Your search keyword '"Castelain, Philippe"' showing total 11 results

1. Evaluation of three methods for the detection of DNA single-strand breaks in human lymphocytes: Alkaline elution, nick translation, and single-cell gel electrophoresis

Author

Leroy, T., Van Hummelen, Paul, Anard, Daniel, Castelain, Philippe, Kirsch-Volders, Micheline, Lauwerys, Robert, Lison, Dominique, Leroy, T., Van Hummelen, Paul, Anard, Daniel, Castelain, Philippe, Kirsch-Volders, Micheline, Lauwerys, Robert, and Lison, Dominique

Abstract

The aim of this study is to assess the ability of three methods, alkaline elution (AE), nick translation (NT), and single-cell gel electrophoresis (SCGE), to detect DNA single-strand breaks (ssb) in human peripheral blood lymphocytes (HPBL) exposed in vitro to three genotoxic agents: -rays, ethyl methanesulfonate (EMS) and benzo[a]pyrene diol epoxide (BPDE). The ultimate objective is to select the most feasible, sensitive, and reproducible method for the monitoring of populations exposed to genotoxic agents. AE and NT do not seem suitable assays. AE is able to detect DNA lesions induced by the three compounds, but only at relatively high doses (2 Gy, 5 mM EMS and 20 μM BPDE). With NT, DNA alterations induced by γ-rays are not detected and ssb are only evidenced after exposure to EMS (80 mM), which already alters the viability of the lymphocytes. Nick translation is able to detect ssb induced by 10 μM BPDE. Compared to the other assays, the sensitivity of the SCGE assay is significantly higher since statistically significant changes were detected after incubation with 0.5 mM EMS and 1.25 μM BDPE. SCGE is a relatively simple method, not time-consuming and applicable to a large number of samples per working day. In conclusion, on the basis of the results of this in vitro comparison, SCGE seems a promising method for the monitoring of populations exposed to genotoxic chemicals. Copyright © 1996 Taylor & Francis., SCOPUS: re.j, info:eu-repo/semantics/published

Published

1996

2. Aneugen‐induced micronuclei (MN) in human lymphocytes may be discerned using image analysis techniques when cell‐cycle stage is taken into account

Author

Van Hummelen, Paul, Nüsse, Michael, Castelain, Philippe, Kirsch-Volders, Micheline, Van Hummelen, Paul, Nüsse, Michael, Castelain, Philippe, and Kirsch-Volders, Micheline

Abstract

We show that for the in vitro cytochalasin‐B human lymphocyte micronucleus (MN) test, the quantification of the DNA content of MN and the difference in DNA content between the two macronuclei in the binucleate cells without MN, as measured by image analysis, gives a first estimation of the aneugenic potential of a test compound. Cultures of isolated human lymphocytes were exposed either to γ‐rays as a clastogen or to carbendazim (MBC) as an an‐eugen. The lymphocytes were stained with Feulgen stain and the MN were analyzed for DNA content with a Magiscan 2A image analyzer. The mean DNA content of MN induced by MBC were statistically higher than γ‐irradiation‐induced MN. It was demonstrated that in culture the lymphocytes, as well as the MN, are in different stages of the cell cycle, but this will not affect the discriminating power of the MN DNA content when only G1 cells are considered, or when DNA content of the MN is expressed relative to the total genome. The identification of Gl and G2 cell populations from image analysis data was performed by extrapolation of DNA content data from Gl‐ and G2‐sorted lymphocytes with a FacStar plus flow sorter. It was demonstrated that in MBC‐treated cells the DNA rearrangement between the macronuclei in binucle‐ates without MN was on the average higher than in γ‐irradiated and untreated cells, which points to aneugenic effects of MBC without the formation of MN. In contrast to DNA content measurements, the area of the MN is not a reliable measure for discriminating clastogens from aneugens. © 1995 Wiley‐Liss, Inc. Copyright © 1995 Wiley‐Liss, Inc. A Wiley Company, SCOPUS: ar.j, FLWNA, info:eu-repo/semantics/published

Published

1995

3. Improved detection of DNA aneuploidy in primary breast cancer using quantitative DNA image analysis in combination with fluorescent in situ hybridization technique

Author

Verdoodt, Berlinda, Castelain, Philippe, Bourgain, Claire, Kirsch-Volders, Micheline, Verdoodt, Berlinda, Castelain, Philippe, Bourgain, Claire, and Kirsch-Volders, Micheline

