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The Clinical Trial of Chinese Herbal Medicine (SaiLuoTong) Capsule

Sponsor
Shineway Pharmaceutical Co.,Ltd (Industry)
Overall Status
Recruiting
CT.gov ID
NCT03789760
Collaborator
(none)
500
Enrollment
28
Locations
2
Arms
47.7
Anticipated Duration (Months)
17.9
Patients Per Site
0.4
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

As a traditional Chinese medicine compound, SaiLuoTong capsule is proven to have beneficial effects on learning and memory ability in animal models of vascular dementia (VaD). According to the result of the phase II study, the efficacy of SaiLuoTong capsule in the treatment of patients with VaD was better than that of placebo group and no difference in safety. So the study hypothesis is also that SaiLuoTong capsule will be effective in the treatment of patients with VaD and will be well tolerated. The purpose of the study is to confirm the efficacy and safety of SaiLuoTong capsule on patients with mild to moderate VaD. The outcome measures include general cognitive function, executive function, daily living skills, and mental behavior changes of symptoms in VaD patients.

Condition or Disease Intervention/Treatment Phase
  • Drug: SaiLuoTong capsule
  • Drug: placebo
 Phase 3

Detailed Description

Vascular dementia (VaD) is a clinical syndrome of acquired intellectual and functional impairment that results from cerebrovascular diseases. SaiLuoTong capsule is a traditional Chinese medicine compound; it is composed of ginseng extract (the main composition: ginseng total saponins), ginkgo biloba extract (the main composition: YinXingTong ester) and safflower extract (the main composition: the west safflower total glycosides). The function of SaiLuoTong capsule is Yiqi Huoxue and Huayu Tongluo in Chinese traditional medicine theory. Pharmacodynamics studies showed that SaiLuoTong capsule can significantly improve neurological symptoms caused by focal cerebral ischemia in animals, and learning and memory ability in animal models of VaD. The result of the phase II study showed that the efficacy of SaiLuoTong capsule in the treatment of patients with VaD was better than that of placebo group and no difference in safety. Based on these previous evidences, the investigators conduct this study to further confirm the efficacy and safety of SaiLuoTong capsule in patients with mild to moderate VaD. This study is a phase III clinical trial of SaiLuoTong capsule for treatment of vascular dementia. The study is a 52-week, multicentre, randomized, double -blind, placebo-controlled study.

Study Design

Study Type:
Interventional
Anticipated Enrollment :
500 participants
Allocation:
Randomized
Intervention Model:
Parallel Assignment
Masking:
Quadruple (Participant, Care Provider, Investigator, Outcomes Assessor)
Primary Purpose:
Treatment
Official Title:
A Phase III, Randomised, Double-blind, Placebo-controlled, Parallel, and Multi-centre Study to Evaluate the Clinical Efficacy and Safety of SaiLuoTong (SLT) in the Treatment of Vascular Dementia
Actual Study Start Date :
Apr 10, 2019
Anticipated Primary Completion Date :
Dec 1, 2022
Anticipated Study Completion Date :
Apr 1, 2023

Arms and Interventions

Arm Intervention/Treatment
Experimental: active group

take two pills (120 mg) of SaiLuoTong capsule each time, twice a day, 0.5 hours before breakfast and dinner, taking with lukewarm water.

Drug: SaiLuoTong capsule
500 subjects are randomly divided into two groups by 3:1. 375 subjects in the active group take two pills(120mg) of SaiLuoTong capsule each time, twice a day, 0.5 hours before breakfast and dinner, taking with lukewarm water.
Other Names:
  • The effects of SaiLuoTong capsule on VaD

    		•
    Placebo Comparator: control group

    take two pills (120 mg) of placebo each time, twice a day, 0.5 hours before breakfast and dinner, taking with lukewarm water.

    Drug: placebo
    500 subjects are randomly divided into two groups by 3:1. 125 subjects in the control group take two pills(120mg) of placebo each time, twice a day, 0.5 hours before breakfast and dinner, taking with lukewarm water.

    Outcome Measures

    Primary Outcome Measures

    1. Vascular Dementia Assessment Scale-cognitive Subscale(VaDAS-cog) [Change from baseline VaDAS-cog score at Week 52]

      The VaDAS-cog comprises the Alzheimer's disease assessment scale(ADAS-cog) plus the Maze and Number Cancellation test to specifically assess executive function. The score of each item is summed to compute a total score. The range of the total score was from 0(no cognitive impairment) to 90(severe cognitive impairment). The data in the table below is the statistical data (mean,SD) of precise scores at screening and week 0 (baseline), while the statistical data of difference value compared to the score of Baseline at weeks 52.

