Y-3 Injection in the Treatment of Acute Ischemic Stroke Phase II Clinical Trial

Acute Ischemic Stroke Clinical Trial

Official title:

Y-3 Injection in the Treatment of Acute Ischemic Stroke Phase II Clinical Trial -- Multicenter, Randomized, Double-blind, Parallel, Placebo-controlled Phase II Clinical Trial

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT06429384
• Other study ID #: Y-3-LC-02
• Status: Completed
• Phase: Phase 2
• Start date: June 4, 2023
• Est. completion date: December 24, 2023

Study information

• Verified date: June 2024
• Source: Beijing Tiantan Hospital
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

The objective of this clinical trial was to explore the efficacy and safety of Y-3 injection at different doses in patients with acute ischemic stroke within 48 hours of onset. A multicenter, randomized, double-blind, parallel, placebo-controlled trial design was designed to include 240 participants. Subjects press 1:1:1: 1 ratio of patients were randomly divided into Y-3 low-dose group (20 mg/ time, qd), medium-dose group (40 mg/ time, qd), high-dose group (60mg/ time, qd) and placebo control group, with 60 cases in each group. Random stratification factors include: Time of onset (≤24 hours, > 24 hours). The patients were treated for 10 consecutive days (10 times) and followed up to 90 days after the first dose. The trial was divided into three phases: screening/baseline, treatment, and follow-up. Screening/baseline period: Subjects enter the screening/baseline period for screening examination after signing the informed consent. Treatment period: Eligible subjects were randomly assigned at a ratio of 1:1:1:1 to receive Y-3 injection low-dose group, medium-dose group, high-dose group and placebo control drug for 10 consecutive days (10 times), during which relevant examinations required by the protocol were conducted and safety was assessed. Follow-up period: Participants who finished treatment were followed up until 90 days after the first dose. Stroke-related scale scores were performed at 10, 30, and 90 days after first use of the investigational drug The scores of Montgomery Depression Rating Scale (MSAS) and Hamilton Anxiety Scale (HAMA) were performed on the 10th and 90th days after the use of experimental drugs. Adverse events were recorded during treatment and follow-up to further assess safety

Description:

A multicenter, randomized, double-blind, parallel, placebo-controlled trial design was designed to include 240 participants, who were randomly assigned to Y-3 low-dose group (20 mg/ time, qd), medium-dose group (40 mg/ time, qd), high-dose group (60 mg/ time, qd) and placebo control group in a ratio of 1:1:1:1. Each group had 60 cases. Random stratification factors included: onset time (≤24 hours, > 24 hours).The patients were treated for 10 consecutive days (10 times) and followed up to 90 days after the first dose. The trial was divided into three phases:screening/baseline, treatment, and follow-up. Screening/baseline period: Subjects enter the screening/baseline period for screening examination after signing the informed consent.Treatment period: Eligible subjects were randomly assigned at a ratio of 1:1:1:1 to receive Y-3 injection low-dose group, medium-dose group, high-dose group and placebo control drug for 10 consecutive days (10 times), during which relevant examinations required by the protocol were conducted and safety was assessed.Follow-up period: Participants who finished treatment were followed up until 90 days after the first dose.Stroke-related scale scores were performed on the 10th, 30th and 90th days after the first use of the experimental drug, and Montgomery Depression Rating Scale (MADRS) and Hamilton Anxiety Scale (HAMA) scores were performed on the 10th and 90th days after the first use of the experimental drug. Adverse events were recorded during treatment and follow-up to further assess safety.

Recruitment information / eligibility

• Status: Completed
• Enrollment: 240
• Est. completion date: December 24, 2023
• Est. primary completion date: November 18, 2023
• Accepts healthy volunteers: No
• Gender: All
• Age group: 18 Years to 80 Years

Eligibility

Inclusion Criteria:

-

Only those who meet all the following criteria can be included in the group:

1. Age = 18 years old and<81 years old, regardless of gender;

2. After the onset of this disease, the National Institutes of Research Stroke Scale score was 6 = NIHSS = 20 points, and the sum of the 5th upper limb and 6th lower limb scores was = 2 points. If patients receiving thrombolysis treatment were screened and evaluated based on the NIHSS score after thrombolysis;

3. Within 48 hours (including 48 hours) of onset;

4. Diagnosed as ischemic stroke according to the "Key Diagnostic Points for Various Major Cerebrovascular Diseases in China 2019", with good recovery after the first or last onset (mRS score = 1 point before this onset);

5. Obtain informed consent from the patient or their legal representative voluntarily signed and approved by the ethics committee. Exclusion Criteria: - Those who meet one of the following criteria during filtering cannot be included in the

group:

1. Intracranial hemorrhagic diseases seen on cranial imaging: hemorrhagic stroke, epidural hematoma, intracranial hematoma, ventricular hemorrhage, subarachnoid hemorrhage, etc; If it is only oozing blood, the researcher can determine whether it is suitable for enrollment;

2. Severe consciousness disorder: The item score of NIHSS's 1a consciousness level is greater than 1 point;

3. Transient ischemic attack (TIA);

4. After controlling the patient's blood pressure, the systolic blood pressure remains = 220mmHg or the diastolic blood pressure remains = 120mmHg;

5. Previously diagnosed patients with severe mental disorders and severe dementia;

6. Patients previously diagnosed with depression or anxiety disorder;

7. Patients undergoing antidepressant or anti anxiety treatment;

8. Diagnosed with severe active liver diseases, such as acute hepatitis, chronic active hepatitis, liver cirrhosis, etc; Or ALT or AST>2.0 × ULN;

