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8. Cover image

Author

Finot, F., primary, Kaddour, A., additional, Morat, L., additional, Mouche, I., additional, Zaguia, N., additional, Cuceu, C., additional, Souverville, D., additional, Négrault, S., additional, Cariou, O., additional, Essahli, A., additional, Prigent, N., additional, Saul, J., additional, Paillard, F., additional, Heidingsfelder, L., additional, Lafouge, P., additional, Al Jawhari, M., additional, Hempel, W. M., additional, El May, M., additional, Colicchio, B., additional, Dieterlen, A., additional, Jeandidier, E., additional, Sabatier, L., additional, Clements, J., additional, and M'Kacher, R., additional

Published
2017
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9. Genotoxic risk of ethyl-paraben could be related to telomere shortening

Author

Finot, F., primary, Kaddour, A., additional, Morat, L., additional, Mouche, I., additional, Zaguia, N., additional, Cuceu, C., additional, Souverville, D., additional, Négrault, S., additional, Cariou, O., additional, Essahli, A., additional, Prigent, N., additional, Saul, J., additional, Paillard, F., additional, Heidingsfelder, L., additional, Lafouge, P., additional, Al Jawhari, M., additional, Hempel, W. M., additional, El May, M., additional, Colicchio, B., additional, Dieterlen, A., additional, Jeandidier, E., additional, Sabatier, L., additional, Clements, J., additional, and M'Kacher, R., additional

Published
2016
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10. O42. Realizing the European Network of Biological Dosimetry ‘RENEB’: Results of 2 intercomparison exercises for the micronucleus assay

Author

Depuydt, J., primary, Baeyens, A., additional, Barnard, S., additional, Beinke, C., additional, Benedek, A., additional, Beukes, P., additional, Buraczewska, I., additional, Darroudi, F., additional, De Sanctis, S., additional, Dominguez, I., additional, Monteiro Gil, O., additional, Hadjidekova, V., additional, Kis, E., additional, Kulka, U., additional, Lista, F., additional, Lumniczky, K., additional, M’kacher, R., additional, Moquet, J., additional, Obreja, D., additional, Oestreicher, U., additional, Pajic, J., additional, Pastor, N., additional, Popova, L., additional, Regalbuto, E., additional, Ricoul, M., additional, Sabatier, L., additional, Slabbert, J.P., additional, Sommer, S., additional, Testa, A., additional, Thierens, H., additional, Wojcik, A., additional, and Vral, A., additional

Published
2016
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11. Realising the European network of biodosimetry : RENEB-status quo

Author

Kulka, U., Ainsbury, L., Atkinson, M., Barnard, S., Smith, R., Barquinero, J. F., Barrios, L., Bassinet, C., Beinke, C., Cucu, A., Darroudi, F., Fattibene, P., Bortolin, E., Della Monaca, S., Gil, O., Gregoire, E., Hadjidekova, V., Haghdoost, Siamak, Hatzi, V., Hempel, W., Herranz, R., Jaworska, A., Lindholm, C., Lumniczky, K., M'kacher, R., Moertl, S., Montoro, A., Moquet, J., Moreno, M., Noditi, M., Ogbazghi, A., Oestreicher, U., Palitti, F., Pantelias, G., Popescu, I., Prieto, M. J., Roch-Lefevre, S., Roessler, U., Romm, H., Rothkamm, K., Sabatier, L., Sebastia, N., Sommer, S., Terzoudi, G., Testa, A., Thierens, H., Trompier, F., Turai, I., Vandevoorde, C., Vaz, P., Voisin, P., Vral, A., Ugletveit, F., Wieser, A., Woda, C., Wojcik, Andrzej, Kulka, U., Ainsbury, L., Atkinson, M., Barnard, S., Smith, R., Barquinero, J. F., Barrios, L., Bassinet, C., Beinke, C., Cucu, A., Darroudi, F., Fattibene, P., Bortolin, E., Della Monaca, S., Gil, O., Gregoire, E., Hadjidekova, V., Haghdoost, Siamak, Hatzi, V., Hempel, W., Herranz, R., Jaworska, A., Lindholm, C., Lumniczky, K., M'kacher, R., Moertl, S., Montoro, A., Moquet, J., Moreno, M., Noditi, M., Ogbazghi, A., Oestreicher, U., Palitti, F., Pantelias, G., Popescu, I., Prieto, M. J., Roch-Lefevre, S., Roessler, U., Romm, H., Rothkamm, K., Sabatier, L., Sebastia, N., Sommer, S., Terzoudi, G., Testa, A., Thierens, H., Trompier, F., Turai, I., Vandevoorde, C., Vaz, P., Voisin, P., Vral, A., Ugletveit, F., Wieser, A., Woda, C., and Wojcik, Andrzej

Abstract

Creating a sustainable network in biological and retrospective dosimetry that involves a large number of experienced laboratories throughout the European Union (EU) will significantly improve the accident and emergency response capabilities in case of a large-scale radiological emergency. A well-organised cooperative action involving EU laboratories will offer the best chance for fast and trustworthy dose assessments that are urgently needed in an emergency situation. To this end, the EC supports the establishment of a European network in biological dosimetry (RENEB). The RENEB project started in January 2012 involving cooperation of 23 organisations from 16 European countries. The purpose of RENEB is to increase the biodosimetry capacities in case of large-scale radiological emergency scenarios. The progress of the project since its inception is presented, comprising the consolidation process of the network with its operational platform, intercomparison exercises, training activities, proceedings in quality assurance and horizon scanning for new methods and partners. Additionally, the benefit of the network for the radiation research community as a whole is addressed.

Published
2015
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12. Telomere shortening: a new prognostic factor for cardiovascular disease post-radiation exposure

Author

M'kacher, R., primary, Girinsky, T., additional, Colicchio, B., additional, Ricoul, M., additional, Dieterlen, A., additional, Jeandidier, E., additional, Heidingsfelder, L., additional, Cuceu, C., additional, Shim, G., additional, Frenzel, M., additional, Lenain, A., additional, Morat, L., additional, Bourhis, J., additional, Hempel, W. M., additional, Koscielny, S., additional, Paul, J. F., additional, Carde, P., additional, and Sabatier, L., additional

Published
2014
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13. Realising the European network of biodosimetry: RENEB--status quo

Author

Kulka, U., primary, Ainsbury, L., additional, Atkinson, M., additional, Barnard, S., additional, Smith, R., additional, Barquinero, J. F., additional, Barrios, L., additional, Bassinet, C., additional, Beinke, C., additional, Cucu, A., additional, Darroudi, F., additional, Fattibene, P., additional, Bortolin, E., additional, Monaca, S. D., additional, Gil, O., additional, Gregoire, E., additional, Hadjidekova, V., additional, Haghdoost, S., additional, Hatzi, V., additional, Hempel, W., additional, Herranz, R., additional, Jaworska, A., additional, Lindholm, C., additional, Lumniczky, K., additional, M'kacher, R., additional, Mortl, S., additional, Montoro, A., additional, Moquet, J., additional, Moreno, M., additional, Noditi, M., additional, Ogbazghi, A., additional, Oestreicher, U., additional, Palitti, F., additional, Pantelias, G., additional, Popescu, I., additional, Prieto, M. J., additional, Roch-Lefevre, S., additional, Roessler, U., additional, Romm, H., additional, Rothkamm, K., additional, Sabatier, L., additional, Sebastia, N., additional, Sommer, S., additional, Terzoudi, G., additional, Testa, A., additional, Thierens, H., additional, Trompier, F., additional, Turai, I., additional, Vandevoorde, C., additional, Vaz, P., additional, Voisin, P., additional, Vral, A., additional, Ugletveit, F., additional, Wieser, A., additional, Woda, C., additional, and Wojcik, A., additional

Published
2014
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15. TELOMERE SHORTENING: A NEW PROGNOSTIC FACTOR FOR CARDIOVASCULAR DISEASE POST-RADIATION EXPOSURE.

