Your search keyword '"Franc B"' showing total 23 results

1. Unsupervised Learning in PET Radiomics.

Author

Liu, G, Liu, G, Huang, S-Y, Franc, B, Seo, Y, Mitra, D, Liu, G, Liu, G, Huang, S-Y, Franc, B, Seo, Y, and Mitra, D

Abstract

In this study, we investigated large scale radoimics on 116 breast cancer patients. We are particularly interested in unsupervised learning to bicluster patients and features in order to associate such biclusters with the disease characteristics. The results show that radiomics features with wavelet features have a better biclustering ability. And 172 radiomics features have shown a better classification capability.

Published

2017

2. Human thyroid tumours, the puzzling lessons from E7 and RET/PTC3 transgenic mice.

Author

Jin, Ling, Burniat, Agnès, Dumont, Jacques Emile, Miot, Françoise, Corvilain, Bernard, Franc, B, Jin, Ling, Burniat, Agnès, Dumont, Jacques Emile, Miot, Françoise, Corvilain, Bernard, and Franc, B

Abstract

Human rearranged RET/PTC3 (papillary thyroid carcinoma) proto-oncogene and high-risk human papillomavirus (HPV) type 16 E7 oncogene induces in the mouse a neoplastic transformation of thyroid follicular cells. We present a detailed immuno-histological study (170 mouse thyroids: RET/PTC3, E7, wild type, 2- to 10-month-old) with cell cycle proliferation and signalling pathway indicators. The characteristics of both models are different. There is an 'oncogene dependent' cellular signature, maintained at all studied ages in the E7 model, less in the RET/PTC3 model. During tumour development a large heterogeneity occurred in the Tg-RET/PTC3 model within a same tumour or within a same thyroid lobe. The Tg-E7 model was less heterogeneous, with a dominant goitrous pattern. The solid tumour already described in the RET/PTC3 models associated with cribriform patterns, suggested 'PTC spindle cell changes' as in humans PTC rather than the equivalent of the solid human PTC. Proliferation and apoptosis in the two thyroid models are related to the causal oncogene rather than reflect a general tumorigenic process. The thyroids of RET/PTC3 mice appeared as a partial and transient model of human PTCs, whereas the Tg-E7 mice do not belong to the usual PTC type., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2008

3. Human thyroid tumours, the puzzling lessons from E7 and RET/PTC3 transgenic mice.

Author

Jin, Ling, Burniat, Agnès, Dumont, Jacques Emile, Miot, Françoise, Corvilain, Bernard, Franc, B, Jin, Ling, Burniat, Agnès, Dumont, Jacques Emile, Miot, Françoise, Corvilain, Bernard, and Franc, B

Abstract

Human rearranged RET/PTC3 (papillary thyroid carcinoma) proto-oncogene and high-risk human papillomavirus (HPV) type 16 E7 oncogene induces in the mouse a neoplastic transformation of thyroid follicular cells. We present a detailed immuno-histological study (170 mouse thyroids: RET/PTC3, E7, wild type, 2- to 10-month-old) with cell cycle proliferation and signalling pathway indicators. The characteristics of both models are different. There is an 'oncogene dependent' cellular signature, maintained at all studied ages in the E7 model, less in the RET/PTC3 model. During tumour development a large heterogeneity occurred in the Tg-RET/PTC3 model within a same tumour or within a same thyroid lobe. The Tg-E7 model was less heterogeneous, with a dominant goitrous pattern. The solid tumour already described in the RET/PTC3 models associated with cribriform patterns, suggested 'PTC spindle cell changes' as in humans PTC rather than the equivalent of the solid human PTC. Proliferation and apoptosis in the two thyroid models are related to the causal oncogene rather than reflect a general tumorigenic process. The thyroids of RET/PTC3 mice appeared as a partial and transient model of human PTCs, whereas the Tg-E7 mice do not belong to the usual PTC type., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2008

4. Genome-wide gene expression profiling suggests distinct radiation susceptibilities in sporadic and post-Chernobyl papillary thyroid cancers.

Author

Detours, V, Detours, V, Delys, L, Libert, F, Weiss Solís, D, Bogdanova, T, Dumont, JE, Franc, B, Thomas, G, Maenhaut, C, Detours, V, Detours, V, Delys, L, Libert, F, Weiss Solís, D, Bogdanova, T, Dumont, JE, Franc, B, Thomas, G, and Maenhaut, C

Abstract

Papillary thyroid cancers (PTCs) incidence dramatically increased in the vicinity of Chernobyl. The cancer-initiating role of radiation elsewhere is debated. Therefore, we searched for a signature distinguishing radio-induced from sporadic cancers. Using microarrays, we compared the expression profiles of PTCs from the Chernobyl Tissue Bank (CTB, n=12) and from French patients with no history of exposure to ionising radiations (n=14). We also compared the transcriptional responses of human lymphocytes to the presumed aetiological agents initiating these tumours, gamma-radiation and H(2)O(2). On a global scale, the transcriptomes of CTB and French tumours are indistinguishable, and the transcriptional responses to gamma-radiation and H(2)O(2) are similar. On a finer scale, a 118 genes signature discriminated the gamma-radiation and H(2)O(2) responses. This signature could be used to classify the tumours as CTB or French with an error of 15-27%. Similar results were obtained with an independent signature of 13 genes involved in homologous recombination. Although sporadic and radio-induced PTCs represent the same disease, they are distinguishable with molecular signatures reflecting specific responses to gamma-radiation and H(2)O(2). These signatures in PTCs could reflect the susceptibility profiles of the patients, suggesting the feasibility of a radiation susceptibility test.

