Combined hormonal contraception


Combined hormonal contraception, or combined birth control, is a form of hormonal contraception which combines both an estrogen and a progestogen in varying formulations.
The different types available include the pill, the patch and the vaginal ring, which are all widely available, and an injection, which is available in only some countries. They work by mainly suppressing luteinising hormone and follicle-stimulating hormone and in turn preventing ovulation.
Its effectiveness depends on how appropriately the woman uses the method, with beneficial effects on health including reduced risks of ovarian, endometrial and colorectal cancer, and better control of some menstrual problems. Adverse effects include a small but higher risk of venous thromboembolism, arterial thromboembolism, breast cancer and cervical cancer.

Types

Types of combined hormonal contraception include:
Widely available
Available in only some countries
Traditionally, to mimick a normal menstrual cycle, CHC is used for 21 consecutive days, followed by either 7 days of no use or in the case of oral CHC, the administration of placebo pills, during which a withdrawal bleed occurs. This regime confers no added benefit and may increase failure rate. Hence, regimes are often tailor-made to the individual with extended periods of use and infrequent hormone-free periods.

Mechanism of action

Combined hormonal contraception works by acting on the hypothalamic–pituitary–ovarian axis to suppress luteinising hormone and follicle-stimulating hormone and in turn prevent ovulation. The addition of progesterone contributes to the contraceptive effect by making changes to the cervical mucus, endometrium and tubal motility.

Effectiveness

The pill, patch and ring have similar effectiveness and this depends largely on the woman using it in the prescribed way. Other factors affecting effectiveness include drug interactions, malabsorption and body weight.

Adverse effects

Although the risk of venous thromboembolism, arterial thromboembolism, breast cancer and cervical cancer in CHC users is small, all CHCs are associated with higher risks of these compared to no use, with the lowest risk for those CHCs containing the progesterones levonorgestrel, norethisterone and norgestimate. CHCs containing higher doses of oestrogen may be associated with an increase in arterial thromboembolism.
Other adverse effects include nausea, headaches, breast pain, skin pigmentation, irregular menstrual bleeding, absent periods and irritation from contact lenses. Changes in libido and mood, decline of liver function and raised blood pressure may also occur.

Drug interactions

Liver enzyme inducing drugs

Medications that induce liver enzymes increase the metabolism of oestradiol and progestogens and subsequently may reduce the effectiveness of CHC. The advice on CHC also depends on whether the liver inducing drug is used short term, for less than two months, or long term, for more than two months.

Ulipristal acetate (ellaOne)

Should a woman have taken ulipristal acetate for emergency contraception, restarting CHC may reduce ellaOne's effectiveness, hence advice is to wait five days before commencing CHC.

Antibiotics

Extra contraceptive precautions are not necessary when using CHC in combination with antibiotics that do not induce liver enzymes, unless the antibiotics cause vomiting and/or diarrhoea.

Antiepileptics

Medications used in the treatment of epilepsy can interact with the combined pill, patch or vaginal ring, resulting in both pregnancy and shift in seizure threshold.

Lamotrigine

Based on a study of 16 women using oral CHC 30 μg ethinyloestradiol/150 μg levonorgestrel and anti-epileptic drug lamotrigine for 6 weeks, it was revealed that the contraceptive effectiveness could be lowered, despite lamotrigine not being an enzyme inducer.
An assessment of risks versus benefits of CHC is recommended in women on lamotrigine who are considering CHC, as the seizure threshold in someone on lamotrigine may be lowered by the oestrogen in CHC. In a similar mechanism, stopping CHC in a woman on lamotrigine can cause lamotrigine toxicity. Long-acting reversible contraception instead may be preferable.

Incorrect usage

If pills are missed or the ring or patch used incorrectly, the chance of pregnancy is increased. In the UK, the Faculty of Sexual and Reproductive Healthcare issue guidance for incorrectly used CHC pills, patches and rings.

Special populations

Following childbirth, the use of CHC depends on factors such as whether the woman is breastfeeding and whether she has other medical conditions including superficial venous thrombosis and dyslipidaemia.

Age

When considering CHC use by age only, use is unrestricted between menarche and age 40, and can be generally used after age 40.

Breastfeeding

CHC should not be used by breastfeeding women in the first six weeks after delivery and are generally not recommended in the first six months after delivery if still breastfeeding. After six months, breastfeeding women may use CHC.

Health benefits

CHCs may reduce the risk of ovarian, endometrial and colorectal cancer.
Other possible benefits include regular and reduced menstrual bleeding, less pain, and control of premenstrual syndrome, polycystic ovary syndrome and endometriosis symptoms.

Epidemiology

In the UK, one survey demonstrated that in 2010–2012, more than 33% of women aged 16–44 years had used oral contraception in the previous year and that it was mostly the combined type.

History

CHC has been used worldwide for more than 60 years, with the first clinical trials on oral CHC beginning in 1956.
The combined injectable contraceptive was developed in 1963 and by 1976, two types of these were in use.
The study of CHC vaginal rings began in the early 1970s and the NuvaRing first became available in 2009. In 2003, the contraceptive patch became available, requiring re-application of a new one every week for three weeks, followed by one week without a patch.