Author

M'kacher, R., Girinsky, T., Colicchio, B., Ricoul, M., Dieterlen, A., Jeandidier, E., Heidingsfelder, L., Cuceu, C., Shim, G., Frenzel, M., Lenain, A., Morat, L., Bourhis, J., Hempel, W. M., Koscielny, S., Paul, J. F., Carde, P., and Sabatier, L.

Subjects
TELOMERES, CARDIOVASCULAR diseases, RADIATION exposure, CARDIOVASCULAR disease related mortality, RADIOTHERAPY complications, CORONARY heart disease risk factors, PROGNOSIS
Abstract

Telomere length has been proposed as a marker of mitotic cell age and as a general index of human organism aging. Telomere shortening in peripheral blood lymphocytes has been linked to cardiovascular-related morbidity and mortality. The authors investigated the potential correlation of conventional risk factors, radiation dose and telomere shortening with the development of coronary artery disease (CAD) following radiation therapy in a large cohort of Hodgkin lymphoma (HL) patients. Multivariate analysis demonstrated that hypertension and telomere length were the only independent risk factors. This is the first study in a large cohort of patients that demonstrates significant telomere shortening in patients treated by radiation therapy who developed cardiovascular disease. Telomere length appears to be an independent prognostic factor that could help determine patients at high risk of developing CAD after exposure in order to implement early detection and prevention. [ABSTRACT FROM AUTHOR]

Published
2015
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16. JC human polyomavirus (JCV) and Epstein-Barr virus (EBV) replicative activities are detected in Hodgkin/Reed Sternberg cells (HRS) and circulating lymphocytes (PBL) of Hodgkin lymphoma (HL) and associated with relapse, especially in younger patients

Author

Carde, P., primary, Andreoletti, L., additional, Koscielny, S., additional, Assaf, E., additional, Girinsky, T., additional, Bosq, J., additional, Bernheim, A., additional, Flamant, S., additional, Violot, D., additional, Parmentier, C., additional, and M’Kacher, R., additional

Published
2006
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21. JC human polyomavirus is associated to chromosomal instability in peripheral blood lymphocytes of Hodgkin’s lymphoma patients and poor clinical outcome.

Author

M'kacher, R., Andreoletti, L., Flamant, S., Milliat, F., Girinsky, T., Dossou, J., Violot, D., Assaf, E., Clausse, B., Koscielny, S., Bourhis, J., Bosq, J., Bernheim, A., Parmentier, C., and Carde, P.

Subjects
*POLYOMAVIRUSES, *EPSTEIN-Barr virus, *LYMPHOCYTES, *HODGKIN'S disease, *B cells
Abstract

Background: B cells are potential sites for latency and reactivation of the human neurotropic JC polyomavirus (JCV). We investigated JCV and Epstein–Barr virus (EBV) status in peripheral blood lymphocytes (PBL) from 74 Hodgkin’s lymphoma (HL) and 91 B-cell non-Hodgkin’s lymphoma (B-NHL) patients. [ABSTRACT FROM PUBLISHER]

Published
2010
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26. Telomere Dysfunction in Pediatric Patients with Differences/Disorders of Sexual Development.

Author

Younoussa H, Gadji M, Soumboundou M, Colicchio B, Said A, Ndoye NA, Junker S, Plesch A, Heidingsfelder L, Diagne NR, Dieterlen A, Voisin P, Carde P, Jeandidier E, and M'kacher R

Abstract

Differences/Disorders of sex development (DSDs) are conditions in which the development of chromosomal, gonadal, and anatomical sexes is atypical. DSDs are relatively rare, but their incidence is becoming alarmingly common in sub-Saharan Africa (SSA). Their etiologies and mechanisms are poorly understood. Therefore, we have investigated cytogenetic profiles, including telomere dysfunction, in a retrospective cohort of Senegalese DSD patients., Materials and Methods: Peripheral blood lymphocytes were sampled from 35 DSD patients (mean age: 3.3 years; range 0-18 years) admitted to two hospital centers in Dakar. Peripheral blood lymphocytes from 150 healthy donors were used as a control. Conventional cytogenetics, telomere, and centromere staining followed by multiplex FISH, as well as FISH with SRY -specific probes, were employed., Results: Cytogenetic analysis identified 19 male and 13 female patients with apparently normal karyotypes, two patients with Turner syndrome, and one patient with Klinefelter syndrome. Additional structural chromosome aberrations were detected in 22% of the patients (8/35). Telomere analysis revealed a reduction in mean telomere lengths of DSD patients compared to those of healthy donors of similar age. This reduction in telomere length was associated with an increased rate of telomere aberrations (telomere loss and the formation of telomere doublets) and the presence of additional chromosomal aberrations., Conclusions: To the best of our knowledge, this study is the first to demonstrate a correlation between telomere dysfunction and DSDs. Further studies may reveal the link between telomere dysfunction and possible mechanisms involved in the disease itself, such as DNA repair deficiency or specific gene mutations. The present study demonstrates the relevance of implementing telomere analysis in prenatal tests as well as in diagnosed genetic DSD disorders.

Published
2024
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27. Multi-omics comparison of malignant and normal uveal melanocytes reveals molecular features of uveal melanoma.

Author

Gentien D, Saberi-Ansari E, Servant N, Jolly A, de la Grange P, Némati F, Liot G, Saule S, Teissandier A, Bourc'his D, Girard E, Wong J, Masliah-Planchon J, Narmanli E, Liu Y, Torun E, Goulancourt R, Rodrigues M, Gaudé LV, Reyes C, Bazire M, Chenegros T, Henry E, Rapinat A, Bohec M, Baulande S, M'kacher R, Jeandidier E, Nicolas A, Ciriello G, Margueron R, Decaudin D, Cassoux N, Piperno-Neumann S, Stern MH, Gibcus JH, Dekker J, Heard E, Roman-Roman S, and Waterfall JJ

Subjects
Humans, Melanocytes metabolism, DNA, Antigens, Neoplasm genetics, Multiomics, Melanoma pathology
Abstract

Uveal melanoma (UM) is a rare cancer resulting from the transformation of melanocytes in the uveal tract. Integrative analysis has identified four molecular and clinical subsets of UM. To improve our molecular understanding of UM, we performed extensive multi-omics characterization comparing two aggressive UM patient-derived xenograft models with normal choroidal melanocytes, including DNA optical mapping, specific histone modifications, and DNA topology analysis using Hi-C. Our gene expression and cytogenetic analyses suggest that genomic instability is a hallmark of UM. We also identified a recurrent deletion in the BAP1 promoter resulting in loss of expression and associated with high risk of metastases in UM patients. Hi-C revealed chromatin topology changes associated with the upregulation of PRAME, an independent prognostic biomarker in UM, and a potential therapeutic target. Our findings illustrate how multi-omics approaches can improve our understanding of tumorigenesis and reveal two distinct mechanisms of gene expression dysregulation in UM., Competing Interests: Declaration of interests P.d.l.G. is a co-founder of Genosplice technology. A.J. and R.G. are employees of Genosplice technology. R.M. is the founder of Cell Environment., (Copyright © 2023 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published
2023
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28. Extended lifespan and improved genome stability in HepaRG-derived cell lines through reprogramming by high-density stress.

