Morton Freytag scite author profile

Carbonic anhydrase IX (CAIX) is involved in pathological processes including tumorgenicity, metastases and poor survival in solid tumors. Twenty-two neuroblastoma samples of patients who were surgically treated at the University Medical Center Hamburg-Eppendorf were evaluated immunohistochemically for expression of CAIX. Results were correlated with clinical parameters and outcome. Neuroblastoma Kelly and SH-EP-Tet-21/N cells were examined for CAIX expression and inhibited with specific inhibitors, FC5-207A and FC8-325A. 32% of neuroblastoma tumors expressed CAIX. This was significantly associated with poorer survival. Kelly and SH-EP-Tet-21/N cells showed a major increase of CAIX RNA under hypoxic conditions. Proliferation of Kelly cells was significantly decreased by CAIX inhibitors, FC5-207A and FC8-325A, while proliferation of SH-EP-Tet-21/N cells was only significantly affected by FC8-325A. CAIX is a potent biomarker that predicts survival in neuroblastoma patients. CAIX-targeted therapy in neuroblastoma cell lines is highly effective and strengthens the potential of CAIX as a clinical therapeutic target in a selected patient collective.

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CAIX furthers tumour progression in the hypoxic tumour microenvironment of esophageal carcinoma and is a possible therapeutic target

Drenckhan

Freytag

Supuran

et al. 2018

Journal of Enzyme Inhibition and Medicinal Chemistry

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The hypoxic tumour microenvironment of solid tumours represents an important starting point for modulating progression and metastatic spread. Carbonic anhydrase IX (CAIX) is a known HIF-1α-dependent key player in maintaining cell pH conditions under hypoxia. We show that CAIX is strongly expressed in esophageal carcinoma tissues. We hypothesize that a moderate CAIX expression facilitates metastases and thereby worsens prognosis. Selective inhibition of CAIX by specific CAIX inhibitors and a CAIX knockdown effectively inhibit proliferation and migration in vitro. In the orthotopic esophageal carcinoma model, the humanized HER2 antibody trastuzumab down-regulates CAIX, possibly through CAIX’s linkage with HER2 in the hypoxic microenvironment. Our results show CAIX to be an essential part of the tumour microenvironment and a possible master regulator of tumour progression. This makes CAIX a highly effective and feasible therapeutic target for selective cancer treatment.

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Influence of hypoxia-dependent factors on the progression of neuroblastoma

et al. 2015

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Metastasising liposarcoma of bone in a young dog

Frase¹,

Freytag

Baumgartner³

et al. 2009

Veterinary Record

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Sagittal section of the distal radius and carpus of a dog with liposarcoma. Tumour tissue arising from the marrow cavity of the distal radius (*) penetrates the cortical bone and infiltrates the adjacent soft tissues. There is periosteal new bone formation proximal to the tumour (arrow) FIG 2: Section of a tumour from the bone marrow of the dog, consisting of sheets of vacuolated cells with round to oval vesicular nuclei: there are numerous mitotic figures (arrows). Haematoxylin and eosin. Bar=50 µm

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Morton Freytag

Carbonic anhydrase IX correlates with survival and is a potential therapeutic target for neuroblastoma

CAIX furthers tumour progression in the hypoxic tumour microenvironment of esophageal carcinoma and is a possible therapeutic target

Influence of hypoxia-dependent factors on the progression of neuroblastoma

Metastasising liposarcoma of bone in a young dog

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