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Oral Contraceptives and Cancer Risk


Oral contraceptives (OCs) first became available to American women in the early 1960s. The convenience, effectiveness, and reversibility of action of birth control pills (popularly known as "the pill") have made them the most popular form of birth control in the United States. However, a correlation between estrogen and increased risk of breast cancer has led to continuing controversy about a possible link between OCs and cancer.
This fact sheet addresses only what is known about OC use and the risk of developing cancer. It does not deal with the most serious side effect of OC use-the increased risk of cardiovascular disease for certain groups of women.
Oral Contraceptives
Currently, two types of OCs are available in the United States. The most commonly prescribed OC contains two synthetic versions of natural female hormones (estrogen and progesterone) that are similar to the hormones the ovaries normally produce. Estrogen stimulates the growth and development of the uterus at puberty, thickens the endometrium (the inner lining of the uterus) during the first half of the menstrual cycle, and stimulates changes in breast tissue at puberty and childbirth. The two types of synthetic estrogens used in OCs are ethinyl estradiol and mestranol.
Progesterone, which is produced during the last half of the menstrual cycle, prepares the endometrium to receive the egg. If the egg is fertilized, progesterone secretion continues, preventing release of additional eggs from the ovaries. For this reason, progesterone is called the "pregnancy-supporting" hormone, and scientists believe it to have valuable contraceptive effects. The synthetic progesterone used in OCs is called progestogen or progestin. Norethindrone and levonorgestrel are examples of synthetic progesterones used in OCs.
The second type of OC available in the United States is called the minipill and contains only a progestogen. The minipill is less effective in preventing pregnancy than the combination pill, so it is prescribed less often.
Because medical research suggests that cancers of the female reproductive organs sometimes depend on naturally occurring sex hormones for their development and growth, scientists have been investigating a possible link between OC use and cancer risk. Medical researchers have focused a great deal of attention on OC users over the past 30 years. This scrutiny has produced a wealth of data on OC use and the development of certain cancers, although results of these studies have not always been consistent.
Breast Cancer
A woman's risk of developing breast cancer depends on several factors, some of which are related to her natural hormones. Hormonal factors that increase the risk of breast cancer include conditions that allow high levels of estrogen to persist for long periods of time, such as early age at first menstruation (before age 12), late age at menopause (after age 55), having children after age 30, and not having children at all. A woman's risk of breast cancer increases with the amount of time she is exposed to estrogen.
Because many of the risk factors for breast cancer are related to natural hormones, and because OCs work by manipulating these hormones, there has been some concern about the possible effects of medicines such as OCs on breast cancer risk, especially if women take them for many years. Sufficient time has elapsed since the introduction of OCs to allow investigators to study large numbers of women who took birth control pills for many years, beginning at a young age, and to follow them as they became older.
Studies examining the use of OCs as a risk factor for breast cancer have produced inconsistent results. Scientists suggest the inconsistent findings may have occurred because participants in different studies used OC in different doses and forms. In addition, other factors that influence baseline hormone levels in the women under study may have led to different results among the studies. In general, most studies have not found an overall increased risk for breast cancer associated with OC use. In June 1995, however, investigators at the National Cancer Institute (NCI) reported an increased risk of developing breast cancer among women under age 35 who had used birth control pills for at least 6 months, compared with those who had never used OCs. They also saw a slightly lower, but still elevated, risk among women ages 35 to 44. In addition, their research showed a higher risk among long-term OC users, especially those who had started taking the pill before age 18.
A 1996 analysis of worldwide epidemiologic data, which included information from the 1995 study, found that women who were current or recent users of birth control pills had a slightly elevated risk of developing breast cancer. However, 10 years or more after they stopped using OCs, their risk of developing breast cancer returned to the same level as if they had never used birth control pills.
To conduct this analysis, the researchers examined the results of 54 studies conducted in 25 countries that involved 53,297 women with breast cancer and 100,239 women without breast cancer. More than 200 researchers participated in this combined exhaustive analysis of their original studies, which represented about 90 percent of the epidemiological studies throughout the world that had investigated the possible relationship between OCs and breast cancer.