Author

Brun C, Allain C, Ferron PJ, Younoussa H, Colicchio B, Jeandidier E, M'Kacher R, Guguen-Guillouzo C, and Bertile F

Subjects
Humans, Cell Differentiation, Cell Line, Cues, Longevity, Cell Transdifferentiation
Abstract

The characteristics and fate of cancer cells partly depend on their environmental stiffness, i.e., the local mechanical cues they face. HepaRG progenitors are liver carcinoma cells exhibiting transdifferentiation properties; however, the underlying mechanisms remain unknown. To evaluate the impact of external physical forces mimicking the tumor microenvironment, we seeded them at very high density for 20 h, keeping the cells round and unanchored to the substrate. Applied without corticoids, spatial confinement due to very high density induced reprogramming of HepaRG cells into stable replicative stem-like cells after replating at normal density. Redifferentiation of these stem-like cells into cells very similar to the original HepaRG cells was then achieved using the same stress but in the presence of corticoids. This demonstrates that the cells retained the memory required to run the complete hepatic differentiation program, after bypassing the Hayflick limit twice. We show that physical stress improved chromosome quality and genomic stability, through greater efficiency of DNA repair and restoration of telomerase activity, thus enabling cells to escape progression to a more aggressive cancer state. We also show the primary importance of high-density seeding, possibly triggering compressive stress, in these processes, rather than that of cell roundness or intracellular tensional signals. The HepaRG-derived lines established here considerably extend the lifespan and availability of this surrogate cell system for mature human hepatocytes. External physical stress is a promising way to create a variety of cell lines, and it paves the way for the development of strategies to improve cancer prognosis.

Published
2023
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29. Modeling Global Genomic Instability in Chronic Myeloid Leukemia (CML) Using Patient-Derived Induced Pluripotent Stem Cells (iPSCs).

Author

Telliam G, Desterke C, Imeri J, M'kacher R, Oudrhiri N, Balducci E, Fontaine-Arnoux M, Acloque H, Bennaceur-Griscelli A, and Turhan AG

Abstract

Methods: We used a patient-specific induced pluripotent stem cell (iPSC) line treated with the mutagenic agent N-ethyl-N-nitrosourea (ENU). Genomic instability was validated using γ-H2AX and micronuclei assays and CGH array for genomic events., Results: An increased number of progenitors (x5-Fold), which proliferated in liquid cultures with a blast cell morphology, was observed in the mutagenized condition as compared to the unmutagenized one. CGH array performed for both conditions in two different time points reveals several cancer genes in the ENU-treated condition, some known to be altered in leukemia (BLM, IKZF1, NCOA2, ALK, EP300, ERG, MKL1, PHF6 and TET1). Transcriptome GEO-dataset GSE4170 allowed us to associate 125 of 249 of the aberrations that we detected in CML-iPSC with the CML progression genes already described during progression from chronic and AP to BC. Among these candidates, eleven of them have been described in CML and related to tyrosine kinase inhibitor resistance and genomic instability., Conclusions: These results demonstrated that we have generated, for the first time to our knowledge, an in vitro genetic instability model, reproducing genomic events described in patients with BC.

Published
2023
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30. High Resolution and Automatable Cytogenetic Biodosimetry Using In Situ Telomere and Centromere Hybridization for the Accurate Detection of DNA Damage: An Overview.

Author

M'Kacher R, Colicchio B, Junker S, El Maalouf E, Heidingsfelder L, Plesch A, Dieterlen A, Jeandidier E, Carde P, and Voisin P

Subjects
Humans, Cytogenetics, Chromosome Aberrations, Radiometry methods, DNA Damage genetics, Cytogenetic Analysis, Lymphocytes, Centromere genetics, Telomere genetics
Abstract

In the event of a radiological or nuclear accident, or when physical dosimetry is not available, the scoring of radiation-induced chromosomal aberrations in lymphocytes constitutes an essential tool for the estimation of the absorbed dose of the exposed individual and for effective triage. Cytogenetic biodosimetry employs different cytogenetic assays including the scoring of dicentrics, micronuclei, and translocations as well as analyses of induced premature chromosome condensation to define the frequency of chromosome aberrations. However, inherent challenges using these techniques include the considerable time span from sampling to result, the sensitivity and specificity of the various techniques, and the requirement of highly skilled personnel. Thus, techniques that obviate these challenges are needed. The introduction of telomere and centromere (TC) staining have successfully met these challenges and, in addition, greatly improved the efficiency of cytogenetic biodosimetry through the development of automated approaches, thus reducing the need for specialized personnel. Here, we review the role of the various cytogenetic dosimeters and their recent improvements in the management of populations exposed to genotoxic agents such as ionizing radiation. Finally, we discuss the emerging potentials to exploit these techniques in a wider spectrum of medical and biological applications, e.g., in cancer biology to identify prognostic biomarkers for the optimal triage and treatment of patients.

Published
2023
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31. A Central Role of Telomere Dysfunction in the Formation of a Unique Translocation within the Sub-Telomere Region Resulting in Duplication and Partial Trisomy.

Author

M'Kacher R, Miguet M, Maillard PY, Colicchio B, Scheidecker S, Najar W, Arnoux M, Oudrhiri N, Borie C, Biehler M, Plesch A, Heidingsfelder L, Bennaceur-Griscelli A, Dieterlen A, Voisin P, Junker S, Carde P, and Jeandidier E

Subjects
Humans, In Situ Hybridization, Fluorescence, Chromosome Banding, Chromosome Aberrations, Telomere genetics, Trisomy genetics, Translocation, Genetic genetics
Abstract

Telomeres play a major role in maintaining genome stability and integrity. Putative involvement of telomere dysfunction in the formation of various types of chromosomal aberrations is an area of active research. Here, we report a case of a six-month-old boy with a chromosomal gain encompassing the 11q22.3q25 region identified by SNP array analysis. The size of the duplication is 26.7 Mb and contains 170 genes (OMIM). The duplication results in partial trisomy of the region in question with clinical consequences, including bilateral renal dysplasia, delayed development, and a heart defect. Moreover, the karyotype determined by R-banding and chromosome painting as well as by hybridization with specific sub-telomere probes revealed the presence of an unbalanced t(9;11)(p24;q22.3) translocation with a unique breakpoint involving the sub-telomere region of the short arm of chromosome 9. The karyotypes of the parents were normal. Telomere integrity in circulating lymphocytes from the child and from his parents was assessed using an automated high-throughput method based on fluorescence in situ hybridization (FISH) with telomere- and centromere-specific PNA probes followed by M-FISH multicolor karyotyping. Very short telomeres, as well as an increased frequency of telomere loss and formation of telomere doublets, were detected in the child's cells. Interestingly, similar telomere profiles were found in the circulating lymphocytes of the father. Moreover, an assessment of clonal telomere aberrations identified chromosomes 9 and 11 with particularly high frequencies of such aberrations. These findings strongly suggest that telomere dysfunction plays a central role in the formation of this specific unbalanced chromosome rearrangement via chromosome end-to-end fusion and breakage-fusion-bridge cycles.