Published

2007

5. Gene expression and the biological phenotype of papillary thyroid carcinomas.

Author

Delys, Laurent, Detours, Vincent, Franc, B, Thomas, G, Bogdanova, T, Tronko, M, Libert, Frédérick, Dumont, Jacques Emile, Maenhaut, Carine, Delys, Laurent, Detours, Vincent, Franc, B, Thomas, G, Bogdanova, T, Tronko, M, Libert, Frédérick, Dumont, Jacques Emile, and Maenhaut, Carine

Abstract

The purpose of this paper is to correlate the molecular phenotype of papillary thyroid carcinoma (PTC) to their biological pathology. We hybridized 26 PTC on microarrays and showed that nearly 44% of the transcriptome was regulated in these tumors. We then combined our data set with two published PTC microarray studies to produce a platform- and study-independent list of PTC-associated genes. We further confirmed the mRNA regulation of 15 genes from this list by quantitative reverse transcription-PCR. Analysis of this list with statistical tools led to several conclusions: (1) there is a change in cell population with an increased expression of genes involved in the immune response, reflecting lymphocyte infiltration in the tumor compared to the normal tissue. (2) The c-jun N-terminal kinase pathway is activated by overexpression of its components. (3) The activation of ERKK1/2 by genetic alterations is supplemented by activation of the epidermal growth factor but not of the insulin-like growth factor signaling pathway. (4) There is a downregulation of immediate early genes. (5) We observed an overexpression of many proteases in accordance with tumor remodeling, and suggested a probable role of S100 proteins and annexin A2 in this process. (6) Numerous overexpressed genes favor the hypothesis of a collective migration mode of tumor cells., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2007

6. Genome-wide gene expression profiling suggests distinct radiation susceptibilities in sporadic and post-Chernobyl papillary thyroid cancers.

Author

Detours, Vincent, Delys, Laurent, Libert, Luc, Weiss Solís, D, Bogdanova, T, Dumont, Jacques Emile, Franc, B, Thomas, G, Maenhaut, Carine, Detours, Vincent, Delys, Laurent, Libert, Luc, Weiss Solís, D, Bogdanova, T, Dumont, Jacques Emile, Franc, B, Thomas, G, and Maenhaut, Carine

Abstract

Papillary thyroid cancers (PTCs) incidence dramatically increased in the vicinity of Chernobyl. The cancer-initiating role of radiation elsewhere is debated. Therefore, we searched for a signature distinguishing radio-induced from sporadic cancers. Using microarrays, we compared the expression profiles of PTCs from the Chernobyl Tissue Bank (CTB, n=12) and from French patients with no history of exposure to ionising radiations (n=14). We also compared the transcriptional responses of human lymphocytes to the presumed aetiological agents initiating these tumours, gamma-radiation and H(2)O(2). On a global scale, the transcriptomes of CTB and French tumours are indistinguishable, and the transcriptional responses to gamma-radiation and H(2)O(2) are similar. On a finer scale, a 118 genes signature discriminated the gamma-radiation and H(2)O(2) responses. This signature could be used to classify the tumours as CTB or French with an error of 15-27%. Similar results were obtained with an independent signature of 13 genes involved in homologous recombination. Although sporadic and radio-induced PTCs represent the same disease, they are distinguishable with molecular signatures reflecting specific responses to gamma-radiation and H(2)O(2). These signatures in PTCs could reflect the susceptibility profiles of the patients, suggesting the feasibility of a radiation susceptibility test., Comparative Study, Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2007

7. Genome-wide gene expression profiling suggests distinct radiation susceptibilities in sporadic and post-Chernobyl papillary thyroid cancers.

Author

Detours, V, Detours, V, Delys, L, Libert, F, Weiss Solís, D, Bogdanova, T, Dumont, JE, Franc, B, Thomas, G, Maenhaut, C, Detours, V, Detours, V, Delys, L, Libert, F, Weiss Solís, D, Bogdanova, T, Dumont, JE, Franc, B, Thomas, G, and Maenhaut, C

Abstract

Papillary thyroid cancers (PTCs) incidence dramatically increased in the vicinity of Chernobyl. The cancer-initiating role of radiation elsewhere is debated. Therefore, we searched for a signature distinguishing radio-induced from sporadic cancers. Using microarrays, we compared the expression profiles of PTCs from the Chernobyl Tissue Bank (CTB, n=12) and from French patients with no history of exposure to ionising radiations (n=14). We also compared the transcriptional responses of human lymphocytes to the presumed aetiological agents initiating these tumours, gamma-radiation and H(2)O(2). On a global scale, the transcriptomes of CTB and French tumours are indistinguishable, and the transcriptional responses to gamma-radiation and H(2)O(2) are similar. On a finer scale, a 118 genes signature discriminated the gamma-radiation and H(2)O(2) responses. This signature could be used to classify the tumours as CTB or French with an error of 15-27%. Similar results were obtained with an independent signature of 13 genes involved in homologous recombination. Although sporadic and radio-induced PTCs represent the same disease, they are distinguishable with molecular signatures reflecting specific responses to gamma-radiation and H(2)O(2). These signatures in PTCs could reflect the susceptibility profiles of the patients, suggesting the feasibility of a radiation susceptibility test.

