Effect of NHS breast screening programme on mortality from breast cancer in England and Wales, 1990-8: comparison of observed with predicted mortality

doi:10.1136/bmj.321.7262.665

BMJ 2000;321:665-669 ( 16 September )

Papers

Effect of NHS breast screening programme on mortality from breast cancer in England and Wales, 1990-8: comparison of observed with predicted mortality

Editorial by Nystrøm

R G Blanks, epidemiologist ^a, S M Moss, associate director ^a, C E McGahan, statistician ^a, M J Quinn, director, National Cancer Intelligence Centre ^b, P J Babb, epidemiologist ^b.

^a Cancer Screening Evaluation Unit, Institute of Cancer Research, Section of Epidemiology, Sutton, Surrey SM2 5NG, ^b Office for National Statistics, Demography and Health Division, London SW1V 2QQ

Correspondence to: S M Moss s.moss{at}icr.ac.uk

Abstract

Top
Abstract
Introduction
Method
Results
Discussion
Appendix
References

Objective: To assess the impact of the NHS breast screeningprogramme on mortality from breast cancer in women aged 55-69years over the period 1990-8.
Design: Age cohort model with data for 1971-89 usedto predict mortality for 1990-8 with assumption of no major effectfrom screening or improvements in treatment until after 1989.Effect of screening and other factors on mortality estimated bycomparing three year moving averages of observed mortality withthose predicted (by five year age groups from 50-54 to 75-79),the effect of screening being restricted to certain agegroups.
Setting: England andWales.
Subjects: Women aged 40 to 79years.
Results: Compared with predicted mortality in the absenceof screening or other effects the total reduction in mortalityfrom breast cancer in 1998 in women aged 55-69 was estimated as21.3%. Direct effect of screening was estimated as 6.4% (rangeof estimates from 5.4-11.8%). Effect of all other factors (improvedtreatment with tamoxifen and chemotherapy, and earlier presentationoutside the screening programme) was estimated as 14.9% (range12.2-14.9%).
Conclusions: By 1998 both screening and other factors,including improvements in treatment, had resulted in substantialreductions in mortality from breast cancer. Many deaths in the1990s will be of women diagnosed in the 1980s and early 1990s,before invitation to screening. Further major effects from screeningand treatment are expected, which together with cohort effectsshould result in further substantial reductions in mortality frombreast cancer, particularly for women aged 55-69, over the next10years.

Introduction

Top
Abstract
Introduction
Method
Results
Discussion
Appendix
References

The NHS breast screening programme was introduced in England and Wales in 1988, on the recommendations of the Forrest committee.¹These recommendations were based on the findings of randomisedcontrolled trials, which showed that mammography could reducemortality from breast cancer in women aged 50 years and over by25-30% over a period of about 10 years. In England and Wales womenaged 50-64 are invited for screening every three years. Evidencefrom the programme itself indicates, and national incidence ratesconfirm, that the build up of activity was gradual and that the"prevalent" round of screening was not completed until1995.

In 1992 the Department of Health set a target for breast cancer of a reduction in mortality of 25% in the age group invitedfor screening by the year 2000.² It was subsequently acknowledgedthat this target should be applied to the age group 55-69 years.Screening would not be expected to affect mortality in the 50-54years age group because the average age at first screening forwomen in the programme is 51.5 years (as women are first invitedbetween the ages of 50 and 52), and in the randomised controlledtrials there was little or no effect of screening in the firstfour years. Also survival from breast cancer in the late 1980swas good (five year relative survival rate was almost 70% and10 year survival over 50%)³ and will have been higher in womendetected by screening because of earlier detection during thepreclinical phase. The programme has set targets relating to uptakeand rates of cancer detection, which, if achieved, should eventuallylead to the target reduction in mortality of 25%.⁴

The targets for cancer detection are based on the detection rates observed in the Swedish two county randomised controlledtrial.⁵ In the analysis of this trial, all deaths from breastcancer in women with date of diagnosis before the date of entryto the trial in both the study and control arms were excluded.In 1989, Day suggested that the reduction in mortality from breastcancer in the target population should be at least 25% after 10years from the start of screening, but only in those women freefrom breast cancer when first invited to screening.⁶ Nationalmortality statistics will include both women who were and werenot free from breast cancer at the time of their first invitation.The further away in time from the start of screening, the greaterwill be the proportion of women in the former category. Many deathsfrom breast cancer in the 1990s will be in women diagnosed withbreast cancer before any invitation to screening, as full coverageof the population of England and Wales did not occur until 1995.Consequently the impact of screening on breast cancer on the nationalmortality statistics by the year 2000 is likely to be much lessthan 25%.²

