Table 1.
Summary of randomised controlled trials
| Study | Objective | Country | Sample size | Attrition | ITT analysis | Oestrogen intervention | Statistical results | Conclusion |
|---|---|---|---|---|---|---|---|---|
| Kantarci et al (2016)7 | Prevention of Alzheimer's disease only | USA | 118 | 50 (42.4%) | No | 0.45 mg/day CEE orally or 50 μg/day 17β-oestradiol transdermally for four years each | Transdermal groupa: odds ratio 0.04 [95% CI 0.004–0.44] Oral groupa: odds ratio 0.01 [95% CI 0.0006–0.23] |
Transdermal 17β-oestradiol was associated with reduced beta-amyloid deposition in APOE ε4 carriers |
| Henderson et al (2000)10 | Prevention and delaying onset of Alzheimer's disease | USA | 42 | 6 (14.3%) | No | 1.25 mg/day CEE orally for 16 weeks | Not applicable | No association between short-term oestrogen therapy and Alzheimer's disease |
| Shumaker et al (2003)11 | Prevention of Alzheimer's disease only | USA | 4532 | 0 (0%) | Yes | 0.625 mg/day CEE orally | Relative risk 1.97 (odds ratio 1.99 [95% CI 1.17–3.38]) | No association between short-term oestrogen therapy and Alzheimer's disease, but oestrogen plus progestin therapy increased risk of probable dementia |
| Shumaker et al (2004)22 | Prevention of Alzheimer's disease only | USA | 7479 | 0 (0%) | Yes | 0.625 mg/day CEE orally | Relative risk 1.36b (odds ratio 1.39 [95% CI 1.01–1.91]) | No association between oestrogen therapy and reducing risk of Alzheimer's disease. Increased risk of probable dementia in both oestrogen-only group and oestrogen plus progestin group |
ITT, intention to treat; CEE, conjugated equine oestrogen; APOE, apolipoprotein E.
a.
Data to calculate relative risk was not available.
b.
Calculated based on the treatment group utilising oestrogen therapy only.