Artigo Revisado por pares

Radiation doses to non-Hodgkin's lymphoma cells and normal bone marrow exposed in vitro. Comparison of an α-emitting radioimmunoconjugate and external γ-irradiation

2002; Taylor & Francis; Volume: 78; Issue: 2 Linguagem: Inglês

10.1080/09553000110094788

ISSN

1362-3095

Autores

E Aurlien, Yngve Kvinnsland, Roy H. Larsen, Øyvind S. Bruland,

Tópico(s)

Effects of Radiation Exposure

Resumo

Purposes : The α -emitting radionuclide 211 At conjugated to the CD20 targeting chimeric monoclonal antibody rituximab was studied to: (a) Estimate radiation dose components to lymphoma and bone marrow (BM) cells exposed in vitro. (b) Calculate the mean absorbed radiation doses in various normal tissues of mice following intravenous injection. Materials and methods : B-lymphoma cells (RAEL) and normal human BM cells were incubated with increasing concentrations of the radioimmunoconjugate. Based on binding kinetics and on measured cellular and nuclear diameters, the radiation doses were calculated using microdosimetric methods. Results : Targeting of 211 At-rituximab to RAEL cells was extensive and stable compared with the binding to BM cells. The absorbed radiation doses from cell-bound activity at an initial activity concentration of 10 kBq ml -1 were 0.645 and 0.021 Gy to RAEL and BM cells, respectively. In comparison, the contribution from unbound conjugate in the medium during 1h exposure was 0.042 and 0.043 Gy. The D 0 value for RAEL cells was 0.55 Gy, but only 0.34 Gy for BM cells, whereas corresponding D 0 values were 0.72 and 1.21 Gy after a single exposure to external 60 Co γ-rays. Mean absorbed doses of 1.31, 0.48 and 0.36 Gy for blood, lungs and heart were calculated in mice injected with 5.4kBq g -1 of 211 At-rituximab. Conclusion : Despite the higher inherent sensitivity of the BM cells to the α -irradiation, there was, related to the radioactivity concentrations of 211 At-rituximab, several logs greater cell kill in RAEL cells, illustrating the tumour-specific nature of the targeting.

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