Abstract

To obtain more information about the relationship between numerical aberrations of chromosome 1 and the overall DNA content of breast cancer cells, fluorescent in situ hybridization with a pericentromeric probe for this chromosome and image analysis based densitometry were carried out on imprints of benign (15 cases, mainly fibroadenomas) and malignant breast disease (31 invasive ductal carcinomas out of 45 cases). The most pronounced aneuploidy was observed in invasive ductal and lobular carcinoma cases both by in situ hybridization and DNA content (76.7 and 75.0% were aneuploid). The frequency of cells with two spots for chromosome 1 was 48.3 and 51.5%, respectively, as compared to 80.3% in control lymphocytes. There was a weak overall correlation (r2 = 0.83) between DNA content and copy number of chromosome 1 in the malignant samples, although some of the DNA diploid/near diploid carcinomas showed a marked aneusomy for this chromosome. Also, some aberrations were present in the benign breast disease samples. Classification of cases by a linear discriminant analysis was most accurate when both techniques were combined (77% of cases correctly classified, according to anatomo-pathological diagnosis). The variables which received the highest weight in the linear discriminant function are the percentage DNA-diploid cells and the fraction of cells with two spots for chromosome 1. The sensitivity and sources of error of both techniques is considered. © 1995 Chapman & Hall., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1995

4. Study of numerical aberrations of chromosome 1 by fluorescent in situ hybridization and DNA content by densitometric analysis on (pre)-malignant cervical lesions

Author

Segers, Pascale, Haesen, Sonja, Castelain, Philippe, Amy, Jean-Jacques, De Sutter, Philippe, Van Dam, Peter, Kirsch-Volders, Micheline, Segers, Pascale, Haesen, Sonja, Castelain, Philippe, Amy, Jean-Jacques, De Sutter, Philippe, Van Dam, Peter, and Kirsch-Volders, Micheline

Abstract

In an attempt to determine whether the fluorescent in situ hybridization (FISH) can be used as a rapid approach for the identification of aneuploidy in premalignant cervical smears, a centromeric probe for chromosome 1 was used. The results from the FISH experiments were compared with measurements of the overall DNA content obtained by means of an image analysis system. With progression to neoplasia, a decrease of the frequency of cells with two spots was observed, due to an increasing polysomy of chromosome 1. As far as the DNA content was concerned, an increasing DNA index and 5C-exceeding ratio (fraction of cells with a DNA content higher than 5C) was observed. Classification of the FISH results by a linear discriminant analysis revealed that 67.6% of the cases were classified in agreement with the CIN classification. These data suggest that chromosome 1 may be considered as a marker chromosome for pre-malignant cervical lesions and that the DNA content measurements are complementary to the FISH results. © 1995 Chapman & Hall., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1995

5. Improved detection of DNA aneuploidy in primary breast cancer using quantitative DNA image analysis in combination with fluorescent in situ hybridization technique

Author

Verdoodt, Berlinda, Castelain, Philippe, Bourgain, Claire, Kirsch-Volders, Micheline, Verdoodt, Berlinda, Castelain, Philippe, Bourgain, Claire, and Kirsch-Volders, Micheline

Abstract

To obtain more information about the relationship between numerical aberrations of chromosome 1 and the overall DNA content of breast cancer cells, fluorescent in situ hybridization with a pericentromeric probe for this chromosome and image analysis based densitometry were carried out on imprints of benign (15 cases, mainly fibroadenomas) and malignant breast disease (31 invasive ductal carcinomas out of 45 cases). The most pronounced aneuploidy was observed in invasive ductal and lobular carcinoma cases both by in situ hybridization and DNA content (76.7 and 75.0% were aneuploid). The frequency of cells with two spots for chromosome 1 was 48.3 and 51.5%, respectively, as compared to 80.3% in control lymphocytes. There was a weak overall correlation (r2 = 0.83) between DNA content and copy number of chromosome 1 in the malignant samples, although some of the DNA diploid/near diploid carcinomas showed a marked aneusomy for this chromosome. Also, some aberrations were present in the benign breast disease samples. Classification of cases by a linear discriminant analysis was most accurate when both techniques were combined (77% of cases correctly classified, according to anatomo-pathological diagnosis). The variables which received the highest weight in the linear discriminant function are the percentage DNA-diploid cells and the fraction of cells with two spots for chromosome 1. The sensitivity and sources of error of both techniques is considered. © 1995 Chapman & Hall., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1995

