Conclusion Our results on nuclear expression of HIF-1α were quite opposite to studies that describe nHIF-1α overexpression as a marker of unfavorable prognosis in human cancer [27–29]. Discrepancies between studies may reflect the balance of multiple effects of HIF status with compartmentalization according to specific functional moments. The HIF-1α mediated hypoxia response is therefore complex and different pathways are likely to be activated in different cell types. In conclusion,
the results obtained selleckchem in this study highlight the more aggressive subtype of CCRCC, associated with overexpression of VEGF-A and cHIF-1α, which may have some clinical implication. Additional studies are needed to understand the significance of nHIF-1α expression associated with better-differentiated tumors. Acknowledgements This work was supported by the Ministry of Science, Education
and Sports of the Republic of Croatia (grant 062-0620095-0082). We are also grateful to Mr. Ozren Štanfel for the excellent technical assistance. References find more 1. Folkman J: Tumor angiogenesis: therapeutic implications. N Engl J Med 1971, 285: 1182–6.CrossRefPubMed 2. Gunningham SP, Currie MJ, Han C, Turner K, Scott PA, Robinson BA, Harris AL, Fox SB: Vascular endothelial growth factor-B and vascular endothelial growth factor-C expression in renal cell carcinomas: regulation by the von Hippel-Lindau gene and hypoxia.
Cancer Res 2001, 61: 3206–11.PubMed 3. Eble JN, Sauter G, Epstein JI, Sesterhenn IA: WHO Classification of Tumours. Rabusertib Pathology and Genetics of Tumours of the Urinary System and Male Genital Organs. Volume 6. IARC Press, Lyon (France); 2004:9–87. 4. Brieger J, Weidt EJ, Schirmacher P, Störkel S, Huber C, Decker HJ: Inverse regulation of Cetuximab datasheet vascular endothelial growth factor and VHL tumor suppressor gene in sporadic renal cell carcinomas is correlated with vascular growth: an in vivo study on 29 tumors. J Mol Med 1999, 77: 505–10.CrossRefPubMed 5. Maranchie JK, Vasselli JR, Riss J, Bonifacino JS, Linehan WM, Klausner RD: The contribution of VHL substrate binding and HIF1-alpha to the phenotype of VHL loss in renal cell carcinoma. Cancer Cell 2002, 1: 247–55.CrossRefPubMed 6. Strefford JC, Stasevich I, Lane TM, Lu YJ, Oliver T, Young BD: A combination of molecular cytogenetic analyses reveals complex genetic alterations in conventional renal cell carcinoma. Cancer Genet Cytogenet 2005, 159: 1–9.CrossRefPubMed 7. Kondo K, Klco J, Nakamura E, Lechpammer M, Kaelin WG Jr: Inhibition of HIF is necessary for tumor suppression by the von Hippel-Lindau protein. Cancer Cell 2002, 1: 237–46.CrossRefPubMed 8. Staehler M, Haseke N, Schoeppler G, Stadler T, Gratzke C, Stief C: Modern therapeutic approaches in Metastatic Renal cell carcinoma. EAU-EBU Update series 2007, 5: 26–37.CrossRef 9.