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5 results on '"B Casto"'

1. Modulation of Ki67, p53 and RARbeta expression in normal, premalignant and malignant human oral epithelial cells by chemopreventive agents

Author

S M, D'Ambrosio, R E, Gibson-D'Ambrosio, G, Wani, B, Casto, G E, Milo, G J, Kelloff, and V E, Steele

Subjects
Retinoids, Ki-67 Antigen, Receptors, Retinoic Acid, Mouth Mucosa, Tumor Cells, Cultured, Anticarcinogenic Agents, Humans, Epithelial Cells, Mouth Neoplasms, Tumor Suppressor Protein p53, Precancerous Conditions, Cell Line
Abstract

Aberrant expression of Ki67, p53 and RARbeta are characteristic of many tumor types including those of the oral cavity. Chemopreventive agents may act by modulating their expression to more normal levels.The effects of 21 chemopreventive agents on the expression of Ki67, p53 and RARbeta were determined using a human in vitro model of normal, premalignant and malignant oral epithelial cell lines.Ki67 and mutant p53 (mtp53) were overexpressed in both the premalignant and malignant cell lines, whereas expression of RARbeta was high in the normal, low in the premalignant and not detectable in the malignant cell lines. Most of the agents selectively inhibited the expression of Ki67 in the premalignant and malignant cell lines. Eight of the 21 agents increased, while four agents decreased, the levels of mtp53 protein in the premalignant cell line. In the malignant cell line, five of the agents increased, while ten agents decreased mtp53 protein levels. The agents increased RARbeta expression to near normal levels in the premalignant cell line.The data suggest that the suppression of Ki67 and mtp53 are good indicators of the effectiveness of agents in premalignant and malignant oral cells, whereas the enhancement of RARbeta is a measure of effectiveness in premalignant oral cells.

Published
2002

2. Differential response of normal, premalignant and malignant human oral epithelial cells to growth inhibition by chemopreventive agents

Author

S M, D'Ambrosio, R, Gibson-D'Ambrosio, G E, Milo, B, Casto, G J, Kelloff, and V E, Steele

Subjects
Retinoids, Curcumin, Eflornithine, Mouth Mucosa, Anticarcinogenic Agents, Humans, Mouth Neoplasms, Precancerous Conditions, Cell Division, Acetylcysteine, Cell Line
Abstract

Squamous cell carcinoma (SCC) of the oral cavity is a multistep process, progressing through a series of discrete, irreversible and complementary alterations in genes that control cell growth, death, and differentiation. In the premalignant state, the oral mucosa progresses through various grades of epithelial dysplasia, with the potential to convert to SCC. Chemopreventive strategies are designed to suppress, reverse, or prevent the formation of premalignant lesions and their subsequent progression to SCC. In the present study, we determined the growth inhibitory effect of 21 chemopreventive agents in a cell culture model using normal, premalignant, and malignant human oral mucosal cell lines. There were significant differences in the growth inhibitory responses of these cell lines to selected retinoids and non-retinoid analogs. Among the retinoids tested, the synthetic retinamides, as a class, showed selective growth inhibition of both premalignant and malignant cells compared to normal human oral epithelial cells in culture. Within the retinamide class, 2CPR exhibited the greatest selectivity in the growth inhibition of premalignant and malignant cells. Among the non-retinoids analyzed, DFMO was a moderate to potent inhibitor of malignant and premalignant oral cell growth, respectively, and stimulated normal oral cell growth at low concentrations. Using this in vitro approach, we have identified several potential chemopreventive agents for oral cancer as selective growth inhibitors of premalignant ahd malignant human oral mucosa cells.

Published
2000

3. Metastatic conversion of chemically transformed human cells

Author

X L, Sun, D, Li, J, Fang, B, Casto, I, Noyes, and G E, Milo

Subjects
Male, Tissue Inhibitor of Metalloproteinase-1, Carcinogenicity Tests, Mice, Nude, Neoplasms, Experimental, DNA, Antisense, Article, Gene Expression Regulation, Neoplastic, Mice, Cell Transformation, Neoplastic, Animals, Humans, Genes, Tumor Suppressor, Matrix Metalloproteinase 1, Neoplasm Metastasis, Cell Line, Transformed
Abstract

A linear model for human cell metastasis has been developed in vitro from chemically transformed normal human cells. The chemically transformed cells are nontumorigenic in nude mice, but can be converted to a tumorigenic phenotype by transfection with a nondirectional cDNA library or antisense cDNA to the ML-1 gene. The primary transfected cell line (TR1T) forms localized, progressively growing tumors in nude mice that do not invade into the surrounding tissue. This tumorigenic TR1T cell line could be advanced into a metastatic stage following an additional transfection (TR2M cell line) with the cDNA expression library or antisense cDNA to the ML-1 gene. Metastatic cells, selected from tumors that were attached to internal organs, exhibited an increase in invasiveness as measured in vitro using an invasion chamber. The metastatic cells also exhibited an increased expression of matrix metalloproteinase-1 (MMP-1), although MMP-1 was not part of the cDNA that was transfected into either the TR1T cells or the doubly transfected metastatic TR2M cells. These data suggest that the increase in MMP-1 expression was a secondary downstream event responding to an upstream genetic change that initiated the conversion of cells from a tumorigenic to a metastatic stage. In summary, human cell lines representing premalignant, malignant, and metastatic phenotypes have been established in culture that can be used to identify gene changes that occur as normal human cells progress to a metastatic stage during tumor development. One gene, ML-1, that is found in the expression library appears to be involved in malignant progression, because ML-1 antisense cDNA will convert chemically transformed cells to both tumorigenic and metastatic stages, and cells from both local and metastatic tumors have a reduced or complete loss of expression of the ML-1 gene.

Published
2000

4. Specific neutralization of human hepatitis type A in marmoset monkeys

Author

A. W. Holmes, G. Froesner, Marcel E. Conrad, B. Casto, F. Deinhardt, D. Paterson, and L. Wolfe

Subjects
endocrine system, animal structures, Cross Reactions, Hepatitis, Animal, Neutralization, Blood serum, Antigen, Species Specificity, Antibody Specificity, Neutralization Tests, biology.animal, medicine, Animals, Humans, Hepatovirus, Antigens, Viral, Hepatitis, Infectivity, Multidisciplinary, biology, Transmission (medicine), Monkey Diseases, Marmoset, Haplorhini, Hepatitis A, medicine.disease, Virology, body regions, Blood chemistry, Immunology
Abstract

THE transmission of human hepatitis type A (infectious hepatitis) to marmoset monkeys, previously reported from this laboratory1–5, has been confirmed by several other laboratories6–9 but questioned by one10,11. To strengthen the case for considering the agents causing experimental hepatitis in marmosets as viruses of human hepatitis type A, and not as latent “marmoset hepatitis viruses” as has been suggested by the dissenting laboratory10,11, it was necessary both to show clearly the lack of induction of disease by normal human serum or plasma and to demonstrate specific neutralization by convalescent human serum of the hepatitis type A agents transmitted from man to marmosets. We describe such neutralization here.

Published
1973

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