Preparation and preclinical evaluation of humanised A33 immunoconjugates for radioimmunotherapy

King, D. J.; Antoniw, Pari; Owens, Raymond J.; Adair, John R.; Haines, A. M. R.; Farnsworth, A. P.; Finney, Helene; Lawson, A D; Lyons, A.; Baker, Terry

doi:10.1038/bjc.1995.516

Cited by 69 publications

(65 citation statements)

References 23 publications

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“…It is also expressed on normal colonic epithelial cells but no other normal tissues (6). The humanized IgG1 antibody huA33 has high affinity for its target antigen (9), is internalized on binding, and is safe and tolerable when given to patients alone (10,11), in combination with chemotherapy (12), and when radiolabeled (13). 131 I-huA33 can cause targeted delivery of radiation to colon cancer cells and is retained in the tumor for 6 wk (13).…”

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confidence: 99%

Targeted Chemoradiation in Metastatic Colorectal Cancer: A Phase I Trial of ¹³¹I-huA33 with Concurrent Capecitabine

et al. 2014

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huA33 is a humanized antibody that targets the A33 antigen, which is highly expressed in intestinal epithelium and more than 95% of human colon cancers but not other normal tissues. Previous studies have shown huA33 can target and be retained in a metastatic tumor for 6 wk but eliminated from normal colonocytes within days. This phase I study used radiolabeled huA33 in combination with capecitabine to target chemoradiation to metastatic colorectal cancer. The primary objective was safety and tolerability of the combination of capecitabine and 131 I-huA33. Pharmacokinetics, biodistribution, immunogenicity, and tumor response were also assessed. Methods: Eligibility included measurable metastatic colorectal cancer, adequate hematologic and biochemical function, and informed consent. An outpatient scout 131 I-huA33 dose was followed by a single-therapy infusion 1 wk later, when capecitabine was commenced. Dose escalation occurred over 5 dose levels. Patients were evaluated weekly, with tumor response assessment at the end of the 12-wk trial. Tumor targeting was assessed using a γ camera and SPECT imaging. Results: Nineteen eligible patients were enrolled. The most frequently observed toxicity included myelosuppression, gastrointestinal symptoms, and asymptomatic hyperbilirubinemia. Biodistribution analysis demonstrated excellent tumor targeting of the known tumor sites, expected transient bowel uptake, but no other normal tissue uptake. 131 I-huA33 demonstrated a mean terminal half-life and serum clearance suited to radioimmunotherapy (T 1/2 β, 100.24 ± 20.92 h, and clearance, 36.72 ± 8.01 mL/h). The mean total tumor dose was 13.8 ± 7.6 Gy (range, 5.1-26.9 Gy). One patient had a partial response, and 10 patients had stable disease. Conclusion: 131 I-huA33 achieves specific targeting of radiotherapy to colorectal cancer metastases and can be safely combined with chemotherapy, providing an opportunity to deliver chemoradiation specifically to metastatic disease in colorectal cancer patients.

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Targeted Chemoradiation in Metastatic Colorectal Cancer: A Phase I Trial of ¹³¹I-huA33 with Concurrent Capecitabine

et al. 2014

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“…In view of the long retention time of mAb A33 in tumors, high tumor uptake, and minimal gut toxicity observed in these trials, a humanized version of mAb A33 was constructed to enable repeated dosing without immunogenicity (21). Two phase I trials with huA33 have been conducted, with huA33 alone and huA33 with chemotherapy in patients with colorectal carcinoma (22,23).…”

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A Phase I Trial of Humanized Monoclonal Antibody A33 in Patients with Colorectal Carcinoma: Biodistribution, Pharmacokinetics, and Quantitative Tumor Uptake

Scott

Lee

Jones³

et al. 2005

Clinical Cancer Research

110

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“…We have been evaluating alternative reagents comprising multivalent Fab's produced by chemical cross-linking. Chemically cross-linked di-Fab (DFM) and tri-Fab (TFM) have been prepared from the mouse-human chimeric Fab' fragment of B72.3 (King et al, 1994) and an engineered human form of the antibody (King et al, 1995). Biodistribution studies with these antibodies have revealed higher tumour accumulation than seen with scFvs, although clearance from the blood is still rapid.…”

