This work aimed to evaluate the influence of two chelators: DOTA(SCN) and DOTA(NHS) on radioimmunotherapy using Lu-DOTA-Rituximab preparations in murine lymphoma xenograft models. Subsequently, based on animal data, the organ radiation-absorbed doses were extrapolated to humans (adult male). Therapeutic efficacy of Lu-DOTA-Rituximab was evaluated in male nude mice bearing either Raji (B lymphocyte, CD20) and Jurkat (T lymphocyte, CD20) xenografts, utilizing an anti-CD20 antibody-Rituximab conjugate with either DOTA(SCN) or DOTA(NHS). The DOTA-Rituximab conjugates were prepared in the form of freeze-dried kits. All radioimmunoconjugates were obtained with high radiolabeling yield (radiochemical purity, RCP > 95%) and specific activity of ca. 0.5 GBq/mg. Therapeutic effects of Lu-DOTA-Rituximab were observed in animals regardless whether DOTA(SCN) or DOTA(NHS) were used for conjugation. Importantly, therapy involving Lu-DOTA-Rituximab was more effective than use of Rituximab alone. The degree of antitumor efficacy was dependent on the type of applied bifunctional chelators conjugated to mAb. However, this difference was not statistically significant. Dosimetry calculations showed that the absorbed radiation doses extrapolated to humans were very low for osteogenic cells regardless of the conjugates. Organs like the liver and spleen, treated with Lu-DOTA(SCN)-Rituximab, showed similar radiation absorbed doses when compared with Lu-DOTA(NHS)-Rituximab.
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http://dx.doi.org/10.1089/cbr.2019.3405 | DOI Listing |
Cancer Biother Radiopharm
October 2020
National Centre for Nuclear Research, Radioisotope Centre POLATOM, Research and Development Department, Otwock, Poland.
This work aimed to evaluate the influence of two chelators: DOTA(SCN) and DOTA(NHS) on radioimmunotherapy using Lu-DOTA-Rituximab preparations in murine lymphoma xenograft models. Subsequently, based on animal data, the organ radiation-absorbed doses were extrapolated to humans (adult male). Therapeutic efficacy of Lu-DOTA-Rituximab was evaluated in male nude mice bearing either Raji (B lymphocyte, CD20) and Jurkat (T lymphocyte, CD20) xenografts, utilizing an anti-CD20 antibody-Rituximab conjugate with either DOTA(SCN) or DOTA(NHS).
View Article and Find Full Text PDFIran J Pharm Res
January 2018
National Centre for Nuclear Research, Radioisotope Centre POLATOM, Otwock, Poland.
This work presents a comparative biological evaluation of Y- and Lu- labelled DOTA-SCN and DOTA-NHS conjugated to Rituximab in tumour-bearing mice. Two DOTA derivatives, p-SCN-Bn-DOTA and DOTA-NHS-ester were conjugated to Rituximab and then freeze-dried kit formulations were prepared, as previously described (1). Tissue distribution was investigated in tumour-bearing (Raji s.
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