Effect of Menopause Hormone Therapy In Postmenopausal Women With CSVD And MCI
NCT ID: NCT05982470
Last Updated: 2023-08-08
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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UNKNOWN
PHASE2
328 participants
INTERVENTIONAL
2023-08-18
2025-10-01
Brief Summary
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The main questions it aims to answer are:
* The efficacy of menopausal hormone mainly estrogen therapy for early menopausal women with CSVD and MCI
* The role of MHT in delaying the progression of cognitive function, CSVD imaging features, and other clinical symptoms and the potential pathophysiological mechanisms.
Participants will be divided randomly into two groups taking MHT drugs and placebo respectively and followed up for 12 months to collect relevant clinical data.
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Detailed Description
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Menopause refers to the permanent cessation of menstruation caused by ovarian failure. During menopause, drastic changes in hormones can have a series of effects on women.Research shows that menopause is an independent risk factor for WMH. Meanwhile, menopause is significantly associated with cognitive impairment, especially with decreased learning, memory, and attention. Menopause can also cause changes in cerebral hemodynamics, damage to the integrity of the Blood-brain barrier and atrophy of cortical structures.
Estrogen not only plays a crucial role in maintaining vascular function, but also has significant neuro-protective effects. Estrogen-based menopausal hormone therapy (MHT) is essentially a treatment measure taken to compensate for ovarian failure caused by aging.
However, it is still unclear whether MHT can effectively alleviate CSVD symptoms and delay CSVD progression. The MHT treatment plan may also be an important reason for the inconsistent conclusions on the impact of MHT on cognitive function in various clinical studies. In previous clinical studies, the MHT regimen was oral estrogen (with or without Progestogen).
Based on the above research background, MHT, especially the MHT regimen using transdermal estrogen, may be an effective treatment method to improve and alleviate the rapid progression of CSVD in perimenopausal women(without contraindications). So far, there have been no RCT studies evaluating the effectiveness and safety of MHT in CSVD patients internationally. Therefore, more research is needed to provide stronger evidence and provide new directions and basis for the treatment of CSVD.
Participates who met the inclusion criteria were randomly divided into two groups. Participants were treated with MHT/placebo followed up for 12 months, and collected and analyzed relevant clinical data to evaluate the efficacy.
Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
QUADRUPLE
Study Groups
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treatment group
Estradiol gel 2.5 g (containing 17β estradiol 1.5mg) once daily (percutaneous application)\* in combination with progesterone soft capsules 100mg once daily (oral) for 12 months
Note :
\* Usage and dosage of estradiol gel: A dose of ruler is applied to the skin of the arm, shoulder, head and neck, abdomen, thigh or face every morning or evening. It is dry about two minutes after application. It is non-irritating, colorless, or milky white and tasteless, and is best used after bathing.
Estradiol Gel
Estradiol gel 2.5 g (containing 17β estradiol 1.5mg) once daily (percutaneous application) for 12 months
Progesterone Soft Capsule
Progesterone soft capsules 100mg once daily (oral) for 12 months
control group
Estradiol placebo gel 2.5g (containing 17β estradiol 0mg) once daily (percutaneous application) \*in combination with progesterone placebo soft capsules(containing progesterone 0mg) 100mg once daily (oral) for 12 months
Note :
\* Usage and dosage of estradiol placebo gel : A dose of ruler is applied to the skin of the arm, shoulder, head and neck, abdomen, thigh or face every morning or evening. It is dry about two minutes after application. It is non-irritating, colorless, or milky white and tasteless, and is best used after bathing.
Estradiol Placebo Gel
Estradiol placebo gel 2.5 g (containing 17β estradiol 1.5mg) once daily (percutaneous application) for 12 months
Progesterone Placebo Soft Capsule
Progesterone placebo soft capsules 100mg once daily (oral) for 12 months
Interventions
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Estradiol Gel
Estradiol gel 2.5 g (containing 17β estradiol 1.5mg) once daily (percutaneous application) for 12 months
Estradiol Placebo Gel
Estradiol placebo gel 2.5 g (containing 17β estradiol 1.5mg) once daily (percutaneous application) for 12 months
Progesterone Soft Capsule
Progesterone soft capsules 100mg once daily (oral) for 12 months
Progesterone Placebo Soft Capsule
Progesterone placebo soft capsules 100mg once daily (oral) for 12 months
Eligibility Criteria
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Inclusion Criteria
2. Female;
3. 1 year ≤ Natural menopause≤ 6 years;
4. FSH ≥ 35 miu/ml and E2 ≤ 25 pg/ml;
5. Head MRI shows CSVD-related image changes, meet one of the following:
1. Parventricular or deep brain white matter hyperintense, Fazekas ≥ 2;
2. Parventricular or deep brain white matter hyperintense, Fazekas = 1, with more than 2 vascular risk factors (hypertension, hyperlipidemia, type 2 diabetes, obesity, current smoking);
