Your search keyword '"Aoi Jitsuki-Takahashi"' showing total 2 results

1. Clinical evidence that a dysregulated master neural network modulator may aid in diagnosing schizophrenia

Author

Joseph T. Coyle, Richard L. Sidman, Brian T. D. Tobe, Aoi Jitsuki-Takahashi, Hiroko Makihara, Fumio Nakamura, Haruko Nakamura, Yoshio Hirayasu, Keisuke Watanabe, Naoya Yamashita, Glenn T. Konopaske, Evan Y. Snyder, Cameron D Pernia, Yoshio Goshima, Munetaka Nomoto, Reina Aoki, Yusuke Saigusa, Toshihiko Baba, Francine M. Benes, and Mari Saito

Subjects

0301 basic medicine, medicine.medical_specialty, collapsin response mediator protein-2 (CRMP2), Nerve Tissue Proteins, blood test, 03 medical and health sciences, 0302 clinical medicine, Mediator, Internal medicine, medicine, Biological neural network, Blood test, Humans, Bipolar disorder, Multidisciplinary, medicine.diagnostic_test, business.industry, cytoskeleton, Biological Sciences, medicine.disease, dendritic morphology, 030104 developmental biology, Endocrinology, Gene Expression Regulation, Schizophrenia, Biomarker (medicine), biomarker, Intercellular Signaling Peptides and Proteins, Collapsin response mediator protein family, medicine.symptom, Nerve Net, business, Mania, 030217 neurology & neurosurgery, Biomarkers, Neuroscience, Genome-Wide Association Study

Abstract

Significance There are no biomarkers for schizophrenia (SCZ), a disorder of dysfunctional neural networks. We demonstrate that a master regulator of cytoskeleton (“CRMP2”) and, hence, neural circuitry, may form the basis for such a biomarker because its activity is uniquely imbalanced in SCZ patients. We show that SCZ patients are characterized by an excess of active CRMP2 not only in their brains (where it is correlated with dendritic abnormalities) but also in their peripheral blood lymphocytes. The abundance of active CRMP2 and insufficiency of opposing inactive p-CRMP2 likely disrupts neuronal function. Because peripheral blood CRMP2 appears to reflect intracerebral processes, it could form the basis of a rapid, minimally invasive, sensitive, and specific clinical diagnostic aid for SCZ in young patients., There are no validated biomarkers for schizophrenia (SCZ), a disorder linked to neural network dysfunction. We demonstrate that collapsin response mediator protein-2 (CRMP2), a master regulator of cytoskeleton and, hence, neural circuitry, may form the basis for a biomarker because its activity is uniquely imbalanced in SCZ patients. CRMP2’s activity depends upon its phosphorylation state. While an equilibrium between inactive (phosphorylated) and active (nonphosphorylated) CRMP2 is present in unaffected individuals, we show that SCZ patients are characterized by excess active CRMP2. We examined CRMP2 levels first in postmortem brains (correlated with neuronal morphometrics) and then, because CRMP2 is expressed in lymphocytes as well, in the peripheral blood of SCZ patients versus age-matched unaffected controls. In the brains and, more starkly, in the lymphocytes of SCZ patients

Published

2021

2. Clinical evidence that a dysregulated master neural network modulator may aid in diagnosing schizophrenia.

Author

Munetaka Nomoto, Konopaske, Glenn T., Naoya Yamashita, Reina Aoki, Aoi Jitsuki-Takahashi, Haruko Nakamura, Hiroko Makihara, Mari Saito, Yusuke Saigusa, Fumio Nakamura, Keisuke Watanabe, Toshihiko Baba, Benes, Francine M., Tobe, Brian T. D., Pernia, Cameron D., Coyle, Joseph T., Sidman, Richard L., Yoshio Hirayasu, Snyder, Evan Y., and Yoshio Goshima

Subjects

PEOPLE with schizophrenia, DIAGNOSIS, NEURAL circuitry, SCHIZOPHRENIA, BIOMARKERS, BIPOLAR disorder, DIALECTICAL behavior therapy

Abstract

There are no validated biomarkers for schizophrenia (SCZ), a disorder linked to neural network dysfunction. We demonstrate that collapsin response mediator protein-2 (CRMP2), a master regulator of cytoskeleton and, hence, neural circuitry, may form the basis for a biomarker because its activity is uniquely imbalanced in SCZ patients. CRMP2's activity depends upon its phosphorylation state. While an equilibrium between inactive (phosphorylated) and active (nonphosphorylated) CRMP2 is present in unaffected individuals, we show that SCZ patients are characterized by excess active CRMP2. We examined CRMP2 levels first in postmortem brains (correlated with neuronal morphometrics) and then, because CRMP2 is expressed in lymphocytes as well, in the peripheral blood of SCZ patients versus age-matched unaffected controls. In the brains and, more starkly, in the lymphocytes of SCZ patients <40 y old, we observed that nonphosphorylated CRMP2 was higher than in controls, while phosphorylated CRMP2 remained unchanged from control. In the brain, these changes were associated with dendritic structural abnormalities. The abundance of active CRMP2 with insufficient opposing inactive p-CRMP2 yielded a unique lowering of the p-CRMP2:CRMP2 ratio in SCZ patients, implying a disruption in the normal equilibrium between active and inactive CRMP2. These clinical data suggest that measuring CRMP2 and p-CRMP2 in peripheral blood might reflect intracerebral processes and suggest a rapid, minimally invasive, sensitive, and specific adjunctive diagnostic aid for early SCZ: increased CRMP2 or a decreased p-CRMP2:CRMP2 ratio may help cinch the diagnosis in a newly presenting young patient suspected of SCZ (versus such mimics as mania in bipolar disorder, where the ratio is high). [ABSTRACT FROM AUTHOR]

Published

2021