6. Study of numerical aberrations of chromosome 1 by fluorescent in situ hybridization and DNA content by densitometric analysis on (pre)-malignant cervical lesions

Author

Segers, Pascale, Haesen, Sonja, Castelain, Philippe, Amy, Jean-Jacques, De Sutter, Philippe, Van Dam, Peter, Kirsch-Volders, Micheline, Segers, Pascale, Haesen, Sonja, Castelain, Philippe, Amy, Jean-Jacques, De Sutter, Philippe, Van Dam, Peter, and Kirsch-Volders, Micheline

Abstract

In an attempt to determine whether the fluorescent in situ hybridization (FISH) can be used as a rapid approach for the identification of aneuploidy in premalignant cervical smears, a centromeric probe for chromosome 1 was used. The results from the FISH experiments were compared with measurements of the overall DNA content obtained by means of an image analysis system. With progression to neoplasia, a decrease of the frequency of cells with two spots was observed, due to an increasing polysomy of chromosome 1. As far as the DNA content was concerned, an increasing DNA index and 5C-exceeding ratio (fraction of cells with a DNA content higher than 5C) was observed. Classification of the FISH results by a linear discriminant analysis revealed that 67.6% of the cases were classified in agreement with the CIN classification. These data suggest that chromosome 1 may be considered as a marker chromosome for pre-malignant cervical lesions and that the DNA content measurements are complementary to the FISH results. © 1995 Chapman & Hall., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1995

7. Aneuploidy for chromosome 1 and overall DNA content in benign and malignant breast disease

Author

Verdoodt, Berlinda, Castelain, Philippe, Bourgain, Claire, Kirsch-Volders, Micheline, Verdoodt, Berlinda, Castelain, Philippe, Bourgain, Claire, and Kirsch-Volders, Micheline

Abstract

Fluorescence in situ hybridization (FISH) with a probe for the pericentromeric region of chromosome 1 and DNA content measurements by image-analysis-based densitometry have been carried out on imprints of benign and malignant breast tissue. In general, an increase in the number of spots per nucleus was observed in the invasive carcinomas, with a large intercellular variation. In comparison with lymphocytes from controls, some cases of benign breast disease already had an increased frequency of aneusomy of chromosome 1, although they were all (near)diploid by DNA-content. However, an overall concordance between the DNA content measurements and the results of FISH was observed, although some exceptions were seen. A statistically significant correlation between the DNA index and the mean number of spots for chromosome 1 per nucleus was found. A linear discriminant analysis was applied on the data; the resulting classification of patients was most accurate when parameters describing DNA content and FISH results were combined. © 1994., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1994

8. Aneuploidy for chromosome 1 and overall DNA content in benign and malignant breast disease

Author

Verdoodt, Berlinda, Castelain, Philippe, Bourgain, Claire, Kirsch-Volders, Micheline, Verdoodt, Berlinda, Castelain, Philippe, Bourgain, Claire, and Kirsch-Volders, Micheline

Abstract

Fluorescence in situ hybridization (FISH) with a probe for the pericentromeric region of chromosome 1 and DNA content measurements by image-analysis-based densitometry have been carried out on imprints of benign and malignant breast tissue. In general, an increase in the number of spots per nucleus was observed in the invasive carcinomas, with a large intercellular variation. In comparison with lymphocytes from controls, some cases of benign breast disease already had an increased frequency of aneusomy of chromosome 1, although they were all (near)diploid by DNA-content. However, an overall concordance between the DNA content measurements and the results of FISH was observed, although some exceptions were seen. A statistically significant correlation between the DNA index and the mean number of spots for chromosome 1 per nucleus was found. A linear discriminant analysis was applied on the data; the resulting classification of patients was most accurate when parameters describing DNA content and FISH results were combined. © 1994., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1994

9. Cytogenetic and genetic alterations during hepatocarcinogenesis

Author

Kirsch-Volders, Micheline, Haesen, Sonja, Deleener, Alain, Castelain, Philippe, Alexandre, Henri, Préat, V, Kirsch-Volders, Micheline, Haesen, Sonja, Deleener, Alain, Castelain, Philippe, Alexandre, Henri, and Préat, V

