Gene/Protein
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Drug
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Gene/Protein
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Target Concepts:
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Query: UNIPROT:P04155 (
pS2
)
1,234
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
pS2 protein
assay was performed with Elsa-
pS2
kit (CIS-Biointernational) on a group of 1,065 patients with operable breast cancer who underwent breast surgery in the years 1982 through 1990. The median follow-up was 57 months. This group included exclusively
infiltrating ductal carcinoma
with primary surgery. Age mean was 58 yr; T0-T1, 33.6%; T2-T4, 66.4%; Differentiation grade I, 29%; node negative, 53%; estrogen receptor (ER) positive, 62.4%; progesterone receptor (PR) positive, 55.2%; mean tumor size, 2.4 cm; local recurrence, 5.2%; metastasis, 17.5%.
pS2
values varied from 0.1 to 707 ng/mg of cytosol protein (median, 5.6; mean 24.5; 95th percentile 112 ng/mg p). There was no significant relationship between the mean level of
pS2
and age, tumor size, nodal status, whereas
pS2
was related to histological grade (P < 10(-3)), ER (P < 10(-5)), and PR (P < 10(-5)). By using 2 ng/mg p as
pS2
cutoff, 77/391 (19.7%) of ER+PR+ tumors were
pS2
-, and 122/345 (35.4%) of ER-PR-tumors were pS2+; with this cutoff, a strong relationship existed between
pS2
and overall survival, but not between
pS2
and relapse-free survival. With Cox multivariate analysis,
pS2 protein
was classified after lymph node status, histological size, ER, differentiation grade, age, clinical stage, PR. In patients with axillary lymph node involvement (N+),
pS2
status could discriminate between good and bad prognosis, specially for patients with small tumors (< 2 cm) and with less than seven invaded nodes. This study showed that
pS2 protein
was a poor prognostic factor in comparison with classical factors.
...
PMID:[PS2 as a prognostic factor in 1065 cases of human breast cancer. A multicenter study]. 770 45
This investigation was carried out to gain insight into the prevalence of
pS2
expression in
invasive ductal breast carcinoma
in the Malaysian population and its correlation with oestrogen receptor (ER) protein expression and tumour aggressiveness. Seventy consecutive infiltrating ductal breast carcinomas treated with mastectomy and axillary lymph node clearance were investigated, using the standard avidin-biotin complex immunoperoxidase method with microwave antigen retrieval and commercial monoclonal antibodies (Dako), for expression of
pS2
and human ER. This was correlated against histological grade (modified Bloom and Richardson) and the presence of axillary lymph node metastasis of these carcinomas. Four (5.7%) were grade 1, 40 (57.1%) grade 2 and 26 (37.1%) grade 3 tumours. A total of 45 (64%) showed histological evidence of axillary lymph node metastasis. Forty (57%) were ER-positive, while 31 (44%) were
pS2
-positive. There was a statistically significant correlation between
pS2
and ER expressions (chi2-test with Yates correction: P<0.005). There was no correlation between
pS2
expression and histological grade (P>0.1) and the presence of lymph node metastasis (P>0.1). Our findings support the views that
pS2
may be a co-marker of endocrine responsiveness in invasive breast cancer and that it does not influence breast cancer biology in terms of potential for metastatic spread.
...
PMID:pS2 expression in infiltrating ductal carcinoma of the breast correlates with oestrogen receptor positivity but not with histological grade and lymph node status. 1152 25
In order to evaluate the influence of hormone dependence on the features of
infiltrating ductal carcinoma
of the breast we have assayed the cytosolic levels of estrogen receptor (ER), progesterone receptor (PR),
pS2
and cathepsin D in 53 women aged over 70 years and in 95 women aged between 55 and 70 years. Tumor size, axillary involvement, distant metastasis, histological grade, ploidy and S-phase were taken into account. Carcinomas of women aged over 70 did not show higher concentrations or higher positive results for ER and PR than those of women in the 55-70-year age group. In older patients, negativity for ER was associated only with higher S-phase fraction, while negativity for PR was not associated with any of the parameters analyzed. In the younger subgroup, negativity for ER was associated with larger tumor size, higher S-phase fraction, lymph node involvement, histological grade 3 and lower
pS2
values. Negativity for PR was associated with the same parameters, as well as with a higher frequency of recurrence. Our results suggest a reduced influence of hormone dependence on the clinicopathological features of breast carcinomas in patients older than 70 years compared with women aged between 55 and 70 years.
...
PMID:Reduced clinicopathological influence of hormone-dependence on breast carcinomas in women older than 70 years. 1840 53
In order to evaluate the influence of hormone dependence on the features of
infiltrating ductal carcinoma
of the breast we have assayed the cytosolic levels of estrogen receptor (ER), progesterone receptor (PR),
pS2
and cathepsin D in 53 women aged over 70 years and in 95 women aged between 55 and 70 years. Tumor size, axillary involvement, distant metastasis, histological grade, ploidy and S-phase were taken into account. Carcinomas of women aged over 70 did not show higher concentrations or higher positive results for ER and PR than those of women in the 55-70-year age group. In older patients, negativity for ER was associated only with higher S-phase fraction, while negativity for PR was not associated with any of the parameters analyzed. In the younger subgroup, negativity for ER was associated with larger tumor size, higher S-phase fraction, lymph node involvement, histological grade 3 and lower
pS2
values. Negativity for PR was associated with the same parameters, as well as with a higher frequency of recurrence. Our results suggest a reduced influence of hormone dependence on the clinicopathological features of breast carcinomas in patients older than 70 years compared with women aged between 55 and 70 years.
...
PMID:Reduced clinicopathological influence of hormone-dependence on breast carcinomas in women older than 70 years. 2820 6
