A M Bilous
Westmead Hospital
4 Papers
A M Bilous is an academic researcher from Westmead Hospital. The author has contributed to research in topics: Progesterone receptor A & Biology. The author has an hindex of 4, co-authored 4 publications.
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Papers
•Journal Article
Characterization of Progesterone Receptor A and B Expression in Human Breast Cancer
J D Graham,C Yeates,Rosemary L. Balleine,S S Harvey,J S Milliken,A M Bilous,Christine L. Clarke +6 more
TL;DR: In PR-positive breast tumors, the ratio of expression of PR-A and B proteins is close to unity, as is seen in a number of other progestin target tissues, but a significant proportion of tumors expressed very low levels ofPR-B and a consequently highPR-A/B ratio.
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Progesterone receptor A and B protein expression in human breast cancer
J D Graham,C Yeates,Rosemary L. Balleine,S S Harvey,Jane S. Milliken,A M Bilous,Christine L. Clarke +6 more
TL;DR: In PR-positive breast tumors the ratio of expression of PR A and B proteins is close to unity as is seen in a number of other progestin target tissues, however, a significant proportion of tumors expressed very low levels of PR B and a consequently high PR A:B ration.
85
Histopathologic indicators of breast cancer biology: insights from population mammographic screening
Lucy Webster,Lucy Webster,A M Bilous,L Willis,Karen Byth,F C Burgemeister,Elizabeth Salisbury,Christine L. Clarke,Christine L. Clarke,Rosemary L. Balleine +9 more
TL;DR: Comparisons of features of breast cancers diagnosed following population mammographic screening with prevalent vs incident detection and screening interval indicate that biology and time both impact on size and LN status of invasive breast cancer, but grade reflects biology alone.
Expression of osteonectin mRNA in human breast tumours is inversely correlated with oestrogen receptor content
TL;DR: The data suggest that ER-mediated suppression of osteonectin gene expression may contribute to the less aggressive characteristics associated with receptor-positive tumours and that loss of ER expression may lead to over-expression of osteanectin and contribute to a poorer differentiated, more invasive phenotype.