In vitro evaluation of 213Bi-rituximab versus external gamma irradiation for the treatment of B-CLL patients: relative biological efficacy with respect to apoptosis induction and chromosomal damage

Vandenbulcke, Katia; Vos, Filip De; Offner, Fritz; Philippé, Jan; Apostolidis, Christos; Molinet, R.; Nikula, Tuomo; Bacher, Klaus; Gelder, Virginie de; Vral, Anne; Lahorte, Christophe; Thierens, Hubert; Dierckx, Rudi; Slegers, Guido

doi:10.1007/s00259-003-1228-8

Cited by 33 publications

(12 citation statements)

References 38 publications

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“…Hence, the findings demonstrate that translocations are a biological marker responding to the external gamma-ray exposure when concerning mixed radiation exposures. This may be correlated with a higher RBE and a higher long-term toxicity by alpha emitters (Vandenbulcke et al 2003) leading to depletion of lethally hit lymphocytes with time.…”

Section: Resultsmentioning

confidence: 99%

mFISH analysis of chromosome aberrations in workers occupationally exposed to mixed radiation

Sotnik

Osovets

Scherthan

et al. 2014

Radiat Environ Biophys

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We performed a study on the presence of chromosome aberrations in a cohort of plutonium workers of the Mayak production association (PA) with a mean age of 73.3 ± 7.2 years to see whether by multi-color fluorescence in situ hybridization (mFISH) translocation analysis can discriminate individuals who underwent occupational exposure with internal and/or external exposure to ionizing radiation 40 years ago. All Mayak PA workers were occupationally exposed to chronic internal alpha-radiation due to incorporated plutonium-239 and/or to external gamma-rays. First, we obtained the translocation yield in control individuals by mFISH to chromosome spreads of age-matched individuals and obtained background values that are similar to previously published values of an international study (Sigurdson et al. in Mutat Res 652:112-121, 2008). Workers who had absorbed a total dose of >0.5 Gy external gamma-rays to the red bone marrow (RBM) displayed a significantly higher frequency of stable chromosome aberrations relative to a group of workers exposed to <0.5 Gy gamma-rays total absorbed RBM dose. Thus, the translocation frequency may be considered to be a biological marker of external radiation exposure even years after the exposure. In a group of workers who were internally exposed and had incorporated plutonium-239 at a body burden >1.48 kBq, mFISH revealed a considerable number of cells with complex chromosomal rearrangements. Linear associations were observed for translocation yield with the absorbed RBM dose from external gamma-rays as well as for complex chromosomal rearrangements with the plutonium-239 body burden.

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Section: Resultsmentioning

confidence: 99%

mFISH analysis of chromosome aberrations in workers occupationally exposed to mixed radiation

Sotnik

Osovets

Scherthan

et al. 2014

Radiat Environ Biophys

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“…4 This makes them highly cytotoxic with a relative biologic effectiveness 5-20 times that of b À -particles. 5,6 Another advantage of a-particles, compared with b À -particles, is that they exhibit a low dependence on dose rate and oxygen enhancement effects. 7 Astatine-211 is the heaviest halogen and it is one of the most promising a-emitters for medical applications.…”

Section: Introductionmentioning

confidence: 99%

Feasibility of the radioastatination of a monoclonal antibody with astatine‐211 purified by wet extraction

Bourgeois

Guérard

Alliot

et al. 2008

Labelled Comp Radiopharmac

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Astatine-211, a most promising α-particle emitter for targeted radiotherapy, is generally obtained by high-temperature distillation. However, a liquid-liquid extraction procedure (wet extraction) has also been described. The purpose of this study was to develop and optimize the labelling of the stannylated-activated ester N-hydroxysuccinimidyl-meta-trimethylstannylbenzoate ester (MeSTB) with astatine-211 extracted in di-isopropylether (DIPE) in the presence of the oxidant N-chlorosuccinimide (NCS). The effect of final volume, incubation duration and NCS amounts on radiolabelling yield was studied. The best yields (85-90%) of N-hydroxysuccinimidyl-meta-[(211)At]astatobenzoate ester (SAB) were obtained with 20 nmol of MeSTB, 100 nmol of NCS in 120 µL of DIPE after 15 min. The astatine-211-labelled-activated ester was then used to radiolabel a monoclonal antibody (mAb). The labelling yield was 20-25% and the radiochemical purity was 97-99%. These results show that mAbs may be efficiently labelled with astatine-211 obtained by wet extraction, a fully automatable technique that may prove to be a useful alternative to dry distillation for high activity labelling of radiopharmaceuticals. Copyright © 2008 John Wiley & Sons, Ltd.