Published

2007

8. Genome-wide gene expression profiling suggests distinct radiation susceptibilities in sporadic and post-Chernobyl papillary thyroid cancers.

Author

Detours, Vincent, Delys, Laurent, Libert, Luc, Weiss Solís, D, Bogdanova, T, Dumont, Jacques Emile, Franc, B, Thomas, G, Maenhaut, Carine, Detours, Vincent, Delys, Laurent, Libert, Luc, Weiss Solís, D, Bogdanova, T, Dumont, Jacques Emile, Franc, B, Thomas, G, and Maenhaut, Carine

Abstract

Papillary thyroid cancers (PTCs) incidence dramatically increased in the vicinity of Chernobyl. The cancer-initiating role of radiation elsewhere is debated. Therefore, we searched for a signature distinguishing radio-induced from sporadic cancers. Using microarrays, we compared the expression profiles of PTCs from the Chernobyl Tissue Bank (CTB, n=12) and from French patients with no history of exposure to ionising radiations (n=14). We also compared the transcriptional responses of human lymphocytes to the presumed aetiological agents initiating these tumours, gamma-radiation and H(2)O(2). On a global scale, the transcriptomes of CTB and French tumours are indistinguishable, and the transcriptional responses to gamma-radiation and H(2)O(2) are similar. On a finer scale, a 118 genes signature discriminated the gamma-radiation and H(2)O(2) responses. This signature could be used to classify the tumours as CTB or French with an error of 15-27%. Similar results were obtained with an independent signature of 13 genes involved in homologous recombination. Although sporadic and radio-induced PTCs represent the same disease, they are distinguishable with molecular signatures reflecting specific responses to gamma-radiation and H(2)O(2). These signatures in PTCs could reflect the susceptibility profiles of the patients, suggesting the feasibility of a radiation susceptibility test., Comparative Study, Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2007

9. Gene expression and the biological phenotype of papillary thyroid carcinomas.

Author

Delys, Laurent, Detours, Vincent, Franc, B, Thomas, G, Bogdanova, T, Tronko, M, Libert, Frédérick, Dumont, Jacques Emile, Maenhaut, Carine, Delys, Laurent, Detours, Vincent, Franc, B, Thomas, G, Bogdanova, T, Tronko, M, Libert, Frédérick, Dumont, Jacques Emile, and Maenhaut, Carine

Abstract

The purpose of this paper is to correlate the molecular phenotype of papillary thyroid carcinoma (PTC) to their biological pathology. We hybridized 26 PTC on microarrays and showed that nearly 44% of the transcriptome was regulated in these tumors. We then combined our data set with two published PTC microarray studies to produce a platform- and study-independent list of PTC-associated genes. We further confirmed the mRNA regulation of 15 genes from this list by quantitative reverse transcription-PCR. Analysis of this list with statistical tools led to several conclusions: (1) there is a change in cell population with an increased expression of genes involved in the immune response, reflecting lymphocyte infiltration in the tumor compared to the normal tissue. (2) The c-jun N-terminal kinase pathway is activated by overexpression of its components. (3) The activation of ERKK1/2 by genetic alterations is supplemented by activation of the epidermal growth factor but not of the insulin-like growth factor signaling pathway. (4) There is a downregulation of immediate early genes. (5) We observed an overexpression of many proteases in accordance with tumor remodeling, and suggested a probable role of S100 proteins and annexin A2 in this process. (6) Numerous overexpressed genes favor the hypothesis of a collective migration mode of tumor cells., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2007

10. Absence of a specific radiation signature in post-Chernobyl thyroid cancers.

Author

Detours, Vincent, Wattel, Sandrine, Venet, David, Hutsebaut, N, Bogdanova, T, Tronko, M, Dumont, Jacques Emile, Franc, B, Thomas, G, Maenhaut, Carine, Detours, Vincent, Wattel, Sandrine, Venet, David, Hutsebaut, N, Bogdanova, T, Tronko, M, Dumont, Jacques Emile, Franc, B, Thomas, G, and Maenhaut, Carine

Abstract

Thyroid cancers have been the main medical consequence of the Chernobyl accident. On the basis of their pathological features and of the fact that a large proportion of them demonstrate RET-PTC translocations, these cancers are considered as similar to classical sporadic papillary carcinomas, although molecular alterations differ between both tumours. We analysed gene expression in post-Chernobyl cancers, sporadic papillary carcinomas and compared to autonomous adenomas used as controls. Unsupervised clustering of these data did not distinguish between the cancers, but separates both cancers from adenomas. No gene signature separating sporadic from post-Chernobyl PTC (chPTC) could be found using supervised and unsupervised classification methods although such a signature is demonstrated for cancers and adenomas. Furthermore, we demonstrate that pooled RNA from sporadic and chPTC are as strongly correlated as two independent sporadic PTC pools, one from Europe, one from the US involving patients not exposed to Chernobyl radiations. This result relies on cDNA and Affymetrix microarrays. Thus, platform-specific artifacts are controlled for. Our findings suggest the absence of a radiation fingerprint in the chPTC and support the concept that post-Chernobyl cancer data, for which the cancer-causing event and its date are known, are a unique source of information to study naturally occurring papillary carcinomas., Comparative Study, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2005

