ABC of breast diseases: Breast cancer---epidemiology, risk factors, and genetics

doi:10.1136/bmj.321.7261.624

BMJ 2000;321:624-628 ( 9 September )

Clinical review

ABC of breast diseases

Breast cancer $---$ epidemiology, risk factors, and genetics

K McPherson, C M Steel, J M Dixon.

With 1 million new cases in the world each year, breast cancer is the commonest malignancy in women and comprises 18% of allfemale cancers. In the United Kingdom, where the age standardisedincidence and mortality is the highest in the world, the incidenceamong women aged 50 approaches two per 1000 women per year, andthe disease is the single commonest cause of death among womenaged 40-50, accounting for about a fifth of all deaths in thisage group. There are more than 14 000 deaths each year, and theincidence is increasing particularly among women aged 50-64, probablybecause of breast screening in this age group.

Worldwide incidence of cancers in women (1980)

Site of cancer No of cases (1000s) % of total

Breast 572 18

Cervix 466 15

Colon and rectum 286 9

Stomach 261 8

Endometrium 149 5

Lung 147 5

Ovary 138 4

Mouth and pharynx 121 4

Oesophagus 108 4

Lymphoma 98 3

Of every 1000 women aged 50, two will recently have had breast cancer diagnosed and about 15 will have had a diagnosis madebefore the age of 50, giving a prevalence of breast cancer ofnearly 2%.

Risk factors for breast cancer

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Risk factors for breast...
Prevention of breast cancer

Age
The incidence of breast cancer increases withage, doubling about every 10 years until the menopause, when therate of increase slows dramatically. Compared with lung cancer,the incidence of breast cancer is higher at younger ages. In somecountries there is a flattening of the age-incidence curve afterthe menopause.

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Percentage of all deaths in women attributable to breast cancer

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Standardised mortality for breast cancer in different countries

Geographical variation
Age adjusted incidence and mortality for breastcancer varies by up to a factor of five between countries. Thedifference between Far Eastern and Western countries is diminishingbut is still about fivefold. Studies of migrants from Japan toHawaii show that the rates of breast cancer in migrants assumethe rate in the host country within one or two generations, indicatingthat environmental factors are of greater importance than geneticfactors.

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Age specific incidence and mortality for breast cancer in United Kingdom

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Annual incidence of breast cancer in Japanese women in Japan, Hawaii, and San Francisco and in white women from San Francisco

Age at menarche and menopause
Women who start menstruating early in lifeor who have a late menopause have an increased risk of developingbreast cancer. Women who have a natural menopause after the ageof 55 are twice as likely to develop breast cancer as women whoexperience the menopause before the age of 45. At one extreme,women who undergo bilateral oophorectomy before the age of 35have only 40% of the risk of breast cancer of women who have anatural menopause.

Established and probable risk factors for breast cancer

   Factor Relative risk    High risk group

Age >10 Elderly

Geographical location 5 Developed country

Age at menarche 3 Menarche before age 11

Age at menopause 2 Menopause after age 54

Age at first full pregnancy 3 First child in early 40s

Family history $>=$ 2 Breast cancer in first degree relative when young

Previous benign disease 4-5 Atypical hyperplasia

Cancer in other breast >4

Socioeconomic group 2 Groups I and II

Diet 1.5 High intake of saturated fat

Body weight:

  Premenopausal 0.7 Body mass index >35

  Postmenopausal 2 Body mass index >35

Alcohol consumption 1.3 Excessive intake

Exposure to ionising radiation 3 Abnormal exposure in young females after age 10

Taking exogenous hormones:

  Oral contraceptives 1.24 Current use

  Hormone replacement   therapy 1.35 Use for $>=$ 10 years

  Diethylstilbestrol 2 Use during pregnancy

Age at first pregnancy
Nulliparity and late age at first birth bothincrease the lifetime incidence of breast cancer. The risk ofbreast cancer in women who have their first child after the ageof 30 is about twice that of women who have their first childbefore the age of 20. The highest risk group are those who havea first child after the age of 35; these women appear to be ateven higher risk than nulliparous women. An early age at birthof a second child further reduces the risk of breast cancer.

Familial breast cancer $---$ criteria for identifying women at substantial increased risk

The following categories identify women who have three or more times the population risk of developing breast cancer

: A woman who has:
: $bullet$ One first degree relative with bilateral breast cancer or breast and ovarian cancer or
: $bullet$ One first degree relative with breast cancer diagnosed under the age of 40 years or one first degree male relative with breast cancer diagnosed at any age or
: $bullet$ Two first or second degree relatives with breast cancer diagnosed under the age of 60 years or ovarian cancer at any age on the same side of the family or
: $bullet$ Three first or second relatives with breast and ovarian cancer on the same side of the family
: First degree relative is mother, sister, or daughter. Second degree female relative is grandmother, granddaughter, aunt, or niece

: $bullet$ Families with four or more relatives affected with either breast or ovarian cancer in three generations and one alive affected relative

Family history
Up to 10% of breast cancer in Western countriesis due to genetic predisposition. Breast cancer susceptibilityis generally inherited as an autosomal dominant with limited penetrance.

