October 2009
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350 Reads
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34 Citations
Annals of Oncology
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October 2009
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350 Reads
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34 Citations
Annals of Oncology
July 2009
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53 Reads
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5 Citations
June 2008
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11 Reads
Bulletin du Cancer
June 2008
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370 Reads
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37 Citations
Cytogenetic and Genome Research
In 1957/58 the British Government conducted a series of nuclear tests in the mid-Pacific codenamed Operation Grapple, which involved several naval vessels from Britain and New Zealand. Two New Zealand frigates with 551 personnel onboard were stationed at various distances between 20 and 150 nautical miles from ground zero. In the present study we applied the cytomolecular technique mFISH (multicolour fluorescent in situ hybridisation) to investigate a potential link between chromosome abnormalities and possible past radiation exposure in New Zealand nuclear test veterans who participated in Operation Grapple. Compared to age matched controls, the veterans showed significantly higher (P < 0.0001) frequencies of chromosomal abnormalities (275 translocations and 12 dicentrics in 9,360 cells vs. 96 translocations and 1 dicentric in 9,548 cells in the controls), in addition to a significant excess of CCRs (complex chromosomal rearrangements) in the veterans. A Kolmogorov-Smirnoff test showed that the distributions of translocations for the two groups were significantly different.
June 2006
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11 Reads
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2 Citations
Journal of Clinical Oncology
7551 Background: The HRS derive from germinal-center B-cells, potential sites for latency and reactivation of JCV in immunosuppressed individuals. Replication of human polyomaviruses (JC, BK, SV40) and EBV was assessed in Hodgkin (HL) and B cell non-Hodgkin (B-NHL) lymphomas. Methods: FISH, immunohistochemistry for oncogenic proteins, PCR and DNA sequencing to identify polyomaviruses and EBV on involved nodes and in PBL before, during and after treatment (N = 73 HL, 91 B-NHL). Controls were 30 healthy donors, 70 solid tumors and 14 acute leukemia patients. Results: using FISH, JCV and EBV DNA were detected in all lymphoma nodes. High genome copy number of JCV and EBV were present in 60% and 63%, respectively, in HL patients versus 11% and 14% in B-NHL patients (P < 10 ⁻⁶ ; P < 10 ⁻⁵ ). Using nest-PCR, JCV DNA sequencing after laser capture microdissection identified the presence and specificity of JCV sequences in HRS. T antigen and LMP1 co-expression, in 34% of HRS, was associated with early HL relapse (P < 10 ⁻⁴ ), particularly in young patients (P < 10 ⁻⁵ ). Only in HL patients PBL, genome copy number of JCV increased significantly during treatment (42%). Rogue cells (cultured lymphocytes with multiple complex chromosomal aberrations indicative of genomic instability) appeared in 40% of patients, and correlated with relapse (p < 10 ⁻⁴ ). The same JCV sequences were found in tumor cells and PBL of HL patients. Co-genomic replication of EBV and JCV was highly correlated in lymph nodes and in PBL in HL. Conclusions: JCV genomic replication was detected for the first time in HRS, and associated to rogue cell emergence in PBL. Co-detections of JCV and EBV genomic replication in HRS and PBL are associated with relapse, especially in young patients. HRS and PBL JCV/EBV infections are linked and worth further studies. No significant financial relationships to disclose.
