| Literature DB >> 24274653 |
Hiroko Masuda, Keith A Baggerly, Ying Wang, Takayuki Iwamoto, Takae Brewer, Lajos Pusztai, Kazuharu Kai, Takahiro Kogawa, Pascal Finetti, Daniel Birnbaum, Luc Dirix, Wendy A Woodward, James M Reuben, Savitri Krishnamurthy, W Symmans, Steven J Van Laere, François Bertucci, Gabriel N Hortobagyi, Naoto T Ueno.
Abstract
INTRODUCTION: Because of its high rate of metastasis, inflammatory breast cancer (IBC) has a poor prognosis compared with non-inflammatory types of breast cancer (non-IBC). In a recent study, Lehmann and colleagues identified seven subtypes of triple-negative breast cancer (TNBC). We hypothesized that the distribution of TNBC subtypes differs between TN-IBC and TN-non-IBC. We determined the subtypes and compared clinical outcomes by subtype in TN-IBC and TN-non-IBC patients.Entities:
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Year: 2013 PMID: 24274653 PMCID: PMC3978878 DOI: 10.1186/bcr3579
Source DB: PubMed Journal: Breast Cancer Res ISSN: 1465-5411 Impact factor: 6.466
Characteristics of patients with TNBC ( = 88)
| 39 | 49 | | |||||
| 49 (26-78) | 56 (28-77) | 0.1681 | |||||
| | | | I | 9 | (19) | 8.904e-09 | |
| | | | II | 17 | (35) | ||
| III | 27 | (69) | III | 18 | (36) | ||
| IV | 5 | (13) | IV | 5 | (10) | ||
| Unknown | 7 | (18) | Unknown | 0 | (0) | ||
| I | 0 | (0) | I | 3 | (6) | 0.2048 | |
| II | 4 | (10) | II | 10 | (20) | ||
| III | 33 | (85) | III | 35 | (72) | ||
| Unknown | 2 | (5) | Unknown | 1 | (2) | ||
| Positive | 24 | (62) | Positive | 3 | (6) | 3.604e-09 | |
| Negative | 12 | (30) | Negative | 20 | (41) | ||
| Unknown | 2 | (8) | Unknown | 26 | (53) | ||
| Positive | 21 | (78) | Positive | 29 | (66) | 0.1684 | |
| Negative | 5 | (18) | Negative | 15 | (34) | ||
| Unknown | 1 | (4) | Unknown | 0 | (0) | ||
Distribution of IBC/non-IBC status by TNBC subtype by using MDA gene signatures
| Subtype 1 (M) | 4 (10.2) | 6 (12.2) | 0.47 |
| Subtype 2 (IM) | 4 (10.2) | 12 (24.4) | |
| Subtype 3 (BL1) | 8 (20.5) | 7 (14.2) | |
| Subtype 4 (BL2) | 3 (7.6) | 2 (4.0) | |
| Subtype 5 (LAR) | 5 (12.8) | 5 (10.2) | |
| Subtype 6 (UNS) | 7 (17.9) | 12 (24.4) | |
| Subtype 7 (MSL) | 8 (20.5) | 5 (10.2) |
Distribution of IBC/non-IBC status by TNBC subtype by using Lehmann’s gene signatures
| M | 5 (12.8) | 9 (18.3) | 0.22 |
| IM | 5 (12.8) | 12 (24.4) | |
| BL1 | 12 (30.7) | 10 (20.4) | |
| BL2 | 1 (2.5) | 4 (8.1) | |
| LAR | 6 (15.3) | 6 (12.2) | |
| UNS | 2 (5.1) | 5 (10.2) | |
| MSL | 8 (20.5) | 3 (6.1) |
Figure 1Kaplan-Meier estimates. (A) Kaplan-Meier estimates for TNBC subtypes (defined by MDA approximated gene signatures) with respect to overall survival (OS) of patients with stage III disease; (B) Kaplan-Meier estimates for TNBC subtypes (defined by MDA approximated gene signatures) with respect to recurrence-free survival (RFS) of patients with stage III disease; (C) Kaplan-Meier estimates for TNBC subtypes (defined by MDA approximated gene signatures) with respect to distance metastasis-free survival (DMFS) of patients with stage III disease. The P values of the log-rank tests are for each pair of TNBC subtypes with respect to OS. The subtypes were classified by using our approximated gene signatures. The Bonferroni-adjusted P value is 0.00238. The P values of the log-rank tests are for each pair of TNBC subtypes with respect to RFS. The subtypes were classified by using our approximated gene signatures. The Bonferroni-adjusted P value is 0.00238. The P values of the log-rank tests are for each pair of TNBC subtypes with respect to DMFS. The subtypes were classified by using our approximated gene signatures. The Bonferroni-adjusted P value is 0.00238.
Figure 2Boxplots of gene expression levels in TNBC subtypes defined by MDA-approximated gene signatures (left panel) or Lehmann’s gene signatures (right panel).
Figure 3IBC versus non-IBC at stage III or above. (A) Those without restriction to TNBC and (B) those within TNBC. Histograms of P values from two-sample t tests for IBC versus non-IBC. The overlaid curves are the fitted BUM models. Counts of significant features with various FDR cutoffs are shown in a comparison of IBC with non-IBC.