Your search keyword '"Kuznicki J"' showing total 5 results

1. LACK OF EVIDENCE THAT CALRETININ IS A CALCIUM BUFFER.

Author

Billing-Marczak, K. and Kuznicki, J.

Subjects

*NEUROCHEMISTRY, *CALCIUM, *CALCIUM-binding proteins, *EVIDENCE

Abstract

The article presents an abstract of the research paper "Lack of Evidence That Calretinin is a Calcium Buffer." Calretinin can serve as either a buffer of intracellular calcium or as a calcium sensor. The conclusion of research study reveals that calretinin expression is not activated by higher calcium levels.

Published

1999

2. Postnatal isoform switch and protein localization of LEF1 and TCF7L2 transcription factors in cortical, thalamic, and mesencephalic regions of the adult mouse brain.

Author

Nagalski, A., Irimia, M., Szewczyk, L., Ferran, J., Misztal, K., Kuznicki, J., and Wisniewska, M.

Subjects

*BRAIN physiology, *LABORATORY mice, *POSTNATAL care, *GENETIC transcription, *LYMPHOID tissue, *BINDING agents

Abstract

β-Catenin signaling, leading to the activation of lymphoid enhancer-binding factor 1/T cell factor (LEF1/TCF) transcription factors, plays a well-established role in transcription regulation during development and tissue homeostasis. In the adult organism, the activity of this pathway has been found in stem cell niches and postmitotic thalamic neurons. Recently, studies show that mutations in components of β-catenin signaling networks have been associated with several psychiatric disorders, indicating the involvement of β-catenin and LEF1/TCF proteins in the proper functioning of the brain. Here, we report a comprehensive analysis of LEF1/TCF protein localization and the expression profile of their isoforms in cortical, thalamic, and midbrain regions in mice. We detected LEF1 and TCF7L2 proteins in neurons of the thalamus and dorsal midbrain, i.e., subcortical regions specialized in the integration of diverse sources of sensory information. These neurons also exhibited nuclear localization of β-catenin, suggesting the involvement of β-catenin/LEF1/TCF7L2 in the regulation of gene expression in these regions. Analysis of alternative splicing and promoter usage identified brain-specific TCF7L2 isoforms and revealed a developmentally coordinated transition in the composition of LEF1 and TCF7L2 isoforms. In the case of TCF7L2, the typical brain isoforms lack the so-called C clamp; in addition, the dominant-negative isoforms are predominant in the embryonic thalamus but disappear postnatally. The present study provides a necessary framework to understand the role of LEF1/TCF factors in thalamic and midbrain development until adulthood and predicts that the regulatory role of these proteins in the adult brain is significantly different from their role in the embryonic brain or other non-neural tissues. [ABSTRACT FROM AUTHOR]

Published

2013

3. Conformationally altered p53: a novel Alzheimer's disease marker?

Author

Lanni, C., Racchi, M., Mazzini, G., Ranzenigo, A., Polotti, R., Sinforiani, E., Olivari, L., Barcikowska, M., Styczynska, M., Kuznicki, J., Szybinska, A., Govoni, S., Memo, M., and Uberti, D.

Subjects

*PARKINSON'S disease, *ALZHEIMER'S disease, *TUMOR markers, *MENTAL health, *HUNTINGTON disease

Abstract

The identification of biological markers of Alzheimer's disease (AD) can be extremely useful to improve diagnostic accuracy and/or to monitor the efficacy of putative therapies. In this regard, peripheral cells may be of great importance, because of their easy accessibility. After subjects were grouped according to diagnosis, the expression of conformationally mutant p53 in blood cells was compared by immunoprecipitation or by a cytofluorimetric assay. In total, 104 patients with AD, 92 age-matched controls, 15 patients with Parkinson's disease and 9 with other types of dementia were analyzed. Two independent methods to evaluate the differential expression of a conformational mutant p53 were developed. Mononuclear cells were analyzed by immunoprecipitation or by flow-cytometric analysis, following incubation with a conformation-specific p53 antibody, which discriminates unfolded p53 tertiary structure. Mononuclear cells from AD patients express a higher amount of mutant-like p53 compared to non-AD subjects, thus supporting the study of conformational mutant p53 as a new putative marker to discriminate AD from non-AD patients. We also observed a strong positive correlation between the expression of p53 and the age of patients. The expression of p53 was independent from the length of illness and from the Mini Mental State Examination value.Molecular Psychiatry (2008) 13, 641–647; doi:10.1038/sj.mp.4002060; published online 7 August 2007 [ABSTRACT FROM AUTHOR]

Published

2008

4. The Alzheimer disease-related calcium-binding protein Calmyrin is present in human forebrain with an altered distribution in Alzheimer's as compared to normal ageing brains.

Author

Bernstein, H.-G., Blazejczyk, M., Rudka, T., Gundelfinger, E. D., Dobrowolny, H., Bogerts, B., Kreutz, M. R., Kuznicki, J., and Wojda, U.

Subjects

*ALZHEIMER'S disease, *CALCIUM-binding proteins, *PROSENCEPHALON, *DEGENERATION (Pathology), *AGING, *BRAIN, *CALCIUM in the body

Abstract

H.-G. Bernstein, M. Blazejczyk, T. Rudka, E. D. Gundelfinger, H. Dobrowolny, B. Bogerts, M. R. Kreutz, J. Kuznicki and U. Wojda (2005)Neuropathology and Applied Neurobiology31,000–000The Alzheimer disease-related calcium-binding protein Calmyrin is present in human forebrain with an altered distribution in Alzheimer's as compared to normal ageing brainsThe EF-hand calcium binding protein Calmyrin (also called CIB-1) was shown to interact with presenilin-2 (PS-2), suggesting that this interaction might play a role in the pathogenesis of Alzheimer's disease (AD). Here we have investigated the distribution of Calmyrin in normal human and AD brain. In normal brain Calmyrin immunoreactivity was unevenly distributed with immunostaining in pyramidal neurones and interneurones of the palaeo- and neocortex, cerebellar granule cells and hypothalamic neurones of the paraventricular, ventromedial and arcuate nuclei. Moderate immunoreactivity was present in hippocampal pyramidal cells and stronger in dentate gyrus neurones. Thalamic and septal neurones were devoid of immunoreactivity. No apparent differences were visible between stainings of brain sections from younger and older nondemented patients. In AD brain a substantial loss of Calmyrin-immunopositive neurones was observed in all regions, especially in cortical areas. Still immunoreactive neurones, however, displayed stronger staining that was especially concentrated in perinuclear regions. Calmyrin immunosignals were in part associated with diffuse and senile plaques. Thus, although protein levels of Calmyrin are low in human forebrain, its cellular localization as well as its altered distribution in AD brain suggest that it may be involved in the pathogenesis of AD. [ABSTRACT FROM AUTHOR]

Published

2005

5. S.04.02 Abnormal myelin and axonal integrity in St8sia2 knockout mice – a model of polysialylation deficiency.

Author

Wisniewska, M.B., Szewczyk, L.M., Nagalski, A., Hildebrandt, H., and Kuznicki, J.

Subjects

*MYELIN, *AXONAL transport, *LABORATORY mice, *MOLECULAR biology, *CELL adhesion, *MEDICAL schools

Published

2015