Published
2022
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32. Patient-Derived iPSCs Reveal Evidence of Telomere Instability and DNA Repair Deficiency in Coats Plus Syndrome.

Author

Oudrhiri N, M'kacher R, Chaker D, Colicchio B, Borie C, Jeandidier E, Dieterlen A, Griscelli F, Bennaceur-Griscelli A, and Turhan AG

Subjects
Ataxia, Brain Neoplasms, Calcinosis, Central Nervous System Cysts, Humans, Leukoencephalopathies, Muscle Spasticity, Retinal Diseases, Seizures, Telomere genetics, Telomere metabolism, Telomere Homeostasis genetics, DNA Repair-Deficiency Disorders, Induced Pluripotent Stem Cells metabolism, Telomerase genetics
Abstract

Coats plus (CP) syndrome is an inherited autosomal recessive condition that results from mutations in the conserved telomere maintenance component 1 gene ( CTC1 ). The CTC1 protein functions as a part of the CST protein complex, a protein heterotrimer consisting of CTC1-STN1-TEN1 which promotes telomere DNA synthesis and inhibits telomerase-mediated telomere elongation. However, it is unclear how CTC1 mutations may have an effect on telomere structure and function. For that purpose, we established the very first induced pluripotent stem cell lines (iPSCs) from a compound heterozygous patient with CP carrying deleterious mutations in both alleles of CTC1 . Telomere dysfunction and chromosomal instability were assessed in both circulating lymphocytes and iPSCs from the patient and from healthy controls of similar age. The circulating lymphocytes and iPSCs from the CP patient were characterized by their higher telomere length heterogeneity and telomere aberrations compared to those in control cells from healthy donors. Moreover, in contrast to iPSCs from healthy controls, the high levels of telomerase were associated with activation of the alternative lengthening of telomere (ALT) pathway in CP-iPSCs. This was accompanied by inappropriate activation of the DNA repair proteins γH2AX, 53BP1, and ATM, as well as with accumulation of DNA damage, micronuclei, and anaphase bridges. CP-iPSCs presented features of cellular senescence and increased radiation sensitivity. Clonal dicentric chromosomes were identified only in CP-iPSCs after exposure to radiation, thus mirroring the role of telomere dysfunction in their formation. These data demonstrate that iPSCs derived from CP patients can be used as a model system for molecular studies of the CP syndrome and underscores the complexity of telomere dysfunction associated with the defect of DNA repair machinery in the CP syndrome.

Published
2022
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33. Lung Fibroblasts from Idiopathic Pulmonary Fibrosis Patients Harbor Short and Unstable Telomeres Leading to Chromosomal Instability.

Author

M'Kacher R, Jaillet M, Colicchio B, Vasarmidi E, Mailleux A, Dieterlen A, Kannengiesser C, Borie C, Oudrhiri N, Junker S, Voisin P, Jeandidier E, Carde P, Fenech M, Bennaceur-Griscelli A, Crestani B, and Borie R

Abstract

Idiopathic pulmonary fibrosis (IPF) is associated with several hallmarks of aging including telomere shortening, which can result from germline mutations in telomere related genes (TRGs). Here, we assessed the length and stability of telomeres as well as the integrity of chromosomes in primary lung fibroblasts from 13 IPF patients (including seven patients with pathogenic variants in TRGs) and seven controls. Automatized high-throughput detection of telomeric FISH signals highlighted lower signal intensity in lung fibroblasts from IPF patients, suggesting a telomere length defect in these cells. The increased detection of telomere loss and terminal deletion in IPF cells, particularly in TRG-mutated cells (IPF-TRG), supports the notion that these cells have unstable telomeres. Furthermore, fibroblasts from IPF patients with TRGs mutations exhibited dicentric chromosomes and anaphase bridges. Collectively, our study indicates that fibroblasts from IPF patients exhibit telomere and chromosome instability that likely contribute to the physiopathology.

Published
2022
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34. Is Response to Genotoxic Stress Similar in Populations of African and European Ancestry? A Study of Dose-Response After in vitro Irradiation.

Author

Soumboundou M, Dossou J, Kalaga Y, Nkengurutse I, Faye I, Guingani A, Gadji M, Yameogo KJ, Zongo H, Mbaye G, Dem A, Diarra M, Adjibade R, Djebou C, Junker S, Oudrhiri N, Hempel WM, Dieterlen A, Jeandidier E, Carde P, El Maalouf E, Colicchio B, Bennaceur-Griscelli A, Fenech M, Voisin P, Rodriguez-Lafrasse C, and M'Kacher R

Abstract

Background: Exposure to genotoxic stress such as radiation is an important public health issue affecting a large population. The necessity of analyzing cytogenetic effects of such exposure is related to the need to estimate the associated risk. Cytogenetic biological dosimetry is based on the relationship between the absorbed dose and the frequency of scored chromosomal aberrations. The influence of confounding factors on radiation response is a topical issue. The role of ethnicity is unclear. Here, we compared the dose-response curves obtained after irradiation of circulating lymphocytes from healthy donors of African and European ancestry. Materials and Methods: Blood samples from six Africans living in Africa, five Africans living in Europe, and five Caucasians living in Europe were exposed to various doses (0-4 Gy) of X-rays at a dose-rate of 0.1 Gy/min using an X-RAD320 irradiator. A validated cohort composed of 14 healthy Africans living in three African countries was included and blood samples were irradiated using the same protocols. Blood lymphocytes were cultured for 48 h and chromosomal aberrations scored during the first mitosis by telomere and centromere staining. The distribution of dicentric chromosomes was determined and the Kruskal-Wallis test was used to compare the dose-response curves of the two populations. Results: No spontaneous dicentric chromosomes were detected in African donors, thus establishing a very low background of unstable chromosomal aberrations relative to the European population. There was a significant difference in the dose response curves between native African and European donors. At 4 Gy, African donors showed a significantly lower frequency of dicentric chromosomes ( p = 8.65 10 -17 ), centric rings ( p = 4.0310 -14 ), and resulting double-strand-breaks (DSB) ( p = 1.32 10 -18 ) than European donors. In addition, a significant difference was found between African donors living in Europe and Africans living in Africa. Conclusion: This is the first study to demonstrate the important role of ethnic and environmental factors that may epigenetically influence the response to irradiation. It will be necessary to establish country-of-origen-specific dose response curves to practice precise and adequate biological dosimetry. This work opens new perspective for the comparison of treatments based on genotoxic agents, such as irradiation., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Soumboundou, Dossou, Kalaga, Nkengurutse, Faye, Guingani, Gadji, Yameogo, Zongo, Mbaye, Dem, Diarra, Adjibade, Djebou, Junker, Oudrhiri, Hempel, Dieterlen, Jeandidier, Carde, El Maalouf, Colicchio, Bennaceur-Griscelli, Fenech, Voisin, Rodriguez-Lafrasse and M’Kacher.)

