Your search keyword '"Nowakowski RS"' showing total 6 results

1. Sex Differences in the Molecular Programs of Pancreatic Cells Contribute to the Differential Risks of Type 2 Diabetes.

Author

Yong HJ, Toledo MP, Nowakowski RS, and Wang YJ

Subjects

Female, Genome-Wide Association Study, Humans, Male, Pancreas metabolism, RNA metabolism, Sex Characteristics, Diabetes Mellitus, Type 2 metabolism, Islets of Langerhans metabolism

Abstract

Epidemiology studies demonstrate that women are at a significantly lower risk of developing type 2 diabetes (T2D) compared to men. However, the molecular basis of this risk difference is not well understood. In this study, we examined the sex differences in the genetic programs of pancreatic endocrine cells. We combined pancreas perifusion data and single-cell genomic data from our laboratory and from publicly available data sets to investigate multiple axes of the sex differences in the human pancreas at the single-cell type and single-cell level. We systematically compared female and male islet secretion function, gene expression program, and regulatory principles of pancreatic endocrine cells. The perifusion data indicate that female endocrine cells have a higher secretion capacity than male endocrine cells. Single-cell RNA-sequencing analysis suggests that endocrine cells in male controls have molecular signatures that resemble T2D. In addition, we identified genomic elements associated with genome-wide association study T2D loci to have differential accessibility between female and male delta cells. These genomic elements may play a sex-specific causal role in the pathogenesis of T2D. We provide molecular mechanisms that explain the differential risk of T2D between women and men. Knowledge gained from our study will accelerate the development of diagnostics and therapeutics in sex-aware precision medicine for diabetes., (© The Author(s) 2022. Published by Oxford University Press on behalf of the Endocrine Society. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2022

2. Differentiation of Amyloid Plaques Between Alzheimer's Disease and Non-Alzheimer's Disease Individuals Based on Gray-Level Co-occurrence Matrix Texture Analysis.

Author

Zaletel I, Milutinović K, Bajčetić M, and Nowakowski RS

Subjects

Aging, Amyloid beta-Peptides metabolism, Brain diagnostic imaging, Brain pathology, Humans, Alzheimer Disease diagnosis, Alzheimer Disease pathology, Plaque, Amyloid pathology

Abstract

Amyloid plaques, one of the main hallmarks of Alzheimer's disease (AD), are classified into diffuse (associated with cognitive impairment) and dense-core types (a common finding in brains of people without Alzheimer's disease (non-AD) and without impaired cognitive function) based on their morphology. We tried to determine the usability of gray-level co-occurrence matrix (GLCM) texture parameters of homogeneity and heterogeneity for the differentiation of amyloid plaque images obtained from AD and non-AD individuals. Images of amyloid-β (Aβ) immunostained brain tissue samples were obtained from the Aging, Dementia and Traumatic Brain Injury Project. A total of 1,039 plaques were isolated from different brain regions of 69 AD and non-AD individuals and used for further GLCM analysis. Images of Aβ stained plaques show higher values of heterogeneity parameters and lower values of homogeneity parameters in AD patients, and vice versa in non-AD patients. Additionally, GLCM analysis shows differences in Aβ plaque texture between different brain regions in non-AD patients and correlates with variables that characterize patient's dementia status. The present study shows that GLCM texture analysis is an efficient method to discriminate between different types of amyloid plaques based on their morphology and thus can prove as a valuable tool in the neuropathological investigation of dementia.

Published

2021

3. Overexpression of p27 Kip 1, probability of cell cycle exit, and laminar destination of neocortical neurons.

Author

Tarui T, Takahashi T, Nowakowski RS, Hayes NL, Bhide PG, and Caviness VS

Subjects

Algorithms, Animals, Antimetabolites pharmacology, Apoptosis physiology, Bromodeoxyuridine pharmacology, Cell Count, Cell Cycle Proteins genetics, Cell Proliferation drug effects, Cyclin-Dependent Kinase Inhibitor p27, Female, Gene Expression, Idoxuridine pharmacology, Immunohistochemistry, In Situ Nick-End Labeling, Kinetics, Mice, Mice, Transgenic, Neocortex anatomy & histology, Neocortex growth & development, S Phase physiology, Tumor Suppressor Proteins genetics, Cell Cycle genetics, Cell Cycle Proteins biosynthesis, Neocortex cytology, Neurons physiology, Tumor Suppressor Proteins biosynthesis

Abstract

Neocortical projection neurons arise from a pseudostratified ventricular epithelium (PVE) from embryonic day 11 (E11) to E17 in mice. The sequence of neuron origin is systematically related to mechanisms that specify neuronal class properties including laminar fate destination. Thus, the neurons to be assembled into the deeper layers are the earliest generated, while those to be assembled into superficial layers are the later generated neurons. The sequence of neuron origin also correlates with the probability of cell cycle exit (Q) and the duration of G1-phase of the cell cycle (T(G1)) in the PVE. Both Q and T(G1) increase as neuronogenesis proceeds. We test the hypothesis that mechanisms regulating specification of neuronal laminar destination, Q and T(G1) are coordinately regulated. We find that overexpression of p27(Kip1) in the PVE from E12 to E14 increases Q but not T(G1) and that the increased Q is associated with a commensurate increase in the proportion of exiting cells that is directed to superficial layers. We conclude that mechanisms that govern specification of neocortical neuronal laminar destination are coordinately regulated with mechanisms that regulate Q and are independent of mechanisms regulatory to cell cycle duration. Moreover, they operate prior to postproliferative mechanisms necessary to neocortical laminar assembly.

