High‐dose radioimmunotherapy combined with extracorporeal depletion in a syngeneic rat tumor model

Mårtensson, Linda; Nilsson, Rune; Ohlsson, Tomas; Sjögren, Hans‐Olov; Strand, Sven‐Erik; Tennvall, Jan

doi:10.1002/cncr.24791

Cited by 13 publications

(13 citation statements)

References 38 publications

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“…12 Må rtensson et al showed that treatment with the MTD resulted in CR in all animals, although metastases were found in 3 of 6 rats. This indicated the need for maintenance treatment.…”

Section: Discussionmentioning

confidence: 99%

“…[8][9][10][11] In an effort to improve RIT, we have used a syngeneic rat colon carcinoma model utilizing the cell line BN7005, in which a complete response (CR) of inoculated tumors was achieved after a single administration of RIT consisting of 177 Lu-labeled mAbs, but with the development of distant metastases in about half of the animals after the treatment. 12 In the present study, we evaluate whether consolidation therapy with unlabeled antibodies after RIT enhances the therapeutic effect and/or delays the clinical symptoms of metastatic disease. The choice of unlabeled antibodies for consolidation therapy is based on the well-established therapeutic effects of various unlabeled antibodies in clinical cancer care.…”

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confidence: 99%

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Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Eriksson

Ohlsson²,

Nilsson³

et al. 2012

Cancer Biotherapy and Radiopharmaceuticals

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Metastatic disease after successful treatment of the primary tumor continues to be a therapeutic challenge. Enhancement of therapeutic effects by the administration of unlabeled monoclonal antibodies (mAbs) after radioimmunotherapy (RIT) may provide a means of preventing or delaying the development of metastatic disease. In the present study, Brown Norway rats with syngeneic grafted colon carcinomas were administered the minimal effective therapeutic dose of 400 MBq/kg lutetium-177 ( 177 Lu)-DOTA-BR96. After 2 weeks, half of the animals were given 15 mg/kg unlabeled mAb BR96 as consolidation therapy. Treatment response and toxicity were monitored 100 days after the treatment with unlabeled BR96. The treatment with unlabeled mAb after RIT resulted in a complete response (CR) in 19 of 19 animals, while RIT alone resulted in a CR in 17 of 19 animals. The additional treatment did not affect the number of animals with metastatic disease or the time to clinical symptoms of metastases. RIT resulted in reversible myelotoxicity. The unlabeled mAb BR96 did not cause any additional toxicity, making it possible to repeat the consolidation therapy.

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“…12 Må rtensson et al showed that treatment with the MTD resulted in CR in all animals, although metastases were found in 3 of 6 rats. This indicated the need for maintenance treatment.…”

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Eriksson

Ohlsson²,

Nilsson³

et al. 2012

Cancer Biotherapy and Radiopharmaceuticals

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“…[76][77][78][79][80][81] In a series of studies, Tennvall et al have demonstrated the utility of extracorporeal affinity adsorption using avidin columns to deplete biotinylated radiolabeled antibodies from circulation. [82][83][84][85][86][87][88][89][90][91][92] In one of the earliest demonstrations of the approach using athymic rats bearing human melanoma and lung cancer xenografts, removal of biotinylated 125 I-labeled antimelanoma (MAb 96.5) and anticarcinoma (MAb L6) antibodies improved the tumor to normal tissue ratios by a factor of four or five. 91 Subsequent studies using a syngeneic model of colorectal cancer in rats with chimeric anti-Lewis Y antibody BR96 demonstrated the benefits of immunoadsorption from the whole blood.…”

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confidence: 99%

“…Direct experimental evidence for the utility of extracorporeal affinity adsorption for increasing the maximum tolerated dose (MTD) of the 90 Y-and 177 Lulabeled BR96 was recently reported. 82 Antibodies were radiolabeled with a trifunctional chelating agent 1033, which contains DOTA and biotin. While the MTDs for 177 Lu-1033-BR96 and 90 Y-1033-BR96 are close to 600 and 350 MBq/kg, respectively, extracorporeal affinity adsorption allowed for administration of 1200 MBq/kg 177 Lu-1033-BR96 and 525 MBq/kg of 90 Y-1033-BR96 without any noticeable increase in the toxicity.…”