Published
2021
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35. Telomere aberrations, including telomere loss, doublets, and extreme shortening, are increased in patients with infertility.

Author

M'kacher R, Colicchio B, Marquet V, Borie C, Najar W, Hempel WM, Heidingsfelder L, Oudrhiri N, Al Jawhari M, Wilhelm-Murer N, Miguet M, Dieterlen A, Deschênes G, Tabet AC, Junker S, Grynberg M, Fenech M, Bennaceur-Griscelli A, Voisin P, Carde P, Jeandidier E, and Yardin C

Subjects
Adult, Case-Control Studies, Chromosomal Instability physiology, Chromosome Duplication physiology, Cytogenetic Analysis methods, Female, Humans, In Situ Hybridization, Fluorescence, Infertility epidemiology, Infertility etiology, Male, Middle Aged, Retrospective Studies, Telomere Shortening genetics, Young Adult, Chromosome Aberrations statistics & numerical data, Infertility genetics, Telomere genetics, Telomere Shortening physiology
Abstract

Objective: To test the hypothesis that telomere shortening and/or loss are risk factors for infertility., Design: Retrospective analysis of the telomere status in patients with infertility using conventional cytogenetic data collected prospectively., Setting: Academic centers., Patient(s): Cytogenetic slides with cultured peripheral lymphocytes from 50 patients undergoing fertility treatment and 150 healthy donors, including 100 donors matched for age., Intervention(s): Cytogenetic slides were used to detect chromosomal and telomere aberrations., Main Outcome Measure(s): Telomere length and telomere aberrations were analyzed after telomere and centromere staining., Result(s): The mean telomere length of patients consulting for infertility was significantly less than that of healthy donors of similar age. Moreover, patients with infertility showed significantly more extreme telomere loss and telomere doublet formation than healthy controls. Telomere shortening and/or telomere aberrations were more pronounced in patients with structural chromosomal aberrations. Dicentric chromosomes were identified in 6/13 patients, with constitutional chromosomal aberrations leading to chromosomal instability that correlated with chromosomal end-to-end fusions., Conclusion(s): Our findings demonstrate the feasibility of analyzing telomere aberrations in addition to chromosomal aberrations, using cytogenetic slides. Telomere attrition and/or dysfunction represent the main common cytogenetic characteristic of patients with infertility, leading to potential implications for fertility assessment. Pending further studies, these techniques that correlate the outcome of assisted reproduction and telomere integrity status may represent a novel and useful diagnostic and/or prognostic tool for medical care in this field., (Copyright © 2020 American Society for Reproductive Medicine. Published by Elsevier Inc. All rights reserved.)

Published
2021
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36. Telomere and Centromere Staining Followed by M-FISH Improves Diagnosis of Chromosomal Instability and Its Clinical Utility.

Author

M'kacher R, Colicchio B, Borie C, Junker S, Marquet V, Heidingsfelder L, Soehnlen K, Najar W, Hempel WM, Oudrhiri N, Wilhelm-Murer N, Miguet M, Arnoux M, Ferrapie C, Kerbrat W, Plesch A, Dieterlen A, Girinsky T, Voisin P, Deschenes G, Tabet AC, Yardin C, Bennaceur-Griscelli A, Fenech M, Carde P, and Jeandidier E

Subjects
Chromosome Aberrations, Cytogenetic Analysis methods, Female, Humans, In Situ Hybridization, Fluorescence methods, Lymphocytes pathology, Male, Metaphase genetics, Middle Aged, Neoplasms classification, Neoplasms genetics, Neoplasms pathology, Centromere genetics, Chromosomal Instability genetics, Neoplasms diagnosis, Telomere genetics
Abstract

Dicentric chromosomes are a relevant marker of chromosomal instability. Their appearance is associated with telomere dysfunction, leading to cancer progression and a poor clinical outcome. Here, we present Telomere and Centromere staining followed by M-FISH (TC+M-FISH) for improved detection of telomere dysfunction and the identification of dicentric chromosomes in cancer patients and various genetic syndromes. Significant telomere length shortening and significantly higher frequencies of telomere loss and deletion were found in the peripheral lymphocytes of patients with cancer and genetic syndromes relative to similar age-matched healthy donors. We assessed our technique against conventional cytogenetics for the detection of dicentric chromosomes by subjecting metaphase preparations to both approaches. We identified dicentric chromosomes in 28/50 cancer patients and 21/44 genetic syndrome patients using our approach, but only 7/50 and 12/44, respectively, using standard cytogenetics. We ascribe this discrepancy to the identification of the unique configuration of dicentric chromosomes. We observed significantly higher frequencies of telomere loss and deletion in patients with dicentric chromosomes ( p < 10 -4 ). TC+M-FISH analysis is superior to classical cytogenetics for the detection of chromosomal instability. Our approach is a relatively simple but useful tool for documenting telomere dysfunction and chromosomal instability with the potential to become a standard additional diagnostic tool in medical genetics and the clinic.

Published
2020
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37. The Use of Natural Agents to Counteract Telomere Shortening: Effects of a Multi-Component Extract of Astragalus mongholicus Bunge and Danazol.

Author

Guinobert I, Blondeau C, Colicchio B, Oudrhiri N, Dieterlen A, Jeandidier E, Deschenes G, Bardot V, Cotte C, Ripoche I, Carde P, Berthomier L, and M'Kacher R

Abstract

A link between telomere shortening and oxidative stress was found in aging people and patients with cancer or inflammatory diseases. Extracts of Astragalus spp. are known to stimulate telomerase activity, thereby compensating telomere shortening. We characterized a multi-component hydroethanolic root extract (HRE) of Astragalus mongholicus Bunge and assessed its effects on telomeres compared to those of danazol. Astragalosides I to IV, flavonoids, amino acids and sugars were detected in the HRE. Samples of peripheral blood lymphocytes with short telomeres from 18 healthy donors (mean age 63.5 years; range 3286 years) were exposed to a single dose of 1 µg/mL HRE or danazol for three days. Telomere length and telomerase expression were then measured. Significant elongation of telomeres associated to a less toxicity was observed in lymphocytes from 13/18 donors following HRE treatment (0.54 kb (0.15-2.06 kb)) and in those from 9/18 donors after danazol treatment (0.95 kb (0.06-2.06 kb)). The rate of cells with short telomeres (<3 kb) decreased in lymphocytes from all donors after exposure to either HRE or danazol, telomere elongation being telomerase-dependent. These findings suggest that the HRE could be used for the management of age-related diseases., Competing Interests: I.G., C.B., V.B. and C.C. are employees of Groupe PiLeJe.

Published
2020
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38. A new tool for genotoxic risk assessment: Reevaluation of the cytokinesis-block micronucleus assay using semi-automated scoring following telomere and centromere staining.