    2. Alzheimer's Disease Cooperative Study-clinical Global Impression of Change(ADCS-CGIC) [Change from baseline ADCS-CGIC score at Week 52]

      The Alzheimer's Disease Cooperative Study-clinical Global Impression of Change(ADCS-CGIC) involves comparison of data acquisition from both home and clinic and the use of both informant-ratings and self-ratings. Important outcomes include clinical global impressions of change (CGIC) as indicators of clinically meaningful change. In week 0 (baseline), the score was to judge the severity of the cognitive, 0(no evaluate),1(normal),2(slight intelligence obstacle),3(mide intelligence obstacle),4(moderate intelligence obstacle),5(significantly intelligence obstacle),6(severe intelligence obstacle),7(intelligent obstacle end-stage). In week 13,26,39,52, the score was to judge the change of the clinical global impression,1(improved significantly),2(improve),3(improve a little),4(no change),5(a little deteriorated),6(deteriorated),7(serious deterioration).

    Secondary Outcome Measures

    1. Alzheimer's Disease Cooperative Study-activities of Daily Living(ADCS-ADL) [Change from baseline ADCS-ADL score at Week 26]

      To assess the daily living activity of the patients, including a subgroup in which there are 23 items to be checked and the total score is 78. A higher score represents a better daily living activity, vice versa. The score of each item is summed to compute a total score. The data in the table below is the statistical data (mean,SD) of precise scores at week 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 26.

    2. Alzheimer's Disease Cooperative Study-activities of Daily Living(ADCS-ADL) [Change from baseline ADCS-ADL score at Week 52]

      To assess the daily living activity of the patients, including a subgroup in which there are 23 items to be checked and the total score is 78. A higher score represents a better daily living activity, vice versa. The score of each item is summed to compute a total score. The data in the table below is the statistical data (mean,SD) of precise scores at week 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 52.

    3. Mini-mental State Examination(MMSE) [Change from baseline MMSE score at Week 26]

      The MMSE is a global test of cognitive function, for which the total score ranges from 0 to 30, with higher scores indicating lesser severity. The score of each item is summed to compute a total score. The data in the table below is the statistical data (mean, SD) of precise scores at screening (baseline), while the statistical data of difference value compared to the score of baseline at weeks 26.

    4. Mini-mental State Examination(MMSE) [Change from baseline MMSE score at Week 52]

      The MMSE is a global test of cognitive function, for which the total score ranges from 0 to 30, with higher scores indicating lesser severity. The score of each item is summed to compute a total score. The data in the table below is the statistical data (mean, SD) of precise scores at screening (baseline), while the statistical data of difference value compared to the score of baseline at weeks 52.

    5. Clinical Dementia Rating(CDR Scale ) [Change from baseline CDR Scale score at Week 26]

      The CDR is a numeric scale used to quantify the severity of symptoms of dementia (i.e. its 'stage'). Talk to the patients or those who know well about the patients and assess the 6 functions (memory, orientation, judgment and problem-solving ability, social activities, household duties and hobbies as well as self-care ability) to obtain the scores and based on the predetermined principles the CDR score is calculated. The diagnostic criteria[68]: normal-CDR=0; suspected dementia-CDR=0.5, mild dementia-CDR=1; moderate dementia- CDR=2; and serious dementia-CDR=3. The data in the table below is the statistical data (mean, SD) of precise scores at baseline and weeks 26.

    6. Clinical Dementia Rating(CDR Scale ) [Change from baseline CDR Scale score at Week 52]

      The CDR is a numeric scale used to quantify the severity of symptoms of dementia (i.e. its 'stage'). Talk to the patients or those who know well about the patients and assess the 6 functions (memory, orientation, judgment and problem-solving ability, social activities, household duties and hobbies as well as self-care ability) to obtain the scores and based on the predetermined principles the CDR score is calculated. The diagnostic criteria[68]: normal-CDR=0; suspected dementia-CDR=0.5, mild dementia-CDR=1; moderate dementia- CDR=2; and serious dementia-CDR=3. The data in the table below is the statistical data (mean, SD) of precise scores at baseline and weeks 52.

    7. Clinical Dementia Rating sum of boxes(CDR-sb) [Change from baseline CDR-sb score at Week 26]

      CDR-sb is the sum of boxes of CDR, with higher scores indicating severer degree of impairment. CDR-sb is the algebraic sum of 6 functional domains with a range of 0(normal) - 18(severe dementia). The data in the table below is the statistical data (mean,SD) of precise scores at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 26.

