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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT03183505
Other study ID # AYPB-MDD-?b-1701
Secondary ID 2017ZX09304-020
Status Completed
Phase Phase 2
First received
Last updated
Start date June 30, 2017
Est. completion date November 29, 2018

Study information

Verified date September 2017
Source Shanghai Mental Health Center
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study is to evaluate the safety and efficacy of Anyu Peibo Capsule comparing with placebo in the treatment of Chinese Patients with Depression. And to provide some scientific evidence for protocol designing in following phase Ⅲ clinical trial.


Recruitment information / eligibility

Status Completed
Enrollment 172
Est. completion date November 29, 2018
Est. primary completion date October 5, 2018
Accepts healthy volunteers No
Gender All
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria:

- Adult with primary diagnosis of major depressive disorder(MDD) based on the criteria of DSM-5, single episode or recurrent episode.

- The total score of MADRS is =24 in both screening visit and baseline visit.

- The total score of HAMD-17 is =18 and the first item (depressed mood) is =2 in both screening visit and baseline visit.

- CGI-S is =4 in both screening visit and baseline visit.

- The subject understands and consents to takes part in this clinical trials. The subjects should sign informed consent form.

Exclusion Criteria:

- The subject has a suicide attempt within recent 1 year, or has a currently significant risk of suicide, or has a score =3 on item 3(suicide assessment) of the HAMD.

- The subject has a current psychiatric diagnosis other than depression.

- When the HAMD-17 score of baseline visit compares with the screening visit, the decreasing rate is =25%.

- Known hypersensitivity to Big Leaf Ju, or at least to two kinds of drugs.

- Any unstable cardiovascular, hepatic, renal, blood, endocrine, or other medical disease.

- Any neurological disease (such as Parkinson's Disease, cerebrovascular accident and epilepsy) or cerebral injury (traumatic or disease related).

- Had a history or a high risk related disease or medication of seizure disorder,except infantile febrile convulsion.

- Had a history of hyperthyroidism or hypothyroidism within recent 1 year and still taking medication.

- With psychotic symptoms.

- The subject has a history of mania episode, including manic, mixed, bipolar depression or rapid cycle attack.

- The subject has a current diagnosis of depression due to a somatic disease.

- The subject could not take medication or has a disease affecting drug absorption, such as active bowel disease, partial or total intestinal obstruction, or chronic diarrhea.

- Clinically significant electrocardiographic(ECG) abnormalities in screening visit. Such as QTc =450 ms in male or =470 ms in female; Sinus bradycardia and HR = 50 bpm; ? atrioventricular block; atrial fibrillation, etc.

- Clinically significant abnormal laboratory values(eg. Routine blood value above or below 1.2 times of the normal range; urine WBC, RBC or protein =++; ALT or AST value above 1.5 times of clinical top-limit; BUN value above 1.2 times of top-limit; Cr value above normal top-limit; thyroid gland function index above or below 1.2 times of the normal range, Fasting plasma glucose value above 1.2 times of normal top-limit; blood fat value above 1.5 times of normal top-limit).

- The subject who used at least two different antidepressants with recommended dose and adequate duration (maximum dosage by at least 4 weeks according to label) treatment still had no respond.

- The subject uses antidepressant drug normally before 2 weeks of screening, and stops using psychotropic drug before randomization less than 7 half-life period (monoamine oxidase inhibitor: at least 2 weeks; fluoxetine: at least 1 month)

- The subject received light therapy within 2 weeks.

- The subject received ECT, trans-cranial magnetic stimulation, or other physics therapy within 3 months.

- The subject received systematic psychotherapy (interpersonal relationship, psychoanalytic therapy, or cognitive behavioral therapy) within 3 months or plan to use systematic psychotherapy during the study period.

- The subject has a history of substance abuse (including alcohol, drug or other psychoactive substance) within 1 year before screening.

- Women who were pregnant, breast-feeding, or serum-HCG(+) on screening; or planning to become pregnant within 3 months after kick-off of clinical trial.

- The subject has participated in a drug clinical trial within 1 month before screening.

- The investigator thinks the subject is unsuitable to enroll in this clinical trial.

Study Design


Intervention

Drug:
Anyu Peibo
Anyu Peibo Capsule, 0.8g twice per day, oral after breakfast and supper
Placebo
Placebo Capsule, twice per day, oral after breakfast and supper

Locations

Country Name City State
China Beijing Anding Hospital,Capital Medical University Beijing Beijing
China Beijing HuiLongGuan Hospital Beijing Beijing
China West China Hospital, Sichuan University Chengdu Sichuan
China Jiangxi Mental Hospital Nanchang Jiangxi
China Shanghai Mental Health Center Shanghai Shanghai
China Brain Hospital of Jilin Province Siping Jilin
China Wuhan Mental Health Center Wuhan Hubei
China XI'AN Mental Health Center Xi'an Shanxi

Sponsors (2)

Lead Sponsor Collaborator
Shanghai Mental Health Center Su Zhou YiHua Biotechnology Co. LTD

Country where clinical trial is conducted

China, 

Outcome

Type Measure Description Time frame Safety issue
Other Physical Examination 6 weeks
Other AE Adverse Events 6 weeks
Other Laboratory Examination Blood RT, Urinalysis, Hepatic function, Renal function, FBG, Lipid, CK, Thyroid Function Test and Serum-HCG(fertile women only) 6 weeks
Other the Change of ECG from baseline 6 weeks
Primary The change of total score from baseline in MADRS scale 6 weeks
Secondary Clinical Response Rate according to MADRS 6 weeks
Secondary Clinical Remission Rate according to MADRS 6 weeks
Secondary Clinical Response Rate according to HAMD-17 6 weeks
Secondary Clinical Remission Rate according to HAMD-17 6 weeks
Secondary the Change of CGI (CGI-S, CGI-I) from baseline 6 weeks
Secondary the Change of total score from baseline in HAMA Hamilton Anxiety Rating Scale 6 weeks
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