Gross tumor volume segmentation for head and neck cancer radiotherapy using deep dense multi-modality network

Gene product expression in normal and chronic hepatitis C virus infection was determined in an attempt to improve our understanding of the molecular events leading to the development of cirrhosis and liver carcinoma. Activation of CD95 (Fas) causes apoptosis of cells and liver failure in mice and has been associated with human liver disorders. c-myc is involved in cell proliferation and EGFR in regeneration of cells. The material of the current study included 50 cases of chronic hepatitis C (CHC) (and negative hepatitis B virus infection), 29 cases of liver cirrhosis and HCV (LC), and 19 cases of hepatocellular carcinoma and HCV (HCC) admitted to the Theodor Bilharz Research Institute (TBRI) during the years 2003-2004. Ten wedge liver biopsies - taken during laparoscopic cholecystectomy - were included in the study as normal controls. Laboratory investigations, including liver function tests, serological markers for viral hepatitis and serum alpha fetoprotein level (alpha-FP), were determined for all cases. Histopathological study and immunohistochemistry using monoclonal antibodies for CD95, c-myc and EGFR were also done. In CHC cases, the histological activity index (HAI) revealed more expression of Fas antigen in liver tissues with active inflammation than in those without active inflammation (p < 0.01). EGFR and c-myc act synergistically in liver tumorigenesis. Upregulation of Fas in chronic hepatitis C infection and of c-myc & EGFR in malignant transformation was concluded from this study. c-myc expression may obstruct the induction of apoptosis of HCC cells and lead to uncontrolled cell growth.

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Circulating miRNAs as Predictor Markers for Activation of Hepatic Stellate Cells and Progression of HCV-Induced Liver Fibrosis

El‐Ahwany¹,

Nagy²,

Zoheiry³

et al. 2016

Electron physician

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IntroductionLiver fibrosis is the excessive accumulation of extracellular matrix that occurs by activation of hepatic stellate cells (HSCs), which has been identified as the major driver of liver fibrosis. Several studies confirmed that miRNAs have regulatory effects on the activation of HSCs by affecting the signaling pathways. The aim of this study was to develop non-invasive diagnostic markers by measuring different circulating miRNAs in serum as predictor markers for early diagnosis of liver fibrosis and its progression.MethodsIn this case-control study, we enrolled 66 subjects with chronic hepatitis C (CHC) with early stage of fibrosis and 65 subjects with CHC with late-stage fibrosis. Also, 40 subjects were included as normal controls. The six main miRNAs, i.e., miR-138, miR-140, miR-143, miR-325, miR-328, and miR-349, were measured using the reverse transcription-polymerase chain reaction.ResultsIn the cases of CHC both with early and late stage of fibrosis, the circulating levels of the six main miRNAs were significantly higher than the levels in the control group. ROC analysis indicated that the sensitivity and specificity of miR-138 were 89.3% and 71.43%, respectively, in the early stage of fibrosis. In the late stage, the sensitivity and specificity of miR-138 were 89.3 and 93.02%, respectively, whereas, for miR-143, they were 75.0 and 88.4%, respectively.ConclusionsCirculating miR-138 could serve as a non-invasive biomarker for the detection of early fibrosis. Also, miR-138 and miR-143 could be specific biomarkers for indicating the late stage of liver fibrosis.

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Pharmacodynamics of pentoxifylline and/or praziquantel in murine schistosomiasis mansoni

El-Lakkany¹,

Nosseir

2007

APMIS

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Pentoxifylline (PTX) was proved to exert both anti-inflammatory and anti-fibrotic effects, and was used therapeutically in this experimental model to investigate its role alone or with praziquantel (PZQ) in Schistosoma mansoni-infected mice, and to explore its impact on the tissue expression of transforming growth factor-beta1 (TGF-beta1). S. mansoni-infected mice were divided into seven groups: Control untreated (I), treated with curative dose of PZQ, 500 mg/kg/day for 2 consecutive days (II), or subcurative dose, 100 mg/kg/day for 2 consecutive days (III), treated with PTX (10 mg/kg/day for 5 days/wk) alone for 4 weeks (IV) or in addition to subcurative dose of PZQ (V), and treated with PTX alone for 8 weeks (VI) or in addition to subcurative dose of PZQ (VII). All animals were killed 10 weeks post infection. Parasitological assessment of worm burden, tissue egg load and oogram pattern was carried out. The degree of granulomatous fibrosis and eosinophilic cell population was quantified in Sirius-red-stained sections and tissue transforming growth factor beta-1 expression was estimated immunohistochemically. Serum ALAT and GGT, as well as hepatic content of reduced GSH, were measured. The results revealed the highest percent of worm reduction and dead ova in groups (II) and (VII) accompanied by significant diminution in granulomatous parameters, collagen content and TGF-beta1 tissue expression. Moreover, treatments with PTX and/or PZQ ameliorated the liver functions. In conclusion, prolonged treatment with PTX has a potent anti-fibrogenic role especially when used in the early stages of infection, with limited toxic effects on schistosome worms and eggs. Thus, PTX can be used as an adjuvant therapeutic tool with anti-helminthic drugs in the treatment of human schistosomiasis.

