Aromatase inhibitors versus tamoxifen in early breast cancer: Patient-level meta-analysis of the randomised trials

R. Bradley; J. Burrett; M. Clarke; C. Davies; F. Duane; V. Evans; L. Gettins; J. Godwin; R. Gray; H. Liu; P. McGale; E. MacKinnon; T. McHugh; S. James; P. Morris; H. Pan; R. Peto; S. Read; C. Taylor; Y. Wang; Z. Wang; M. Dowsett; J. F. Forbes; J. Ingle; A. Coates; J. Cuzick; M. Gnant; T. Aihara; J. Bliss; F. Boccardo; R. C. Coombes; P. Dubsky; M. Kaufmann; L. Kilburn; F. Perrone; D. Rea; B. Thürlimann; C. Van De Velde; M. Baum; A. Buzdar; I. Sestak; C. Markopoulos; C. Fesl; R. Jakesz; M. Colleoni; R. Gelber; M. Regan; G. Von Minckwitz; C. Snowdon; C. Geyer; Early Breast Cancer Trialists’ Collaborative Group

doi:10.1016/S0140-6736(15)61074-1

Aromatase inhibitors versus tamoxifen in early breast cancer: Patient-level meta-analysis of the randomised trials

R. Bradley, J. Burrett, M. Clarke, C. Davies, F. Duane, V. Evans, L. Gettins, J. Godwin, R. Gray, H. Liu, P. McGale, E. MacKinnon, T. McHugh, S. James, P. Morris, H. Pan, R. Peto, S. Read, C. Taylor, Y. WangZ. Wang, M. Dowsett, J. F. Forbes, J. Ingle, A. Coates, J. Cuzick, M. Gnant, T. Aihara, J. Bliss, F. Boccardo, R. C. Coombes, P. Dubsky, M. Kaufmann, L. Kilburn, F. Perrone, D. Rea, B. Thürlimann, C. Van De Velde, M. Baum, A. Buzdar, I. Sestak, C. Markopoulos, C. Fesl, R. Jakesz, M. Colleoni, R. Gelber, M. Regan, G. Von Minckwitz, C. Snowdon, C. Geyer, Early Breast Cancer Trialists’ Collaborative Group