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Preparation, characterisation and tumour targeting of cross-linked divalent and trivalent anti-tumour Fab' fragments

Casey

King²,

Chaplin³

et al. 1996

Br J Cancer

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Summary The monoclonal anti-CEA antibody, A5B7, has previously been administered to patients for radioimmunotherapy (RIT). Long circulation time and the formation of an immune response have limited therapeutic success in the clinic. Antibody fragments can be used to reduce the in vivo circulation time, but the best combination of fragment and radioisotope to use for therapy is far from clear. In this study we have compared the biodistribution of A5B7 IgG and F(ab')2 with chemically cross-linked divalent (DFM) and trivalent (TFM) A5B7 Fab' fragments in nude mice bearing human colorectal tumour xenografts. The crosslinkers were designed to allow site-specific labelling using yttrium 90 (90Y), a high-energy f-emitter. We have also compared the above antibody forms conjugated to both 13'I and 9'Y. Both DFM and TFM were fully immunoreactive and remained intact after radiolabelling and incubation in serum at 37°C for 24 h. Biodistribution results showed similar tumour uptake levels and an identical blood clearance pattern for F(ab')2 and DFM with high tumour-blood ratios generated in each case. However, unacceptably high kidney accumulation for both F(ab')2 and DFM and elevated splenic uptake of DFM labelled with 9'Y was observed.Kinetic analysis of antigen binding revealed that DFM had the fastest association rate (kass = 1.6 x 105 Ms-1) of the antibody forms, perhaps owing to increased flexibility of the cross-linker. This advantage implies that DFM may be more suitable than F(ab')2 radiolabelled with 13'I for RIT. TFM cleared from the blood significantly faster than A5B7 IgG when labelled with both 13'I and 9'Y, producing an improved therapeutic tumour-blood ratio. Kidney accumulation was not observed for [90Y]TFM, but a slightly higher splenic uptake was observed that may indicate reticuloendothelial system (RES) uptake. Overall, tumour uptake was higher for 90Y-labelled antibodies than for '3'I-labelled antibodies. Because of the faster clearance, it should be possible to administer a higher total dose of 90Y-labelled TFM than IgG, which is attractive for RIT. Both A5B7 DFM and TFM, therefore, show favourable properties compared with their parent antibody forms.

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Preparation and preclinical evaluation of humanised A33 immunoconjugates for radioimmunotherapy

Cited by 69 publications

References 23 publications

Targeted Chemoradiation in Metastatic Colorectal Cancer: A Phase I Trial of ¹³¹I-huA33 with Concurrent Capecitabine

Targeted Chemoradiation in Metastatic Colorectal Cancer: A Phase I Trial of ¹³¹I-huA33 with Concurrent Capecitabine

A Phase I Trial of Humanized Monoclonal Antibody A33 in Patients with Colorectal Carcinoma: Biodistribution, Pharmacokinetics, and Quantitative Tumor Uptake

Preparation, characterisation and tumour targeting of cross-linked divalent and trivalent anti-tumour Fab' fragments

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Preparation and preclinical evaluation of humanised A33 immunoconjugates for radioimmunotherapy

Cited by 69 publications

References 23 publications

Targeted Chemoradiation in Metastatic Colorectal Cancer: A Phase I Trial of 131I-huA33 with Concurrent Capecitabine

Targeted Chemoradiation in Metastatic Colorectal Cancer: A Phase I Trial of 131I-huA33 with Concurrent Capecitabine

A Phase I Trial of Humanized Monoclonal Antibody A33 in Patients with Colorectal Carcinoma: Biodistribution, Pharmacokinetics, and Quantitative Tumor Uptake

Preparation, characterisation and tumour targeting of cross-linked divalent and trivalent anti-tumour Fab' fragments

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Targeted Chemoradiation in Metastatic Colorectal Cancer: A Phase I Trial of ¹³¹I-huA33 with Concurrent Capecitabine

Targeted Chemoradiation in Metastatic Colorectal Cancer: A Phase I Trial of ¹³¹I-huA33 with Concurrent Capecitabine