Oligo/amenorrhoeic premenopausal women: positive effect of oral contraceptives on bone mineral density
| Study design | Reference | No of patients | OC exposure | Measurement of BMD/bone metabolism | Results |
|---|---|---|---|---|---|
| OC, Oral contraceptive; BMD, bone mineral density; RCT, randomised controlled trial; EE, ethinyl oestradiol; DXA, dual energy x ray absorptiometry; DPA, dual photon absorptiometry; SPA, single photon absorptiometry; NS, non-significant;’. | |||||
| RCT (level 1b) | Hergenroeder et al62 | 24 women with hypothalamic amenorrhoea (ages 14–28) | 35 μg EE+0.5–1 mg norethindrone (n = 5) v 10 mg medroxyprogesterone (n = 5) v placebo (n = 5) for 12 months | Lumbar spine, total body, femoral neck DXA | Increase in lumbar spine & total body BMD in OC treated group v placebo; no change in BMD at any site in medroxyprogesterone treated group |
| Castelo-Branco et al63 | 64 women with hypothalamic oligomenorrhoea (ages 19–35) | 30 μg EE+0.15 mg desogestrel (n = 24) v 20 μg EE+0.15 mg desogestrel (n = 22) v control (n = 18) for 12 months | Lumbar spine DXA | Increase in lumbar spine BMD in both OC treated groups; decrease in BMD in control group | |
| Cohort (level 2b,64,67,68 level 465,66) | De Creé et al64 | 11 sportswomen with athletic menstrual irregularity (ages 18–29) | 50 μg EE+2 mg cyproterone acetate (n = 7) v control (n = 4) for 8 months | Lumbar spine DPA, radius SPA | 9.5% increase in lumbar spine BMD in OC treated group |
| Gulekli et al65 | 85 women with past (n = 33) or current (n = 52) history of amenorrhoea (ages 17–40) | Synthetic oestrogens (10–50 μg EE) (n = 40) v natural oestrogens (Premarin or oestradiol valerate) (n = 10) v 50 mg transdermal estradiol (n = 8) v bromocriptine (n = 9) v weight gain (n = 6) v control (untreated) (n = 12) for 3 years | Lumbar spine DXA | Increase in BMD in all treatment groups, but weight gain was most effective treatment; NS decrease in BMD in control group | |
| Haenggi et al66 | 21 women with hypothalamic or ovarian amenorrhoea, 123 healthy controls (ages 18–45) | 30 μg EE+0.15 mg desogestrel (n = 15) v control (n = 123) for 24 months | Lumbar spine, proximal femur DXA | Initial BMD was lower in amenorrhoeic women than in healthy women; increase in lumbar spine, Ward’s triangle BMD in OC treated group | |
| Cumming67 | 13 female runners with amenorrhoea (ages 23–34) | Oestrogen treated (0.0625 mg conjugated oestrogen (n = 6) or 50 μg transdermal estradiol (n = 2)) v control (n = 5) for 24 months | Lumbar spine, femoral neck, Ward’s triangle DXA | Increase in lumbar spine, femoral neck BMD in oestrogen treated group; NS decrease in BMD in control group | |
| Rickenlund et al68 | 38 women (26 athletes (13 eumenorrhoeic, 13 oligoamenorrhoeic), 12 eumenorrhoeic non-athletes) (ages 16–35) | Each group received 30 μg EE+150 μg levonorgestrel for 10 months | Lumbar spine, total body DXA before and after 10 months of OC use | Increase in lumbar spine BMD in oligoamenorrhoeic athletes (especially those with low BMD at baseline); increase leg BMD in eumenorrhoeic athletes (related to weight-bearing exercise?) | |