Mortality from breast cancer began falling in England and Wales from around 1990, before the programme could have been expectedto have a major impact.⁷ By 1994, in the age group 55-69 years,where mortality would be affected by screening, there was a 12%reduction compared with prescreening rates in the late 1980s.An explanation for some of this reduction may be the use of adjuvanttamoxifen, which by 1990 was in widespread use for women agedover 50 years. It has been pointed out, however, that there isno direct evidence for such an effect and that by 1993 some reductionin mortality (albeit rather small) would have been expected fromscreening.⁸

Breast cancer mortality in this period may also have been affected by changes in stage at presentation, possibly because ofincreased publicity about breast cancer during the introductionof the screening programme, and by birth cohort effects.⁹ Cohorteffects may cause mortality to increase or decrease in differentage groups and result in the true reduction attributable to screeningand improvements in treatment being over or underestimated. Theterm "improvements in treatment" is used here to include effectsof both changes in treatment and other factors including earlierpresentation outside the age range of women invited for screeningand structural changes in the NHS after the Calman-Hine report.¹⁰

We used an age cohort model based on mortality data for 1971-89 (which would not have been affected by screening) to predictthe mortality from breast cancer for 1990-8. By comparing theobserved mortality in different age groups with that predictedby the model we estimated the separate effects of screening andof improvements in treatment and otherfactors.

Method

Top
Abstract
Introduction
Method
Results
Discussion
Appendix
References

We obtained data on mortality from breast cancer for England and Wales from the database of deaths at the Office for NationalStatistics for 1971-99 by single year of age and calendar yearof death. We reconstructed these data into five year age groups(from 40-44 to 75-79 years) and cohort groups from 1896 to 1946.We corrected the annual numbers of deaths for coding changes thatoccurred in 1984 and 1993 as a result of revised interpretationof WHO rule 3 and for other procedural changes in 1993; the overalladjustment was only a few percentage points for women aged 50-74but greater for younger and older age groups.⁷

We assumed that use of tamoxifen, other treatment changes, and screening would not have had any substantial impact on mortalityuntil 1990 and that age and birth cohort effects were the majorinfluences on mortality from 1971 to1989.

We fitted an age cohort model using five year age groups from 40-44 to 75-79 for 1971-89 using log linear Poisson modellingwith the generalised linear models command in the statisticalpackage STATA. Although we considered that an age cohort modelwas likely to give the best fit we also used age (alone) and ageperiod models for comparison, according to the methods of Claytonand Shifflers.¹¹ The age cohort model was highly significant(P< <0.001) when tested against the age model alone. Other models,such as an age period model did not fit the data well. Althoughthe age cohort model provided a good fit to the data, the 1946cohort estimate was based on only few data and had wide confidencelimits. To provide a better estimate for this cohort we extrapolatedthe rate ratios for the 1896 to 1941 cohorts to 1946 by fittinga quadratic model, after noting that the rate ratios increasedup to the 1926 cohort and decreased thereafter. The final modelwas used to predict the mortality from breast cancer in the absenceof screening or treatment effects for 1990-8 for each five yearagegroup.

From the mid-1980s the use of tamoxifen in women with breast cancer increased rapidly. By 1990 in the Thames regions over90% of women aged over 50 years and over 50% below the age of50 received tamoxifen.¹² Results of randomised controlled trialssuggest a fairly uniform effect of tamoxifen across the age range50-79 years.¹³ The effect of screening, in contrast, will bemore age dependent because of the age range of women invited.Screening will reduce mortality in older age groups as time progresses,influencing mortality in women aged 55-74 by 2000 and those aged55-79 by2005.

Three year moving averages of mortality were used to increase statistical stability: the results in table 1 for 1998 arebased on the average mortality for 1997, 1998, and 1999. We comparedthe observed mortality from national statistics from 1990 to 1998with that predicted by the model for each five year age groupfrom 50-54 to 75-79. For 1990-5 we assumed mortality in age groups50-54, 70-74, and 75-79 to be affected only by factors other thanscreening, and assumed mortality in age groups 55-59, 60-64 and65-69 to be affected by these factors plus screening. After 1995mortality in the 70-74 age group will have been partly affectedby screening (the only age groups not affected by screening are50-54 and 75-79).