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confidence: 99%

“…While the MTDs for 177 Lu-1033-BR96 and 90 Y-1033-BR96 are close to 600 and 350 MBq/kg, respectively, extracorporeal affinity adsorption allowed for administration of 1200 MBq/kg 177 Lu-1033-BR96 and 525 MBq/kg of 90 Y-1033-BR96 without any noticeable increase in the toxicity. 82 The feasibility and utility of extracorporeal elimination of radioimmunoconjugates has also been demonstrated in human subjects. In lung and breast carcinoma patients, Lear et al tested the utility of extracorporeal immunoadsorption of 111 In-labeled murine antibody using a goat anti-mouse antibody column.…”

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confidence: 99%

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Emerging Trends for Radioimmunotherapy in Solid Tumors

Jain

Gupta

Kaur

et al. 2013

Cancer Biotherapy and Radiopharmaceuticals

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Due to its ability to target both known and occult lesions, radioimmunotherapy (RIT) is an attractive therapeutic modality for solid tumors. Poor tumor uptake and undesirable pharmacokinetics, however, have precluded the administration of radioimmunoconjugates at therapeutically relevant doses thereby limiting the clinical utility of RIT. In solid tumors, efficacy of RIT is further compromised by heterogeneities in blood flow, tumor stroma, expression of target antigens and radioresistance. As a result significant efforts have been invested toward developing strategies to overcome these impediments. Further, there is an emerging interest in exploiting shortrange, high energy a-particle emitting radionuclides for the eradication of minimal residual and micrometastatic disease. As a result several modalities for localized therapy and models of minimal disease have been developed for preclinical evaluation. This review provides a brief update on the recent efforts toward improving the efficacy of RIT for solid tumors, and development of RIT strategies for minimal disease associated with solid tumors. Further, some of promising approaches to improve tumor targeting, which showed promise in the past, but have now been ignored are also discussed.

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Hematological, biochemical, and toxicopathic effects of subchronic acetamiprid toxicity in Wistar rats

Chakroun

Ezzi

Grissa

et al. 2016

Environ Sci Pollut Res

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Acetamiprid is one of the most widely used neonicotinoids. This study investigates toxic effects of repeated oral administration of three doses of acetamiprid (1/20, 1/10, and 1/5 of LD) during 60 days. For this, male Wistar rats were divided into four different groups. Hematological, biochemical, and toxicopathic effects of acetamiprid were evaluated. According to the results, a significant decrease in the body weight gain at the highest dose 1/5 of LD of acetamiprid was noticed. An increase in the relative liver weight was also observed at this dose level. The hematological constituents were affected. A significant decrease in RBC, HGB, and HCT in rats treated with higher doses of acetamiprid (1/10 and 1/5 of LD) was noted. However, a significant increase in WBC and PLT were observed at the same doses. Furthermore, acetamiprid induced liver toxicity measured by the increased activities of aspartate aminotransferase (AST), alanine aminotransferase (ALT), alkaline phosphates (ALPs), and lactate dehydrogenase (LDH) which may be due to the loss of hepatic membrane architecture and hepatocellular damage. In addition, exposure to acetamiprid resulted in a significant decrease in the levels of superoxide dismutase and catalase activities (p ≤ 0.01) with concomitant increase in lipid peroxidation in rat liver. These findings highlight the subchronic hepatotoxicity of acetamiprid.

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High‐dose radioimmunotherapy combined with extracorporeal depletion in a syngeneic rat tumor model

Cited by 13 publications

References 38 publications

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Emerging Trends for Radioimmunotherapy in Solid Tumors

Hematological, biochemical, and toxicopathic effects of subchronic acetamiprid toxicity in Wistar rats

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High‐dose radioimmunotherapy combined with extracorporeal depletion in a syngeneic rat tumor model

Cited by 13 publications

References 38 publications

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with 177Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with 177Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Emerging Trends for Radioimmunotherapy in Solid Tumors

Hematological, biochemical, and toxicopathic effects of subchronic acetamiprid toxicity in Wistar rats

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Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model