Abstract

info:eu-repo/semantics/published

Published

1988

10. The influence of phenobarbital and butylated hydroxytoluene on the ploidy rate in rat hepatocarcinogenesis.

Author

Haesen, Sonja, Derijcke, T, Deleener, Alain, Castelain, Philippe, Alexandre, Henri, Préat, V, Kirsch-Volders, Micheline, Haesen, Sonja, Derijcke, T, Deleener, Alain, Castelain, Philippe, Alexandre, Henri, Préat, V, and Kirsch-Volders, Micheline

Abstract

The effect of the 'promoters' phenobarbital (PB) and butylated hydroxytoluene (BHT) on the ploidy changes during hepatocarcinogenesis in rats was compared in a densitometric analysis of Feulgen-stained nuclei on paraffin-embedded tissue slices. The triphasic Gerlans protocol for liver-cancer induction was applied. Initiation with a single dose of diethylnitrosamine (DEN), and selection with 2-acetylamino-fluorene (2-AAF) combined with a proliferative stimulus (CCl4 administration), was followed by a treatment with PB or BHT for periods up to 22 weeks. Control animals received no treatment after the initiation and selection procedure. Despite intra- and inter-individual variations, an increase in the amount of 2N nuclei is found in the putative preneoplastic lesions of animals that received initiation and selection (I-S) and 3 weeks basal diet (BD). When the diet is supplemented with PB (after I-S), the increase of diploid nuclei starts earlier. At the time carcinoma arise (22 weeks PB treatment) a decrease in the frequency of 2N nuclei is found. BHT-treated animals which develop no carcinoma within the considered timespan, show a clear increased amount of 2N nuclei in the precancerous lesions only after 14 weeks treatment. It seems that there is a positive correlation between the outgrowth of putative preneoplastic foci and nodules in rat liver and an increase of diploid nuclei in these lesions. PB, as promoter used after initiation and selection, speeds up the development of carcinoma in rat liver, and therefore also the shift to diploidization in these rats starts earlier in comparison with I-S-treated rats. Although BHT does not promote liver carcinogenesis, an increase of diploid nuclei is also observed here during lesion formation. It may, therefore, be concluded that the phenomenon of diploidization is closely linked to and probably necessary for preneoplastic development, but that it is not an absolute indicator for neoplastic transformation., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1988

11. Changes in nucleolar transcriptional activity and nuclear DNA content during the first steps of rat hepatocarcinogenesis.

Author

Deleener, Alain, Castelain, Philippe, Préat, V, de Gerlache, Jacques, Alexandre, Henri, Kirsch-Volders, Micheline, Deleener, Alain, Castelain, Philippe, Préat, V, de Gerlache, Jacques, Alexandre, Henri, and Kirsch-Volders, Micheline

Abstract

Two complementary genetic parameters were followed in liver parenchymal cells during the first steps of rat hepatocarcinogenesis: the expression of nucleolar genes estimated from their silver stainability and the nuclear DNA content determined after Feulgen staining. Putative preneoplastic lesions as foci and nodules were induced by the triphasic 'Gerlans protocol'. Initiation with a single dose of diethylnitrosamine (DEN) was followed by a selection of initiated cells with 2-acetylaminofluorene (2-AAF) in combination with a single necrogenic dose of CCl4 as a proliferative stimulus. Finally after 1 week of normal diet, the animals were treated or not with phenobarbital (PB) for periods up to 2 months. Serial sections were analysed after silver staining (AgNO3), methyl-green--pyronin staining (Unna-Brachet) and Feulgen staining with densitometric and morphometric methods. Silver staining, which is known to stain an acidic protein associated with rRNA synthesis, increased gradually with the duration of the PB treatment. Morphometry revealed an increase in both nucleolar and nuclear volume; the fraction of nuclei with one nucleolus also increased. These results seem to point towards an increase of nucleolar activity in the early steps of PB promotion. Moreover, this shift cannot be ascribed to an increase of DNA content. Indeed, a parallel study on neighbouring sections stained with Feulgen revealed a shift towards a population of diploid nuclei, in contrast to normal liver cells, which are mostly tetraploid. The observed diploidisation may therefore provide a functional advantage for the expansion of putative preneoplastic cells., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

1987