N. L. P. Barnes scite author profile

Cyclooxygenase-2 (COX-2) is associated with poor-prognosis breast cancer. We used a nude mouse xenograft model to determine the effects of COX-2 inhibition in breast cancer. Oestrogen receptor (ER)-positive MCF7/HER2-18 and ER-negative MDAMB231 breast cancer cell lines were injected into nude mice and allowed to form tumours. Mice then received either chow containing Celecoxib (a COX-2 inhibitor) or control and tumour growth measured. Tumour proliferation, apoptosis, COX-2, lymphangiogenesis and angiogenesis were assessed by immunohistochemistry (IHC), Western blotting or Q-PCR. Celecoxib inhibited median tumour growth in MCF7/HER2-18 (58.7%, P ¼ 0.029) and MDAMB231 (46.3%, P ¼ 0.0002) cell lines compared to control. Cyclooxygenase-2 expression decreased following Celecoxib treatment (MCF7/HER2-18 median control 65.3% vs treated 22.5%, P ¼ 0.0001). Celecoxib increased apoptosis in MCF7/HER2-18 tumours (TUNEL 0.52% control vs 0.73% treated, P ¼ 0.0004) via inactivation of AKT (median pAKT ser473 57.3% control vs 35.5% treated, P ¼ 0.0001 -confirmed at Western blotting). Q-PCR demonstrated decreased podoplanin RNA (lymphangiogenesis marker) in the MCF7/HER2-18 -median 2.9 copies treated vs 66.6 control (P ¼ 0.05) and MDAMB231-treated groups -median 160.7 copies vs 0.05 control copies (P ¼ 0.015), confirmed at IHC. Cyclooxygenase-2 is associated with high levels of activated AKT ser473 and lymphangiogenesis in breast cancer. Cyclooxygenase-2 inhibition decreases tumour growth, and may potentially decrease recurrence, by inactivating AKT and decreasing lymphangiogenesis.

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Survivin expression in in situ and invasive breast cancer relates to COX-2 expression and DCIS recurrence

Barnes

Haywood

Flint

et al. 2006

Br J Cancer

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In lung cancer cyclooxygenase-2 (COX-2) expression has been reported to stabilise survivin, an inhibitor of apoptosis (IAP) which prevents cell death by blocking activated caspases. COX-2 expression limits the ubiquitination of survivin, protecting it from degradation. To determine if COX-2 expression in breast cancer showed an association with survivin expression, we assessed the levels of each protein in ductal carcinoma in situ (DCIS) and invasive breast cancer (IBC); relating expression patterns to recurrence of DCIS after surgery. Patterns of COX-2 and survivin expression were determined by intensity-graded immunohistochemistry of the primary tumours. Patients with DCIS (n ¼ 161) which had either recurred (n ¼ 47) or shown no evidence of recurrence (n ¼ 114) 5 years following primary surgery were studied. These were compared to 58 cases of IBC. Survivin was expressed in the cytoplasm of 59% of DCIS and 17% of IBC. High levels of both cytoplasmic survivin and COX-2 expression significantly correlated to DCIS recurrence. COX-2 expression was present in 72% of DCIS, and levels of expression positively correlated with cytoplasmic survivin expression in DCIS and invasive disease. The majority of DCIS that recurred expressed both proteins (69%) vs 39% nonrecurrent. Recurrence was not seen in DCIS lacking both proteins at 5 years (P ¼ 0.001). Expression of the IAP survivin is increased in DCIS and correlates closely with COX-2 expression. Increased expression of IAP, (leading to reduced apoptosis) may explain the effect of COX-2 in increasing recurrence of DCIS after surgical treatment.

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Relationship between hormone receptor status and tumour size, grade and comedo necrosis in ductal carcinoma in situ

Barnes

Boland

Davenport

et al. 2005

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N. L. P. Barnes

Molecular phenotypes of DCIS predict overall and invasive recurrence

Cyclooxygenase-2 inhibition: effects on tumour growth, cell cycling and lymphangiogenesis in a xenograft model of breast cancer

Survivin expression in in situ and invasive breast cancer relates to COX-2 expression and DCIS recurrence

Relationship between hormone receptor status and tumour size, grade and comedo necrosis in ductal carcinoma in situ

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