Internal Medicine

Research output: Contribution to journal › Article › peer-review

1004 Scopus citations

Abstract

Background The optimal ways of using aromatase inhibitors or tamoxifen as endocrine treatment for early breast cancer remains uncertain. Methods We undertook meta-analyses of individual data on 31 920 postmenopausal women with oestrogen-receptorpositive early breast cancer in the randomised trials of 5 years of aromatase inhibitor versus 5 years of tamoxifen; of 5 years of aromatase inhibitor versus 2-3 years of tamoxifen then aromatase inhibitor to year 5; and of 2-3 years of tamoxifen then aromatase inhibitor to year 5 versus 5 years of tamoxifen. Primary outcomes were any recurrence of breast cancer, breast cancer mortality, death without recurrence, and all-cause mortality. Intention-to-treat log-rank analyses, stratifi ed by age, nodal status, and trial, yielded aromatase inhibitor versus tamoxifen fi rst-event rate ratios (RRs). Findings In the comparison of 5 years of aromatase inhibitor versus 5 years of tamoxifen, recurrence RRs favoured aromatase inhibitors signifi cantly during years 0-1 (RR 0.64, 95% CI 0.52-0.78) and 2-4 (RR 0.80, 0.68-0.93), and non-signifi cantly thereafter. 10-year breast cancer mortality was lower with aromatase inhibitors than tamoxifen (12.1% vs 14.2%; RR 0.85, 0.75-0.96; 2p=0.009). In the comparison of 5 years of aromatase inhibitor versus 2-3 years of tamoxifen then aromatase inhibitor to year 5, recurrence RRs favoured aromatase inhibitors signifi cantly during years 0-1 (RR 0.74, 0.62-0.89) but not while both groups received aromatase inhibitors during years 2-4, or thereafter; overall in these trials, there were fewer recurrences with 5 years of aromatase inhibitors than with tamoxifen then aromatase inhibitors (RR 0.90, 0.81-0.99; 2p=0.045), though the breast cancer mortality reduction was not signifi cant (RR 0.89, 0.78-1.03; 2p=0.11). In the comparison of 2-3 years of tamoxifen then aromatase inhibitor to year 5 versus 5 years of tamoxifen, recurrence RRs favoured aromatase inhibitors signifi cantly during years 2-4 (RR 0.56, 0.46-0.67) but not subsequently, and 10-year breast cancer mortality was lower with switching to aromatase inhibitors than with remaining on tamoxifen (8.7% vs 10.1%; 2p=0.015). Aggregating all three types of comparison, recurrence RRs favoured aromatase inhibitors during periods when treatments diff ered (RR 0.70, 0.64-0.77), but not signifi cantly thereafter (RR 0.93, 0.86-1.01; 2p=0.08). Breast cancer mortality was reduced both while treatments diff ered (RR 0.79, 0.67-0.92), and subsequently (RR 0.89, 0.81-0.99), and for all periods combined (RR 0.86, 0.80-0.94; 2p=0.0005). All-cause mortality was also reduced (RR 0.88, 0.82-0.94; 2p=0.0003). RRs diff ered little by age, body-mass index, stage, grade, progesterone receptor status, or HER2 status. There were fewer endometrial cancers with aromatase inhibitors than tamoxifen (10-year incidence 0.4% vs 1.2%; RR 0.33, 0.21-0.51) but more bone fractures (5-year risk 8.2% vs 5.5%; RR 1.42, 1.28-1.57); non-breast-cancer mortality was similar. Interpretation Aromatase inhibitors reduce recurrence rates by about 30% (proportionately) compared with tamoxifen while treatments diff er, but not thereafter. 5 years of an aromatase inhibitor reduces 10-year breast cancer mortality rates by about 15% compared with 5 years of tamoxifen, hence by about 40% (proportionately) compared with no endocrine treatment.

Original language	English (US)
Pages (from-to)	1341-1352
Number of pages	12
Journal	The Lancet
Volume	386
Issue number	10001
DOIs	https://doi.org/10.1016/S0140-6736(15)61074-1
State	Published - Oct 3 2015

ASJC Scopus subject areas

General Medicine

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10.1016/S0140-6736(15)61074-1

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Bradley, R., Burrett, J., Clarke, M., Davies, C., Duane, F., Evans, V., Gettins, L., Godwin, J., Gray, R., Liu, H., McGale, P., MacKinnon, E., McHugh, T., James, S., Morris, P., Pan, H., Peto, R., Read, S., Taylor, C., ... Early Breast Cancer Trialists’ Collaborative Group (2015). Aromatase inhibitors versus tamoxifen in early breast cancer: Patient-level meta-analysis of the randomised trials. The Lancet, 386(10001), 1341-1352. https://doi.org/10.1016/S0140-6736(15)61074-1

Bradley, R, Burrett, J, Clarke, M, Davies, C, Duane, F, Evans, V, Gettins, L, Godwin, J, Gray, R, Liu, H, McGale, P, MacKinnon, E, McHugh, T, James, S, Morris, P, Pan, H, Peto, R, Read, S, Taylor, C, Wang, Y, Wang, Z, Dowsett, M, Forbes, JF, Ingle, J, Coates, A, Cuzick, J, Gnant, M, Aihara, T, Bliss, J, Boccardo, F, Coombes, RC, Dubsky, P, Kaufmann, M, Kilburn, L, Perrone, F, Rea, D, Thürlimann, B, Van De Velde, C, Baum, M, Buzdar, A, Sestak, I, Markopoulos, C, Fesl, C, Jakesz, R, Colleoni, M, Gelber, R, Regan, M, Von Minckwitz, G, Snowdon, C, Geyer, C & Early Breast Cancer Trialists’ Collaborative Group 2015, 'Aromatase inhibitors versus tamoxifen in early breast cancer: Patient-level meta-analysis of the randomised trials', The Lancet, vol. 386, no. 10001, pp. 1341-1352. https://doi.org/10.1016/S0140-6736(15)61074-1

