 2019-A026 approved on March 25, 2019).http://www.nrronline.org/article.asp?issn=1673-5374;year=2021;volume=16;issue=7;spage=1258;epage=1265;aulast=Sugenocns regeneration; cortex; crmp2; hemoglobin; metabolic pathway; spinal cord injury; spine; transcriptome
collection DOAJ
language English
format Article
sources DOAJ
author Ayaka Sugeno
Wenhui Piao
Miki Yamazaki
Kiyofumi Takahashi
Koji Arikawa
Hiroko Matsunaga
Masahito Hosokawa
Daisuke Tominaga
Yoshio Goshima
Haruko Takeyama
Toshio Ohshima
spellingShingle Ayaka Sugeno
Wenhui Piao
Miki Yamazaki
Kiyofumi Takahashi
Koji Arikawa
Hiroko Matsunaga
Masahito Hosokawa
Daisuke Tominaga
Yoshio Goshima
Haruko Takeyama
Toshio Ohshima
Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in mice
Neural Regeneration Research
cns regeneration; cortex; crmp2; hemoglobin; metabolic pathway; spinal cord injury; spine; transcriptome
author_facet Ayaka Sugeno
Wenhui Piao
Miki Yamazaki
Kiyofumi Takahashi
Koji Arikawa
Hiroko Matsunaga
Masahito Hosokawa
Daisuke Tominaga
Yoshio Goshima
Haruko Takeyama
Toshio Ohshima
author_sort Ayaka Sugeno
title Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in mice
title_short Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in mice
title_full Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in mice
title_fullStr Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in mice
title_full_unstemmed Cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in CRMP2 knock-in mice
title_sort cortical transcriptome analysis after spinal cord injury reveals the regenerative mechanism of central nervous system in crmp2 knock-in mice
publisher Wolters Kluwer Medknow Publications
series Neural Regeneration Research
issn 1673-5374
publishDate 2021-01-01
description Recent studies have shown that mutation at Ser522 causes inhibition of collapsin response mediator protein 2 (CRMP2) phosphorylation and induces axon elongation and partial recovery of the lost sensorimotor function after spinal cord injury (SCI). We aimed to reveal the intracellular mechanism in axotomized neurons in the CRMP2 knock-in (CRMP2KI) mouse model by performing transcriptome analysis in mouse sensorimotor cortex using micro-dissection punching system. Prior to that, we analyzed the structural pathophysiology in axotomized or neighboring neurons after SCI and found that somatic atrophy and dendritic spine reduction in sensorimotor cortex were suppressed in CRMP2KI mice. Further analysis of the transcriptome has aided in the identification of four hemoglobin genes Hba-a1, Hba-a2, Hbb-bs, and Hbb-bt that are significantly upregulated in wild-type mice with concomitant upregulation of genes involved in the oxidative phosphorylation and ribosomal pathways after SCI. However, we observed substantial upregulation in channel activity genes and downregulation of genes regulating vesicles, synaptic function, glial cell differentiation in CRMP2KI mice. Moreover, the transcriptome profile of CRMP2KI mice has been discussed wherein energy metabolism and neuronal pathways were found to be differentially regulated. Our results showed that CRMP2KI mice displayed improved SCI pathophysiology not only via microtubule stabilization in neurons, but also possibly via the whole metabolic system in the central nervous system, response changes in glial cells, and synapses. Taken together, we reveal new insights on SCI pathophysiology and the regenerative mechanism of central nervous system by the inhibition of CRMP2 phosphorylation at Ser522. All these experiments were performed in accordance with the guidelines of the Institutional Animal Care and Use Committee at Waseda University, Japan (2017-A027 approved on March 21, 2017; 2018-A003 approved on March 25, 2018; 2019-A026 approved on March 25, 2019).
topic cns regeneration; cortex; crmp2; hemoglobin; metabolic pathway; spinal cord injury; spine; transcriptome
url http://www.nrronline.org/article.asp?issn=1673-5374;year=2021;volume=16;issue=7;spage=1258;epage=1265;aulast=Sugeno
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