Nuclear Medicine and Biology
Volume 36, Issue 6 , Pages 659-669, August 2009

Treatment of HER2-positive breast carcinomatous meningitis with intrathecal administration of α-particle-emitting 211At-labeled trastuzumab

  • Abraham Boskovitz

      Affiliations

    • Department of Pathology, Duke University Medical Center, Durham, NC 27710 USA
    • ,
  • Roger E. McLendon

      Affiliations

    • Department of Pathology, Duke University Medical Center, Durham, NC 27710 USA
    • ,
  • Tatsunori Okamura

      Affiliations

    • Department of Pathology, Duke University Medical Center, Durham, NC 27710 USA
    • ,
  • John H. Sampson

      Affiliations

    • Department of Surgery, Duke University Medical Center, Durham, NC 27710 USA
    • ,
  • Darell D. Bigner

      Affiliations

    • Department of Pathology, Duke University Medical Center, Durham, NC 27710 USA
    • ,
  • Michael R. Zalutsky

      Affiliations

    • Department of Radiology, Duke University Medical Center, Durham, NC 27710 USA
    • Corresponding Author InformationCorresponding author. Tel.: +1 919 684 7708; fax: +1 919 684 7121.

Received 28 January 2009; received in revised form 19 February 2009; accepted 2 April 2009.

Abstract 

Introduction

Carcinomatous meningitis (CM) is a devastating disease characterized by the dissemination of malignant tumor cells into the subarachnoid space along the brain and spine. Systemic treatment with monoclonal antibody (mAb) trastuzumab can be effective against HER2-positive systemic breast carcinoma but, like other therapies, is ineffective against CM. The goal of this study was to evaluate the therapeutic effect of α-particle emitting 211At-labeled trastuzumab following intrathecal administration in a rat model of breast carcinoma CM.

Methods

Athymic rats were injected intrathecally with MCF-7/HER2-18 breast carcinoma cells through a surgically implanted indwelling intrathecal catheter. In Experiment 1, animals received 33 or 66 μCi 211At-labeled trastuzumab, cold trastuzumab or saline. In Experiment 2, animals were inoculated with a lower tumor burden and received 46 or 92 μCi 211At-labeled trastuzumab or saline. In Experiment 3, animals received 28 μCi 211At-labeled trastuzumab, 30 μCi 211At-labeled TPS3.2 control mAb or saline. Histopathological analysis of the neuroaxis was performed at the end of the study.

Results

In Experiment 1, median survival increased from 21 days for the saline and cold trastuzumab groups to 45 and 48 days for 33 and 66 μCi 211At-labeled trastuzumab, respectively. In Experiment 2, median survival increased from 23 days for saline controls to 68 and 92 days for 46 and 92 μCi 211At-labeled trastuzumab, respectively. In Experiment 3, median survival increased from 20 days to 29 and 36 days for animals treated with 211At-labeled TPS3.2 and 211At-labeled trastuzumab, respectively. Long-term survivors were observed exclusively in the 211At-trastuzumab-treated groups.

Conclusion

Intrathecal 211At-labeled trastuzumab shows promise as a treatment for patients with HER2-positive breast CM.

Keywords: Astatine-211, Radioimmunotherapy, Trastuzumab, HER2, Targeted radiotherapy

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 This work was supported by Grants CA42324 and NS20023 from the National Institutes of Health and Grant DOE-FG02-08ER64697 from the Department of Energy.

PII: S0969-8051(09)00087-0

doi:10.1016/j.nucmedbio.2009.04.003

Nuclear Medicine and Biology
Volume 36, Issue 6 , Pages 659-669, August 2009

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