The return of risk to normal levels after 10 years or more of not taking OCs was consistent regardless of family history of breast cancer, reproductive history, geographic area of residence, ethnic background, differences in study designs, dose and type of hormone, and duration of use. The change in risk also generally held true for age at first use; however, for reasons that were not fully understood, there was a continued elevated risk among women who had started to use OCs before age 20.
Scientists suggest that the slightly elevated risk seen in both current OC users and those who had stopped use less than 10 years previously may not be due to the contraceptive itself. The slightly elevated risk may result from the potential of estrogen to promote the growth of breast cancer cells that are already present, rather than its potential to initiate changes in normal cells leading to the development of cancer.
Furthermore, the observation that the slightly elevated risk of developing breast cancer that was seen in this study peaked during use, declined gradually after OC use had stopped, then returned to normal risk levels 10 years or more after stopping, is not consistent with the usual process of carcinogenesis (the process by which normal cells are transformed into cancer cells). It is more typical for cancer risk to peak decades after exposure, not immediately afterward. Cancer usually is more likely to occur with increased duration and/or degree of exposure to a carcinogen (cancer-causing substance). In this analytical study, neither the dose and type of hormone nor the duration of use affected the risk of developing breast cancer.
Ovarian and Endometrial Cancers
Many studies have found that using OCs reduces a woman's risk of ovarian cancer by 40 to 50 percent compared with women who have not used OCs. The Centers for Disease Control and Prevention's (CDC) Cancer and Steroid Hormone Study (CASH), along with other research conducted over the past 20 years, shows that the longer a woman uses OCs, the lower her risk of ovarian cancer. Moreover, this lowered risk persists long after OC use ceases. The CASH study found that the reduced risk of ovarian cancer is seen in women who have used OCs for as little as 3 to 6 months, and that it continues for 15 years after use ends. Other studies have confirmed that the reduced risk of ovarian cancer continues for at least 10 to 15 years after a woman has stopped taking OCs. Several hypotheses have been offered to explain how oral contraceptives might protect against ovarian cancer, such as a reduction in the number of ovulations a woman has during her lifetime, but the exact mechanism is still not known.
Researchers have also found that OC use may reduce the risk of endometrial cancer. Findings from the CASH study and other reports show that combination OC use can protect against the development of endometrial cancer. The CASH study found that using combination OCs for at least 1 year reduced the risk of developing endometrial cancer to half of that seen for women who never took birth control pills. In addition, the beneficial effect of OC use persisted for at least 15 years after OC users stopped taking birth control pills. Some researchers have found that the protective effect of OCs against endometrial cancer increases with the length of time combination OCs are used, but results have not been consistent.
The reduction in risk of ovarian and endometrial cancers from OC use does not apply to the sequential type of pill, in which each monthly cycle contains 16 estrogen pills followed by 5 estrogen-plus-progesterone pills. (Sequential OCs were taken off the market in 1976, so few women have been exposed to them.) Researchers believe OCs reduce cancer risk only when the estrogen content of birth control pills is balanced by progestogen in the same pill.
Cancer of the Cervix
There is some evidence that long-term use of OCs may increase the risk of cancer of the cervix (the narrow, lower portion of the uterus). The results of studies conducted by NCI scientists and other researchers support a relationship between extended use of the pill (5 or more years) and a slightly increased risk of cervical cancer. However, the exact nature of the association between OC use and risk of cervical cancer remains unclear.
One reason that the association is unclear is that two of the major risk factors for cervical cancer (early age at first intercourse, especially age 16 or younger, and a history of multiple sex partners) are related to sexual behavior. Because these risk factors may be different between women who use OCs and those who have never used them, it is difficult for researchers to determine the exact role that OCs may play in the development of cervical cancer.
The two major risk factors that contribute to the development of cervical cancer are also risk factors that contribute to the development of human papillomavirus (HPV) infection in the cervix. Of the more than 100 types of HPV, over 30 types can be passed from one person to another through sexual contact. HPV is one of the most common sexually transmitted diseases. Certain HPVs, particularly HPV type 16, are known to cause cervical cancer. Compared to non-OC users, women who use OCs may be less likely to use barrier methods of contraception (such as condoms). Since condoms can prevent the transmission of HPVs, OC users who do not use them may be at increased risk of becoming infected with HPVs. Therefore, the increased risk of cervical cancer that some studies found to be caused by prolonged OC use may actually be the result of HPV infection.
