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Low dose 25 mg oestradiol implants and 1 mg norethisterone as continuous combined hormone therapy: a prospective study
Author(s) -
Panay N.,
Zamblera D.,
Sands R.,
Jones J.,
AlaghbandZadeh J.,
Studd J.W.W.
Publication year - 2002
Publication title -
bjog: an international journal of obstetrics and gynaecology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.157
H-Index - 164
eISSN - 1471-0528
pISSN - 1470-0328
DOI - 10.1111/j.1471-0528.2002.00308.x
Subject(s) - medicine , progestogen , norethisterone , urology , osteoporosis , n terminal telopeptide , prospective cohort study , endocrinology , bone density , bone resorption , bone remodeling , estrogen , population , chemistry , alkaline phosphatase , biochemistry , environmental health , osteocalcin , research methodology , enzyme
The anxiety regarding no‐bleed regimens is that breakthrough bleeding and endometrial hyperplasia may occur. We aimed to demonstrate that 25 mg oestradiol implants can be adequately opposed by a low dose of progestogen protecting against osteoporosis. Twenty‐two patients were recruited to the study. The mean age was 62 years and body mass index of 26.5. Median oestradiol rose from 77 pmol/L at baseline to 275 pmol/L at one year. Median endometrial thickness remained unchanged at 4 mm and only two women withdrew with bleeding problems. There was one case of proliferative endometrium at one year—all others samples were either atrophic or secretory. Lumbar bone density (L2–L4) rose significantly from 0.939 to 0.992 g/cm 2 ( +5.6% , P = 0.005 ) and the total femoral density rose from 0.872 to 0.890 g/cm 2 (+2.1%) . Bone formation markers increased significantly (serum type 1 procollagen C terminal peptide, P1CP = 112–114, P = 0.0376 ) and bone resorption fell (serum type 1 collagen C terminal telopeptide, 1CTP = 3.0–2.9, P = 0.2863 ). E25 implants and low dose progestogen appear to avoid endometrial hyperplasia and bleeding problems while increasing bone density.