March 2005
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126 Reads
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17 Citations
European Journal of Nuclear Medicine and Molecular Imaging
The aim of this study was to evaluate the frequency of chromosomal abnormalities in thyroid cancer patients before and after radioactive iodine administration in order to assess cytogenetic particularity in Polynesian thyroid cancer patients. Chromosomal abnormalities were studied in 30 Polynesian patients with differentiated thyroid cancer, prior to and 4 days after 131I administration. Unstable chromosomal abnormalities were counted in peripheral blood lymphocytes using a conventional cytogenetic method. Peripheral blood was irradiated in vitro at different doses (0.5, 1 and 2 Gy) in order to establish the dose-response of the lymphocytes. Control groups were composed of 50 European thyroid cancer patients before and after first administration of 131I, and of ten European healthy donors. In addition, in vitro irradiation assays were performed at different doses (0.5, 1 and 2 Gy). The relative risk of spontaneous dicentrics before any radiation treatment was 2.9 (95% CI 1.7-5.1) times higher among Polynesian thyroid patients than among European thyroid cancer patients. After in vitro irradiation, the rise in frequency of dicentrics was similar in the Polynesian thyroid cancer group and the European thyroid patients and healthy donors. Four days after administration of 3.7 GBq 131I, the relative risk for a dicentric per cell was 1.3 (95% CI 1.0-1.5) times higher in Polynesian than in European patients. This can be explained by higher 131I retention in Polynesian compared with European patients. The results obtained revealed an increased frequency of cytogenetic abnormalities in Polynesian thyroid cancer patients compared with European control patients. These preliminary findings are compatible with possible previous environmental aggression and therefore imply a need for further investigations on larger series including, in particular, French Polynesian healthy donors. In addition to French Polynesians, Maori and Hawaiian control groups could be useful.
October 2003
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89 Reads
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33 Citations
International Journal of Radiation Oncology*Biology*Physics
To study chromosomal abnormalities in 49 patients with Hodgkin's lymphoma (HL), before and after treatment and at several times during a 2-year period. Simple chromosomal aberrations (CAs) and complex chromosomal rearrangements (CCRs) were counted in peripheral lymphocytes by painting of chromosomes 1, 3, and 4 (fluorescence in situ hybridization). A control population was composed of 20 healthy donors and 69 untreated cancer patients who had undergone various radiologic scans. A greater frequency (p < 10(-4)) of spontaneous cytogenetic abnormalities was observed in untreated HL patients compared with the control populations. CCRs were observed exclusively in the HL population (p < 10(-4)). Chemotherapy was associated with a significant increase in the frequency of CAs (p < 10(-4)), according to the chemotherapy regimen (p = 0.002). Immediately after radiotherapy, a significant increase (p < 10(-4)) was observed in CAs according to the size of the irradiation field. Conversely, the significant increases in the frequency of CCRs observed after treatment did not correlate with the chemotherapy regimens, radiotherapy dose, or size of the irradiation field. The evolution of CAs vs. CCRs over time was also dissociated: during the follow-up of these patients, a significant decrease was observed in the frequency of CAs at 6 months and 1 and 2 years. In contrast, after an initial decrease for up to 6 months after treatment, the frequency of CCRs remained constant for up to 2 years. Increased cytogenetic abnormalities were observed in untreated HL patients compared with the control populations. The greater frequency of cytogenetic abnormalities persisted in some patients. The presence of CCRs supports the concept of a unique genetic environment in HL patients that persists in response to potentially noxious treatments.
October 2003
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202 Reads
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44 Citations
Oncogene
Mantle cell lymphomas (MCL) are characterized by their aggressive behavior and poor response to chemotherapy regimens. We report here evidence of increased in vitro radiation sensitivity in two cell lines that we have generated from two MCL patients (UPN1 and UPN2). However, despite their increased radiation sensitivity, UPN2 cells were totally resistant to apoptotic cell death, whereas UPN1 cells underwent massive apoptosis 6 h after irradiation. The frequency of induced chromosomal abnormalities was higher in UPN1 as compared to UPN2. Distinct mechanisms have been found to contribute to this phenotype: a major telomere shortening (UPN1 and UPN2), deletion of one ATM allele and a point mutation in the remaining allele in UPN2, mutation of p53 gene (UPN1 and UPN2) with absence of functional p53 as revealed by functional yeast assays. After irradiation, Ku70 levels in UPN1 increased and decreased in UPN2, whereas in the same conditions, DNA-PKcs protein levels decreased in UPN1 and remained unchanged in UPN2. Thus, irradiation-induced apoptotic cell death can occur despite the nonfunctional status of p53 (UPN1), suggesting activation of a unique pathway in MCL cells for the induction of this event. Overall, our study demonstrates that MCL cells show increased radiation sensitivity, which can be the result of distinct molecular events. These findings could clinically be exploited to increase the dismal response rates of MCL patients to the current chemotherapy regimens.