There is evidence that pill users who never use a barrier method of contraception or who have a history of genital infections are at a higher risk for developing cervical cancer. This association supports the theory that OCs may act together with sexually transmitted agents (such as HPVs) in the development of cervical cancer. Researchers continue to investigate the exact nature of the relationship between OC use and cancer of the cervix.
OC product labels have been revised to inform women of the possible risk of cervical cancer. The product labels also warn that birth control pills do not protect against human immunodeficiency virus (HIV) and other sexually transmitted diseases such as HPV, chlamydia, and genital herpes.
Liver Tumors
There is some evidence that OCs may increase the risk of certain malignant (cancerous) liver tumors. However, the risk is difficult to evaluate because of different patterns of OC use and because these tumors are rare in American women (the incidence is approximately 2 cases per 100,000 women). A benign (noncancerous) tumor of the liver called hepatic adenoma has also been found to occur, although rarely, among OC users. These tumors do not spread, but they may rupture and cause internal bleeding.
Reducing Risks Through Screening
Studies have found that breast cancer screening with mammograms reduces the number of deaths from breast cancer for women age 40 to 69. Women who are at increased risk for breast cancer should seek medical advice about when to begin having mammograms and how often to be screened. A high-quality mammogram, with a clinical breast exam (an exam done by a professional health care provider), is the most effective way to detect breast cancer early.
Women who are or have been sexually active or are in their late teens or older can reduce their risk for cervical cancer by having regular Pap tests. Abnormal changes in the cervix can often be detected by the Pap test and treated before cancer develops.
Women who are concerned about their risk for cancer are encouraged to talk with their doctor. More information is also available from the Cancer Information Service (see below).
References:
Breast Cancer
Brinton LA, Daling JR, Liff JM, et al. Oral contraceptives and breast cancer risk among younger women. Journal of the National Cancer Institute 1995; 87(13):827-835.
The Centers for Disease Control and the National Institute of Child Health and Human Development. Oral contraceptive use and the risk of breast cancer: The Centers for Disease Control and the National Institute of Child Health and Human Development Cancer and Steroid Hormone Study. New England Journal of Medicine 1986; 315:405-411.
Chilvers C, McPherson K, Pike MC, et al. Oral contraceptive use and breast cancer risk in young women. Lancet 1989; 1:973-982.
McPherson K, Vessey MP, Neil A, et al. Early oral contraceptive use and breast cancer: Results of another case-control study. British Journal of Cancer 1987; 56:653-660.
Meirik O, Lund E, Adami HO, et al. Oral Contraceptive use and breast cancer in young women: A joint national study in Sweden and Norway. Lancet 1986; 2:650-654.
Miller DR, Rosenberg L, Kaufman DW, et al. Breast cancer before age 45 and oral contraceptive use: New findings. American Journal of Epidemiology 1989; 129:269-280.
Olsson H, Olsson ML, Moeller TR, et al. Oral contraceptive use and breast cancer in young women in Sweden. Lancet 1985; 1:748-749.
Paul C, Skegg DCG, Spears GFS. Oral contraceptives and risk of breast cancer. International Journal of Cancer 1990; 46:366-373.
Pike MC, Henderson BE, Krailo MD, et al. Breast cancer in young women and use of oral contraceptives: Possible modifying effect of formulation and age at use. Lancet 1983; 2:926-930.
Romiu I, Berlin JA, Colditz G. Oral contraceptives and breast cancer: Review and meta-analysis. Cancer 1990; 66:2253-2263.
Rookus MA, Van Leeuwen FE. Oral contraceptives and risk of breast cancer in women aged 25B54 years: The Netherlands Oral Contraceptives and Breast Cancer Study Group. Lancet 1994; 344:844-851.
Thomas DB. Oral contraceptives and breast cancer: Review of the epidemiologic literature. Contraception 1991; 43(6):597-642.