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Family tree of family with genetically inherited breast cancer

This means that it can be transmitted through either sex and that some family members may transmit the abnormal gene withoutdeveloping cancer themselves. It is not yet known how many breastcancer genes there may be. Two breast cancer genes, BRCA1 andBRCA2, which are located on the long arms of chromosomes 17 and13 respectively, have been identified and account for a substantialproportion of very high risk families $---$ ie those with four or morebreast cancers among close relatives. Both genes are very largeand mutations can occur at almost any position, so that molecularscreening to detect mutation for the first time in an affectedindividual or family is technically demanding. Certain mutationsoccur at high frequency in defined populations. For instance,some 2% of Ashkenazi Jewish women carry either BRCA1 185 del AG(deletion of two base pairs in position 185), BRCA1 5382 ins C(insertion of an extra base pair at position 5382) or BRCA 6174del T (deletion of a single base pair at position 6174), whileBRCA2 999 del 5 (deletion of five base pairs at position 999)accounts for about half of all familial breast cancer in Iceland.Inherited mutations in two other genes, p53 and PTEN, are associatedwith familial syndromes (Li-Fraumeni and Cowden's respectively)that include a high risk of breast cancer but both are rare. Theseare almost certainly other (as yet unidentified) genes that increasethe risk of disease by only a moderate degree $---$ perhaps three orfour-fold above the general population level. These are unlikelyto generate florid multi-case families but they are probably rathercommon and therefore account for a substantial part of the overallgenetic contribution to breastcancer.

Many families affected by breast cancer show an excess of ovarian, colon, prostatic, and other cancers attributable to thesame inherited mutation. Patients with bilateral breast cancer,those who develop a combination of breast cancer and another epithelialcancer, and women who get the disease at an early age are mostlikely to be carrying a genetic mutation that has predisposedthem to developing breast cancer. Most breast cancers that aredue to a genetic mutation occur before the age of 65, and a womanwith a strong family history of breast cancer of early onset whois still unaffected at 65 has probably not inherited the geneticmutation.

A woman's risk of breast cancer is two or more times greater if she has a first degree relative (mother, sister, or daughter)who developed the disease before the age of 50, and the youngerthe relative when she developed breast cancer the greater therisk. For example, a woman whose sister developed breast canceraged 30-39 has a cumulative risk of 10% of developing the diseaseherself by age 65, but that risk is only 5% (close to the populationrisk) if the sister was aged 50-54 at diagnosis. The risk increasesby between four and six times if two first degree relatives developthe disease. For example, a woman with two affected relatives,one who was aged under 50 at diagnosis, has a 25% chance of developingbreast cancer by the age of 65.

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Severe atypical lobular hyperplasia

Previous benign breast disease
Women with severe atypical epithelial hyperplasiahave a four to five times higher risk of developing breast cancerthan women who do not have any proliferative changes in theirbreast. Women with this change and a family history of breastcancer (first degree relative) have a ninefold increase in risk.Women with palpable cysts, complex fibroadenomas, duct papillomas,sclerosis adenosis, and moderate or florid epithelial hyperplasiahave a slightly higher risk of breast cancer (1.5-3 times) thanwomen without these changes, but this increase is not clinicallyimportant.

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Relation between breast cancer mortality in various countries and fat consumption

Radiation
A doubling of risk of breast cancer was observedamong teenage girls exposed to radiation during the Second WorldWar. Ionising radiation also increases risk later in life, particularlywhen exposure is during rapid breast formation. Mammographic screeningis associated with a net decrease in mortality from breast canceramong women aged over50.

Lifestyle

Diet
Although there is a close correlation betweenthe incidence of breast cancer and dietary fat intake in populations,the true relation between fat intake and breast cancer does notappear to be particularly strong or consistent.

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Cumulative risk of breast cancer in women who were aged 10-19 years when exposed to radiation from atomic bombs during the Second World War

Weight
Obesity is associated with a twofold increasein the risk of breast cancer in postmenopausal women whereas amongpremenopausal women it is associated with a reducedincidence.

Alcohol intake
Some studies have shown a link between alcoholconsumption and incidence of breast cancer, but the relation isinconsistent and the association may be with other dietary factorsrather thanalcohol.

Smoking
Smoking is of no importance in the aetiologyof breastcancer.