Author

Zaguia N, Laplagne E, Colicchio B, Cariou O, Al Jawhari M, Heidingsfelder L, Hempel WM, Jrad BBH, Jeandidier E, Dieterlen A, Carde P, Voisin P, and M'kacher R

Subjects
Aneugens pharmacology, Centromere genetics, Cytokinesis drug effects, Cytokinesis genetics, DNA Damage genetics, Humans, Lymphocytes drug effects, Micronuclei, Chromosome-Defective drug effects, Micronucleus Tests, Mutagens toxicity, Risk Assessment, Telomere genetics, Centromere drug effects, DNA Damage drug effects, Mutagenicity Tests, Telomere drug effects
Abstract

Background: The cytokinesis-block micronucleus (CBMN) assay is an internationally recognized method for measuring DNA damage after exposure to genotoxic agents, as well as a biomarker for DNA repair and chromosomal instability. The high baseline level of micronuclei (MN) in the healthy population has limited the sensitivity and application of the CBMN assay for the follow-up of exposed populations. We reevaluated the sensitivity of the CBNM assay using semi-automated MN scoring following telomere and centromere (TC) staining after in vitro exposure to genotoxic agents (mitomycin or radiation) or aneugenic agents (vinblastine)., Materials and Methods: Blood samples from 12 healthy donors were exposed to 137 Cs at seven doses from 0.1-4 Gy and cultured for 72 h. Cytochalasin B was added at 46 h of culture. The exposure of chemical agents (mitomycin or vinblastine) was performed after 48 h of culture for 3 h. Cytochalasin B was added after treatment and slides were prepared 24 h after. MN was semi-automatically scored following TC staining. Nucleoplasmic bridges (NPBs) and nuclear buds (NBUDs) were assessed in a human cell line after TC staining., Results: The introduction TC staining to the scoring of MN not only renders MN scoring more efficient and robust, but also permits discrimination between exposure to clastogenic (MN with only telomere signals) and aneugenic agents (MN with both TC signals). The resulting improvement of MN detection led to an increase in the sensitivity of the CBMN assay following low-dose radiation exposure (0.3 versus 0.1 Gy). Hyperradiosensitivity phenomenon was observed after low dose exposure. A dose-response curve was obtained for up to 4 Gy. In addition, TC staining permits assessment of the nature of NPBs and NBUDs as biomarkers for genotoxicity and chromosomal instability., Conclusion: These approaches can be potentially used to follow-up populations exposed to genotoxic agents and assess cancer risk., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020. Published by Elsevier B.V.)

Published
2020
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39. Benefit of an association of an antioxidative substrate and a traditional chinese medicine on telomere elongation.

Author

M'kacher R, Breton L, Colicchio B, Puget H, Hempel WM, Al Jawhari M, Jeandidier E, and Frey M

Subjects
Adolescent, Adult, Aged, Astragalus Plant metabolism, Child, Child, Preschool, Humans, Lymphocytes metabolism, Middle Aged, Polysaccharides administration & dosage, Polysaccharides chemistry, S-Adenosylmethionine administration & dosage, S-Adenosylmethionine chemistry, Telomere Shortening, Young Adult, Antioxidants administration & dosage, Dietary Supplements, Medicine, Chinese Traditional, Telomere metabolism
Abstract

Telomere shortening is involved in age-related disorders, such as cancer and cardiovascular diseases. Recently, telomerase re-activation strategies have been proposed to counteract telomere shortening and its consequences. Here, we investigated the benefit of dietary supplementation with a mix of S-adenosyl-methionine (SAMe) and a polysaccharide extract of Astragalus (APS) on telomere length of circulating lymphocytes of healthy volunteers. Blood lymphocytes of a cohort of 26 healthy volunteers who were administrated the mix of SAMe and APS in a food supplement for one year were collected. In vitro treatment of blood lymphocytes of healthy volunteers with the mix was also performed. A cohort of 150 healthy volunteers was used as a control. Telomere length was measured by Q-FISH. The micronucleus assay was performed to detect genotoxicity of the mix. The telomeres of circulating lymphocytes of the cohort of 26 donors supplemented with the mix were significantly longer than those of matched controls (p &lt; 10-4). This elongation was essentially observed in the lymphocytes of older donors. Similarly, in vitro treatment of circulating lymphocytes with the mix significantly increased telomere length and decrease the proportion of cells with short telomeres. Here, we observed an increase in telomere length after in vivo and in vitro administration of a mix with SAMe and APS.  The benefit of dietary supplementation with this mix opens a new horizon for the battle against aging and could be used in the treatment of chronic age-related disorders.

Published
2019

40. Biological Dosimetry Network in Africa: Establishment of a Dose-Response Curve Using Telomere and Centromere Staining.

Author

Soumboundou M, Nkengurutse I, Dossou J, Colicchio B, Djebou C, Gadji M, Houenon G, Dem A, Dedjan A, Diarra M, Adjibade R, Finot F, Hempel W, Dieterlen A, Jeandidier E, Rodriguez-Lafrasse C, and M'kacher R

Subjects
Adult, Africa, Blood Cells radiation effects, Female, Humans, Lymphocytes radiation effects, Male, Radiation Dosage, Radiation Protection, Radiation, Ionizing, Radiometry instrumentation, Radiometry standards, X-Rays, Young Adult, Blood Cells metabolism, Centromere metabolism, Chromosome Aberrations radiation effects, Lymphocytes metabolism, Radiometry methods, Staining and Labeling methods, Telomere metabolism
Abstract

Purpose: Biological dosimetry, based on the relationship between the absorbed dose after exposure to ionizing radiation and the frequency of scored aberrations, has been and continues to be an important tool for estimating the dose after exposure. Dicentric chromosomes are considered to be the most specific and sensitive aberration related to radiation exposure. Here, we established the dose-response curve following in vitro irradiation of circulating lymphocytes from healthy donors from three African countries after scoring unstable chromosomal aberrations., Materials and Methods: Blood samples from 16 African donors were exposed to various doses (0 to 4 Gy) using an X-RAD320 x-ray system with a maximum photon energy of 250 kV at a dose rate of 0.1 Gy min. Blood lymphocytes were cultured for 48 h, and chromosomal aberrations were scored during the first mitosis by telomere and centromere staining. The distribution of dicentric chromosomes was determined., Results: No dicentric chromosomes were found after the analysis of 2,669 first-division metaphases before in vitro exposure. We established a linear-quadratic dose-response curve based on the frequency of dicentric and ring chromosomes and calculated double-strand breaks, taking into account all scored aberrations., Conclusion: The generation of a specific dose-response curve for African donors will allow the practice of precise biological dosimetry in these countries. This work is the first step towards realizing an African biodosimetry network and the establishment of a biological dosimetry laboratory, which could play a major role in the application of radioprotection norms.

Published
2019
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41. Erratum: Cuceu, C., et al. Independent Mechanisms Lead to Genomic Instability in Hodgkin Lymphoma: Microsatellite or Chromosomal Instability. Cancers 2018, 10 , 233.

Author

Cuceu C, Colicchio B, Jeandidier E, Junker S, Plassa F, Shim G, Mika J, Frenzel M, Al Jawhari M, Hempel WM, Kabacik S, Lenain A, Morat L, Girinsky T, Dieterlen A, Polanska J, Badie C, Carde P, and M'Kacher R

Abstract

The authors wish to make the following corrections to this paper [...].

Published
2019
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43. Establishment and Characterization of a Reliable Xenograft Model of Hodgkin Lymphoma Suitable for the Study of Tumor Origin and the Design of New Therapies.