White E, Malone KE, Weiss NS, et al. Breast cancer among young U.S. women in relation to oral contraceptive use. Journal of the National Cancer Institute 1994; 86: 505-514.
Wingo PA, Lee NC, Ory HW, et al. Age-specific differences in the relationship between oral contraceptive use and breast cancer. Cancer Supplement 1993; 71(4):1506-1517.
Ovarian and Endometrial Cancers
Brinton LA, Huggins GR, Lehman HF, et al. Long-term use of oral contraceptives and risk of invasive cervical cancer. International Journal of Cancer 1986; 38:339-344.
The Centers for Disease Control. Oral contraceptive use and the risk of ovarian cancer: The Centers for Disease Control Cancer and Steroid Hormone Study. Journal of the American Medical Association 1983; 249:1596-1599.
The Centers for Disease Control. Combination oral contraceptive use and the risk of endometrial cancer: The Cancer and Steroid Hormone Study of the Centers for Disease Control and the National Institute of Child Health and Human Development. Journal of the American Medical Association 1987; 257(6):796-800.
The Centers for Disease Control and the National Institute of Child Health and Human Development. The reduction in risk of ovarian cancer associated with oral contraceptive use: The Cancer and Steroid Hormone Study of the Centers for Disease Control and the National Institute of Child Health and Human Development. New England Journal of Medicine 1987; 316:650-655.
Stanford JL, Brinton LA, Berman ML, et al. Oral contraceptives and endometrial cancer: Do other risk factors modify the association? International Journal of Cancer 1993; 54(2):243-248.
Cervical Cancer
Brinton LA. Epidemiology of cervical cancer-overview. IARC Scientific Publications 1992; 119:3-23.
Brinton LA. Oral contraceptives and cervical neoplasia. Contraception 1991; 43(6):581-595.
Brinton LA, Huggins GR, Lehman HF, et al. Long-term use of oral contraceptives and risk of invasive cervical cancer. International Journal of Cancer 1986; 38(3):399-444.
Daling JR, Madeleine MM, McKnight B, et al. The relationship of human papillomavirus-related cervical tumors to cigarette smoking, oral contraceptive use, and prior herpes simplex virus type 2 infection. Cancer Epidemiology, Biomarkers, and Prevention 1996; 5(7):541-548.
Giuliano AR, Papenfuss M, Schneider A, et al. Risk factors for high-risk type human papillomavirus infection among Mexican-American women. Cancer Epidemiology, Biomarkers, and Prevention 1999; 8(7):615-620.
Gram IT, Macaluso M, Stalsberg H. Oral contraceptive use and the incidence of cervical intraepithelial neoplasia. American Journal of Obstetrics and Gynecology 1992; 167(1):40-44.
Kjellberg L, Hallmans G, Ahren AM, et al. Smoking, diet, pregnancy and oral contraceptive use as risk factors for cervical intra-epithelial neoplasia in relation to human papillomavirus infection. British Journal of Cancer 2000; 82:1332-1338.
Lacey JV Jr., Brinton LA, Abbas FM, et al. Oral contraceptives as risk factors for cervical adenocarcinomas and squamous cell carcinomas. Cancer Epidemiology, Biomarkers, and Prevention 1999; 8(12):1079-1085.
Munoz N, Bosch FX, de Sanjose S, et al. The causal link between human papillomavirus and invasive cervical cancer: A population-based case-control study in Colombia and Spain. International Journal of Cancer 1992; 52(5):743-749.
Ylitalo N, Sorensen P, Josefsson A, et al. Smoking and oral contraceptives as risk factors for cervical carcinoma in situ. International Journal of Cancer 1999; 81(3):357-365.
Liver Cancer
Palmer J, Rosenberg L, Kaufman DW, et al. Oral contraceptive use and liver cancer. American Journal of Epidemiology 1989; 130:878-882.
Rooks JB, Ory HW, Ishak KG, et al. Epidemiology of hepatocellular adenoma: The role of oral contraceptive use. Journal of the American Medical Association 1979; 242:644-648.
Tao, LC. Oral contraceptive-associated liver cell adenoma and hepatocellular carcinoma. Cancer 1991; 68:341-347.

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