Human CRMP4 mutation and disrupted Crmp4 expression in mice are associated with ASD characteristics and sexual dimorphism

Tsutiya, Atsuhiro; Nakano, Yoritaka; Hansen-Kiss, Emily; Kelly, Benjamin J.; Nishihara, Masugi; Goshima, Yoshio; Corsmeier, Don; White, Peter; Herman, Gail E.; Ohtani-Kaneko, Ritsuko

doi:10.1038/s41598-017-16782-8

Cited by 18 publications

(40 citation statements)

References 76 publications

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“…Besides, the migraine attack is a paroxysmal dysfunctional alteration or inflow-outflow dysfunctional modulation of multiple sensory systems [ 9 ]. Various neuroimaging outcomes have demonstrated correlation of functional connectivity between the subregions in SMN, and the central executive network (CEN) [ 6 ], salience network (SN) [ 10 ] as well as default mode network (DMN) [ 11 ] in patients with MwoA. The functional connectivity strength of SMN has been shown to significantly illuminate the perception of pain intensity and therapeutic effect in MwoA [ 12 ].…”

Section: Introductionmentioning

confidence: 99%

Impaired effective functional connectivity of the sensorimotor network in interictal episodic migraineurs without aura

Wei

Chen

et al. 2020

J Headache Pain

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Background Resting-state functional magnetic resonance imaging (Rs-fMRI) has confirmed sensorimotor network (SMN) dysfunction in migraine without aura (MwoA). However, the underlying mechanisms of SMN effective functional connectivity in MwoA remain unclear. We aimed to explore the association between clinical characteristics and effective functional connectivity in SMN, in interictal patients who have MwoA. Methods We used Rs-fMRI to acquire imaging data in 40 episodic patients with MwoA in the interictal phase and 34 healthy controls (HCs). Independent component analysis was used to profile the distribution of SMN and calculate the different SMN activity between the two groups. Subsequently, Granger causality analysis was used to analyze the effective functional connectivity between the SMN and other brain regions. Results Compared to the HCs, MwoA patients showed higher activity in the bilateral postcentral gyri (PoCG), but lower activity in the left midcingulate cortex (MCC). Moreover, MwoA patients showed decreased effective functional connectivity from the SMN to left middle temporal gyrus, right putamen, left insula and bilateral precuneus, but increased effective functional connectivity to the right paracentral lobule. There was also significant effective functional connectivity from the primary visual cortex, right cuneus and right putamen to the SMN. In the interictal period, there was positive correlation between the activity of the right PoCG and the frequency of headache. The disease duration was positively correlated with abnormal effective functional connectivity from the left PoCG to right precuneus. In addition, the headache impact scores were negatively correlated with abnormal effective functional connectivity from the left MCC to right paracentral lobule, as well as from the right precuneus to left PoCG. Conclusions These differential, resting-state functional activities of the SMN in episodic MwoA may contribute to the understanding of migraine-related intra- and internetwork imbalances associated with nociceptive regulation and chronification.

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Section: Introductionmentioning

confidence: 99%

Impaired effective functional connectivity of the sensorimotor network in interictal episodic migraineurs without aura

Wei

Chen

et al. 2020

J Headache Pain

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“…Sexual dimorphism has been reported in other mouse models with mutations in chromatin remodeling proteins, including CHD8 and MeCP2, where females are unaffected by loss of the protein of interest or are affected differently [75][76][77] . In humans, neurological disorders such as autismspectrum disorders tend to preferentially affect males rather than females, possibly due to combinatorial contributions of hormonal and genetic factors in a phenomenon known as the female protective effect [78][79][80] , and this is regularly supported with mouse models [81][82][83] . The presence of estrogen and estrogen receptor in the female brain has been shown to be neuroprotective and leads to enhanced Schaffer-collateral LTP 84 .…”

Section: Discussionmentioning

confidence: 99%

Atrx deletion in neurons leads to sexually-dimorphic dysregulation of miR-137 and spatial learning and memory deficits

Tamming

Dumeaux

Langlois

et al. 2019

Preprint

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statement: Ablation of the ATRX chromatin remodeler specifically in forebrain excitatory neurons of mice causes male-specific deficits in long-term spatial memory associated with miR-137 overexpression, transcriptional changes and structural alterations corresponding to pre-and post-synaptic abnormalities. AbstractMutations in the ATRX chromatin remodeler are associated with syndromic and non-syndromic intellectual disability. Emerging evidence points to key roles for ATRX in preserving neuroprogenitor cell genomic stability, whereas ATRX function in differentiated neurons and memory processes are still unresolved. Here, we show that Atrx deletion in mouse forebrain glutamatergic neurons causes distinct hippocampal structural defects identified by magnetic resonance imaging. Ultrastructural analysis revealed fewer presynaptic vesicles and an enlarged postsynaptic area at CA1 apical dendrite-axon junctions. These synaptic defects are associated with impaired long-term contextual memory in male, but not female mice. Mechanistically, we identify ATRXdependent and sex-specific alterations in synaptic gene expression linked to Mir137 levels, a known regulator of presynaptic processes and spatial memory. We conclude that ablation of Atrx in excitatory forebrain neurons leads to sexually dimorphic outcomes on miR-137 and on spatial memory, identifying a promising therapeutic target for neurological disorders caused by ATRX dysfunction.

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“…Currently, the nomenclature has been unified by calling the family members ''CRMP1'' through ''CRMP5'' ( Supplementary Table S1); CRMP-62 has been renamed as CRMP2. The CRMP family of proteins are now recognized as multifunctional proteins, not only being involved in neuronal development, regeneration and inflammation, but also in various neurological and psychiatric disease states (Tobe et al, 2017;Tsutiya et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

Collapsin Response Mediator Proteins: Their Biological Functions and Pathophysiology in Neuronal Development and Regeneration

Nakamura

Ohshima

Goshima

2020

Front. Cell. Neurosci.

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Collapsin response mediator proteins (CRMPs), which consist of five homologous cytosolic proteins, are one of the major phosphoproteins in the developing nervous system. The prominent feature of the CRMP family proteins is a new class of microtubuleassociated proteins that play important roles in the whole process of developing the nervous system, such as axon guidance, synapse maturation, cell migration, and even in adult brain function. The CRMP C-terminal region is subjected to posttranslational modifications such as phosphorylation, which, in turn, regulates the interaction between the CRMPs and various kinds of proteins including receptors, ion channels, cytoskeletal proteins, and motor proteins. The gene-knockout of the CRMP family proteins produces different phenotypes, thereby showing distinct roles of all CRMP family proteins. Also, the phenotypic analysis of a non-phosphorylated form of CRMP2-knockin mouse model, and studies of pharmacological responses to CRMP-related drugs suggest that the phosphorylation/dephosphorylation process plays a pivotal role in pathophysiology in neuronal development, regeneration, and neurodegenerative disorders, thus showing CRMPs as promising target molecules for therapeutic intervention.

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Human CRMP4 mutation and disrupted Crmp4 expression in mice are associated with ASD characteristics and sexual dimorphism

Cited by 18 publications

References 76 publications

Impaired effective functional connectivity of the sensorimotor network in interictal episodic migraineurs without aura

Impaired effective functional connectivity of the sensorimotor network in interictal episodic migraineurs without aura

Atrx deletion in neurons leads to sexually-dimorphic dysregulation of miR-137 and spatial learning and memory deficits

Collapsin Response Mediator Proteins: Their Biological Functions and Pathophysiology in Neuronal Development and Regeneration

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