11. Absence of a specific radiation signature in post-Chernobyl thyroid cancers.

Author

Detours, Vincent, Wattel, Sandrine, Venet, David, Hutsebaut, N, Bogdanova, T, Tronko, M, Dumont, Jacques Emile, Franc, B, Thomas, G, Maenhaut, Carine, Detours, Vincent, Wattel, Sandrine, Venet, David, Hutsebaut, N, Bogdanova, T, Tronko, M, Dumont, Jacques Emile, Franc, B, Thomas, G, and Maenhaut, Carine

Abstract

Thyroid cancers have been the main medical consequence of the Chernobyl accident. On the basis of their pathological features and of the fact that a large proportion of them demonstrate RET-PTC translocations, these cancers are considered as similar to classical sporadic papillary carcinomas, although molecular alterations differ between both tumours. We analysed gene expression in post-Chernobyl cancers, sporadic papillary carcinomas and compared to autonomous adenomas used as controls. Unsupervised clustering of these data did not distinguish between the cancers, but separates both cancers from adenomas. No gene signature separating sporadic from post-Chernobyl PTC (chPTC) could be found using supervised and unsupervised classification methods although such a signature is demonstrated for cancers and adenomas. Furthermore, we demonstrate that pooled RNA from sporadic and chPTC are as strongly correlated as two independent sporadic PTC pools, one from Europe, one from the US involving patients not exposed to Chernobyl radiations. This result relies on cDNA and Affymetrix microarrays. Thus, platform-specific artifacts are controlled for. Our findings suggest the absence of a radiation fingerprint in the chPTC and support the concept that post-Chernobyl cancer data, for which the cancer-causing event and its date are known, are a unique source of information to study naturally occurring papillary carcinomas., Comparative Study, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2005

12. Correlation between the loss of thyroglobulin iodination and the expression of thyroid-specific proteins involved in iodine metabolism in thyroid carcinomas

Author

UCL - MD/MNOP - Département de morphologie normale et pathologique, UCL - MD/MINT - Département de médecine interne, UCL - (SLuc) Service d'endocrinologie et de nutrition, Gérard, Anne-Catherine, Daumerie, Chantal, Mestdagh, C., Gohy, Sophie, De Burbure, Claire, Costagliola, Sabine, Miot, Françoise, Nollevaux, Marie-Cécile, Denef, Jean-François, Rahier, Jacques, Franc, B., De Vijlder, Jan J. M., Colin, Idesbald, Many, Marie-Christine, UCL - MD/MNOP - Département de morphologie normale et pathologique, UCL - MD/MINT - Département de médecine interne, UCL - (SLuc) Service d'endocrinologie et de nutrition, Gérard, Anne-Catherine, Daumerie, Chantal, Mestdagh, C., Gohy, Sophie, De Burbure, Claire, Costagliola, Sabine, Miot, Françoise, Nollevaux, Marie-Cécile, Denef, Jean-François, Rahier, Jacques, Franc, B., De Vijlder, Jan J. M., Colin, Idesbald, and Many, Marie-Christine

Abstract

Progress in biotechnology has provided useful tools for tracing proteins involved in thyroid hormone synthesis in vivo. Mono- or polyclonal antibodies are now available to detect on histological sections the Na(+)/I(-) symporter (NIS) at the basolateral pole of the cell, the putative iodide channel (pendrin) at the apical plasma membrane, thyroperoxidase (TPO), and members of the NADPH-oxidase family, thyroid oxidase 1 and 2 (ThOXs), part of the H(2)O(2)-generating system. The aim of this study was to correlate thyroglobulin (Tg) iodination with the presence of these proteins. Tg, T(4)-containing Tg, NIS, pendrin, TPO, ThOXs, and TSH receptor (TSHr) were detected by immunohistochemistry on tissue sections of normal thyroids and various benign and malignant thyroid disorders. Tg was present in all cases. T(4)-containing Tg was found in the adenomas, except in Hurthle cell adenomas. It was never detected in carcinomas. NIS was reduced in all types of carcinomas, whereas it was detected in noncancerous tissues. Pendrin was not expressed in carcinomas, except in follicular carcinomas, where weak staining persisted. TPO expression was present in insular, follicular carcinomas and in follicular variants of papillary carcinomas, but in a reduced percentage of cells. It was below the level of detection in papillary carcinomas. The H(2)O(2)-generating system, ThOXs, was found in all carcinomas and was even increased in papillary carcinomas. Its staining was apical in normal thyroids, whereas it was cytoplasmic in carcinomas. The TSHr was expressed in all cases, but the intensity of the staining was decreased in insular carcinomas. In conclusion, our work shows that all types of carcinomas lose the capacity to synthesize T(4)-rich, iodinated Tg. In follicular carcinomas, this might be due to a defect in iodide transport at the basolateral pole of the cell. In papillary carcinomas, this defect seems to be coupled to an altered apical transport of iodide and probably TPO activi

Published

2003

13. Correlation between the loss of thyroglobulin iodination and the expression of thyroid-specific proteins involved in iodine metabolism in thyroid carcinomas.