Published

2005

4. Cell output, cell cycle duration and neuronal specification: a model of integrated mechanisms of the neocortical proliferative process.

Author

Caviness VS Jr, Goto T, Tarui T, Takahashi T, Bhide PG, and Nowakowski RS

Subjects

Animals, Cell Cycle physiology, Cell Division physiology, Cerebral Ventricles cytology, Cerebral Ventricles embryology, Computer Simulation, Culture Techniques, Epithelium embryology, Gene Expression Regulation, Developmental, Mice, Mice, Knockout, Microfilament Proteins deficiency, Microfilament Proteins genetics, Neocortex cytology, Neurons classification, Neurons cytology, Microfilament Proteins metabolism, Models, Neurological, Muscle Proteins, Neocortex embryology, Neocortex physiology, Neurons physiology

Abstract

The neurons of the neocortex are generated over a 6 day neuronogenetic interval that comprises 11 cell cycles. During these 11 cell cycles, the length of cell cycle increases and the proportion of cells that exits (Q) versus re-enters (P) the cell cycle changes systematically. At the same time, the fate of the neurons produced at each of the 11 cell cycles appears to be specified at least in terms of their laminar destination. As a first step towards determining the causal interrelationships of the proliferative process with the process of laminar specification, we present a two-pronged approach. This consists of (i) a mathematical model that integrates the output of the proliferative process with the laminar fate of the output and predicts the effects of induced changes in Q and P during the neuronogenetic interval on the developing and mature cortex and (ii) an experimental system that allows the manipulation of Q and P in vivo. Here we show that the predictions of the model and the results of the experiments agree. The results indicate that events affecting the output of the proliferative population affect both the number of neurons produced and their specification with regard to their laminar fate.

Published

2003

5. Cyclin E-p27 opposition and regulation of the G1 phase of the cell cycle in the murine neocortical PVE: a quantitative analysis of mRNA in situ hybridization.

Author

Delalle I, Takahashi T, Nowakowski RS, Tsai LH, and Caviness VS Jr

Subjects

Animals, Cyclin B metabolism, Cyclin-Dependent Kinase 2, Cyclin-Dependent Kinases metabolism, In Situ Hybridization, Mice, Neocortex embryology, Protein Serine-Threonine Kinases metabolism, Proto-Oncogene Proteins p21(ras) metabolism, CDC2-CDC28 Kinases, Cyclin E metabolism, G1 Phase physiology, Gene Products, rex metabolism, Neocortex metabolism, RNA, Messenger metabolism

Abstract

We have analyzed the expression patterns of mRNAs of five cell cycle related proteins in the ventricular zone of the neocortical cerebral wall over the course of the neuronogenetic interval in the mouse. One set of mRNAs (cyclin E and p21) are initially expressed at high levels but expression then falls to a low asymptote. A second set (p27, cyclin B and cdk2) are initially expressed at low levels but ascend to peak levels only to decline again. These patterns divide the overall neuronogenetic interval into three phases. In phase 1 cyclin E and p21 levels of mRNA expression are high, while those of mRNAs of p27, cdk2 and cyclin B are low. In this phase the fraction of cells leaving the cycle after each mitosis, Q, is low and the duration of the G1 phase, TG1, is short. In phase 2 levels of expression of cyclin E and p21 fall to asymptote while levels of expression of mRNA of the other three proteins reach their peaks. Q increases to approach 0.5 and TG1 increases even more rapidly to approach its maximum length. In phase 3 levels of expression of cyclin E and p21 mRNAs remain low and those of the mRNAs of the other three proteins fall. TG1 becomes maximum and Q rapidly increases to 1.0. The character of these phases can be understood in part as consequences of the reciprocal regulatory influence of p27 and cyclin E and of the rate limiting functions of p27 at the restriction point and of cyclin E at the G1 to S transition.

Published

1999

6. A gradient in the duration of the G1 phase in the murine neocortical proliferative epithelium.

Author

Miyama S, Takahashi T, Nowakowski RS, and Caviness VS Jr

Subjects

Animals, Epithelial Cells cytology, Epithelium embryology, Gestational Age, Mice, Mice, Inbred Strains, Models, Neurological, S Phase, Cell Cycle, Embryonic and Fetal Development physiology, Neocortex cytology, Neocortex embryology

Abstract

Neuronogenesis in the neocortical pseudostratified ventricular epithelium (PVE) is initiated rostrolaterally and progresses caudo-medially as development progresses. Here we have measured the cytokinetic parameters and the fractional neuronal output parameter, Q, of laterally located early-maturing regions over the principal embryonic days (E12-E15) of neocortical neuronogenesis in the mouse. These measures are compared with ones previously made of a medial, late-maturing portion of the PVE. Laterally, as medially, the duration of the neuronogenetic interval is 6 days and comprises 11 integer cell cycles. Also, in both lateral and medial areas the length of G1 phase (TG1) increases nearly 4-fold and is the only cell cycle parameter to change. Q progresses essentially identically laterally and medially with respect to the succession of integer cell cycles. Most importantly, from E12 to E13 there is a steeply declining lateral to medial gradient in TG1. The gradient is due both to the lateral to medial graded stage of neuronogenesis and to the stepwise increase in TG1 with each integer cycle during the neuronogenetic interval. To our knowledge this gradient in TG1 of the cerebral PVE is the first cell biological gradient to be demonstrated experimentally in such an extensive proliferative epithelial sheet. We suggest that this gradient in TG1 is the cellular mechanism for positionally encoding a protomap of the neocortex within the PVE.

Published

1997