Folia Biologica
Journal of Cellular and Molecular Biology, Charles University 

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Fol. Biol. 2003, 49, 26-32

https://doi.org/10.14712/fb2003049010026

Local IFN-γ Therapy of HPV16-Associated Tumours

Romana Mikyšková1, J. Bieblová1, J. Šímová1, M. Indrová1, T. Jandlová1, V. Vonka2, M. Šmahel2, J. Bubeník1, L. Mendoza1

1Institute of Molecular Genetics, Academy of Sciences of the Czech Republic, Prague, Czech Republic
2Department of Experimental Virology, Institute of Haematology and Blood Transfusion, Prague, Czech Republic

Received October 2002
Accepted November 2002

We have examined whether peritumoral administration of IFN-γ can inhibit growth of HPV16associated, MHC class I- tumour MK16/1/IIIABC (MK16) transplanted in syngeneic mice. It has been found that peritumoral administration of recombinant IFN-γ performed on days 0-11 after tumour challenge inhibited growth of MK16 s.c. tumour transplants. If the therapy with IFN-γ was started when the tumours had already reached a palpable size, the IFN-γ administration was without any effect. To investigate the antitumour effects of IFN-γ in a clinically more relevant setting, surgical minimal residual tumour disease was utilized. Subcutaneously growing MK16 carcinomas, 8-12 mm in diameter, were removed and the operated mice were injected with IFN-γ on days 3-14 after the operation at the site of surgery. Treatment with IFN-γ resulted in a moderate, reproducible, but statistically insignificant inhibition of tumour recurrences. In the next experiments we have addressed the question whether the tumour-inhibitory effect of IFN-γ was due to the upregulation of MHC class I molecule expression on MK16 tumour cells. IFN-γ-treated and control mice were sacrificed, their tumours were explanted, and the expression of MHC class I molecules on the MK16 tumour cells was examined. As presumed, the MHC class I expression on the cells of IFN-γ-treated tumours, as well as on their lung metastases, was upregulated. However, an unexpected moderate upregulation of the MHC class I expression was also observed on MK16 tumours from the control, exogenous IFN-γ-uninjected mice. Cytofluorometric analysis of the in vivo transplanted MK16 tumours from both groups has excluded that the increased percentage of the MHC class I molecules on the tumour cell populations could be due to the infiltration of the tumours with MHC class I+ leukocytes, since no expression of MHC class II, CD11b, CD80/CD86, and CD11c molecules in the MK16 cell population was observed.

Funding

This work was supported by grants Nos. NC 7148-3 and NC5900-3 from the Grant Agency of the Ministry of Health of the Czech Republic, No. 301/01/0985 from the Grant Agency of the Czech Republic and by the League Against Cancer, Prague.

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