Author

Gérard, A-C, Daumerie, Chantal, Mestdagh, C, Gohy, S, de Burbure, Claire, Costagliola, Sabine, Miot, Françoise, Nollevaux, M. C., Denef, Jean François, Rahier, J, Franc, B, De Vijlder, J J M, Colin, Ides M, Many, Marie-Christine, Gérard, A-C, Daumerie, Chantal, Mestdagh, C, Gohy, S, de Burbure, Claire, Costagliola, Sabine, Miot, Françoise, Nollevaux, M. C., Denef, Jean François, Rahier, J, Franc, B, De Vijlder, J J M, Colin, Ides M, and Many, Marie-Christine

Abstract

Progress in biotechnology has provided useful tools for tracing proteins involved in thyroid hormone synthesis in vivo. Mono- or polyclonal antibodies are now available to detect on histological sections the Na(+)/I(-) symporter (NIS) at the basolateral pole of the cell, the putative iodide channel (pendrin) at the apical plasma membrane, thyroperoxidase (TPO), and members of the NADPH-oxidase family, thyroid oxidase 1 and 2 (ThOXs), part of the H(2)O(2)-generating system. The aim of this study was to correlate thyroglobulin (Tg) iodination with the presence of these proteins. Tg, T(4)-containing Tg, NIS, pendrin, TPO, ThOXs, and TSH receptor (TSHr) were detected by immunohistochemistry on tissue sections of normal thyroids and various benign and malignant thyroid disorders. Tg was present in all cases. T(4)-containing Tg was found in the adenomas, except in Hurthle cell adenomas. It was never detected in carcinomas. NIS was reduced in all types of carcinomas, whereas it was detected in noncancerous tissues. Pendrin was not expressed in carcinomas, except in follicular carcinomas, where weak staining persisted. TPO expression was present in insular, follicular carcinomas and in follicular variants of papillary carcinomas, but in a reduced percentage of cells. It was below the level of detection in papillary carcinomas. The H(2)O(2)-generating system, ThOXs, was found in all carcinomas and was even increased in papillary carcinomas. Its staining was apical in normal thyroids, whereas it was cytoplasmic in carcinomas. The TSHr was expressed in all cases, but the intensity of the staining was decreased in insular carcinomas. In conclusion, our work shows that all types of carcinomas lose the capacity to synthesize T(4)-rich, iodinated Tg. In follicular carcinomas, this might be due to a defect in iodide transport at the basolateral pole of the cell. In papillary carcinomas, this defect seems to be coupled to an altered apical transport of iodide and probably TPO activi, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2003

14. Correlation between the loss of thyroglobulin iodination and the expression of thyroid-specific proteins involved in iodine metabolism in thyroid carcinomas.

Author

Gérard, A-C, Daumerie, Chantal, Mestdagh, C, Gohy, S, de Burbure, Claire, Costagliola, Sabine, Miot, Françoise, Nollevaux, M. C., Denef, Jean François, Rahier, J, Franc, B, De Vijlder, J J M, Colin, Ides M, Many, Marie-Christine, Gérard, A-C, Daumerie, Chantal, Mestdagh, C, Gohy, S, de Burbure, Claire, Costagliola, Sabine, Miot, Françoise, Nollevaux, M. C., Denef, Jean François, Rahier, J, Franc, B, De Vijlder, J J M, Colin, Ides M, and Many, Marie-Christine

Abstract

Progress in biotechnology has provided useful tools for tracing proteins involved in thyroid hormone synthesis in vivo. Mono- or polyclonal antibodies are now available to detect on histological sections the Na(+)/I(-) symporter (NIS) at the basolateral pole of the cell, the putative iodide channel (pendrin) at the apical plasma membrane, thyroperoxidase (TPO), and members of the NADPH-oxidase family, thyroid oxidase 1 and 2 (ThOXs), part of the H(2)O(2)-generating system. The aim of this study was to correlate thyroglobulin (Tg) iodination with the presence of these proteins. Tg, T(4)-containing Tg, NIS, pendrin, TPO, ThOXs, and TSH receptor (TSHr) were detected by immunohistochemistry on tissue sections of normal thyroids and various benign and malignant thyroid disorders. Tg was present in all cases. T(4)-containing Tg was found in the adenomas, except in Hurthle cell adenomas. It was never detected in carcinomas. NIS was reduced in all types of carcinomas, whereas it was detected in noncancerous tissues. Pendrin was not expressed in carcinomas, except in follicular carcinomas, where weak staining persisted. TPO expression was present in insular, follicular carcinomas and in follicular variants of papillary carcinomas, but in a reduced percentage of cells. It was below the level of detection in papillary carcinomas. The H(2)O(2)-generating system, ThOXs, was found in all carcinomas and was even increased in papillary carcinomas. Its staining was apical in normal thyroids, whereas it was cytoplasmic in carcinomas. The TSHr was expressed in all cases, but the intensity of the staining was decreased in insular carcinomas. In conclusion, our work shows that all types of carcinomas lose the capacity to synthesize T(4)-rich, iodinated Tg. In follicular carcinomas, this might be due to a defect in iodide transport at the basolateral pole of the cell. In papillary carcinomas, this defect seems to be coupled to an altered apical transport of iodide and probably TPO activi, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2003