    8. Clinical Dementia Rating sum of boxes(CDR-sb) [Change from baseline CDR-sb score at Week 52]

      CDR-sb is the sum of boxes of CDR, with higher scores indicating severer degree of impairment. CDR-sb is the algebraic sum of 6 functional domains with a range of 0(normal) - 18(severe dementia). The data in the table below is the statistical data (mean,SD) of precise scores at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 52.

    9. Blood biomarker: Brain-derived neurotrophic factor(BDNF) [Change from baseline BDNF at Week 26]

      The data in the table below is the statistical data (mean,SD) of precise measurement at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 26.

    10. Blood biomarker: Brain-derived neurotrophic factor(BDNF) [Change from baseline BDNF at Week 52]

      The data in the table below is the statistical data (mean,SD) of precise measurement at weeks 0(baseline), while the statistical data of difference value compared to the score of baseline at weeks 52.

    11. Blood biomarker: Vascular endothelial growth factor(VEGF) [Change from baseline VEGF at Week 26]

      The data in the table below is the statistical data (mean,SD) of precise measurement at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 26.

    12. Blood biomarker: Vascular endothelial growth factor(VEGF) [Change from baseline VEGF at Week 52]

      The data in the table below is the statistical data (mean,SD) of precise measurement at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 52.

    13. Blood biomarker: Matrix metalloproteinase-9(MMP-9) [Change from baseline MMP-9 at Week 26]

      The data in the table below is the statistical data (mean,SD) of precise measurement at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 26.

    14. Blood biomarker: Matrix metalloproteinase-9(MMP-9)) [Change from baseline MMP-9 at Week 52]

      The data in the table below is the statistical data (mean,SD) of precise measurement at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 52.

    15. Blood biomarker: Interleukin-6(IL-6) [Change from baseline MMP-9 at Week 26]

      The data in the table below is the statistical data (mean,SD) of precise measurement at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 26.

    16. Blood biomarker: Interleukin-6(IL-6) [Change from baseline MMP-9 at Week 52]

      The data in the table below is the statistical data (mean,SD) of precise measurement at weeks 0 (baseline), while the statistical data of difference value compared to the score of baseline at weeks 52.

    17. Vascular Dementia Assessment Scale-cognitive Subscale(VaDAS-cog) [Change from baseline VaDAS-cog score at week 13]

      The VaDAS-cog comprises the ADAS-cog plus the Maze and Number Cancellation test to specifically assess executive function. The score of each item is summed to compute a total score. The range of the total score was from 0(no cognitive impairment) to 90(severe cognitive impairment). The data in the table below is the statistical data (mean,SD) of precise scores at screening and week 0 (baseline), while the statistical data of difference value compared to the score of Baseline at weeks 13.

    18. Vascular Dementia Assessment Scale-cognitive Subscale(VaDAS-cog) [Change from baseline VaDAS-cog score at week 26]

      The VaDAS-cog comprises the ADAS-cog plus the Maze and Number Cancellation test to specifically assess executive function. The score of each item is summed to compute a total score. The range of the total score was from 0(no cognitive impairment) to 90(severe cognitive impairment). The data in the table below is the statistical data (mean,SD) of precise scores at screening and week 0 (baseline), while the statistical data of difference value compared to the score of Baseline at weeks 26.

    19. Vascular Dementia Assessment Scale-cognitive Subscale(VaDAS-cog) [Change from baseline VaDAS-cog score at week 39]

      The VaDAS-cog comprises the ADAS-cog plus the Maze and Number Cancellation test to specifically assess executive function. The score of each item is summed to compute a total score. The range of the total score was from 0(no cognitive impairment) to 90(severe cognitive impairment). The data in the table below is the statistical data (mean,SD) of precise scores at screening and week 0 (baseline), while the statistical data of difference value compared to the score of Baseline at weeks 39.

    20. Alzheimer's Disease Cooperative Study-clinical Global Impression of Change(ADCS-CGIC) [Change from baseline ADCS-CGIC score at week 13]

      The ADCS-CGIC involves comparison of data acquisition from both home and clinic and the use of both informant-ratings and self-ratings. Important outcomes include clinical global impressions of change (CGIC) as indicators of clinically meaningful change. In week 0 (baseline), the score was to judge the severity of the cognitive, 0(no evaluate),1(normal),2(slight intelligence obstacle),3(mide intelligence obstacle),4(moderate intelligence obstacle),5(significantly intelligence obstacle),6(severe intelligence obstacle),7(intelligent obstacle end-stage). In week 13,26,39,52, the score was to judge the change of the clinical global impression,1(improved significantly),2(improve),3(improve a little),4(no change),5(a little deteriorated),6(deteriorated),7(serious deterioration).