@article{2ca8f8cf62ce43bf8f0ff7eab4e3bc39,

title = "Aromatase inhibitors versus tamoxifen in early breast cancer: Patient-level meta-analysis of the randomised trials",

abstract = "Background The optimal ways of using aromatase inhibitors or tamoxifen as endocrine treatment for early breast cancer remains uncertain. Methods We undertook meta-analyses of individual data on 31 920 postmenopausal women with oestrogen-receptorpositive early breast cancer in the randomised trials of 5 years of aromatase inhibitor versus 5 years of tamoxifen; of 5 years of aromatase inhibitor versus 2-3 years of tamoxifen then aromatase inhibitor to year 5; and of 2-3 years of tamoxifen then aromatase inhibitor to year 5 versus 5 years of tamoxifen. Primary outcomes were any recurrence of breast cancer, breast cancer mortality, death without recurrence, and all-cause mortality. Intention-to-treat log-rank analyses, stratifi ed by age, nodal status, and trial, yielded aromatase inhibitor versus tamoxifen fi rst-event rate ratios (RRs). Findings In the comparison of 5 years of aromatase inhibitor versus 5 years of tamoxifen, recurrence RRs favoured aromatase inhibitors signifi cantly during years 0-1 (RR 0.64, 95% CI 0.52-0.78) and 2-4 (RR 0.80, 0.68-0.93), and non-signifi cantly thereafter. 10-year breast cancer mortality was lower with aromatase inhibitors than tamoxifen (12.1% vs 14.2%; RR 0.85, 0.75-0.96; 2p=0.009). In the comparison of 5 years of aromatase inhibitor versus 2-3 years of tamoxifen then aromatase inhibitor to year 5, recurrence RRs favoured aromatase inhibitors signifi cantly during years 0-1 (RR 0.74, 0.62-0.89) but not while both groups received aromatase inhibitors during years 2-4, or thereafter; overall in these trials, there were fewer recurrences with 5 years of aromatase inhibitors than with tamoxifen then aromatase inhibitors (RR 0.90, 0.81-0.99; 2p=0.045), though the breast cancer mortality reduction was not signifi cant (RR 0.89, 0.78-1.03; 2p=0.11). In the comparison of 2-3 years of tamoxifen then aromatase inhibitor to year 5 versus 5 years of tamoxifen, recurrence RRs favoured aromatase inhibitors signifi cantly during years 2-4 (RR 0.56, 0.46-0.67) but not subsequently, and 10-year breast cancer mortality was lower with switching to aromatase inhibitors than with remaining on tamoxifen (8.7% vs 10.1%; 2p=0.015). Aggregating all three types of comparison, recurrence RRs favoured aromatase inhibitors during periods when treatments diff ered (RR 0.70, 0.64-0.77), but not signifi cantly thereafter (RR 0.93, 0.86-1.01; 2p=0.08). Breast cancer mortality was reduced both while treatments diff ered (RR 0.79, 0.67-0.92), and subsequently (RR 0.89, 0.81-0.99), and for all periods combined (RR 0.86, 0.80-0.94; 2p=0.0005). All-cause mortality was also reduced (RR 0.88, 0.82-0.94; 2p=0.0003). RRs diff ered little by age, body-mass index, stage, grade, progesterone receptor status, or HER2 status. There were fewer endometrial cancers with aromatase inhibitors than tamoxifen (10-year incidence 0.4% vs 1.2%; RR 0.33, 0.21-0.51) but more bone fractures (5-year risk 8.2% vs 5.5%; RR 1.42, 1.28-1.57); non-breast-cancer mortality was similar. Interpretation Aromatase inhibitors reduce recurrence rates by about 30% (proportionately) compared with tamoxifen while treatments diff er, but not thereafter. 5 years of an aromatase inhibitor reduces 10-year breast cancer mortality rates by about 15% compared with 5 years of tamoxifen, hence by about 40% (proportionately) compared with no endocrine treatment.",

