Charles-André Vogel scite author profile

Charles-André Vogel

3Publications

21Citation Statements Received

40Citation Statements Given

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Affiliations

University Hospital of Lausanne, University of Lausanne

Publications

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Carcinoembryonic antigen expression, antibody localisation and immunophotodetection of human colon cancer liver metastases in nude mice: A model for radioimmunotherapy

et al. 1996

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2Division of Nuclear Medicine,Colorectal cancer frequently disseminates through the portal vein into the liver. In this study, outbred Swiss nude mice were adapted to facilitate the induction of liver metastases by a pre-grafting treatment with 6 Gy total body irradiation and i.v.injection of anti-asialo GM I antibody. One day later, cultured LS I74T human colon cancer cells were injected into the surgically exposed spleen, which was resected 3 min later. In 48 of 65 mice, a few to several hundred liver metastases were macroscopically observed at dissection 3 to 4 weeks after transplantation. Ten of I 0 mice, followed-up for survival, died with multiple large confluent liver metastases. By reducing the radiation dose to 4 or 0 Gy, or omitting the anti-asialo GM I antibody injection, only 60%. 37% or 50% of mice, respectively, had visible metastases 3 weeks after transplantation. Carcinoembryonic antigen (CEA) measured in tumour extracts was in the mean 25.6 pg/g in liver metastases compared with 9.2 pg/g in S.C. turnours. Uptake of radiolabelled anti-CEA monoclonal antibody (MAb) in the metastases 12, 24 and 48 hr after injection gave a mean value of 39% of the injected dose per gram of tissue (ID/g). In comparison, MAb uptake in S. C. and intrasplenic turnours or lung metastases gave a mean percentage ID/g of 20, I 8 and 15, respectively. Laser-induced fluorescence after injection of Indocyanin-MAb conjugate allowed direct visual detection of small liver metastases, including some that were not visible under normal light, Preliminary results showed that mice, pre-treated with 4 Gy irradiation and the anti-asialo GM I injection, were tolerant to radioimmunotherapy with a total dose of 500 pCi I 3 ' l labeled anti-CEA intact MAbs given in 3 injections.o 1996 Wiley-Liss, Inc.

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Direct comparison of a radioiodinated intact chimeric anti-CEA MAb with its F(ab')2 fragment in nude mice bearing different human colon cancer xenografts

Vogel

Bischof-Delaloye²,

Mach³

et al. 1993

Br J Cancer

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Tumour localisation and tumour to normal tissue ratios of a chimeric anti-carcinoembryonic antigen (CEA) monoclonal antibody (MAb), in intact form and as an F(ab')2 fragment labelled with 125I and 131I, were compared in groups of nude mice bearing four different colon cancer xenografts, T380, Co112 or LoVo, of human origin, or a rat colon cancer transfected with human CEA cDNA, called '3G7'. For each tumour, three to four mice per time point were analysed 6, 12, 24, 48 and 96 h after MAb injection. In the different tumours, maximal localisation of intact MAb was obtained at 24 to 48 h, and of F(ab')2 fragment 12 to 24 h after injection. Among the different tumours, localisation was highest with colon cancer T380, with 64% of the injected dose per gram (% ID/g) for the intact MAb and 57% for its F(ab')2 fragment, while in the three other tumours, maximal localisation ranged from 14 to 22% ID g-1 for the intact MAb and was about 11% for the F(ab')2. Tumour to normal tissue ratios of intact MAb increased rapidly until 24 h after injection and remained stable or showed only a minor increase thereafter. In contrast, for the F(ab')2 fragment, the tumour to normal tissue ratios increased steadily up to 4 days after injection reaching markedly higher values than those obtained with intact MAb. For the four different xenografts, tumour to blood ratios of F(ab')2 were about 2, 3 and 5 to 16 times higher than those of intact antibodies at 12, 24 and 96 h after injection, respectively.

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Fluorescence in situ hybridization (FISH) may accurately select patients likely to benefit from herceptin monotherapy

Cobleigh¹,

Vogel²,

Tripathy³

et al. 2001

European Journal of Cancer

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