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Role of fibrogenic markers in chronic hepatitis C and associated hepatocellular carcinoma

et al. 2012

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Detection and follow up of fibrogenesis in chronic hepatitis C (CHC) is mandatory for early treatment and risk stratification. The current study included 120 patients with CHC, of whom 30 had liver cirrhosis (LC) and 30 had hepatocellular carcinoma (HCC). 15 wedge liver biopsies, taken during laparoscopic cholecystectomy, were included as normal controls. Cases were subjected to laboratory investigations, serologic markers for viral hepatitis and assessment of circulating levels of hyaluronic acid (HA) and platelet-derived growth factor (PDGF). Immunohistochemical expression of connective tissue growth factor (CTGF), PDGF and transforming growth factor-β1 (TGF-β1) was also carried out. A significant increase (p < 0.01) in serum HA was noticed in CHC, LC and HCC compared to controls. Although, a significant decrease in serum PDGF was detected in CHC and LC compared to controls, HCC values were comparable. A significant up-regulation of CTGF was detected in CHC, LC and HCC (p < 0.01) in contrast to its limited mild expression in normal livers. Intense PDGF positive staining was noticed in CHC, LC and HCC compared to scattered faint expression in controls. The significant expression and marked intensity of PDGF staining matched the progress to tumorigenesis. A positive TGF-β1 immunostaining was also noticed in CHC, LC and HCC. An intense and extensive cytoplasmic expression of TGF-β1 was encountered in patients with LC revealing that CTGF, PDGF and TGF-β1 act synergistically in LC. Data revealed that HA and CTGF may be implicated as important diagnostic parameters for assessment of hepatic fibrosis and PDGF for monitoring malignant transformation in CHC.

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Experiments with 4-Thiopyrones and with 2,2',6,6'-Tetraphenyl-4,4'-dipyrylene. The Piezochromism of Diflavylene

Schönberg¹,

Elkaschef²,

Nosseir³

et al. 1958

J. Am. Chem. Soc.

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A. SCHONBERG, M. ELKASCHEF, M. NOSSEIR AND M. ill. SIDKY VOl. 80 solute ethanol was hydrogenated over 3 mg. of 1Oyo palladium-on-carbon a t atmospheric pressure and room temperature. The measured volume of hydrogen consunled was 1.53 cc. (calcd. for 1 equivalent, 1.25 cc.). The catalyst was removed by centrifugation and washed with several portions of ether. Evaporation of the solvents yielded an depression. oil which partially crystallized when scratched with a glass stirring rod. The product was dissolved in 1 cc. of methanol and suffkient water added t o make the solution cloudy. Cooling in an ice-bath with scratching caused crystallization t o occur. The crystalline acid was separated by centrifugation and had m.p. 53-56'. Sublimation a t 75" (15 mm.) afforded 3.5 mg. (41.5%) of the pure acid, m.p. 55.5-57' (reportedg 5 8 " ) . Mixed melting point comparison with 'in

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Über die eigenschaften von polyvinylcarbanilat in lösung. 1. Die molekulargewichtsabhängigkeit von trägheitsradius, 2. Virialkoeffizienten und staudingerindex in dioxan sowie in einem Θ‐lösungsmittel

Burchard¹,

Nosseir²

1965

Makromol. Chem.

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ZUSAMMENFASSUNG:Die molekularen Parameter von Polyvinylcarbanilat in Dioxan und einem 0-Losungsmittel wurden durch Streulicht-und Viskositatsmessungen bestimmt. Es zeigte sich, daI3die aus den STAUDINGERindiCes berechneten Tragheitsradien gut mit den direkt gemessenen iibereinstimmen. Die Molekulargewichtsabhangigkeit des Expansionskoeffizienten a2 erlaubt eine Priifung der Theorie von KURATA, STOCKMAYER und R O I G~~) .Bis zu Werten von a2 = 1,6 ist die Theorie erfiillt, bei hoheren Werten treten Abweichungen auf, die auch bei Polymethylmethacrylat beobachtet werden. Die Eztrapolation der STAUDIiVGERindiCes nach KURATA und STOCKMAYER~) ergibt fur die Messungen in Dioxan den gleichen Ordinatenabschnitt wie fiir die Messungen in dem @-Losungsmittel, jedoch erhalt man bei den Dioxanlosungen statt der von der Theorie geforderten Geraden eine gekrummte Kurve. Die Abhingigkeit des 2. Virialkoeffizienten vom Molekulargewicht kann durch keine der bekannten Theorien beschrieben werden. SUMMARY:The molecular data of polyvinylcarbanilate in dioxane and a @-solvent have been determined by light scattering and viscosity measurement. The radii of gyration calculated from the intrinsic viscosity correspond well with the directly measured ones. The molecular weight dependence of the expansion coefficient u2 permits an improvement of the theory of KURATA, STOCKMAYER, and R O I G~~) .Up to values of a2 = 1,6 the K-ST-R theory is valid, at higher values deviations are observed. In dioxane and the @-solvent the KURATA-STOCKMAYER-plot of the intrinsic viscosity yields the same intercept but instead of the theoretical straight line a curve is obtained for dioxane solutions. The molecular weight dependence of the 2. virialcoefficient cannot be described by any of the known theories. A. EinleitungObwohl die Losungseigenschaften von Vinylpolymeren von den verschiedenen Gruppen linearer Makromolekiile bisher am eingehendsten untersucht wwrden und nach der zusammenfassenden Arbeit von KURATA

