Osama El-Sayed scite author profile

Western blotting confirmed the activation of the hypertrophic signaling cascades in aortas of profilin 1 mice. Phospho-ERK1/2 was significantly higher in profilin 1 than 88R/L and control (512.3 and 361.7%, respectively, p < 0.05). Profilin 1 mice had significant increases in phospho-JNK as compared with 88R/L and control (371.4 and 346%, respectively, p < 0.05). However, there were no differences between 88R/L and control mice in both kinases. There was a significant increase in ROCK II kinase in the aorta of profilin 1 mice compared with controls (>400%, p < 0.05). Tail cuff and circadian monitoring of blood pressure showed significant increases in systolic and mean arterial blood pressures of profilin 1 mice starting at age 6 months compared with controls (ϳ25 mm Hg, p < 0.05). These results suggest that increased actin polymerization in blood vessels triggers activation of the hypertrophic signaling cascades and results in elevation of blood pressure at advanced age.

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Precision annotation of digital samples in NCBI’s gene expression omnibus

Hadley

Pan

El-Sayed

et al. 2017

Sci Data

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The Gene Expression Omnibus (GEO) contains more than two million digital samples from functional genomics experiments amassed over almost two decades. However, individual sample meta-data remains poorly described by unstructured free text attributes preventing its largescale reanalysis. We introduce the Search Tag Analyze Resource for GEO as a web application (http://STARGEO.org) to curate better annotations of sample phenotypes uniformly across different studies, and to use these sample annotations to define robust genomic signatures of disease pathology by meta-analysis. In this paper, we target a small group of biomedical graduate students to show rapid crowd-curation of precise sample annotations across all phenotypes, and we demonstrate the biological validity of these crowd-curated annotations for breast cancer. STARGEO.org makes GEO data findable, accessible, interoperable and reusable (i.e., FAIR) to ultimately facilitate knowledge discovery. Our work demonstrates the utility of crowd-curation and interpretation of open ‘big data’ under FAIR principles as a first step towards realizing an ideal paradigm of precision medicine.

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Cardiac remodeling caused by transgenic overexpression of a corn Rac gene

Elnakish

Awad

Hassona

et al. 2011

American Journal of Physiology-Heart and Circulatory Physiology

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Rac1-GTPase activation plays a key role in the development and progression of cardiac remodeling. Therefore, we engineered a transgenic mouse model by overexpressing cDNA of a constitutively active form of Zea maize Rac gene (ZmRacD) specifically in the hearts of FVB/N mice. Echocardiography and MRI analyses showed cardiac hypertrophy in old transgenic mice, as evidenced by increased left ventricular (LV) mass and LV mass-to-body weight ratio, which are associated with relative ventricular chamber dilation and systolic dysfunction. LV hypertrophy in the hearts of old transgenic mice was further confirmed by an increased heart weight-to-body weight ratio and histopathology analysis. The cardiac remodeling in old transgenic mice was coupled with increased myocardial Rac-GTPase activity (372%) and ROS production (462%). There were also increases in α(1)-integrin (224%) and β(1)-integrin (240%) expression. This led to the activation of hypertrophic signaling pathways, e.g., ERK1/2 (295%) and JNK (223%). Pravastatin treatment led to inhibition of Rac-GTPase activity and integrin signaling. Interestingly, activation of ZmRacD expression with thyroxin led to cardiac dilation and systolic dysfunction in adult transgenic mice within 2 wk. In conclusion, this is the first study to show the conservation of Rho/Rac proteins between plant and animal kingdoms in vivo. Additionally, ZmRacD is a novel transgenic model that gradually develops a cardiac phenotype with aging. Furthermore, the shift from cardiac hypertrophy to dilated hearts via thyroxin treatment will provide us with an excellent system to study the temporal changes in cardiac signaling from adaptive to maladaptive hypertrophy and heart failure.

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Intact Toll-like receptor 9 signaling in neutrophils modulates normal thrombogenesis in mice

El-Sayed

Dewyer

Luke

et al. 2016

Journal of Vascular Surgery

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Background Deletion of Toll-like receptor 9 (Tlr9) signaling, which is important for sterile inflammatory processes, results in impaired venous thrombosis (VT) resolution in mice. The purpose of this study was to determine if deletion of Tlr9 affected sterile necrosis, apoptosis, and neutrophil extracellular trap (NET) production in VT. Methods Stasis and non-stasis murine models of VT were used in wild type (WT and Tlr9−/− mice, with assessment of VT size, and determination of neutrophil extracellular traps (NETs), necrosis and apoptosis markers. Anti-PMN and anti-platelet antibody strategies were used to determine the cellular roles and their roles in WT and Tlr9−/− mice. Results At 2d, stasis thrombi in Tlr9−/− mice were 62% larger (n = 6–10) with 1.4 fold increased uric acid levels, 1.7 fold more apoptotic cells, 2 fold increased citrullinated histones (cit-H3), 2 fold increased peptidylarginine deiminase – 4 and 1.5 fold increased elastase, with a 2.4 fold reduction in tissue factor pathway inhibitor (TFPI) as compared with WT (all n = 4–7; P < .05). In contrast, non-stasis VT sizes were not significantly different in Tlr9−/− mice (n = 4–6), and did not have elevated necrosis or NET markers. Stasis VT size was not reduced at the 2d time-point in WT or TLR9−/− mice that received treatment with DNAse-I, or in PAD4−/− mice, which are incapable of forming NETs. Stasis VT size was reduced 18% inTlr9−/− mice undergoing PMN depletion (n = 8–10), and was associated with 29 fold decreased cit H3, 1.3 fold decreased elastase, and 1.5 fold increased TFPI (all n = 6; P < .05). Lastly, platelet depletion (>90% reduction) did not significantly reduce stasis VT inTlr9−/− mice. Conclusions These data suggest the thrombogenic model impacts Tlr9 thrombogenic mechanisms, and that functional Tlr9 signaling in PMN, but not platelets or NETs, is an important mechanism in early stasis experimental venous thrombogenesis.

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Cardiac resynchronization therapy in patients with postero-lateral scar by cardiac magnetic resonance: A systematic review and meta-analysis

Daoulah

Alsheikh‐Ali

Al-Faifi

et al. 2015

Journal of Electrocardiology

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Osama El-Sayed

Vascular Hypertrophy and Hypertension Caused by Transgenic Overexpression of Profilin 1

Precision annotation of digital samples in NCBI’s gene expression omnibus

Cardiac remodeling caused by transgenic overexpression of a corn Rac gene

Intact Toll-like receptor 9 signaling in neutrophils modulates normal thrombogenesis in mice

Cardiac resynchronization therapy in patients with postero-lateral scar by cardiac magnetic resonance: A systematic review and meta-analysis

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