| Literature DB >> 23820253 |
T M Brewer1, H Masuda, D D Liu, Y Shen, P Liu, T Iwamoto, K Kai, C M Barnett, W A Woodward, J M Reuben, P Yang, G N Hortobagyi, N T Ueno.
Abstract
BACKGROUND: Some studies have suggested that statins, which have cholesterol-lowering and anti-inflammatory properties, may have antitumor effects. Effects of statins on inflammatory breast cancer (IBC) have never been studied.Entities:
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Year: 2013 PMID: 23820253 PMCID: PMC3721387 DOI: 10.1038/bjc.2013.342
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Statin classification based on the log partition coefficient, adopted from a Danish nationwide prospective cohort study conducted by Ahern
| Lipophilic | Simvastatin | C10AA01 | 4.7 |
| | Lovastatin | C10AA02 | 4.3 |
| | Fluvastatin | C10AA04 | 3.5 |
| | Cerivastatin | C10AA06 | 3.6 |
| Hydrophilic | Atorvastatin | C10AA05 | 1.5 |
| | Pravastatin | C10AA03 | −0.47 |
| Rosuvastatin | C10AA07 | 1.6 |
Reproduced with kind permission of Oxford University Press from Ahern .
Partition coefficient for atorvastatin and pravastatin were reported by Kubota . Remaining partition coefficients were ascertained from the National Center for Biotechnology Information Pub Chem database (http://pubchem.ncbi.nlm.hih.gov/).
Frequency and percentage of statin users by statin type
| L-statin | Fluvastatin | 1 (3.4%) |
| | Lovastatin | 1 (3.4%) |
| | Simvastatin | 27 (93.1%) |
| H-statin | Atorvastatin | 29 (65.9%) |
| | Pravastatin | 9 (20.5%) |
| | Pravastatin and rosuvastatin | 1 (2.3%) |
| Rosuvastatin | 5 (11.4%) |
Abbreviations: L-statin=lipophilic statin; H-statin=hydrophilic to weakly lipophilic statin.
The classification of statins is from Ahern , as shown in Table 1.
Patient characteristics by statin type
| Age | <50 | 359 (55.2%) | 5 (17.2%) | 6 (13.6%) | <0.01 |
| | ⩾50 | 291 (44.8%) | 24 (82.8%) | 38 (86.4%) | |
| Race | White | 562 (86.5%) | 26 (89.7%) | 41 (93.2%) | 0.71 |
| | Black | 63 (9.7%) | 3 (10.3%) | 3 (6.8%) | |
| | Other | 25 (3.8%) | 0 | 0 | |
| BMI | <25 | 162 (26.5%) | 6 (25%) | 4 (10%) | 0.07 |
| | ⩾25 and <30 | 199 (32.5%) | 5 (20.8%) | 13 (32.5%) | |
| | ⩾30 | 251 (41%) | 13 (54.2%) | 23 (57.5%) | |
| Menopausal status | Post | 313 (48.6%) | 24 (82.8%) | 38 (88.4%) | <0.01 |
| | Pre | 331 (51.4%) | 5 (17.2%) | 5 (11.6%) | |
| ER | Negative | 334 (56.1%) | 17 (60.7%) | 20 (50%) | 0.66 |
| | Positive | 261 (43.9%) | 11 (39.3%) | 20 (50%) | |
| PR | Negative | 394 (67.4%) | 22 (81.5%) | 26 (65%) | 0.28 |
| | Positive | 191 (32.6%) | 5 (18.5%) | 14 (35%) | |
| HR | Negative | 304 (51.2%) | 16 (57.1%) | 16 (40%) | 0.31 |
| | Positive | 290 (48.8%) | 12 (42.9%) | 24 (60%) | |
| HER2 | Negative | 316 (61.4%) | 19 (79.2%) | 27 (71.1%) | 0.12 |
| | Positive | 199 (38.6%) | 5 (20.8%) | 11 (28.9%) | |
| TNBC | Non-TNBC | 420 (75.3%) | 16 (64%) | 28 (71.8%) | 0.41 |
| | TNBC | 138 (24.7%) | 9 (36%) | 11 (28.2%) | |
| Nuclear grade | I | 6 (1%) | 0 | 0 | 0.18 |
| | II | 102 (17.4%) | 8 (29.6%) | 12 (29.3%) | |
| | III | 478 (81.6%) | 19 (70.4%) | 29 (70.7%) | |
| Lymphatic invasion | Negative | 209 (35.9%) | 11 (42.3%) | 19 (46.3%) | 0.34 |
| | Positive | 373 (64.1%) | 15 (57.7%) | 22 (53.7%) | |
| Vascular invasion | Negative | 268 (46.2%) | 11 (42.3%) | 20 (50%) | 0.82 |
| | Positive | 312 (53.8%) | 15 (57.7%) | 20 (50%) | |
| Lymphatic/vascular invasion | Either negative | 277 (47.8%) | 11 (42.3%) | 20 (50%) | 0.82 |