    21. Alzheimer's Disease Cooperative Study-clinical Global Impression of Change(ADCS-CGIC) [Change from baseline ADCS-CGIC score at week 26]

      The ADCS-CGIC involves comparison of data acquisition from both home and clinic and the use of both informant-ratings and self-ratings. Important outcomes include clinical global impressions of change (CGIC) as indicators of clinically meaningful change. In week 0 (baseline), the score was to judge the severity of the cognitive, 0(no evaluate),1(normal),2(slight intelligence obstacle),3(mide intelligence obstacle),4(moderate intelligence obstacle),5(significantly intelligence obstacle),6(severe intelligence obstacle),7(intelligent obstacle end-stage). In week 13,26,39,52, the score was to judge the change of the clinical global impression,1(improved significantly),2(improve),3(improve a little),4(no change),5(a little deteriorated),6(deteriorated),7(serious deterioration).

    22. Alzheimer's Disease Cooperative Study-clinical Global Impression of Change(ADCS-CGIC) [Change from baseline ADCS-CGIC score at week 39]

      The ADCS-CGIC involves comparison of data acquisition from both home and clinic and the use of both informant-ratings and self-ratings. Important outcomes include clinical global impressions of change (CGIC) as indicators of clinically meaningful change. In week 0 (baseline), the score was to judge the severity of the cognitive, 0(no evaluate),1(normal),2(slight intelligence obstacle),3(mide intelligence obstacle),4(moderate intelligence obstacle),5(significantly intelligence obstacle),6(severe intelligence obstacle),7(intelligent obstacle end-stage). In week 13,26,39,52, the score was to judge the change of the clinical global impression,1(improved significantly),2(improve),3(improve a little),4(no change),5(a little deteriorated),6(deteriorated),7(serious deterioration).

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    40 Years to 75 Years
    Sexes Eligible for Study:
    All
    Accepts Healthy Volunteers:
    No
    Inclusion Criteria:

    • 40 years≤Age≤75 years, female or male.

    • With an education at more than (including) 6 years.

    • Meet the diagnostic criteria for dementia in Diagnostic and Statistical Manual of Mental Disorders-5th Edition (DSM-V).

    • Meet the National Institute of Neurological Disorders and Stroke-Association Internationale pour la Recherche etl'Enseignement en Neurosciences(NINDS-AIREN) Criteria of Probable Vascular Dementia (1993).

    • MRI (magnetic resonance imaging) supports the presence of ischemic cerebrovascular disease, and meets NINDS-AIREN Imaging Criteria; the diameter of each infarct≤ 30mm(And the perivascular spaces and cerebral microbleeds were excluded).

    • Modified Hachinski Ischemic (mHIS) Scale ≥ 4.

    • Hamilton depression scale (HAMD) ≤ 17.

    • Patients with mild or moderate VaD: 10 ≤ MMSE ≤ 26 and 1 ≤ CDR ≤ 2.

    • Willing to participate in this study and could sign the informed consent form by him/herself and lawful guardian prior to the study.

    • The subjects must have a care giver who are cognitively normal (MMSE scores: illiteracy> 17 points, 1 - 6 years of education > 20 points, 7 years and above of education > 24 points). The care giver shall also be able to take care of the patient at least 4 days a week for more than 4 hours a day while he or she can accompany the subjects to attend each visit. During the trial, a new caregiver must have MMSE score and the results would be presented in forms of subjects in the attachment.

    Exclusion Criteria:

    • Patients with dementia caused by a brain disease other than VaD (such as Alzheimer's disease, dementia with Lewy bodies, frontotemporal dementia, Parkinson's disease, central nervous system demyelinative diseases, tumour, hydrocephalus, trauma, central nervous system infection, such as syphilis, AIDS and Creutzfeldt-Jakob disease);

    • Patients with serious neurological impairment to finish the examination: hand hemiplegia, aphasia, and visual or hearing impairment.

    • Laboratory anomalies: hemoglobin (Hb) level less than 80g/L , platelet count (Plt) level less than 50×109/L, activated partial thromboplastin time (APTT) exceeds 2.5 times the normal upper level, fibrinogen(FIB) level less than 0.5g/L, prothrombin time (PT) exceeds 2.5 times the normal upper level, Serum creatinine (Scr) exceeds 3 times the normal upper level, alanine aminotransferase (ALT) exceed 5 times the normal upper level , aspartate aminotransferase (AST) exceed 5 times the normal upper level, alkaline phosphates (ALP) exceed 5 times the normal upper level , γ-glutamyl transferase (γ-GT) exceed 5 times the normal upper level, total bilirubin (TBiL) exceeds 3 times the normal upper level.