June 2003
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34 Reads
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31 Citations
Cancer Genetics and Cytogenetics
Mantle cell lymphoma (MCL) is characterized by the t(11;14)(q13;q32), which is associated with cyclin D1 hyperexpression and a poor prognosis. MCL cases have been shown to progress to a more aggressive disease but the molecular events responsible of this phenomenon have not been determined. We have established two cell lines from the pleural effusions of two patients with MCL that we have used for further cytogenetic characterization to better define the incidence and nature of secondary chromosome abnormalities using multicolor fluorescence in situ hybridization, whole chromosome paint, and specific probes. Both cell lines grew independently without growth factors. Using CCND1/IGH-specific probes, patient UPN1 was found to have a masked t(11;14). Numerous and complex chromosomal abnormalities were found in both cell lines affecting chromosomes 2, 8, 13, 18, 22, X, and Y. These abnormalities included 8p losses, suggesting the presence of an anti-oncogene in this region, rearrangements of 8q24, MYC gene, and translocations involving 8, X, and Y chromosomes, which might be significant in the pathogenesis of MCL progression. The use of the cell lines (UPN1) allowed us to generate a mouse model of human MCL, mimicking a disseminated lymphoma and leading to the death of the animals in 4 weeks. This blastoid MCL model could be of major interest to determine molecular events involved in MCL progression, allowing isolation of involved genes and their functional characterization, and to study the effects of new chemotherapy regimens in mouse models.
May 2003
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49 Reads
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29 Citations
Cancer Genetics and Cytogenetics
Mantle cell lymphoma (MCL) is characterized by the t(11;14)(q13;q32), which is associated with cyclin D1 hyperexpression and a poor prognosis. MCL cases have been shown to progress to a more aggressive disease but the molecular events responsible of this phenomenon have not been determined. We have established two cell lines from the pleural effusions of two patients with MCL that we have used for further cytogenetic characterization to better define the incidence and nature of secondary chromosome abnormalities using multicolor fluorescence in situ hybridization, whole chromosome paint, and specific probes. Both cell lines grew independently without growth factors. Using CCND1/IGH-specific probes, patient UPN1 was found to have a masked t(11;14). Numerous and complex chromosomal abnormalities were found in both cell lines affecting chromosomes 2, 8, 13, 18, 22, X, and Y. These abnormalities included 8p losses, suggesting the presence of an anti-oncogene in this region, rearrangements of 8q24, MYC gene, and translocations involving 8, X, and Y chromosomes, which might be significant in the pathogenesis of MCL progression. The use of the cell lines (UPN1) allowed us to generate a mouse model of human MCL, mimicking a disseminated lymphoma and leading to the death of the animals in 4 weeks. This blastoid MCL model could be of major interest to determine molecular events involved in MCL progression, allowing isolation of involved genes and their functional characterization, and to study the effects of new chemotherapy regimens in mouse models.
... The etiological role of JCV in lymphoma is still debated [139][140][141][142][143]. We have demonstrated that the prevalence of the JCV antibody is significantly higher in the blood of HL patients than that of NHL patients and controls (data not shown). The presence of T-antigen and agnoprotein has been detected in HL lymph nodes [144] (Figure 3). In addition, the co-activation of JCV and EBV and the presence of rogue cells [145] were observed in the peripheral blood lymphocytes of HL patients and were associated with high a risk of relapse and the mechanisms of "hit and run" [146] in HL was proposed [147]. ...
June 2006
Journal of Clinical Oncology
... The adrenal disease is invariably bilateral, commencing as hyperplasia as in this case, and progressing to the development of frank phaechromocytoma. Bilateral adrenalectomy is indicated for the management of the adrenal involvement in multiple endocrine neoplasia type 2 on account of the frequent bilaterality of the phaeochromocytomas and the associated adrenal hyperplasia [13,14]. A patient with predominant MCT, may have a past history of adrenalectomy for phaeochromocytoma. ...
January 1995
... The benefits of postoperative radiotherapy for local tumour control have undergone poor, and only retrospective, evaluation. External beam radiotherapy (EBRT) may be indicated to improve locoregional disease control in high-risk patients, especially in cases of microscopic and even macroscopic residual tumour in the neck after incomplete surgery, or severe local extratumoural spreading (34). For distant metastases that cannot be approached surgically, EBRT can be indicated for palliative treatment of painful bone metastases or prevention of paraplegia upon threat of spinal cord involvement; it can also be indicated as an adjuvant therapy after surgery (11). ...