Author

M'kacher R, Frenzel M, Al Jawhari M, Junker S, Cuceu C, Morat L, Bauchet AL, Stimmer L, Lenain A, Dechamps N, Hempel WM, Pottier G, Heidingsfelder L, Laplagne E, Borie C, Oudrhiri N, Jouni D, Bennaceur-Griscelli A, Colicchio B, Dieterlen A, Girinsky T, Boisgard R, Bourhis J, Bosq J, Mehrling T, Jeandidier E, and Carde P

Abstract

To identify the cells responsible for the initiation and maintenance of Hodgkin lymphoma (HL) cells, we have characterized a subpopulation of HL cells grown in vitro and in vivo with the aim of establishing a reliable and robust animal model for HL. To validate our model, we challenged the tumor cells in vivo by injecting the alkylating histone-deacetylase inhibitor, EDO-S101, a salvage regimen for HL patients, into xenografted mice. Methodology: Blood lymphocytes from 50 HL patients and seven HL cell lines were used. Immunohistochemistry, flow cytometry, and cytogenetics analyses were performed. The in vitro and in vivo effects of EDO-S101 were assessed. Results: We have successfully determined conditions for in vitro amplification and characterization of the HL L428-c subline, containing a higher proportion of CD30-/CD15- cells than the parental L428 cell line. This subline displayed excellent clonogenic potential and reliable reproducibility upon xenografting into immunodeficient NOD-SCID-gamma (-/-)(NSG) mice. Using cell sorting, we demonstrate that CD30-/CD15- subpopulations can gain the phenotype of the L428-c cell line in vitro. Moreover, the human cells recovered from the seventh week after injection of L428-c cells into NSG mice were small cells characterized by a high frequency of CD30-/CD15- cells. Cytogenetic analysis demonstrated that they were diploid and showed high telomere instability and telomerase activity. Accordingly, chromosomal instability emerged, as shown by the formation of dicentric chromosomes, ring chromosomes, and breakage/fusion/bridge cycles. Similarly, high telomerase activity and telomere instability were detected in circulating lymphocytes from HL patients. The beneficial effect of the histone-deacetylase inhibitor EDO-S101 as an anti-tumor drug validated our animal model. Conclusion: Our HL animal model requires only 10³ cells and is characterized by a high survival/toxicity ratio and high reproducibility. Moreover, the cells that engraft in mice are characterized by a high frequency of small CD30-/CD15- cells exhibiting high telomerase activity and telomere dysfunction.

Published
2018
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44. Independent Mechanisms Lead to Genomic Instability in Hodgkin Lymphoma: Microsatellite or Chromosomal Instability † .

Author

Cuceu C, Colicchio B, Jeandidier E, Junker S, Plassa F, Shim G, Mika J, Frenzel M, Al Jawhari M, Hempel WM, O'Brien G, Lenain A, Morat L, Girinsky T, Dieterlen A, Polanska J, Badie C, Carde P, and M'Kacher R

Abstract

Background : Microsatellite and chromosomal instability have been investigated in Hodgkin lymphoma (HL). Materials and Methods : We studied seven HL cell lines (five Nodular Sclerosis (NS) and two Mixed Cellularity (MC)) and patient peripheral blood lymphocytes (100 NS-HL and 23 MC-HL). Microsatellite instability (MSI) was assessed by PCR. Chromosomal instability and telomere dysfunction were investigated by FISH. DNA repair mechanisms were studied by transcriptomic and molecular approaches. Results : In the cell lines, we observed high MSI in L428 (4/5), KMH2, and HDLM2 (3/5), low MSI in L540, L591, and SUP-HD1, and none in L1236. NS-HL cell lines showed telomere shortening, associated with alterations of nuclear shape. Small cells were characterized by telomere loss and deletion, leading to chromosomal fusion, large nucleoplasmic bridges, and breakage/fusion/bridge (B/F/B) cycles, leading to chromosomal instability. The MC-HL cell lines showed substantial heterogeneity of telomere length. Intrachromosmal double strand breaks induced dicentric chromosome formation, high levels of micronucleus formation, and small nucleoplasmic bridges. B/F/B cycles induced complex chromosomal rearrangements. We observed a similar pattern in circulating lymphocytes of NS-HL and MC-HL patients. Transcriptome analysis confirmed the differences in the DNA repair pathways between the NS and MC cell lines. In addition, the NS-HL cell lines were radiosensitive and the MC-cell lines resistant to apoptosis after radiation exposure. Conclusions : In mononuclear NS-HL cells, loss of telomere integrity may present the first step in the ongoing process of chromosomal instability. Here, we identified, MSI as an additional mechanism for genomic instability in HL.

Published
2018
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45. The Transition between Telomerase and ALT Mechanisms in Hodgkin Lymphoma and Its Predictive Value in Clinical Outcomes.

Author

M'kacher R, Cuceu C, Al Jawhari M, Morat L, Frenzel M, Shim G, Lenain A, Hempel WM, Junker S, Girinsky T, Colicchio B, Dieterlen A, Heidingsfelder L, Borie C, Oudrhiri N, Bennaceur-Griscelli A, Moralès O, Renaud S, Van de Wyngaert Z, Jeandidier E, Delhem N, and Carde P

Abstract

Background : We analyzed telomere maintenance mechanisms (TMMs) in lymph node samples from HL patients treated with standard therapy. The TMMs correlated with clinical outcomes of patients. Materials and Methods : Lymph node biopsies obtained from 38 HL patients and 24 patients with lymphadenitis were included in this study. Seven HL cell lines were used as in vitro models. Telomerase activity (TA) was assessed by TRAP assay and verified through hTERT immunofluorescence expression; alternative telomere lengthening (ALT) was also assessed, along with EBV status. Results : Both TA and ALT mechanisms were present in HL lymph nodes. Our findings were reproduced in HL cell lines. The highest levels of TA were expressed in CD30-/CD15- cells. Small cells were identified with ALT and TA. Hodgkin and Reed Sternberg cells contained high levels of PML bodies, but had very low hTERT expression. There was a significant correlation between overall survival ( p < 10 -3 ), event-free survival ( p < 10 -4 ), and freedom from progression ( p < 10 -3 ) and the presence of an ALT profile in lymph nodes of EBV+ patients. Conclusion : The presence of both types of TMMs in HL lymph nodes and in HL cell lines has not previously been reported. TMMs correlate with the treatment outcome of EBV+ HL patients.

Published
2018
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46. Chromosomal Instability in Hodgkin Lymphoma: An In-Depth Review and Perspectives.

Author

Cuceu C, Hempel WM, Sabatier L, Bosq J, Carde P, and M'kacher R

Abstract

The study of Hodgkin lymphoma (HL), with its unique microenvironment and long-term follow-up, has provided exceptional insights into several areas of tumor biology. Findings in HL have not only improved our understanding of human carcinogenesis, but have also pioneered its translation into the clinics. HL is a successful paradigm of modern treatment strategies. Nonetheless, approximately 15-20% of patients with advanced stage HL still die following relapse or progressive disease and a similar proportion of patients are over-treated, leading to treatment-related late sequelae, including solid tumors and organ dysfunction. The malignant cells in HL are characterized by a highly altered genomic landscape with a wide spectrum of genomic alterations, including somatic mutations, copy number alterations, complex chromosomal rearrangements, and aneuploidy. Here, we review the chromosomal instability mechanisms in HL, starting with the cellular origin of neoplastic cells and the mechanisms supporting HL pathogenesis, focusing particularly on the role of the microenvironment, including the influence of viruses and macrophages on the induction of chromosomal instability in HL. We discuss the emerging possibilities to exploit these aberrations as prognostic biomarkers and guides for personalized patient management., Competing Interests: The authors declare no conflict of interest.