15. Characterization of autonomous thyroid adenoma: metabolism, gene expression, and pathology.

Author

Deleu, Sandrine, Allory, Y, Radulescu, A, Pirson, Isabelle, Carrasco, N, Corvilain, Bernard, Salmon, Isabelle, Franc, B, Dumont, Jacques Emile, Van Sande, Jacqueline, Maenhaut, Carine, Deleu, Sandrine, Allory, Y, Radulescu, A, Pirson, Isabelle, Carrasco, N, Corvilain, Bernard, Salmon, Isabelle, Franc, B, Dumont, Jacques Emile, Van Sande, Jacqueline, and Maenhaut, Carine

Abstract

Fifty-one in vivo characterized autonomous single adenomas have been studied for functional parameters in vitro, for gene and protein expression and for pathology, and have been systematically compared to the corresponding extratumoral quiescent tissue. The adenomas were characterized by a high level of iodide trapping that corresponds to a high level of Na+ /iodide symporter gene expression, a high thyroperoxidase mRNA and protein content, and a low H2O2 generation. This explains the iodide metabolism characteristics demonstrated before, ie, the main cause of the "hot" character of the adenomas is their increased iodide transport. The adenomas spontaneously secreted higher amounts of thyroid hormone than the quiescent tissue and in agreement with previous in vivo data, this secretion could be further enhanced by thyrotropin (TSH). Inositol uptake was also increased but there was no spontaneous increase of the generation of inositol phosphates and this metabolism could be further activated by TSH. These positive responses to TSH are in agreement with the properties of TSH-stimulated thyroid cells in vitro and in vivo. They are compatible with the characteristics of mutated TSH receptors whose constitutive activation accounts for the majority of autonomous thyroid adenomas in Europe. The number of cycling cells, as evaluated by MIB-1 immunolabeling was low but increased in comparison with the corresponding quiescent tissue or normal tissue. The cycling cells are observed mainly at the periphery; there was very little apoptosis. Both findings account for the slow growth of these established adenomas. On the other hand, by thyroperoxidase immunohistochemistry, the whole lesion appeared hyperfunctional, which demonstrates a dissociation of mitogenic and functional stimulations. Thyroglobulin, TSH receptor, and E-cadherin mRNA accumulations were not modified in a consistent way, which confirms the near-constitutive expression of the corresponding genes in normal differen, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2000

16. Characterization of autonomous thyroid adenoma: metabolism, gene expression, and pathology.

Author

Deleu, Sandrine, Allory, Y, Radulescu, A, Pirson, Isabelle, Carrasco, N, Corvilain, Bernard, Salmon, Isabelle, Franc, B, Dumont, Jacques Emile, Van Sande, Jacqueline, Maenhaut, Carine, Deleu, Sandrine, Allory, Y, Radulescu, A, Pirson, Isabelle, Carrasco, N, Corvilain, Bernard, Salmon, Isabelle, Franc, B, Dumont, Jacques Emile, Van Sande, Jacqueline, and Maenhaut, Carine

Abstract

Fifty-one in vivo characterized autonomous single adenomas have been studied for functional parameters in vitro, for gene and protein expression and for pathology, and have been systematically compared to the corresponding extratumoral quiescent tissue. The adenomas were characterized by a high level of iodide trapping that corresponds to a high level of Na+ /iodide symporter gene expression, a high thyroperoxidase mRNA and protein content, and a low H2O2 generation. This explains the iodide metabolism characteristics demonstrated before, ie, the main cause of the "hot" character of the adenomas is their increased iodide transport. The adenomas spontaneously secreted higher amounts of thyroid hormone than the quiescent tissue and in agreement with previous in vivo data, this secretion could be further enhanced by thyrotropin (TSH). Inositol uptake was also increased but there was no spontaneous increase of the generation of inositol phosphates and this metabolism could be further activated by TSH. These positive responses to TSH are in agreement with the properties of TSH-stimulated thyroid cells in vitro and in vivo. They are compatible with the characteristics of mutated TSH receptors whose constitutive activation accounts for the majority of autonomous thyroid adenomas in Europe. The number of cycling cells, as evaluated by MIB-1 immunolabeling was low but increased in comparison with the corresponding quiescent tissue or normal tissue. The cycling cells are observed mainly at the periphery; there was very little apoptosis. Both findings account for the slow growth of these established adenomas. On the other hand, by thyroperoxidase immunohistochemistry, the whole lesion appeared hyperfunctional, which demonstrates a dissociation of mitogenic and functional stimulations. Thyroglobulin, TSH receptor, and E-cadherin mRNA accumulations were not modified in a consistent way, which confirms the near-constitutive expression of the corresponding genes in normal differen, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2000