author = "R. Bradley and J. Burrett and M. Clarke and C. Davies and F. Duane and V. Evans and L. Gettins and J. Godwin and R. Gray and H. Liu and P. McGale and E. MacKinnon and T. McHugh and S. James and P. Morris and H. Pan and R. Peto and S. Read and C. Taylor and Y. Wang and Z. Wang and M. Dowsett and Forbes, {J. F.} and J. Ingle and A. Coates and J. Cuzick and M. Gnant and T. Aihara and J. Bliss and F. Boccardo and Coombes, {R. C.} and P. Dubsky and M. Kaufmann and L. Kilburn and F. Perrone and D. Rea and B. Th{\"u}rlimann and {Van De Velde}, C. and M. Baum and A. Buzdar and I. Sestak and C. Markopoulos and C. Fesl and R. Jakesz and M. Colleoni and R. Gelber and M. Regan and {Von Minckwitz}, G. and C. Snowdon and C. Geyer and {Early Breast Cancer Trialists{\textquoteright} Collaborative Group}",

note = "Funding Information: Clinical Trial Service Unit (CTSU) staff policy excludes honoraria or consultancy fees for any member of the Early Breast Cancer Trialists' Collaborative Group Secretariat. EBCTCG is funded by Cancer Research UK and UK Medical Research Council grants to the CTSU. JB reports grants, personal fees, and non-financial support from Pfizer during the conduct of the study; outside the submitted work she reports grants from Pfizer, GlaxoSmithKline, Novartis, AstraZeneca, Clovis, and Janssen-Cilag. RCC reports financial and non-financial support from Pfizer to Imperial College, London during the conduct of the study; outside the submitted work he has received personal fees (speaker fees) from Pfizer. JC reports grants from AstraZeneca, outside the submitted work. MD reports grants from Pfizer, Novartis, and AstraZeneca, and personal fees from Pfizer and AstraZeneca, outside the submitted work. PD reports grants and non-financial support from Agendia and Sividon, grants from Nanostring Technologies, personal fees and travel support from AstraZeneca, personal fees from Pfizer and TEVA-ratiopharm, and travel support from Novartis, outside the submitted work. JFF reports grants from National Health & Medical Research Council, during the conduct of the study. MG reports grants and personal fees from Novartis, Roche, and GlaxoSmithKline, grants from Sanofi-Aventis, Pfizer, and Smith Medical, and personal fees from AstraZeneca, Nanostring Technologies, and Accelsiors, outside the submitted work. LK reports funding from Pfizer for the IES study. FP reports grants and non-financial support from AstraZeneca and non-financial support from Novartis, during the conduct of the study. BT reports grants, personal fees, and compensation received by the hospital for research work from Novartis, grants and personal fees from AstraZeneca, and grants from OSKK, during the conduct of the study, outside the submitted work, contracts for clinical research and honoraria for other services were received by the hospital from Novartis, AstraZeneca, and Pfizer; BT also holds stock in Novartis. TA, FB, RB, AC, CD, RG, JI, MK, HP, RP, DR, and CvdV declare no competing interests. Publisher Copyright: {\textcopyright} Early Breast Cancer Trialists{\textquoteright} Collaborative Group (EBCTCG).",

year = "2015",

month = oct,

day = "3",

doi = "10.1016/S0140-6736(15)61074-1",

language = "English (US)",

volume = "386",

pages = "1341--1352",

journal = "The Lancet",

issn = "0140-6736",

publisher = "Elsevier Limited",

number = "10001",

}

TY - JOUR

T1 - Aromatase inhibitors versus tamoxifen in early breast cancer

T2 - Patient-level meta-analysis of the randomised trials

AU - Bradley, R.

