Advertisement

Cancer Chemotherapy and Pharmacology

, Volume 49, Supplement 1, pp 21–24 | Cite as

Microencapsulated, CYP2B1-transfected cells activating ifosfamide at the site of the tumor: the magic bullets of the 21st century

  • Matthias Löhr
  • Frank Hummel
  • Grit Faulmann
  • Jörg Ringel
  • Robert Saller
  • Johannes Hain
  • Walter H. Günzburg
  • Brian Salmons

Heading

Abstract

Background. Conventional chemotherapy of pancreatic carcinoma is only marginally effective. This is in part due to the severity of side effects following systemic administration of the cytostatic drug. The aim was to create a therapeutic tool allowing the targeting of the conversion site of a cytotoxic prodrug to the site of the tumor. This was realized by transfection of the CYP2B1 gene, the major ifosfamide-converting P450 enzyme, in cells with subsequent microencapsulation and administration of these microcapsules to or into the tumor. The enzyme activity (resorufin assay) remained stable for weeks in vitro and in vivo within the microencapsulated CYP2B1-expressing cells. We demonstrated a significant antitumor effect of the intratumorally injected capsules against xenotransplanted human pancreatic carcinomas in the nude mouse. Angiographic experiments in the pig confirmed the feasibility of an intraarterial placement of the capsules into the pancreas. A clinical protocol was established and approved.

Patients, material and methods. L293 cells were transfected with the CYP2B1 gene, microencapsulated (diameter 0.7 mm) under GCP conditions and packed sterile. Patients with confirmed inoperable adenocarcinoma of the pancreas underwent angiography, and capsules were injected into a vessel leading into the tumor. The patients were monitored for 48 h to exclude allergic reactions or pancreatitis. A day later, ifosfamide was administered for three consecutive days to be repeated on days 21–23. The patients were followed up for 5 months.

Results. A total of 17 patients were enrolled. The patients tolerated the procedure without any complications. No allergic reactions or pancreatitis were encountered. Chemotherapy was uneventful. All patients had stable disease, and two patients a partial remission. The median survival was 44 weeks which compared favorably with that of a historical control group (22 weeks).

Conclusions. The intraarterial administration of microcapsules for targeted chemotherapy was well tolerated. Control of local tumor growth was achieved.

Ifosfamide CYP2B1-transfected cells 

Preview

Unable to display preview. Download preview PDF.

Unable to display preview. Download preview PDF.

Copyright information

© Springer-Verlag 2002

Authors and Affiliations

  • Matthias Löhr
    • 1
  • Frank Hummel
    • 1
  • Grit Faulmann
    • 1
  • Jörg Ringel
    • 1
  • Robert Saller
    • 2
  • Johannes Hain
    • 2
  • Walter H. Günzburg
    • 3
  • Brian Salmons
    • 4
  1. 1.Molecular Gastroenterology, Department of Medicine II, Medical Faculty Mannheim, University of Heidelberg, Theodor Kutzer Ufer, 68135 Mannheim, Germany
  2. 2.Bavarian Nordic Research Institute, Fraunhoferstr. 18b, 82152 Martinsried, Germany
  3. 3.Institute of Virology, University of Veterinary Sciences, Veterinärplatz 1, 1210 Vienna, Austria
  4. 4.Austrianova Biotherapeutics, Veterinärplatz 1, 1210 Vienna, Austria

Personalised recommendations