Combination Photoimmunotherapy and Cisplatin: Effects on Human Ovarian Cancer Ex Vivo

doi:10.1093/jnci/91.18.1557

JNCI Journal of the National Cancer Institute 1999 91(18):1557-1563; doi:10.1093/jnci/91.18.1557
© 1999 by Oxford University Press

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Journal of the National Cancer Institute, Vol. 91, No. 18, 1557-1563, September 15, 1999
© 1999 Oxford University Press

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Combination Photoimmunotherapy and Cisplatin: Effects on Human Ovarian Cancer Ex Vivo

Linda R. Duska, Michael R. Hamblin, Jaimie L. Miller, Tayyaba Hasan

Affiliations of authors: L. R. Duska, Wellman Laboratories of Photomedicine and Vincent Memorial Obstetrics and Gynecology Service, Harvard Medical School, Massachusetts General Hospital, Boston; M. R. Hamblin, J. L. Miller, T. Hasan, Department of Dermatology, Wellman Laboratories of Photomedicine, Harvard Medical School, Massachusetts General Hospital.

Correspondence to: Tayyaba Hasan, Ph.D., Department of Dermatology, Wellman Laboratories of Photomedicine, Harvard Medical School, Massachusetts General Hospital, 55 Fruit St., Boston, MA 02114 (e-mail: hasan{at}helix.harvard.mgh.edu).

BACKGROUND: Patients with ovarian cancer that is clinicallyresistant to cisplatin-based chemotherapy have little hope ofa cure of their disease. Photoimmunotherapy, which involvesthe antibody-targeted delivery of a nontoxic photosensitizerthat is activated to a cytotoxic state with visible light, mayoffer a new treatment option. Photoimmunotherapy may be applied intraperitoneallyto target disseminated tumor. We tested the hypothesis thatthis treatment in combination with cisplatin potentiates cytotoxicityin ovarian cancer cell lines and primary cultures of human tumors.METHODS: Five human cancer cell lines (ovarian and breast) and19 primary cultures were studied. The primary cultures werefrom solid and ascites tumor samples obtained from 14 patientswith ovarian cancer who were undergoing primary surgery. The photosensitizerchlorin e₆ was conjugated to the F(ab')₂ fragment of the murinemonoclonal antibody OC-125, which is directed against the antigenCA 125. Cytotoxicity was measured by the microculture tetrazoliumassay. Treatments consisted of cisplatin alone, photoimmunotherapyalone, and photoimmunotherapy followed by cisplatin. The fractionalproduct method was used to assess synergy in treatment effects.Ex vivo cultured human cells exhibiting 80% or greater survivalat cisplatin concentrations of 10 µM for 24 hours weredefined as cisplatin resistant for this study. RESULTS: When allcell types (cisplatin sensitive and cisplatin resistant) wereconsidered together, combination treatment yielded cytotoxicitythat was, on average, 6.9 times (95% confidence interval = 1.86-11.94)greater than that of cisplatin alone (two-sided P = .023). Cisplatin-resistantcells showed a synergistic effect of the two treatments (two-sidedP = .044), while cisplatin-sensitive cells showed an additiveeffect. CONCLUSION: These ex vivo data suggest that platinumresistance in human ovarian cancer cells may be reversible bypretreatment with OC-125-targeted photoimmunotherapy. Furtherstudies are required to confirm the efficacy of this approachin vivo.

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