    • The subjects have nutritional and metabolic diseases and endocrine system diseases that cannot been controlled by therapy - thyroid diseases, parathyroid disease, vitamin or element deficiency.

    • Patients with serious circulatory system diseases, respiratory system diseases, urinary system diseases, digestive system diseases, haemopoietic system diseases (such as unstable angina, uncontrollable asthma and active gastrorrhagia) and cancer.

    • Serious mental disease (such as depression and schizophrenia) and epilepsy.

    • Gastrointestinal diseases that may affect the absorption, distribution, and metabolism of the investigational drug.

    • Alcohol and drug abuse.

    • Patients who have been given any drug that can affect the cognitive function (including Chinese herbal preparations containing any one of these: ginseng, ginkgo leaf, and saffron; Western medicines such as donepezil, karbalatine, rivastigmine, huperzine a, memantine and similar drugs, etc; Butylphthalide and other drugs with the same effect such as runeirergine, aniracetam, cytosporine, dihydroergine, nimodipine, etc) within one month before the start of this study and cannot be discontinued.

    • Patients who are allergic to more than 2 drugs or any component of the SLT capsules.

    • Pregnant or lactating women.

    • Patients who have participated in other clinical studies within 3 months prior to this study.

    • Cannot accept magnetic resonance imaging (MRI) examination.

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 Xuan Wu Hospital of Capital Medical University Beijing Beijing China 100053
    2 Peking University Shougang Hospital Beijing Beijing China 100144
    3 Xiyuan Hospital Beijing Beijing China
    4 Liuzhou Worker's Hospital Liuzhou Guangxi China
    5 Affiliated Hospital of Hebei University Baoding Hebei China
    6 Affiliated Hospital of Chengde Medical College Chengde Hebei China 067000
    7 Handan First Hospital Handan Hebei China 056000
    8 The Third Hospital of Hebei Medical University Shijiazhuang Hebei China 050051
    9 The Fourth Hospital of Medical University Harbin Hei Longjiang China
    10 The First People's Hospital of Luoyang Luoyang Henan China 471000
    11 Nanyang Second People's Hospital Nanyang Henan China 473003
    12 The First Hospital of Changsha Changsha Hunan China 41000
    13 Xiangya Boai Rehability Hospital Changsha Hunan China
    14 Yueyang Second People's Hospital Yueyang Hunan China 414000
    15 Baogang Hospital Baotou Inner Mongolia China 014000
    16 Inner Mongolia International Mongolian Hospital Hohhot Inner Mongolia China
    17 Taizhou Hospital of Chinese Medicine Taizhou Jiangsu China 225300
    18 Jiujiang University Clinical Medical College ▪ Jiujiang University Hospital Jiujiang Jiangxi China 332000
    19 The Fourth Affiliated Hospital of Nanchang University Nanchang Jiangxi China 330000
    20 Nanchang Hongdu Hospital of TCM Nanchang Jiangxi China
    21 Changzhi People's Hospital Changzhi Shanxi China 046000
    22 Jinzhong First People's Hospital Jinzhong Shanxi China
    23 Xianyang Hospital of Yan'an University Xianyang Shanxi China 712000
    24 Yuncheng Central Hospital Yuncheng Shanxi China
    25 The Second people's Hospital of Neijiang Neijiang Sichuan China
    26 The Second Hospital of Xingjiang Medical University Ürümqi Xingjiang China
    27 The Central Hospital of Lishui City Lishui Zhejiang China 323000
    28 Wenzhou Hospital of Traditional Chinese Medicine Wenzhou Zhejiang China 325000

    Sponsors and Collaborators

    • Shineway Pharmaceutical Co.,Ltd

    Investigators

    • Principal Investigator: Jianping Jia, Professor, Xuan Wu Hospital of Capital Medical University

    Study Documents (Full-Text)

    None provided.

    More Information

    Publications

    None provided.
    Responsible Party:
    Shineway Pharmaceutical Co.,Ltd
    ClinicalTrials.gov Identifier:
    NCT03789760
    Other Study ID Numbers:
    • SW003
    First Posted:
    Dec 31, 2018
    Last Update Posted:
    Dec 27, 2021
    Last Verified:
    Dec 1, 2021
    Studies a U.S. FDA-regulated Drug Product:
    No
    Studies a U.S. FDA-regulated Device Product:
    No
    Keywords provided by Shineway Pharmaceutical Co.,Ltd
    Vascular Dementia
    cognitive
    Additional relevant MeSH terms:
    Dementia
    Dementia, Vascular

    Study Results

    No Results Posted as of Dec 27, 2021