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Expression of the forkhead box transcription factor FOXP1 is associated with oestrogen receptor alpha, oestrogen receptor beta and improved survival in familial breast cancers
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Background:
The role of FOXP1 in sporadic breast cancers has been widely studied but its role in familial breast cancers is yet unexplored.
Aims:
To investigate FOXP1 expression in different molecular subtypes of familial breast cancers and to correlate its expression with clinicopathological parameters, oestrogen receptors (ER) and survival.
Methods:
Immunohistochemical staining for FOXP1 was performed in 126 familial breast carcinomas comprising 35 BRCA1, 34 BRCA2 and 57 BRCAX.
Results:
Nuclear FOXP1 expression ranged from focal weak to widespread strong expression. Expression of FOXP1 was higher in familial breast cancers (54%) compared with sporadic cancers (46%) (p<0.001). There was a significant correlation between FOXP1 with ERα (p = 0.038) and ERβ (p = 0.007) in familial breast cancers. FOXP1 was more highly expressed in familial breast cancers compared with sporadic cancers for luminal (p = 0.021) and basal (p<0.001), but not HER2 and null phenotypes (both p>0.05). The absence of FOXP1 expression was associated with a shorter relapse-free (p = 0.025) and overall survival (p = 0.009) in familial breast cancer. Negativity for FOXP1 was associated with a significantly worse overall survival in BRCA2 cancers (p = 0.021) and there was a non-significant separation of the survival curves for BRCA1 cancers (p = 0.183). No differences in survival were seen for BRCAX cancers (p = 0.762).
Conclusion:
Results suggest that FOXP1 demonstrates different expression patterns in familial breast cancers than sporadic tumours, even in tumours showing similar phenotypes. They also suggest a different role of FOXP1 as a tumour suppressor in familial tumours, which is unrelated to ER expression and may impact on therapeutic options.
Title: Expression of the forkhead box transcription factor FOXP1 is associated with oestrogen receptor alpha, oestrogen receptor beta and improved survival in familial breast cancers
Description:
Background:
The role of FOXP1 in sporadic breast cancers has been widely studied but its role in familial breast cancers is yet unexplored.
Aims:
To investigate FOXP1 expression in different molecular subtypes of familial breast cancers and to correlate its expression with clinicopathological parameters, oestrogen receptors (ER) and survival.
Methods:
Immunohistochemical staining for FOXP1 was performed in 126 familial breast carcinomas comprising 35 BRCA1, 34 BRCA2 and 57 BRCAX.
Results:
Nuclear FOXP1 expression ranged from focal weak to widespread strong expression.
Expression of FOXP1 was higher in familial breast cancers (54%) compared with sporadic cancers (46%) (p<0.
001).
There was a significant correlation between FOXP1 with ERα (p = 0.
038) and ERβ (p = 0.
007) in familial breast cancers.
FOXP1 was more highly expressed in familial breast cancers compared with sporadic cancers for luminal (p = 0.
021) and basal (p<0.
001), but not HER2 and null phenotypes (both p>0.
05).
The absence of FOXP1 expression was associated with a shorter relapse-free (p = 0.
025) and overall survival (p = 0.
009) in familial breast cancer.
Negativity for FOXP1 was associated with a significantly worse overall survival in BRCA2 cancers (p = 0.
021) and there was a non-significant separation of the survival curves for BRCA1 cancers (p = 0.
183).
No differences in survival were seen for BRCAX cancers (p = 0.
762).
Conclusion:
Results suggest that FOXP1 demonstrates different expression patterns in familial breast cancers than sporadic tumours, even in tumours showing similar phenotypes.
They also suggest a different role of FOXP1 as a tumour suppressor in familial tumours, which is unrelated to ER expression and may impact on therapeutic options.
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