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“…Insight into these mechanisms could lead to improved strategies for radioimmunotherapy with a-emitters. Incubation of human prostate cancer cells and lymphocytes from leukemia patients with 213 Bi-immunoconjugates has been reported to activate apoptotic pathways (11,12), whereas treatment of gastric cancer cells expressing d9-E-cadherin with 213 Bi-d9MAb triggered nonapoptotic pathways (10).…”

Section: Introductionmentioning

confidence: 99%

“…BrdUrd was removed completely by repeated washings with BrdUrd-free culture medium. At defined time points after start of irradiation (4,6,12, and 24 h), cells were detached with 1 mmol/L EDTA in PBS and fixed in 80% ethanol. For preparation of nuclei, cells were treated with RNase A (Sigma) and subsequently incubated with pepsin (Merck; 0.7 FIP-U/mg; 5% in 0.05 N HCl) for 10 min at 37jC.…”

mentioning

confidence: 99%

213Bi-induced death of HSC45-M2 gastric cancer cells is characterized by G2 arrest and up-regulation of genes known to prevent apoptosis but induce necrosis and mitotic catastrophe

Seidl¹,

Port

Gilbertz

et al. 2007

Molecular Cancer Therapeutics

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Tumor cells are efficiently killed after incubation with A-emitter immunoconjugates targeting tumor-specific antigens. Therefore, application of A-emitter immunoconjugates is a promising therapeutic option for treatment of carcinomas that are characterized by dissemination of single tumor cells in the peritoneum like ovarian cancer or gastric cancer. In diffuse-type gastric cancer, 10% of patients express mutant d9-E-cadherin on the surface of tumor cells that is targeted by the monoclonal antibody d9MAb. Coupling of the A-emitter 213 Bi to d9MAb provides an efficient tool to eliminate HSC45-M2 gastric cancer cells expressing d9-E-cadherin in vitro and in vivo. Elucidation of the molecular mechanisms triggered by A-emitters in tumor cells could help to improve strategies of A-emitter radioimmunotherapy. For that purpose, gene expression of 213 Bi-treated tumor cells was quantified using a real time quantitative-PCR low-density array covering 380 genes in combination with analysis of cell proliferation and the mode of cell death. We could show that 213 Bi-induced cell death was initiated by G 2 arrest; up-regulation of tumor necrosis factor (TNF), SPHK1, STAT5A, p21, MYT1, and SSTR3; and down-regulation of SPP1, CDC25 phosphatases, and of genes involved in chromosome segregation. Together with morphologic changes, these results suggest that 213 Bi activates death cascades different from apoptosis. Furthermore, 213 Bitriggered up-regulation of SSTR3 could be exploited for improvement of the therapeutic regimen. [Mol Cancer Ther 2007;6(8):2346 -59]

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In vitro evaluation of 213Bi-rituximab versus external gamma irradiation for the treatment of B-CLL patients: relative biological efficacy with respect to apoptosis induction and chromosomal damage

Cited by 33 publications

References 38 publications

mFISH analysis of chromosome aberrations in workers occupationally exposed to mixed radiation

mFISH analysis of chromosome aberrations in workers occupationally exposed to mixed radiation

Feasibility of the radioastatination of a monoclonal antibody with astatine‐211 purified by wet extraction

213Bi-induced death of HSC45-M2 gastric cancer cells is characterized by G2 arrest and up-regulation of genes known to prevent apoptosis but induce necrosis and mitotic catastrophe

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