AU - Burrett, J.

AU - Clarke, M.

AU - Davies, C.

AU - Duane, F.

AU - Evans, V.

AU - Gettins, L.

AU - Godwin, J.

AU - Gray, R.

AU - Liu, H.

AU - McGale, P.

AU - MacKinnon, E.

AU - McHugh, T.

AU - James, S.

AU - Morris, P.

AU - Pan, H.

AU - Peto, R.

AU - Read, S.

AU - Taylor, C.

AU - Wang, Y.

AU - Wang, Z.

AU - Dowsett, M.

AU - Forbes, J. F.

AU - Ingle, J.

AU - Coates, A.

AU - Cuzick, J.

AU - Gnant, M.

AU - Aihara, T.

AU - Bliss, J.

AU - Boccardo, F.

AU - Coombes, R. C.

AU - Dubsky, P.

AU - Kaufmann, M.

AU - Kilburn, L.

AU - Perrone, F.

AU - Rea, D.

AU - Thürlimann, B.

AU - Van De Velde, C.

AU - Baum, M.

AU - Buzdar, A.

AU - Sestak, I.

AU - Markopoulos, C.

AU - Fesl, C.

AU - Jakesz, R.

AU - Colleoni, M.

AU - Gelber, R.

AU - Regan, M.

AU - Von Minckwitz, G.

AU - Snowdon, C.

AU - Geyer, C.

AU - Early Breast Cancer Trialists’ Collaborative Group

N1 - Funding Information: Clinical Trial Service Unit (CTSU) staff policy excludes honoraria or consultancy fees for any member of the Early Breast Cancer Trialists' Collaborative Group Secretariat. EBCTCG is funded by Cancer Research UK and UK Medical Research Council grants to the CTSU. JB reports grants, personal fees, and non-financial support from Pfizer during the conduct of the study; outside the submitted work she reports grants from Pfizer, GlaxoSmithKline, Novartis, AstraZeneca, Clovis, and Janssen-Cilag. RCC reports financial and non-financial support from Pfizer to Imperial College, London during the conduct of the study; outside the submitted work he has received personal fees (speaker fees) from Pfizer. JC reports grants from AstraZeneca, outside the submitted work. MD reports grants from Pfizer, Novartis, and AstraZeneca, and personal fees from Pfizer and AstraZeneca, outside the submitted work. PD reports grants and non-financial support from Agendia and Sividon, grants from Nanostring Technologies, personal fees and travel support from AstraZeneca, personal fees from Pfizer and TEVA-ratiopharm, and travel support from Novartis, outside the submitted work. JFF reports grants from National Health & Medical Research Council, during the conduct of the study. MG reports grants and personal fees from Novartis, Roche, and GlaxoSmithKline, grants from Sanofi-Aventis, Pfizer, and Smith Medical, and personal fees from AstraZeneca, Nanostring Technologies, and Accelsiors, outside the submitted work. LK reports funding from Pfizer for the IES study. FP reports grants and non-financial support from AstraZeneca and non-financial support from Novartis, during the conduct of the study. BT reports grants, personal fees, and compensation received by the hospital for research work from Novartis, grants and personal fees from AstraZeneca, and grants from OSKK, during the conduct of the study, outside the submitted work, contracts for clinical research and honoraria for other services were received by the hospital from Novartis, AstraZeneca, and Pfizer; BT also holds stock in Novartis. TA, FB, RB, AC, CD, RG, JI, MK, HP, RP, DR, and CvdV declare no competing interests. Publisher Copyright: © Early Breast Cancer Trialists’ Collaborative Group (EBCTCG).

