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. 2006 Jul 19;2006(3):CD005214.
doi: 10.1002/14651858.CD005214.pub2.

Depot medroxyprogesterone versus norethisterone oenanthate for long-acting progestogenic contraception

B H Draper  1 C MorroniM HoffmanJ SmitM BeksinskaJ HapgoodL Van der Merwe
Affiliations

Depot medroxyprogesterone versus norethisterone oenanthate for long-acting progestogenic contraception

B H Draper et al. Cochrane Database Syst Rev. .

Abstract

Background: There are two injectable progestogen-only contraceptives (IPCs) that have been available in many countries in the world since 1983. They are both still extensively used in many developing countries, forming a large proportion of the health system's expenditure on contraception. These are depot medroxyprogesterone acetate (DMPA) and norethisterone oenanthate (NET-EN). These are both highly effective contraceptives that receive wide acceptance amongst women in their fertile years. They differ in frequency of administration that has implications on patient uptake. They also differ in cost that may significantly affect budgeting in the health system. A systematic comparison will aid to ensure their rational use.

Objectives: To determine if there are differences between depot medroxyprogesterone acetate given at a dose of 150 mg IM every 3 months and norethisterone oenanthate given at a dose of 200mg IM every 2 months, in terms of contraceptive effectiveness, reversibility and discontinuation patterns, minor effects and major effects.

Search strategy: We searched the computerized databases MEDLINE using PubMed, Popline, Cochrane Controlled Trials Register, Biblioline, LILACS, EMBASE and PASCAL for randomised controlled trials of DMPA versus NET-EN for long-acting progestogenic contraception. Studies were included regardless of language, and all databases were reviewed from the time that injectable progestogens have been in use.

Selection criteria: All randomised controlled comparisons of DMPA acetate given at a dose of 150 mg IM every 3 months versus NET-EN given at a dose of 200mg IM every 2 months, used for contraception, were included. Trials had to report on contraceptive efficiency and return to fertility, discontinuation risks and reasons for discontinuation, and clinical effects, both menstrual and non-menstrual.

Data collection and analysis: BD and CM evaluated the titles and abstracts obtained through applying the search strategy and applied the eligibility criteria. BD attempted to contact authors where clarification of the data was required, and contacted all main manufacturers of the contraceptives. After inclusion of the two studies, the data was abstracted and analysed with RevMan 4.2.

Main results: Two trials were included in this review. There was no significant difference between the two treatment groups for the frequency of discontinuation for either contraceptive, although the women on NET-EN were 4% more likely to discontinue for personal reasons than those on DPMA. Discontinuation because of accidental pregnancy did not differ between the groups. Although the duration of bleeding and spotting events was the same in each group, women on DPMA were 21% more likely to develop amenorrhoea. Mean changes in body weight at 12 and 24 months, and in systolic and diastolic blood pressure at 12 months did not differ significantly between the studies.

Authors' conclusions: While the choice between DPMA and NET-EN as injectable progestogen contraceptives may vary between both health providers and patients, data from randomized controlled trials indicate little difference between the effects of these methods, except that women on DMPA are more likely to develop amenorrhoea. There is inadequate data to detect differences in some non-menstrual major and minor clinical effects.

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Conflict of interest statement

No conflict of interest exists in the research for this review.

Figures

1.1
1.1. Analysis
Comparison 1 DMPA vs NET‐EN, Outcome 1 Discontinuation rates.
1.2
1.2. Analysis
Comparison 1 DMPA vs NET‐EN, Outcome 2 Reasons for discontinuation at 12 months.
1.3
1.3. Analysis
Comparison 1 DMPA vs NET‐EN, Outcome 3 Proportion of women with bleeding / spotting.
1.4
1.4. Analysis
Comparison 1 DMPA vs NET‐EN, Outcome 4 Duration of bleeding and spotting episodes.
1.5
1.5. Analysis
Comparison 1 DMPA vs NET‐EN, Outcome 5 Amenorrhoea.
1.6
1.6. Analysis
Comparison 1 DMPA vs NET‐EN, Outcome 6 Mean increase in body weight.
1.7
1.7. Analysis
Comparison 1 DMPA vs NET‐EN, Outcome 7 Mean decrease in blood pressure.
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Update of

  • doi: 10.1002/14651858.CD005214

References

References to studies included in this review

Salem HT {published data only}
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WHO {published data only}
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References to studies excluded from this review

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References to ongoing studies

Beksinska M part 2 {published data only}
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