Once the baseline predictions of what the mortality would have been over the period 1990-8 in the absence of screening areestablished, our method of apportioning any reduction in mortalitybetween screening and other factors is deterministic. It is thereforenot possible to put conventional confidence intervals around thetwo proportions. We therefore explored the sensitivity of ourresults to changes in the age cohort model by considering twoalternative sets of predicted mortality. Firstly, we assumed thatmortality in each age group would have remained at its rate beforescreening $---$ that is, the rates in each year from 1990 to 1998 inclusivewere taken to be the same as those in 1989. This is more neutralthan the cohort effects predicted by our model, which give decreasingrates in women up to the 60-64 age group and increasing ratesin those over 70 (see below and fig 1). Secondly, we assumed thatthe curvature in the cohort rate ratios (see table in Appendix )was more marked (by 5% points in the youngest and oldest cohorts,pro rata for the others) giving a more extreme divergence in predictedmortality by agegroup.

Results

Top
Abstract
Introduction
Method
Results
Discussion
Appendix
References

Figure 1 shows the observed mortality from breast cancer from 1971 to 1999 by five year age group (solid line) together withthe modelled rates from 1990 to 1998 (dotted lines). Throughoutthe whole period 1971 to 1998, mortality was higher in each successiveage group. Mortality in all age groups increased after 1971, butby the early 1980s the rate in the youngest women (50-54 years)had more or less stabilised. Mortality began to fall soon afterscreening started; the falls seem to have been larger in womenaged 55-69 years than in the other age groups. Details of themodel estimates are shown in the table in the Appendix . The cohortrate ratios show that mortality from breast cancer peaked in womenin the 1926 cohort, with a declining risk in later cohorts. Themodel predicts declining mortality in women under 65 years for1990-8 but an increasing rate in women over 70.

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Fig 1. Mortality from breast cancer by year of death for selected age groups, England and Wales, 1971-99

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Fig 2. Mortality from breast cancer by year of birth for selected age groups, England and Wales, 1971-99

Figure 2 shows the data by year of birth rather than year of death for age groups 50-54 (in which mortality will be affectedonly by improvements in treatment), 55-69 (affected by screeningand improvements in treatment), and 75-79 (affected only by improvementsin treatment). Deaths in 1971 to 1989 have been distinguishedfrom those in 1990 to 1998. The age group 70-74 has been omittedbecause women will have been affected by screening from 1995.The trends in mortality, albeit at different levels, in the threeage groups were similar until screening was introduced. Thereafter,mortality in women aged 55-69 dropped considerably more than inthe other two agegroups.

Table 1 compares observed mortality with that predicted by the model for the two years 1993 and 1998. By 1993 only a smalldirect effect of screening would be expected; 1998 is the lastcomplete year for which three year moving average data are available.The average reduction in mortality in 1993 in age groups 50-54,70-74, and 75-79 was 5.6%. This is assumed to be the contributionfrom improvements in treatment. In the age groups 55-59, 60-64,and 65-69 the average reduction was 8.8%, attributable to bothtreatment and screening. The estimated reduction in mortalitydirectly from screening is therefore 3.2%. In 1998 the averagereduction in mortality in age groups 50-54 and 75-79 had increasedto 14.9% and that in age groups 55-59, 60-64, and 65-69 to 21.3%,giving an estimated direct contribution from screening of 6.4%.

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Table 1. Modelled and observed mortality (rates based on three year averages) from breast cancer per 100 000 in 1993 and 1998 by age group

The overall reductions in mortality in 1998 from the two alternative predictions of mortality are shown in table 2. The correspondingdirect effects of screening were 11.8% and 5.4% and of improvementsin treatment were 12.2% and 12.6%. Consequently, the best estimateof the direct effect of screening is a 6.4% reduction in mortalitywith a range of estimates of 5.4-11.8%, and the best estimatefor improvements in treatment is 14.9% (12.2-14.9%).

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Table 2. Modelled and observed mortality (rates based on three year averages) from breast cancer per 100 000 in 1998 by age group: two alternative estimates

	Discussion

Top Abstract Introduction Method Results Discussion Appendix References

From 1990 to 1998 our analyses show a reduction of up to 21% in mortality from breast cancer that is directly attributableto improvements in treatment, earlier presentation outside ofscreening, and screening itself, after allowance for cohort effectsand changes of coding for breastcancer.