PY - 2015/10/3

Y1 - 2015/10/3

N2 - Background The optimal ways of using aromatase inhibitors or tamoxifen as endocrine treatment for early breast cancer remains uncertain. Methods We undertook meta-analyses of individual data on 31 920 postmenopausal women with oestrogen-receptorpositive early breast cancer in the randomised trials of 5 years of aromatase inhibitor versus 5 years of tamoxifen; of 5 years of aromatase inhibitor versus 2-3 years of tamoxifen then aromatase inhibitor to year 5; and of 2-3 years of tamoxifen then aromatase inhibitor to year 5 versus 5 years of tamoxifen. Primary outcomes were any recurrence of breast cancer, breast cancer mortality, death without recurrence, and all-cause mortality. Intention-to-treat log-rank analyses, stratifi ed by age, nodal status, and trial, yielded aromatase inhibitor versus tamoxifen fi rst-event rate ratios (RRs). Findings In the comparison of 5 years of aromatase inhibitor versus 5 years of tamoxifen, recurrence RRs favoured aromatase inhibitors signifi cantly during years 0-1 (RR 0.64, 95% CI 0.52-0.78) and 2-4 (RR 0.80, 0.68-0.93), and non-signifi cantly thereafter. 10-year breast cancer mortality was lower with aromatase inhibitors than tamoxifen (12.1% vs 14.2%; RR 0.85, 0.75-0.96; 2p=0.009). In the comparison of 5 years of aromatase inhibitor versus 2-3 years of tamoxifen then aromatase inhibitor to year 5, recurrence RRs favoured aromatase inhibitors signifi cantly during years 0-1 (RR 0.74, 0.62-0.89) but not while both groups received aromatase inhibitors during years 2-4, or thereafter; overall in these trials, there were fewer recurrences with 5 years of aromatase inhibitors than with tamoxifen then aromatase inhibitors (RR 0.90, 0.81-0.99; 2p=0.045), though the breast cancer mortality reduction was not signifi cant (RR 0.89, 0.78-1.03; 2p=0.11). In the comparison of 2-3 years of tamoxifen then aromatase inhibitor to year 5 versus 5 years of tamoxifen, recurrence RRs favoured aromatase inhibitors signifi cantly during years 2-4 (RR 0.56, 0.46-0.67) but not subsequently, and 10-year breast cancer mortality was lower with switching to aromatase inhibitors than with remaining on tamoxifen (8.7% vs 10.1%; 2p=0.015). Aggregating all three types of comparison, recurrence RRs favoured aromatase inhibitors during periods when treatments diff ered (RR 0.70, 0.64-0.77), but not signifi cantly thereafter (RR 0.93, 0.86-1.01; 2p=0.08). Breast cancer mortality was reduced both while treatments diff ered (RR 0.79, 0.67-0.92), and subsequently (RR 0.89, 0.81-0.99), and for all periods combined (RR 0.86, 0.80-0.94; 2p=0.0005). All-cause mortality was also reduced (RR 0.88, 0.82-0.94; 2p=0.0003). RRs diff ered little by age, body-mass index, stage, grade, progesterone receptor status, or HER2 status. There were fewer endometrial cancers with aromatase inhibitors than tamoxifen (10-year incidence 0.4% vs 1.2%; RR 0.33, 0.21-0.51) but more bone fractures (5-year risk 8.2% vs 5.5%; RR 1.42, 1.28-1.57); non-breast-cancer mortality was similar. Interpretation Aromatase inhibitors reduce recurrence rates by about 30% (proportionately) compared with tamoxifen while treatments diff er, but not thereafter. 5 years of an aromatase inhibitor reduces 10-year breast cancer mortality rates by about 15% compared with 5 years of tamoxifen, hence by about 40% (proportionately) compared with no endocrine treatment.