3. Parventricular or deep brain white matter hyperintense, Fazekas = 1, with more than 1 vascular-derived lacunae;
4. Recent small subcortical infarction within the last 3 months
6. Mild cognitive dysfunction (18 ≤ MoCA \<26);
7. Independent in daily life (mRS ≤ 1)
8. Sign informed consent.
Note:
1. Natural menopause: The self-reported last menstrual date of the subject
2. CSVD related image changes: evaluated according to the STRIVE2 standard issued in 2023;
3. Fazekas score: The total score is 6 , which is the sum of Fazekas scores for subcortical and periventricular white matter lesions;
4. Recent subcortical small infarcts: lesions with a diameter of\<20mm in the subcortical, basal ganglia, or brainstem regions that exhibit high signal intensity (ADC diffusion limitation) on DWI imaging, with or without corresponding clinical symptoms; With new clinical symptoms, FLAIR hyperintense lesions (\<20mm in diameter) in subcortical, basal ganglia or corresponding parts of pons can be seen in FLAIR sequence of head MRI.
5. MoCA: Montreal Cognitive Assessment; If the subject's education period ≤ 12 years, then increase by 1 point, with a maximum score of 30 points;
6. mRS: Modified Rankin Scale
Exclusion Criteria
2. Confirmed neurodegenerative diseases, such as AD and PD;
3. Clear non-vascular white matter lesions, such as multiple sclerosis, adult brain white matter dysplasia, metabolic encephalopathy, etc.
4. History of intracranial hemorrhagic disease within the recent 6 months, including cerebral parenchymal hemorrhage, intraventricular hemorrhage, subarachnoid hemorrhage, subdural / extradural hematoma, etc., as well as untreated aneurysms (diameter\> 3mm) and cerebrovascular malformations.
5. Cardiovascular and cerebrovascular events within the past 6 months, such as myocardial infarction, unstable angina pectoris, cerebral infarction, etc.
6. Previously received or initiated menopausal hormone therapy.
7. Previous Hysterectomy
8. Vaginal bleeding of unknown origin
9. Intra- and extra- cranial Atherosclerosis large artery stenosis (50-99%) or occlusion.
10. Active venous or arterial thromboembolic diseases, such as Deep vein thrombosis, Pulmonary embolism, myocardial infarction, angina pectoris or congestive heart failure, in the last 6 months.
11. Used drugs and Phytoestrogen supplements that affect estrogen levels in the past 3 months, such as soybean concentrate or extract, Kuntai capsule, Dingkundan, Lifumin, etc.
12. Endometrial hyperplasia, vaginal ultrasound indicates endometrial ≥ 5mm (note: those confirmed as benign lesions by pathology can be included).
13. Severe liver and kidney dysfunction: severe liver dysfunction refers to Alanine transaminase\>3 times the upper limit of normal value or cereal grass Transaminase\>3 times the upper limit of normal value; Severe renal insufficiency refers to blood creatinine\>3.0 mg/dl (265.2 μmol/L) or glomerular filtration rate\<30 ml/min/1.73m\^2;
14. Hypertension is still difficult to control after standardized treatment (blood pressure\>160/100mmHg); Type 2 diabetes is still difficult to control after standard treatment (Glycated hemoglobin ≥ 8%).
15. Known or suspected to have sex hormone dependent malignant tumors, such as breast cancer, endometrial cancer, cervical adenocarcinoma, ovarian cancer, and meningioma.
16. Suffering from severe organic diseases with an expected survival time of\<5 years.
17. Other situations that are not suitable for menopausal hormone treatment, such as porphyria, otosclerosis, etc.
18. Mental disorders diagnosed according to DSM-5 diagnostic criteria, or previous mental system diseases that cannot be fully communicated.
19. Allergies to the active ingredients or any of the excipients of the research drug.
20. Contraindications to MRI examination, such as Claustrophobia, metal implants in the body, etc.
21. Unable to cooperate in completing follow-up due to geographical or other reasons.
22. Situations deemed unsuitable by other researchers to participate in the study.
23. Participating in other interventional clinical trials. -
40 Years
60 Years
FEMALE
No
Sponsors
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Beijing Tiantan Hospital
OTHER
Responsible Party
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yilong Wang
Vice President of Beijing Tiantan Hospital
Principal Investigators
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yilong wang, MD,PhD
Role: PRINCIPAL_INVESTIGATOR
Beiiing Tiantan Hospital
Locations
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Beijing Tiantan Hospital
Beijing, , China
Countries
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Central Contacts
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Facility Contacts
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yilong Wang, MD, PhD
Role: primary
Other Identifiers
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KY2023-117
Identifier Type: -
Identifier Source: org_study_id
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