Published
2018
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47. Triradial and quadriradial chromosomes detected in a case of B-cell prolymphocytic leukaemia.

Author

Ittel A, Gervais C, Galoisy AC, M'Kacher R, Mauvieux L, and Fornecker LM

Subjects
Aged, Biomarkers, Bone Marrow Cells metabolism, Bone Marrow Cells pathology, Female, Genomic Instability, Humans, Immunophenotyping, In Situ Hybridization, Fluorescence, Chromosome Aberrations, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma diagnosis, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma genetics
Published
2017
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48. Transmission of Induced Chromosomal Aberrations through Successive Mitotic Divisions in Human Lymphocytes after In Vitro and In Vivo Radiation.

Author

Kaddour A, Colicchio B, Buron D, El Maalouf E, Laplagne E, Borie C, Ricoul M, Lenain A, Hempel WM, Morat L, Al Jawhari M, Cuceu C, Heidingsfelder L, Jeandidier E, Deschênes G, Dieterlen A, El May M, Girinsky T, Bennaceur-Griscelli A, Carde P, Sabatier L, and M'kacher R

Subjects
Chromosomal Instability, Chromosomes, Human genetics, Giant Cells cytology, Humans, Lymphocytes metabolism, Reproducibility of Results, Telomere metabolism, Chromosome Aberrations, Gamma Rays, Lymphocytes cytology, Lymphocytes radiation effects, Mitosis radiation effects
Abstract

The mechanisms behind the transmission of chromosomal aberrations (CA) remain unclear, despite a large body of work and major technological advances in chromosome identification. We reevaluated the transmission of CA to second- and third-division cells by telomere and centromere (TC) staining followed by M-FISH. We scored CA in lymphocytes of healthy donors after in vitro irradiation and those of cancer patients treated by radiation therapy more than 12 years before. Our data demonstrate, for the first time, that dicentric chromosomes (DCs) decreased by approximately 50% per division. DCs with two centromeres in close proximity were more efficiently transmitted, representing 70% of persistent DCs in ≥M3 cells. Only 1/3 of acentric chromosomes (ACs), ACs with four telomeres, and interstitial ACs, were paired in M2 cells and associated with specific DCs configurations. In lymphocytes of cancer patients, 82% of detected DCs were characterized by these specific configurations. Our findings demonstrate the high stability of DCs with two centromeres in close proximity during cell division. The frequency of telomere deletion increased during cell cycle progression playing an important role in chromosomal instability. These findings could be exploited in the follow-up of exposed populations.

Published
2017
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49. Genotoxic risk of ethyl-paraben could be related to telomere shortening.

Author

Finot F, Kaddour A, Morat L, Mouche I, Zaguia N, Cuceu C, Souverville D, Négrault S, Cariou O, Essahli A, Prigent N, Saul J, Paillard F, Heidingsfelder L, Lafouge P, Al Jawhari M, Hempel WM, El May M, Colicchio B, Dieterlen A, Jeandidier E, Sabatier L, Clements J, and M'Kacher R

Subjects
Activation, Metabolic, Animals, Cell Culture Techniques, Cell Line, Tumor, Humans, Lymphocytes drug effects, Lymphocytes pathology, Mice, Micronuclei, Chromosome-Defective statistics & numerical data, Microsomes, Liver metabolism, Rats, Sprague-Dawley, Micronuclei, Chromosome-Defective chemically induced, Mutagens toxicity, Parabens toxicity, Telomere Shortening drug effects
Abstract

The ability of parabens to promote the appearance of multiple cancer hallmarks in breast epithelium cells provides grounds for regulatory review of the implication of the presence of parabens in human breast tissue. It is well documented that telomere dysfunction plays a significant role in the initiation of genomic instability during carcinogenesis in human breast cancer. In the present study, we evaluated the genotoxic effect of ethyl 4-hydroxybenzoate (ethyl-paraben), with and without metabolic activation (S9), in studies following OECD guidelines. We observed a significant increase in genotoxic damage using the Mouse Lymphoma Assay and in vitro micronucleus (MN) tests in the L5178Y cell line in the presence of S9 only after a short exposure. A high frequency of MN was observed in the TK6 cells after a short exposure (3 h) in the presence of S9 and a long exposure (26 h) without S9. We found significant increases in the MN frequency and induced chromosomal aberrations in the lymphocytes of only one donor after ethyl-paraben exposure in the presence of S9 after a short exposure. Cytogenetic characterization of the paraben-treated cells demonstrated telomere shortening associated with telomere loss and telomere deletions in L5178Y and TK6 cells and lymphocytes of the paraben sensitive-donor. In a control cohort of 68 human lymphocytes, telomere length and telomere aberrations were age-dependent and showed high inter-individual variation. This study is the first to link telomere shortening and the genotoxic effect of ethyl paraben in the presence of S9 and raises the possibility that telomere shortening may be a proxy for underlying inter-individual sensitivity to ethyl-paraben. Copyright © 2016 John Wiley & Sons, Ltd., (Copyright © 2016 John Wiley & Sons, Ltd.)

Published
2017
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50. RENEB intercomparison exercises analyzing micronuclei (Cytokinesis-block Micronucleus Assay).

Author

Depuydt J, Baeyens A, Barnard S, Beinke C, Benedek A, Beukes P, Buraczewska I, Darroudi F, De Sanctis S, Dominguez I, Monteiro Gil O, Hadjidekova V, Kis E, Kulka U, Lista F, Lumniczky K, M'kacher R, Moquet J, Obreja D, Oestreicher U, Pajic J, Pastor N, Popova L, Regalbuto E, Ricoul M, Sabatier L, Slabbert J, Sommer S, Testa A, Thierens H, Wojcik A, and Vral A

Subjects
Biological Assay standards, Europe, Humans, Lymphocytes radiation effects, Radiation Monitoring standards, Reproducibility of Results, Sensitivity and Specificity, Biological Assay methods, Chromosome Aberrations radiation effects, Micronucleus Tests methods, Quality Assurance, Health Care, Radiation Exposure analysis, Radiation Monitoring methods
Abstract

Purpose: In the framework of the 'Realizing the European Network of Biodosimetry' (RENEB) project, two intercomparison exercises were conducted to assess the suitability of an optimized version of the cytokinesis-block micronucleus assay, and to evaluate the capacity of a large laboratory network performing biodosimetry for radiation emergency triages. Twelve European institutions participated in the first exercise, and four non-RENEB labs were added in the second one., Materials and Methods: Irradiated blood samples were shipped to participating labs, whose task was to culture these samples and provide a blind dose estimate. Micronucleus analysis was performed by automated, semi-automated and manual procedures., Results: The dose estimates provided by network laboratories were in good agreement with true administered doses. The most accurate estimates were reported for low dose points (≤ 0.94 Gy). For higher dose points (≥ 2.7 Gy) a larger variation in estimates was observed, though in the second exercise the number of acceptable estimates increased satisfactorily. Higher accuracy was achieved with the semi-automated method., Conclusion: The results of the two exercises performed by our network demonstrate that the micronucleus assay is a useful tool for large-scale radiation emergencies, and can be successfully implemented within a large network of laboratories.

Published
2017
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