Oral contraceptive
While women are taking oral contraceptivesand for 10 years after stopping these agents, there is a smallincrease in the relative risk of developing breast cancer. Thereis no significantly increased risk of having breast cancer diagnosed10 or more years following cessation of the oral contraceptiveagent. Cancers diagnosed in women taking the oral contraceptiveare less likely to be advanced clinically than those diagnosedin women who have never used these agents, relative risk 0.88(0.81-0.95). Duration of use, age at first use, dose and typeof hormone within the contraceptives appear to have no significanteffect on breast cancer risk. Women who begin use before the ageof 20 appear to have a higher relative risk than women who beginoral contraceptive use at an older age. This higher relative riskapplies at an age when the incidence of breast cancer is howeververy low.

Relative risk of breast cancer in relation to use of oral contraceptives

Relative risk 95% CI

>10 years after stopping 1

Current user 1.24 0.96-1.05

1-5 years since stopping 1.16 1.08-1.23

5-9 years since stopping 1.07 1.02-1.13

Hormone replacement therapy
Among current users of HRT and those who haveceased use 1-4 years previously the relative risk of having breastcancer diagnosed increases by a factor of 1.023 (1.011-1.036)for each year of use. This increase is consistent with the effectof a delay in the menopause, because the relative risk of breastcancer increases in never users by a factor of 1.028 (1.021-1.034)for each year older at the menopause. The risk of breast cancerappears higher with combined oestrogen and progestogen combinations.HRT increases breast density and reduces the sensitivity and specificityof breast screening. Cancers diagnosed in women taking HRT tendto be less advanced clinically than those diagnosed in women whohave not used HRT. Current evidence suggests that HRT does notincrease breast cancermortality.

Prevention of breast cancer

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Risk factors for breast...
Prevention of breast cancer

Screening as currently practised can reduce mortality but not incidence, and then only in a particular age group. Advancesin treatment have produced significant but modest survival benefits.A better appreciation of factors important in the aetiology ofbreast cancer would raise the possibility of disease prevention.

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The effect of tamoxifen on the incidence of breast cancer in the NSABP Prevention Study in relation to age

Relationship of HRT to breast cancer development

   Time on HRT Breast cancers
over the
20 years from
age 50-70
Extra breast
cancers in
HRT users
Individual
risk of women
over 20 years

Never 45 per 1000 $---$ 1 in 22

5 years use 47 per 1000 2 per 1000 1 in 21

10 years use 51 per 1000 6 per 1000 1 in 19

15 years use 57 per 1000 12 per 1000 1 in 17-18

Hormonal control
One promising avenue for primary preventionis influencing the hormonal milieu of women at risk. During trialsof tamoxifen as an adjuvant treatment for breast cancer, the numberof contralateral breast cancers was less than expected, suggestingthat this drug might have a role in preventing breast cancer.Studies comparing tamoxifen with placebo in women at high riskof breast cancer have been reported and show conflicting results.The NSABP study randomised 3338 women with a risk equal to thatof a 60 year old woman and showed a 47% reduction in the riskof invasive breast cancer and a 50% reduction in the rate of non-invasivebreast cancer in women taking tamoxifen. Benefits of tamoxifenwere observed in all age groups. The effect found for tamoxifenalso reduced the overall incidence of osteoporotic fractures ofthe hip, spine and radius by 19%. It increased the relative riskof endometrial cancer by 2.5 but this risk was limited to womenaged 50 or older. More women over 50 in the tamoxifen group developeddeep venous thrombosis, pulmonary emboli and stroke. An Italianstudy and a UK study have failed to confirm the benefits of tamoxifenbut overall evidence suggests there is a benefit of tamoxifenin preventing breast cancer. The ongoing UK trial should demonstratewhether this translates into a reduction in deaths from breastcancer. Raloxifene, a tamoxifen-like compound, has been evaluatedin a population of 10 355 postmenopausal women being treated forosteoporosis and has demonstrated a 54% decrease in the numberof breast cancers in the raloxifene group. Both the tamoxifenand raloxifene studies show a selective reduction in the incidenceof oestrogen receptor positive breast cancers.

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Mammograms of patient before and after three years of hormone replacement therapy showing increase in density caused by treatment

Dietary intervention
If specific dietary factors are found to beassociated with an increased risk of breast cancer dietary interventionwill be possible. However, reduction of dietary intake of sucha factor in whole communities may well be difficult to achievewithout major social and cultural changes. Weight gain by morethan 10-20 kg from the weight at age 18 does seem to be associatedwith an increasedrisk.