AB - Background The optimal ways of using aromatase inhibitors or tamoxifen as endocrine treatment for early breast cancer remains uncertain. Methods We undertook meta-analyses of individual data on 31 920 postmenopausal women with oestrogen-receptorpositive early breast cancer in the randomised trials of 5 years of aromatase inhibitor versus 5 years of tamoxifen; of 5 years of aromatase inhibitor versus 2-3 years of tamoxifen then aromatase inhibitor to year 5; and of 2-3 years of tamoxifen then aromatase inhibitor to year 5 versus 5 years of tamoxifen. Primary outcomes were any recurrence of breast cancer, breast cancer mortality, death without recurrence, and all-cause mortality. Intention-to-treat log-rank analyses, stratifi ed by age, nodal status, and trial, yielded aromatase inhibitor versus tamoxifen fi rst-event rate ratios (RRs). Findings In the comparison of 5 years of aromatase inhibitor versus 5 years of tamoxifen, recurrence RRs favoured aromatase inhibitors signifi cantly during years 0-1 (RR 0.64, 95% CI 0.52-0.78) and 2-4 (RR 0.80, 0.68-0.93), and non-signifi cantly thereafter. 10-year breast cancer mortality was lower with aromatase inhibitors than tamoxifen (12.1% vs 14.2%; RR 0.85, 0.75-0.96; 2p=0.009). In the comparison of 5 years of aromatase inhibitor versus 2-3 years of tamoxifen then aromatase inhibitor to year 5, recurrence RRs favoured aromatase inhibitors signifi cantly during years 0-1 (RR 0.74, 0.62-0.89) but not while both groups received aromatase inhibitors during years 2-4, or thereafter; overall in these trials, there were fewer recurrences with 5 years of aromatase inhibitors than with tamoxifen then aromatase inhibitors (RR 0.90, 0.81-0.99; 2p=0.045), though the breast cancer mortality reduction was not signifi cant (RR 0.89, 0.78-1.03; 2p=0.11). In the comparison of 2-3 years of tamoxifen then aromatase inhibitor to year 5 versus 5 years of tamoxifen, recurrence RRs favoured aromatase inhibitors signifi cantly during years 2-4 (RR 0.56, 0.46-0.67) but not subsequently, and 10-year breast cancer mortality was lower with switching to aromatase inhibitors than with remaining on tamoxifen (8.7% vs 10.1%; 2p=0.015). Aggregating all three types of comparison, recurrence RRs favoured aromatase inhibitors during periods when treatments diff ered (RR 0.70, 0.64-0.77), but not signifi cantly thereafter (RR 0.93, 0.86-1.01; 2p=0.08). Breast cancer mortality was reduced both while treatments diff ered (RR 0.79, 0.67-0.92), and subsequently (RR 0.89, 0.81-0.99), and for all periods combined (RR 0.86, 0.80-0.94; 2p=0.0005). All-cause mortality was also reduced (RR 0.88, 0.82-0.94; 2p=0.0003). RRs diff ered little by age, body-mass index, stage, grade, progesterone receptor status, or HER2 status. There were fewer endometrial cancers with aromatase inhibitors than tamoxifen (10-year incidence 0.4% vs 1.2%; RR 0.33, 0.21-0.51) but more bone fractures (5-year risk 8.2% vs 5.5%; RR 1.42, 1.28-1.57); non-breast-cancer mortality was similar. Interpretation Aromatase inhibitors reduce recurrence rates by about 30% (proportionately) compared with tamoxifen while treatments diff er, but not thereafter. 5 years of an aromatase inhibitor reduces 10-year breast cancer mortality rates by about 15% compared with 5 years of tamoxifen, hence by about 40% (proportionately) compared with no endocrine treatment.

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UR - http://www.scopus.com/inward/citedby.url?scp=84944162380&partnerID=8YFLogxK

U2 - 10.1016/S0140-6736(15)61074-1

DO - 10.1016/S0140-6736(15)61074-1

M3 - Article

C2 - 26211827

AN - SCOPUS:84944162380

SN - 0140-6736

VL - 386

SP - 1341

EP - 1352

JO - The Lancet

JF - The Lancet

IS - 10001

ER -

Aromatase inhibitors versus tamoxifen in early breast cancer: Patient-level meta-analysis of the randomised trials

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