Breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.

BACKGROUND: There is increasing evidence that breast cancer is a heterogeneous disease presented by different phenotypes and that white women have a higher breast cancer incidence rate, whereas black women have a higher mortality rate. It is also well known that white women have lower incidence rate...

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Main Authors: Michael X Gleason, Tengiz Mdzinarishvili, Simon Sherman
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3498165?pdf=render
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spelling doaj-ee85d6e94be240529df42d823bfaa7792020-11-25T00:12:14ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01711e4935910.1371/journal.pone.0049359Breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.Michael X GleasonTengiz MdzinarishviliSimon ShermanBACKGROUND: There is increasing evidence that breast cancer is a heterogeneous disease presented by different phenotypes and that white women have a higher breast cancer incidence rate, whereas black women have a higher mortality rate. It is also well known that white women have lower incidence rates than black women until approximately age 40, when rate curves cross over and white women have higher rates. The goal of this study was to validate the risk of white and black women to breast cancer phenotypes, stratified by statuses of the estrogen (ER) and progesterone (PR) receptors. METHODOLOGY/PRINCIPAL FINDINGS: SEER17 data were fractioned by receptor status into [ER+, PR+], [ER-, PR-], [ER+, PR-], and [ER-, PR+] phenotypes. It was shown that in black women compared to white women, cumulative age-specific incidence rates are: (i) smaller for the [ER+, PR+] phenotype; (ii) larger for the [ER-, PR-] and [ER-, PR+] phenotypes; and (iii) almost equal for the [ER+, PR-] phenotype. Clemmesen's Hook, an undulation unique to women's breast cancer age-specific incidence rate curves, is shown here to exist in both races only for the [ER+, PR+] phenotype. It was also shown that for all phenotypes, rate curves have additional undulations and that age-specific incidence rates are nearly proportional in all age intervals. CONCLUSIONS/SIGNIFICANCE: For black and white women, risk for the [ER+, PR+], [ER-, PR-] and [ER-, PR+] phenotypes are race dependent, while risk for the [ER+, PR-] phenotype is almost independent of race. The processes of carcinogenesis in aging, leading to the development of each of the considered breast cancer phenotypes, are similar in these racial groups. Undulations exhibited on the curves of age-specific incidence rates of the considered breast cancer phenotypes point to the presence of several subtypes (to be determined) of each of these phenotypes.http://europepmc.org/articles/PMC3498165?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Michael X Gleason
Tengiz Mdzinarishvili
Simon Sherman
spellingShingle Michael X Gleason
Tengiz Mdzinarishvili
Simon Sherman
Breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.
PLoS ONE
author_facet Michael X Gleason
Tengiz Mdzinarishvili
Simon Sherman
author_sort Michael X Gleason
title Breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.
title_short Breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.
title_full Breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.
title_fullStr Breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.
title_full_unstemmed Breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.
title_sort breast cancer incidence in black and white women stratified by estrogen and progesterone receptor statuses.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description BACKGROUND: There is increasing evidence that breast cancer is a heterogeneous disease presented by different phenotypes and that white women have a higher breast cancer incidence rate, whereas black women have a higher mortality rate. It is also well known that white women have lower incidence rates than black women until approximately age 40, when rate curves cross over and white women have higher rates. The goal of this study was to validate the risk of white and black women to breast cancer phenotypes, stratified by statuses of the estrogen (ER) and progesterone (PR) receptors. METHODOLOGY/PRINCIPAL FINDINGS: SEER17 data were fractioned by receptor status into [ER+, PR+], [ER-, PR-], [ER+, PR-], and [ER-, PR+] phenotypes. It was shown that in black women compared to white women, cumulative age-specific incidence rates are: (i) smaller for the [ER+, PR+] phenotype; (ii) larger for the [ER-, PR-] and [ER-, PR+] phenotypes; and (iii) almost equal for the [ER+, PR-] phenotype. Clemmesen's Hook, an undulation unique to women's breast cancer age-specific incidence rate curves, is shown here to exist in both races only for the [ER+, PR+] phenotype. It was also shown that for all phenotypes, rate curves have additional undulations and that age-specific incidence rates are nearly proportional in all age intervals. CONCLUSIONS/SIGNIFICANCE: For black and white women, risk for the [ER+, PR+], [ER-, PR-] and [ER-, PR+] phenotypes are race dependent, while risk for the [ER+, PR-] phenotype is almost independent of race. The processes of carcinogenesis in aging, leading to the development of each of the considered breast cancer phenotypes, are similar in these racial groups. Undulations exhibited on the curves of age-specific incidence rates of the considered breast cancer phenotypes point to the presence of several subtypes (to be determined) of each of these phenotypes.
url http://europepmc.org/articles/PMC3498165?pdf=render
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