By 1998 the NHS breast screening programme had directly produced a reduction in annual mortality from breast cancer of 6-7%in women aged 55-69, although the sensitivity analysis indicateda probable range of 5-12%. The best estimate of number of deathsfrom breast cancer in the 55-69 year age group prevented by screeningin 1998 was 320 (range 270 to 590). The number of deaths preventedby screening is expected to increase over the coming years asfrom 1995 all women aged 50-64 were invited for screening. Theexpected further effects from screening, together with improvedtreatments such as the use of tamoxifen for five years and theimpact of cohort effects all suggest that mortality in women aged55-69 will continue to decrease over the next 10years.

Methodological difficulties
There are several inherent problems that limitthe precision of our estimate of the reduction in mortality resultingfrom screening. These include errors inherent in projecting mortalityinto future years, such as the fit of the model and the greaterinstability in the numbers of deaths in younger age groups beingprojected forward in time to predict rates in older women. Theage cohort model has, however, also been found by others to bethe best model, and the rate ratios from our model are closelysimilar.¹⁴ Our assumption that an age cohort model would stillhave fitted the data in 1990 to 1998 in the absence of improvementsin treatment and screening effects is impossible to test; butthe potential errors in the observed rates, which are each basedon an average of three years' data, will be relatively small.It could be argued that screening affects the older women in theage range 50-54; if the only group considered to be unaffectedby screening is 75-79 years, the direct reduction in mortalityfrom screening in 1998 increases from 6.4% to 8.5%. Our analysesusing alternative predictions of mortality for 1990-8 have ledto estimates of the mortality reduction from screening of between5.4% and 11.8%. This range indicates the limitations in our methods,but clearly shows that the mortality in women aged 55-69 has decreasedmore than in the adjacent age groups and that this is directlyrelated to the screeningprogramme.

Population screening and randomised controlled trials
It is important to emphasise that deaths inwomen diagnosed with breast cancer before invitation to screeningwill cause a severe dilution of the effect of the screening programmeon national mortality statistics, particularly in the first decadeof screening, compared with the results from randomised controlledtrials. The extent and timing of a reduction in mortality dueto screening will depend on several factors. These include theproportion of deaths from breast cancer in a given year occurringin women diagnosed with the disease before their first invitationto screening and the time period over which 100% coverage of thetarget population is achieved. Given the relatively good survivalrates in the 1980s and that there is excess mortality in womenwith breast cancer 15-20 years after diagnosis ¹⁵ ¹⁶ a largenumber of the deaths that occurred in the 1990s would have beenin women who were diagnosed with breast cancer before invitationto screening. If we take these factors into account and allowfor the fact that in the first years of screening the sensitivityof the process in detecting cancers¹⁷ was some 25% lower thananticipated on the basis of the Swedish two county study,⁵it is likely to be between 2005 and 2010 before the full effectof screening is seen in national breast cancer mortalitystatistics.

Results from a computer simulated model (MISCAN) suggested that 70% of the reported 12% reduction in mortality seen by 1994 $---$ thatis, about 8% $---$ may be due to screening.¹⁸ Our lower estimatedreductions due to screening may be consistent with the lower sensitivityof the screening programme in the early years of screening.¹⁷The earlier "shortfall" in detection of invasive cancer in theprogramme was mostly due to a low sensitivity for small invasivecancers $---$ those least likely to have metastasised and the most importantto detect to achieve a high reduction in mortality. The "steadystate" effect of screening, if we assume the same sensitivityand improvement in prognosis as achieved in the Swedish two countystudy and an uptake of around 70%, has been estimated as a 25%reduction in mortality from breast cancer in women aged 55-69.¹⁸

There are several reasons why the effect of screening in the population screening programme could be different from that observedin the Swedish two county randomised controlled trial. The stageof breast cancers in women diagnosed before the introduction ofscreening in England and Wales may have differed from that inthe control group of the Swedish two county study. A tendencytowards a late stage at presentation would in theory result ina greater potential for the effect of earlier diagnosis. In addition,the effect of screening on mortality is likely to vary accordingto the treatment of early stage disease and in particular theextent to which tamoxifen isused.