17. Graves-Basedow disease goiter: a model of Bax-Bcl2 regulated apoptosis.

Author

Labat-Moleur, F, Chabre, O, Guillermet, C, Chaffanjon, P, Blumet-Rondeu, F, Bauchet, A, Franc, B, Brambilla, E, Bachelot, I, Dumont, Jacques Emile, Negoescu, A, Labat-Moleur, F, Chabre, O, Guillermet, C, Chaffanjon, P, Blumet-Rondeu, F, Bauchet, A, Franc, B, Brambilla, E, Bachelot, I, Dumont, Jacques Emile, and Negoescu, A

Abstract

This study demonstrates the involvement of a Bax-Bcl2-dependent apoptotic process in Graves-Basedow thyroid disease, a pathological condition known for its spontaneously oscillating evolution. A continuous series of 86 cases of surgically treated Graves' thyroid was evaluated for apoptotic cell content identified by histological criteria and confirmed by terminal desoxynucleotidyl transferase-mediated desoxyuridine triphosphate nick end-labeling (TUNEL). A significant correlation was found between tissue features of Graves' disease (epithelial hyperplasia, cellular hypertrophy, colloid content) and the amount of apoptotic cells. No correlation was found with lymphocytic infiltrates. Significantly, 11 cases (about 12% of the series) with high-level apoptosis displayed the typical features of active Graves' disease over all tissue sections. In contrast, cases with no detectable apoptosis exhibited regressive tissue features of Graves' disease. An intermediate group of cases was characterized by tissue heterogeneity with hyperactive foci, rich in apoptosis, alternating with regressive areas lacking apoptosis. In this group the participation of apoptosis to the remodeling of Graves' thyroid parenchyma, in a tight balance with cell proliferation, was best illustrated. Moreover, the thyroid follicle by accumulating apoptotic cells and bodies, allowed a tentative chronological ordering of apoptosis steps in correlation with Bax-Bcl2 tissue distribution and cellular pattern. Our observations suggest that the initiation of apoptosis corresponds to a loss of cellular cohesion, a drop in Bcl2 expression, and a delocalization of Bax from a putative Golgi storage location to a mitochondrial distribution., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1999

18. Graves-Basedow disease goiter: a model of Bax-Bcl2 regulated apoptosis.

Author

Labat-Moleur, F, Chabre, O, Guillermet, C, Chaffanjon, P, Blumet-Rondeu, F, Bauchet, A, Franc, B, Brambilla, E, Bachelot, I, Dumont, Jacques Emile, Negoescu, A, Labat-Moleur, F, Chabre, O, Guillermet, C, Chaffanjon, P, Blumet-Rondeu, F, Bauchet, A, Franc, B, Brambilla, E, Bachelot, I, Dumont, Jacques Emile, and Negoescu, A

Abstract

This study demonstrates the involvement of a Bax-Bcl2-dependent apoptotic process in Graves-Basedow thyroid disease, a pathological condition known for its spontaneously oscillating evolution. A continuous series of 86 cases of surgically treated Graves' thyroid was evaluated for apoptotic cell content identified by histological criteria and confirmed by terminal desoxynucleotidyl transferase-mediated desoxyuridine triphosphate nick end-labeling (TUNEL). A significant correlation was found between tissue features of Graves' disease (epithelial hyperplasia, cellular hypertrophy, colloid content) and the amount of apoptotic cells. No correlation was found with lymphocytic infiltrates. Significantly, 11 cases (about 12% of the series) with high-level apoptosis displayed the typical features of active Graves' disease over all tissue sections. In contrast, cases with no detectable apoptosis exhibited regressive tissue features of Graves' disease. An intermediate group of cases was characterized by tissue heterogeneity with hyperactive foci, rich in apoptosis, alternating with regressive areas lacking apoptosis. In this group the participation of apoptosis to the remodeling of Graves' thyroid parenchyma, in a tight balance with cell proliferation, was best illustrated. Moreover, the thyroid follicle by accumulating apoptotic cells and bodies, allowed a tentative chronological ordering of apoptosis steps in correlation with Bax-Bcl2 tissue distribution and cellular pattern. Our observations suggest that the initiation of apoptosis corresponds to a loss of cellular cohesion, a drop in Bcl2 expression, and a delocalization of Bax from a putative Golgi storage location to a mitochondrial distribution., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1999

19. Comparison of morphonuclear features in normal, benign and neoplastic thyroid tissue by digital cell image analysis.

Author

Salmon, Isabelle, Kiss, Robert, Franc, B, Gasperin, Plínio, Heimann, R, Pasteels, Jean Lambert, Verhest, Alain, Salmon, Isabelle, Kiss, Robert, Franc, B, Gasperin, Plínio, Heimann, R, Pasteels, Jean Lambert, and Verhest, Alain

