BACKGROUND Although hepatocellular carcinoma (HCC) is one of the most vascular solid tumors, antiangiogenic therapy has not induced the expected results. AIM To uncover immunohistochemical (IHC) aspects of angiogenesis in HCC. METHODS A retrospective cohort study was performed and 50 cases of HCC were randomly selected. The angiogenesis particularities were evaluated based on the IHC markers Cyclooxygenase-2 (COX-2), vascular endothelial growth factor (VEGF) A and the endothelial area (EA) was counted using the antibodies CD31 and CD105. RESULTS The angiogenic phenotype evaluated with VEGF-A was more expressed in small tumors without vascular invasion (pT1), whereas COX-2 was rather expressed in dedifferentiated tumors developed in non-cirrhotic liver. The CD31-related EA value decreased in parallel with increasing COX-2 intensity but was higher in HCC cases developed in patients with cirrhosis. The CD105-related EA was higher in tumors developed in patients without associated hepatitis. CONCLUSION In patients with HCC developed in cirrhosis, the newly formed vessels are rather immature and their genesis is mediated via VEGF. In patients with non-cirrhotic liver, COX-2 intensity and number of mature neoformed vessels increases in parallel with HCC dedifferentiation.
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Department of Pathology, University of Medicine,Pharmacy, Sciences and TechnologyDepartment of Pathology, University of Medicine,Pharmacy, Sciences and Technology
Decebal Fodor
Ioan Jung
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Department of Pathology, University of Medicine,Pharmacy, Sciences and TechnologyDepartment of Pathology, University of Medicine,Pharmacy, Sciences and Technology
Ioan Jung
Sabin Turdean
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Department of Pathology, University of Medicine,Pharmacy, Sciences and TechnologyDepartment of Pathology, University of Medicine,Pharmacy, Sciences and Technology
Sabin Turdean
Catalin Satala
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Department of Pathology, University of Medicine,Pharmacy, Sciences and TechnologyDepartment of Pathology, University of Medicine,Pharmacy, Sciences and Technology
Catalin Satala
Simona Gurzu
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Department of Pathology, University of Medicine,Pharmacy, Sciences and Technology
Research Center (CCAMF), University of Medicine, Pharmacy, Sciences and TechnologyDepartment of Pathology, University of Medicine,Pharmacy, Sciences and Technology
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Univ Calif San Francisco, Dept Pathol, 505 Parnassus Ave,M552,Box 0102, San Francisco, CA 94143 USAUniv Calif San Francisco, Dept Pathol, 505 Parnassus Ave,M552,Box 0102, San Francisco, CA 94143 USA
Choi, Won-Tak
Kakar, Sanjay
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Univ Calif San Francisco, Dept Pathol, 505 Parnassus Ave,M552,Box 0102, San Francisco, CA 94143 USAUniv Calif San Francisco, Dept Pathol, 505 Parnassus Ave,M552,Box 0102, San Francisco, CA 94143 USA
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Duke Univ Hlth Syst, Div Med Oncol, Dept Med, Duke Box 3233, Durham, NC 27710 USADuke Univ Hlth Syst, Div Med Oncol, Dept Med, Duke Box 3233, Durham, NC 27710 USA
Morse, Michael A.
Sun, Weijing
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Univ Kansas, Sch Med, Div Mol Med, Kansas City, KS USADuke Univ Hlth Syst, Div Med Oncol, Dept Med, Duke Box 3233, Durham, NC 27710 USA
Sun, Weijing
Kim, Richard
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H Lee Moffitt Canc Ctr & Res Inst, Dept Gastrointestinal Oncol, Tampa, FL USADuke Univ Hlth Syst, Div Med Oncol, Dept Med, Duke Box 3233, Durham, NC 27710 USA
Kim, Richard
He, Aiwu Ruth
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Georgetown Univ, Med Ctr, Dept Med, Washington, DC 20007 USADuke Univ Hlth Syst, Div Med Oncol, Dept Med, Duke Box 3233, Durham, NC 27710 USA
He, Aiwu Ruth
Abada, Paolo B.
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Eli Lilly & Co, Indianapolis, IN 46285 USADuke Univ Hlth Syst, Div Med Oncol, Dept Med, Duke Box 3233, Durham, NC 27710 USA
Abada, Paolo B.
Mynderse, Michelle
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Syneos Hlth, Clin Solut, Raleigh, NC USA
PRA Hlth Sci, Raleigh, NC USADuke Univ Hlth Syst, Div Med Oncol, Dept Med, Duke Box 3233, Durham, NC 27710 USA
Mynderse, Michelle
Finn, Richard S.
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Univ Calif Los Angeles, Geffen Sch Med, Dept Med, Div Hematol Oncol, Los Angeles, CA USADuke Univ Hlth Syst, Div Med Oncol, Dept Med, Duke Box 3233, Durham, NC 27710 USA