Treatment and other effects
We estimated the effect of tamoxifen and otherfactors, excluding the direct effect of screening by 1998, tohave been a reduction in mortality of between 12.2% and 14.9%.The randomised controlled trials for tamoxifen often report onearly stage disease in women who are positive for oestrogen receptor.As about one third of women are negative for oestrogen receptor,and many women with breast cancer do not present with early stagedisease, the benefit of tamoxifen to the population of women withbreast cancer is difficult to predict from the results of randomisedcontrolled trials. Peto has suggested that the absolute benefitproduced by a few years of adjuvant tamoxifen for patients withbreast cancer is not large (50% survival may be increased to 55%or 60%),¹⁹ but the treatment is widely given and the diseaseis common. Improvements in chemotherapy and other factors, includingstructural changes in the NHS, will also have contributed to thisreduction in mortality. Recent work has suggested an additionaleffect of the massive publicity surrounding breast cancer wherebysince the mid-1980s there has been a shift to earlier diagnosisof tumours.⁹ This may explain why mortality from breast cancerdecreased so rapidly in the early 1990s with treatment and earlierpresentation outside the screening programme together with cohorteffects in women under age 70 all contributing to the apparentfalls.

Improvements in screening
Since the early years of screening there havebeen substantial improvements in sensitivity, particularly forsmall invasive cancers,²⁰ as a result of the increased use oftwo view mammography, the use of higher film densities, and increasingexperience ofradiologists.

Conclusions
There has been considerable recent debateover the attribution of the reduction in mortality from breastcancer to improvements in treatment or screening. The purposeof screening is to detect cancers at an earlier stage, when treatmentis more effective. Our research indicates that for 1990-8 improvementsin treatment and screening both probably have major roles in thereduction in mortality from breast cancer. The difficulties inproducing quantitative estimates of the effect of a national screeningprogramme (or improvements in treatment) on mortality are wellrecognised.¹⁸ Such difficulties illustrate the importance ofcarrying out well conducted randomised controlled trials beforethe introduction of population based screening. Continuous monitoringof the performance of the NHS breast screening programme is essential.Recent results of such monitoring suggest that the effect of theprogramme on mortality will increase substantially in future years.²⁰

What is already known on this topic

Screening for breast cancer with mammography has been shown to reduce mortality by 25-30% in randomised controlled trials

Women in England and Wales started to be invited for screening between 1988 and 1995

What this study adds

Analysis of the mortality from breast cancer in England and Wales between 1971 and 1999 shows that between 1990 and 1998 there was a real fall of 21.3% in women aged 55-69

Of this fall, 6.4% has been attributed to screening and 14.9% to improvements in treatment and other factors

The effect of screening on national statistics has been slower to take effect compared with randomised controlled trials partly because many deaths from breast cancer in the 1990s will be in women diagnosed before any invitation to screening

Substantial improvements in screening and the decreasing proportion of deaths of women in whom breast cancer was diagnosed before screening will lead to a continuing decline in mortality in women aged 55-69 over the next ten years

	Acknowledgments

We thank Professor N E Day and Professor M Vessey and the referees for comments on earlier drafts of thispaper.

Contributors: SM and RB initiated the research. RB and CMcG carried out the analysis of the data. The paper was written jointly by SM, RB, MQ, and PB. MQ and PB were responsible for supplying the data and advising on the analysis. SMM is guarantor for the paper.

Footnotes

Funding: The Cancer Screening Evaluation Unit receives support from the Department of Health; the views expressed in thispaper are those of the authors and not necessarily those of theDepartment ofHealth.

Competing interests: Nonedeclared.

Appendix

Top
Abstract
Introduction
Method
Results
Discussion
Appendix
References

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Multiplicative age cohort model with Poisson regression used to estimate mortality from breast cancer, 1990-8

	References

Top Abstract Introduction Method Results Discussion Appendix References

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(Accepted 11 May 2000)

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Smith, R. A., Saslow, D., Andrews Sawyer, K., Burke, W., Costanza, M. E., Evans, W. P. III, Foster, R. S. Jr., Hendrick, E., Eyre, H. J., Sener, S. (2003). American Cancer Society Guidelines for Breast Cancer Screening: Update 2003. CA Cancer J Clin 53: 141-169 [Abstract] [Full text]
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Rapid Responses:

Read all Rapid Responses

The title of the press release.: Luis Gerk de Azevedo Quadros
bmj.com, 15 Sep 2000 [Full text]
Effect of breast cancer screening on breast cancer mortality: Anthony B Miller
bmj.com, 25 Sep 2000 [Full text]
Effect of the NHS breast screening programme on mortality from breast cancer: Graham Layer
bmj.com, 28 Sep 2000 [Full text]