January 1991
... In an early case series of 4 patients with metastatic thyroid cancers (2 RAI-refractory PTCs, and 2 'insular' DTCs/PDTCs), 111 In-pentetreotide scintigraphy revealed uptake in the tumors in both patients with insular variant, and in one PTC patient (75). Several other studies have evaluated 111 In-labeled SSA scintigraphic uptake patterns in DTCs, including varying combinations of PTC, FTC, HTC, and PDTCs, with vast scintigraphy positivity rates ranging from 19% to 100% (51,(76)(77)(78)(79)(80)(81)(82)(83)(84). Binse et al. evaluated the diagnostic utility of 68 Ga-DOTATOC in 15 consecutive patients with 18 F-FDG-negative, RAI-refractory DTC with rising serum thyroglobulin (Tg) (85). ...
July 1996
The Journal of Clinical Endocrinology and Metabolism
... The ATM gene is located on chromosome 11q22-23 and plays a major role in the activation of signaling pathways by DNA damage. Missense and truncation mutations in the ATM gene have been found in adult leukemia [61][62][63][64], as well as Mantle cell lymphoma patients [56,[65][66][67][68]. Several studies have investigated the possible involvement of the ATM gene in the pathogenesis of pediatric HL [69,70]. ...
May 2003
Cancer Genetics and Cytogenetics
... Often the answer to the first question has been " the set of covariates that are common causes of treatment and outcome " or " all observed pretreatment covariates " , hereinafter referred to as 'the common cause criterion' and 'the pretreatment criterion', respectively. However, in response to Rubin (2007), in a series of letters to the editor and author's replies (Shrier, 2008; Rubin, 2008a; Pearl, 2009b; Sjölander, 2009; Rubin, 2009) and later on in VanderWeele and Shpitser (2011) it was discussed under what circumstances conditioning on the covariate set defined by the common cause criterion or the pretreatment criterion will in fact induce bias in the causal effect estimate instead of reducing it. In an attempt to mediate between the standpoints of Pearl, Shrier, Sjölander and Rubin VanderWeele and Shpitser (2011) proposed an alternative covariate selection criterion, 'the disjunctive cause criterion'. ...
July 2009
... "Rogue cells" are cells with multiple and complex chromosomal aberrations (e.g., dicentric, tricentric, translocations, insertions, deletions, and acentric chromosomes) related to the activation of viral infection [100,101]. A significant increase in induced chromosomal aberrations has been detected in the presence of rogue cells [102][103][104][105]. Further studies are needed to investigate the role of viral infection in the formation of radiation-induced chromosomal aberrations. ...
October 2009
Annals of Oncology
... 50 Clinical trials involving the HRS3 antibody began in the early 1990s, focusing on biodistribution studies in patients with cHL. 51 The HRS3 binding module has an affinity of 25 nM. It was successfully humanized for CAR-T cell therapy, proving to be non-inferior in anti-tumor activity compared to the original antibody in the NCG mice model. ...
October 1992
Annals of Oncology
... The survival benefit is more difficult to determine, although there are data suggesting a longer OS for patients treated with higher single doses (400 mCi) and in patients showing a symptomatic response and biochemical improvement after therapy [79]. Reported overall survival ranges from 16 months to more than 50 months [89][90][91], with a 5-year survival rate ranging from 45% to 85% [82,85]. ...
October 1991
Journal of nuclear biology and medicine (Turin, Italy: 1991)
... 154 It was hypothesized that somatic mutations in TSHR may be present in thyroid tumors following the identification of somatic activating Gα S mutations in pituitary adenoma and thyroid tumors. 155,156 In 1993, heterozygous mutations in TSHR were identified in the tumor tissue of three patients which affected two residues in ICL3. 154 This led to constitutive activation of adenylyl cyclase, and therefore was mechanistically similar to the 10 TSHR can couple to both G s -AC-cAMP and G q/11 -PLC pathways. ...
Reference:
GPCR's and Endocrinology
May 1991
Oncogene