| Literature DB >> 23587222 |
Lorella Maniscalco1, Yolanda Millán, Selina Iussich, Mauro Denina, Raquel Sánchez-Céspedes, Francesca Gattino, Bartolomeo Biolatti, Nobuo Sasaki, Takayuki Nakagawa, Maria Flavia Di Renzo, Juana Martín de Las Mulas, Raffaella De Maria.
Abstract
BACKGROUND: Triple negative breast cancer (TNBC) in humans is defined by the absence of oestrogen receptor (ER), progesterone receptor (PR) and HER2 overexpression. Mammalian target of rapamycin (mTOR) is overexpressed in TNBC and it represents a potential target for the treatment of this aggressive tumour. Feline mammary carcinoma (FMC) is considered to be a model for hormone-independent human breast cancer. This study investigated mTOR and p-mTOR expression in FMC in relation to triple negative (TN) phenotype.Entities:
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Year: 2013 PMID: 23587222 PMCID: PMC3637810 DOI: 10.1186/1746-6148-9-80
Source DB: PubMed Journal: BMC Vet Res ISSN: 1746-6148 Impact factor: 2.741
Figure 1DFI in patients with TN and no-TN feline mammary carcinomas. Kaplan–Meier estimates for disease free interval probability in TN-FMCs (TN) and no TN_FMCs (no-TN) (P >0.05).
Figure 2mTOR expression in tubulopapillary carcinoma. a. Mammary gland. I grade tubulopapillary carcinoma. Neoplastic cells are characterised by diffuse and moderate cytoplasmic immunopositivity for mTOR. Streptavidin-biotin-peroxidase method. Mayer’s haematoxylin counterstaining. Scale bar = 50 μM b. Mammary gland. III grade tubulopapillary carcinoma. Neoplastic cells are characterised by diffuse and moderate cytoplasmic immunopositivity for mTOR. Streptavidin-biotin-peroxidase method. Mayer’s haematoxylin counterstaining. Scale bar = 50 μM.
Figure 3- phospho-mTOR expression in tubulopapillary carcinoma. Mammary gland. III grade tubulopapillary carcinoma. About 60% of neoplastic cells are characterised by strong nuclear immunopositivity for p-mTOR. Streptavidin-biotin-peroxidase method. Mayer’s haematoxylin counterstaining. Scale bar = 100 μM.
Relationships between tumour characteristics and expression of mTOR and p-mTOR
| Triple negative | 22 (42.31%) | 9 (17.31%) | 0.03 | 24 (41.38%) | 7 (12.07%) | 0.0005 |
| Non-triple negative | 11 (21.15%) | 16 (30.77%) | | 8 (13.79%) | 19 (32.76%) | |
| Total | 33 | 25 | | 32 | 26 | |
| | | | mTOR + | 24 (41.38%) | 8 (13.79%) | 0.0032 |
| | | | mTOR - | 9 (17.31%) | 17 (29.31%) | |
| | | | | 32 | 26 | |
| | | | * | | | *** |
| HER2 + | 7 (12.07%) | 12 (20.69%) | 0.0479 | 4 (6.9%) | 15 (25.86%) | 0.0005 |
| HER2 - | 26 (44.83%) | 13 (22.41%) | | 28 (48.28%) | 11 (18.97%) | |
| Total | 33 | 25 | | 32 | 26 | |
| >1 cm | 27 (46.55%) | 16 (27.59%) | >0.05 | 22 (42.31%) | 20 (30.48%) | 0.05 |
| ≤1 cm | 8 (13.79%) | 7 (12.07%) | | 10 (17.24%) | 6 (10.34%) | |
| | 35 | 23 | | 32 | 26 | |
| Grade I | 5 (8.62%) | 4 (6.90%) | >0.05 | 4 (6.90%) | 5 (8.62%) | >0.05 |
| Grade II | 12 (20.69%) | 12 (20.69%) | | 14 (24.14%) | 10 (17.24%) | |
| Grade III | 16 (27.59%) | 9 (15.52%) | | 14 (24.14%) | 11 (21.15%) | |
| Total | 33 | 25 | | 32 | 26 | |
| Vascular invasion | 7 (12.07%) | 7 (12.07%) | >0.05 | 6 (10.34%) | 8 (13.79%) | >0.05 |
| No vascular invasion | 26 (44.83%) | 18 (31.03%) | | 26 (44.83%) | 18 (31.03) | |
| Total | 33 | 25 | | 32 | 26 | |
| Relapsed | 25 (43.10%) | 20 (30.48%) | >0.05 | 17 (29.31%) | 28 (48.28%) | >0.05 |
| Not relapsed | 8 (13.79%) | 5 (8.62%) | | 7 (12.07%) | 6 (10.34%) | |
| Total | 33 | 25 | | 24 | 34 | |
| Relapsed 0–6 months | 17 (37.78%) | 14 (31.11%) | >0.05 | 9 (20.00%) | 22 (48.89%) | >0.05 |
| Relapsed 6–12 months | 4 (8.89%) | 3 (31.03%) | | 4 (8.89%) | 3 (31.03%) | |
| Relapsed >12 months | 4 (8.89%) | 3 (31.03%) | | 4 (8.89%) | 4 (31.03%) | |
| Total | 25 | 20 | | 17 | 28 | |
| Mitotic indexa 1 | 4 (6.90%) | 2 (3.45%) | >0.05 | 3 (5.17%) | 3 (5.17%) | >0.05 |
| Mitotic index 2 | 7 (12.07%) | 8 (13.79%) | | 8 (13.79%) | 7 (12.07%) | |
| Mitotic index 3 | 22 (42.31%) | 15 (25.86%) | | 21 (36.21%) | 16 (27.59%) | |
| Total | 33 | 25 | 32 | 26 |
aMitotic index of the histological grading system [27].
Figure 4Western blot. a. Western blot analysis of HER2, oestrogen receptor α (ERα), progesterone receptor (PR), mTOR and p-mTOR expression in FYCp (lane 1), P248m (lane 2), FMCp (lane 3), FMCm (lane 4), FKNp (lane 5) and FNNm (lane 6) cell lines. α Tubulin expression was used as the loading control. b. Measure of band intensity normalized to α tubulin. Error bars demonstrate standard deviation.