Other preventive agents
Retinoids affect the growth and differentiationof epithelial cells, and experiments suggest that they may havea role in preventing breast cancer. A clinical trial of fenretinoidhas been reported. In a study of 2972 women with breast cancerrandomly allocated to fenretinoid or no treatment, no significantdifference was seen in contralateral breast cancer between thetwo groups. There was a significant interaction with treatmentand menopausal status with a beneficial effect being seen in premenopausalpatients (adjusted hazard ratio 0.66, 95% CI 0.14-1.07) and anopposite trend on postmenopausal women. Selenium is another possiblecancer preventing agent.

Key references

$bullet$   Bilimoria M, Morrow M. The woman at increased risk for breast cancer: evaluation and management strategies. Cancer J Clin 1995;45:263-78. $bullet$ Futreal PA, Liu Q, Shattuck-Eidens D et al. BRCA1 mutations in primary breast and ovarian carcinomas. Science 1994;266:120-2.

$bullet$   Black DM. The genetics of breast cancer. Eur J Cancer 1994;30a:1957-61. $bullet$ Hill ADK, Doyle JM, McDermott EW, et al. Hereditary breast cancer. Br J Surg 1997;84:1334-9.

$bullet$   Brinton LA, Devesa SS. Etiology and pathogenesis of breast cancer: incidence, demographics and environmental factors. In: Harris JR, Lippman ME, Morrow M, Hellman S, eds. Diseases of the breast. Philadelphia: Lippincott-Raven, 1996:159-68. $bullet$ Isaacs CJD, Peshkin BN, Lerman C. Evaluation and management of women with a strong family history of breast cancer. In: Harris JR, Lippman ME, Morrow M, Osborne CK, eds. Disease of the Breast. Philadelphia: Lippincott Williams & Wilkins, 2000:237-54.

$bullet$   Collaborative Group on Hormonal Factors in Breast Cancer. Breast cancer and hormonal contraceptives: collaborative reanalysis of individual data on 53 297 women with breast cancer and 100 239 women without breast cancer from 54 epidemiological studies. Lancet 1996;347:1713-27. $bullet$ Jordan CV, Costa AF. Chemoprevention. In: Harris JR, Lippman ME, Morrow M, Osborne CK, eds. Disease of the Breast. Philadelphia: Lippincott Williams & Wilkins, 2000:265-80.

$bullet$   Collaborative Group on Hormonal Factors in Breast Cancer. Breast cancer and hormone replacement therapy: collaborative reanalysis of data from 51 epidemiological studies of 52 705 women with breast cancer and 108 411 without breast cancer. Lancet 1997;350:1047-59. $bullet$ Jordan VC, Glusman JE, Eckert S, et al. Raloxifene reduces incident primary breast cancers: integrated data from multicenter double blind placebo controlled, randomised trials in postmenopausal women. Breast Cancer Res Treat 1998;50:227 (abst no 2).

$bullet$   Decker D. Prophylactic mastectomy for familial breast cancer. JAMA 1993;269:2608-9. $bullet$ Powles TJ, Eeles R, Ashley S, et al. Interim analysis of the incident breast cancer in the Royal Marsden Hospital tamoxifen randomised chemoprevention trial. Lancet 1998;362:98.

$bullet$ DeMichele A, Weber BL. Inherited genetic factors. In: Harris JR, Lippman ME, Morrow M, Osborne CK, eds. Disease of the Breast. Philadelphia: Lippincott Williams & Wilkins, 2000:221-36. $bullet$ Veronesi U, Maisonneuve P, Costa A, et al. Prevention of breast cancer with tamoxifen: preliminary findings from the Italian randomised trial among hysterectomised women. Lancet 1998;362:93.

$bullet$   Fisher B, Constantino JP, Wickerman DL et al. Tamoxifen for the prevention of breast cancer: report of the National Surgical Adjuvant Breast and Bowel Project P-1 study. J Natl Cancer Inst 1998;90:1371. $bullet$ Willett WC, Rockhill B, Hankinson SE, et al. Epidemiology and nongenetic causes of breast cancer. In: Harris JR, Lippman ME, Morrow M, Osborne CK, eds. Disease of the Breast. Philadelphia: Lippincott Williams & Wilkins, 2000:175-220.

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The National Surgical Adjuvant Breast and Bowel Project (NSABP) data illustrate the effects of tamoxifen on both invasive and non-invasive breast cancer. Data from the Royal Marsden and the Italian studies include only the number of invasive cancers. The raloxifene data include both invasive and non-invasive breast cancers

Footnotes

K McPherson is professor of public health epidemiology, London School of Hygiene and Tropical Medicine, London, C M Steelis professor of medical and biological sciences, University ofSt Andrews, St Andrews, and J M Dixon is consultant surgeon andsenior lecturer in surgery, Edinburgh Breast Unit, Western GeneralHospital,Edinburgh.

The ABC of breast diseases is edited by J MichaelDixon.

© BMJ 2000

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