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Cyclooxygenase‐2 expression on urothelial and inflammatory cells of cystoscopic biopsies and urine cytology as a possible predictive marker for bladder carcinoma

Moussa¹,

Omran²,

Nosseir³

et al. 2009

APMIS

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Cyclooxygenase-2 (COX-2) is a key inducible enzyme involved in the production of prostaglandins. It contributes to human carcinogenesis by various mechanisms. The aim of the current study was to elucidate the possible involvement of COX-2 in human bladder carcinoma by examining its expression on both urothelial and inflammatory cells in tissue biopsies and urine cytology samples of different urinary bladder lesions. A total of 65 patients were included in the study and were selected from cases admitted to Urology Department, Theodor Bilharz Research Institute (TBRI), Giza, Egypt. They represented seven control cases with almost normal-looking bladder tissue; pure chronic cystitis (n=12); premalignant lesions (18) in the form of squamous metaplasia (n=8) or urothelial dysplasia (n=10) as well as transitional cell carcinoma (TCC) (n=18), and squamous cell carcinoma (SqCC) (n=10). Immunohistochemistry of formalin-fixed, paraffin-embedded tissue sections and urine cytology samples was performed for all cases using COX-2 (H-62): sc-7951, a rabbit polyclonal antibody. The study revealed positive COX-2 expression on the urothelial and inflammatory cells of cystoscopic biopsies from all cases of pure chronic cystitis, squamous metaplasia and SqCC compared with 42.8% and 71.4% of normal controls, respectively. The score of urothelial COX-2 expression was sequentially up-regulated from normal to chronic cystitis (either pure or associated with premalignant changes) (p<0.05) to malignant changes (p<0.05). However, the inflammatory cellular expression was down-regulated with malignant transformation compared with chronic cystitis (p<0.05). In TCC, COX-2 was over-expressed on both urothelial and inflammatory cells in advanced tumors. Urine cytology samples were positive for COX-2 in a comparable manner to that observed in cystoscopic biopsies. Accordingly, the results of the current study have provided new information in two aspects: First, is the possibility of using the differential COX-2 expression on both inflammatory and urothelial cells as markers for premalignant or malignant transformation; second, besides cystoscopy, urine cytology was found to have a high sensitivity for COX-2 expression and hence proved to be valuable in malignancy as a non-invasive substitute for cystoscopy.

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Immunohistopathological and biochemical changes in Schistosoma mansoni-infected mice treated with artemether

Botros

Mahmoud

Moussa

et al. 2007

Journal of Infection

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M. H. Nosseir

Immunohistochemical expression of CD95 (Fas), c‐myc and epidermal growth factor receptor in hepatitis C virus infection, cirrhotic liver disease and hepatocellular carcinoma

Circulating miRNAs as Predictor Markers for Activation of Hepatic Stellate Cells and Progression of HCV-Induced Liver Fibrosis

Pharmacodynamics of pentoxifylline and/or praziquantel in murine schistosomiasis mansoni

Role of fibrogenic markers in chronic hepatitis C and associated hepatocellular carcinoma

Experiments with 4-Thiopyrones and with 2,2',6,6'-Tetraphenyl-4,4'-dipyrylene. The Piezochromism of Diflavylene

Über die eigenschaften von polyvinylcarbanilat in lösung. 1. Die molekulargewichtsabhängigkeit von trägheitsradius, 2. Virialkoeffizienten und staudingerindex in dioxan sowie in einem Θ‐lösungsmittel

Cyclooxygenase‐2 expression on urothelial and inflammatory cells of cystoscopic biopsies and urine cytology as a possible predictive marker for bladder carcinoma

Immunohistopathological and biochemical changes in Schistosoma mansoni-infected mice treated with artemether

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