| | Positive/positive | 302 (52.2%) | 15 (57.7%) | 20 (50%) | |
| Neoadjuvant chemotherapy | No | 52 (8%) | 0 | 3 (6.8%) | 0.32 |
| | Yes | 598 (92%) | 29 (100%) | 41 (93.2%) | |
| Neoadjuvant hormonal therapy | No | 636 (97.8%) | 29 (100%) | 44 (100%) | 1.00 |
| | Yes | 14 (2.2%) | 0 | 0 | |
| Adjuvant chemotherapy | No | 343 (52.8%) | 25 (86.2%) | 25 (56.8%) | <0.01 |
| | Yes | 307 (47.2%) | 4 (13.8%) | 19 (43.2%) | |
| Adjuvant hormonal therapy | No | 449 (69.1%) | 21 (72.4%) | 25 (56.8%) | 0.21 |
| | Yes | 201 (30.9%) | 8 (27.6%) | 19 (43.2%) | |
| Radiation therapy | No | 165 (25.4%) | 6 (20.7%) | 11 (25%) | 0.85 |
| | Yes | 485 (74.6%) | 23 (79.3%) | 33 (75%) | |
| Diabetes mellitus | No | 601 (92.5%) | 20 (69%) | 29 (65.9%) | <0.01 |
| | Yes | 49 (7.5%) | 9 (31%) | 15 (34.1%) | |
| Insulin | No | 637 (98%) | 25 (86.2%) | 40 (90.9%) | <0.01 |
| | Yes | 13 (2%) | 4 (13.8%) | 4 (9.1%) | |
| Metformin | No | 627 (96.5%) | 24 (82.8%) | 36 (81.8%) | <0.01 |
| | Yes | 23 (3.5%) | 5 (17.2%) | 8 (18.2%) | |
| Hypertension | No | 520 (80%) | 9 (31%) | 19 (43.2%) | <0.01 |
| | Yes | 130 (20%) | 20 (69%) | 25 (56.8%) | |
| ACEI or ARB | No | 562(86.5%) | 16 (55.2%) | 23 (52.3%) | <0.01 |
| | Yes | 88 (13.5%) | 13 (44.8%) | 21 (47.7%) | |
| Beta-blocker | No | 568 (87.4%) | 17 (58.6%) | 26 (59.1%) | <0.01 |
| | Yes | 82 (12.6%) | 12 (41.4%) | 18 (40.9%) | |
| Bisphosphonate | No | 606 (93.2%) | 24 (82.8%) | 42 (95.5%) | 0.09 |
| | Yes | 44 (6.8%) | 5 (17.2%) | 2 (4.5%) | |
| Surgery within 1 year | No | 77 (11.8%) | 2 (6.9%) | 5 (11.4%) | 0.84 |
| Yes | 573 (88.2%) | 27 (93.1%) | 39 (88.6%) |
Abbreviations: ACEI=angiotensin-converting enzyme inhibitor; ARB=angiotensin receptor blocker; BMI=body mass index; ER=oestrogen receptor; HER2=human epidermal growth factor receptor 2; HR=hazard ratio; PR=progesterone receptor; TNBC=triple-negative breast cancer.
Univariate and multicovariate cox model for PFS, OS, and DSS for H-statin and L-statin when compared with non-statin users
| | ||||
|---|---|---|---|---|
| Statin L | 0.94 (0.57–1.55) | 0.81 | 0.76 (0.41–1.41) | 0.38 |
| H | 0.55 (0.35–0.87) | 0.01 | 0.49 (0.28–0.84) | <0.01 |
| Statin L | 1.23 (0.71–2.15) | 0.46 | 1.46 (0.73–2.90) | 0.28 |
| H | 0.75 (0.46–1.20) | 0.23 | 0.80 (0.43–1.49) | 0.49 |
| Statin L | 1.11 (0.61–2.03) | 0.74 | 1.18 (0.54–2.55) | 0.68 |
| H | 0.71 (0.43–1.17) | 0.18 | 0.85 (0.46–1.57) | 0.59 |
Abbreviations: CI=confidence interval; DSS=disease-specific survival; L=lipophilic statin users; H=weakly lipophilic and hydrophilic statin users; N=non-statin users; OS=overall survival; PFS=progression-free survival.
Multicovariate models included radiation therapy, hormonal receptor status and HER2 status as the stratification factors and adjusted for lymphatic/vascular invasion for PFS and lymphatic/vascular invasion, nuclear grade and surgery within 1 year (Yes vs No) for OS and DSS.
Figure 1Kaplan–Meier curve for PFS comparing H-statin users, L-statin users, and non-statin users.
Multicovariate Cox model for PFS, OS, and DSS comparing atorvastatin and simvastatin users vs non-statin users
| | ||
|---|---|---|
| Statin Atorva | 0.48 (0.25–0.95) | 0.03 |
| Simva | 0.72 (0.38–1.36) | 0.30 |
| Statin Atorva | 1.00 (0.49–2.05) | 0.99 |
| Simva | 1.38 (0.67–2.85) | 0.38 |
| Statin Atorva | 1.05 (0.51–2.17) | 0.89 |
| Simva | 1.07 (0.47–2.46) | 0.87 |
Abbreviations: CI=confidence interval; DSS=disease-specific survival; N=non-statin users; OS=overall survival, PFS=progression-free survival.