Abstract

We analyzed the morphonuclear features of thyroid cell nuclei from 10 normal tissues (10 multinodular goiters), 10 benign tissues (10 adenomas) and 10 neoplastic tissues (10 carcinomas--2 follicular, 2 medullary and 6 papillary). These morphonuclear features quantitatively described the nuclear size, DNA content and chromatin texture of 200-400 Feulgen-stained cell nuclei that were digitized by means of a cell image processor. Nuclear DNA estimations revealed that the benign thyroid tumors showed an aneuploidy level that was not different from that of the neoplastic tissues. Morphometric measurements showed a significant and positive correlation between an increase in nuclear area and the development of thyroid pathology--i.e. from normal to a neoplastic stage. We also observed a significant decrease in chromatin condensation and heterogeneity from normal to neoplastic thyroid tissue. In the specific case of thyroid tumors, such criteria were not found sufficient per se for a diagnosis of malignancy. More detailed data banks will be necessary for this purpose., Comparative Study, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1992

20. Comparison of morphonuclear features in normal, benign and neoplastic thyroid tissue by digital cell image analysis.

Author

Salmon, Isabelle, Kiss, Robert, Franc, B, Gasperin, Plínio, Heimann, R, Pasteels, Jean Lambert, Verhest, Alain, Salmon, Isabelle, Kiss, Robert, Franc, B, Gasperin, Plínio, Heimann, R, Pasteels, Jean Lambert, and Verhest, Alain

Abstract

We analyzed the morphonuclear features of thyroid cell nuclei from 10 normal tissues (10 multinodular goiters), 10 benign tissues (10 adenomas) and 10 neoplastic tissues (10 carcinomas--2 follicular, 2 medullary and 6 papillary). These morphonuclear features quantitatively described the nuclear size, DNA content and chromatin texture of 200-400 Feulgen-stained cell nuclei that were digitized by means of a cell image processor. Nuclear DNA estimations revealed that the benign thyroid tumors showed an aneuploidy level that was not different from that of the neoplastic tissues. Morphometric measurements showed a significant and positive correlation between an increase in nuclear area and the development of thyroid pathology--i.e. from normal to a neoplastic stage. We also observed a significant decrease in chromatin condensation and heterogeneity from normal to neoplastic thyroid tissue. In the specific case of thyroid tumors, such criteria were not found sufficient per se for a diagnosis of malignancy. More detailed data banks will be necessary for this purpose., Comparative Study, Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

1992

21. Davenport, past and present; including the early history, and personal and anecdotal reminiscences of Davenport; together with biographies, likenesses of its prominent men; compendious articles upon the physical, industrial, social and political characteristics of the city. By Franc B. Wilkie.

Author

Wilkie, Franc B., Wilkie, Franc B. (Franc Bangs), 1832-1892., Wilkie, Franc B., and Wilkie, Franc B. (Franc Bangs), 1832-1892.

Abstract

We have determined this item to be in the public domain according to US copyright law through information in the bibliographic record and/or US copyright renewal records. The digital version is available for all educational uses worldwide. Please contact HathiTrust staff at hathitrust-help@umich.edu with any questions about this item., Davenport (Iowa)--History., Davenport (Iowa)., (OCoLC)691999., 3649660., Sdr-ia-srlf3649660., F629.D2 W6., Http://hdl.handle.net/2027/uc2.ark:/13960/t9765kh7j.

22. Davenport, past and present: including the early history, and personal and anecdotal reminiscences of Davenport ; together with biographies, likenesses of its prominent men ; compendious articles upon physical, industrial, social and political characteristics of the city ; statistics of every department of note or interest, & c. / by Franc B.Wilkie.

Author

Wilkie, Franc B. (Franc Bangs), 1832-1892., Wilkie, Franc B. (Franc Bangs), 1832-1892., Wilkie, Franc B. (Franc Bangs), 1832-1892., and Wilkie, Franc B. (Franc Bangs), 1832-1892.

Abstract

333, [1] p. : ill. ; 22 cm., Electronic text and image data. Ann Arbor, Mich. : University of Michigan, Digital Library Initiatives, 1996. Includes both TIFF files and keyword searchable text. [Making of America] This volume is made possible by a grant from the Andrew W. Mellon Foundation., Making of America (MOA), (dlps) AFK4431.0001.001, (lccallno) See URL for access, http://quod.lib.umich.edu/t/text/accesspolicy.html

23. Davenport, past and present: including the early history, and personal and anecdotal reminiscences of Davenport ; together with biographies, likenesses of its prominent men ; compendious articles upon physical, industrial, social and political characteristics of the city ; statistics of every department of note or interest, & c. / by Franc B.Wilkie.

Author

Wilkie, Franc B. (Franc Bangs), 1832-1892., Wilkie, Franc B. (Franc Bangs), 1832-1892., Wilkie, Franc B. (Franc Bangs), 1832-1892., and Wilkie, Franc B. (Franc Bangs), 1832-1892.

Abstract

333, [1] p. : ill. ; 22 cm., Electronic text and image data. Ann Arbor, Mich. : University of Michigan, Digital Library Initiatives, 1996. Includes both TIFF files and keyword searchable text. [Making of America] This volume is made possible by a grant from the Andrew W. Mellon Foundation., Making of America (MOA), (dlps) AFK4431.0001.001, (lccallno) See URL for access, http://quod.lib.umich.edu/t/text/accesspolicy.html