Preclinical and clinical evidence of activity of pazopanib in solitary fibrous tumour.

[severe combined immunodeficiency]

To explore the activity of pazopanib in solitary fibrous tumour (SFT ).In a preclinical study , we compared the activity of pazopanib , sorafenib , sunitinib , regorafenib , axitinib and bevacizumab in a dedifferentiated-SFT (DSFT ) xenotransplanted into Severe Combined Immunodeficiency (SCID ) mice . Antiangiogenics were administered at their reported optimal doses when mean tumour volume (TV ) was 80 mm (3 ). Drug activity was assessed as TV inhibition percentage (TVI %). From May 2012 , six consecutive patients with advanced SFT received pazopanib , on a national name-based programme . In one case sunitinib was administered after pazopanib failure .In the xenograft model , pazopanib showed the lowest antitumour activity (21 %TVI ), while regorafenib was the most active (95 %TVI ). Sorafenib , bevacizumab , sunitinib were markedly active (78 /70 /65 %TVI ). Axitinib was marginally active (51 %TVI ). In the retrospective case-series , three patients carried malignant -SFT (MSFT ), three DSFT . Best Response Evaluation Criteria in Solid Tumour (RECIST ) responses were : three stable disease (SD ), all MSFT , three progressive disease (PD ), all DSFT , corresponding to one partial response (PR ), two SD , three PD by Choi criteria . Median-progression-free survival was 3 months (range 1 -15 ). In one patient , sunitinib was started after pazopanib failure , with a response .In dedifferentiated-SFT xenograft pazopanib induced a marginal antitumour activity , while regorafenib appeared the most active and promising agent . When administered in patients , pazopanib showed a modest activity in terms of tumour growth stabilisation , observed only in non-dedifferentiated cases .