9. Diagnosed with severe active kidney disease or renal insufficiency; Or serum creatinine>1.5 × ULN;

10. After the onset of the disease, drugs with brain cytoprotection in the instructions have been used, such as edaravone, concentrated solution of edaravone and dextranol for injection, nimodipine, ganglioside, CDPC, piracetam, oxiracetam, butylphenylpeptide, human urinary kallidinogenase (Urinary Kallidinogenase), cinepazide, rat nerve growth factor, cerebrolysin (cerebroprotein hydrolysate), calf serum deproteinized injection Calf blood deproteinized extract injection, etc;

11. After the onset of this disease, thrombectomy or interventional therapy has been applied or planned to be applied;

12. Previously diagnosed with concurrent malignant tumors and undergoing anti-tumor treatment;

13. Previously diagnosed with severe systemic diseases, with an estimated survival period of<90 days;

14. The patient is in pregnancy, lactation, and there is a possibility of pregnancy in the patient/patient partner who plans to conceive during the trial period;

15. Previously known allergies to this product or any of its excipients (15-hydroxystearic acid polyethylene glycol ester, propylene glycol, sodium hydroxide);

16. A history of major surgeries within 4 weeks prior to enrollment and assessed by the researcher as affecting neurological function scores or affecting 90 day survival;

17. Have participated in other clinical studies or are currently participating in other clinical studies within the first 30 days of randomization;

18. The researcher believes that it is not suitable to participate in this clinical study.

Related Conditions & MeSH terms

• Acute Ischemic Stroke
• Cerebral Infarction
• Ischemia
• Ischemic Stroke
• Stroke

Intervention

Drug:
• Y-3 Injection/Y-3 blank injection
The first dose should be completed as soon as possible after randomization; The time from the second dose to the first dose shall not be less than 12h, but not more than 24h+1h; The time interval of each subsequent administration is 24h±1h;

Locations

Country	Name	City	State
China	Inner Mongolia Baotou Steel Hospital	Baotou	Inner Mongolia Autonomous Region
China	The First Affiliated Hospital of Baotou Medical College, Inner Mongolia University of Science and Technology	Baotou	Inner Mongolia Autonomous Region
China	Beijing Tiantan Hospital, Capital Medical University Beijing	Beijing	Beijing
China	Beipiao Central Hospital	Beipiao	Liaoning
China	Cangzhou Central Hospital	Cangzhou	Hebei
China	Hunan Provincial People's Hospital	Changsha	Hunan
China	Daqing Oilfield General Hospital	Daqing	Heilongjiang
China	Daqing People's Hospital	Daqing	Heilongjiang
China	Dongyang City People's Hospital	Dongyang	Zhejiang
China	Harrison International Peace Hospital	Hengshui	Hebei
China	Inner Mongolia International Mongolian Medicine Hospital	Hohhot	Inner Mongolia Autonomous Region
China	Huai 'an First People's Hospital	Huai'an	Jiangsu
China	Shandong Third Hospital	Jinan	Shandong
China	The First Affiliated Hospital of Jinzhou Medical University	Jinzhou	Liaoning
China	Lianyungang First People's Hospital	Lianyungang	Jiangsu
China	Lianyungang Second People's Hospital	Lianyungang	Jiangsu
China	Liaocheng People's Hospital	Liaocheng	Shandong
China	Tancheng County First People's Hospital	Linyi	Shandong
China	Liuzhou Workers Hospital	Liuzhou	Guangxi
China	Nanyang Second People's Hospital	Nanyang	Henan
China	Nanyang South Stone Hospital	Nanyang	Henan
China	The First Affiliated Hospital of Nanyang Medical College	Nanyang	Henan
China	Pingxiang People's Hospital	Pingxiang	Jiangxi
China	Chinese People's Liberation Army Northern Theater Command General Hospital	Shenyang	Liaoning
China	Shenyang First People's Hospital	Shenyang	Liaoning
China	Taizhou Second People's Hospital	Taizhou	Jiangsu
China	Tengzhou Central People's Hospital	Tengzhou	Shandong
China	Xuzhou Central Hospital (Old Hospital Area)	Xuzhou	Jiangsu
China	Xuzhou Central Hospital(New compound)	Xuzhou	Jiangsu
China	Xuzhou First People's Hospital	Xuzhou	Jiangsu

Sponsors (2)

Lead Sponsor	Collaborator
Beijing Tiantan Hospital	NeuroDawn Pharmaceutical Co., Ltd.

Country where clinical trial is conducted

China, 

References & Publications (23)

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* Note: There are 23 references in all — Click here to view all references

Outcome

Type	Measure	Description	Time frame	Safety issue
Other	Montgomery Depression Rating Scale scores on day 10 and day 90 were &lt, respectively; Proportion of patients with scores of 12, =12, and =22;	Montgomery Depression Rating Scale scores on day 10 and day 90 were <, respectively; Proportion of patients with scores of 12, =12, and =22.There are 10 items in the scale, with a total score of 60 points. The higher the score, the higher the degree of depression. MADRS < 12 indicates no depressive symptoms, 12=MADRS < 22 indicates mild depression, 22=MADRS < 30 indicates moderate depression, and MADRS=30 indicates severe depression.	On the 10th and 90th day of treatment
Other	Hamilton Anxiety Scale scores on day 10 and day 90 were &lt, respectively; Proportion of patients with scores of 7, =7, and =14.	Hamilton Anxiety Scale (HAMA) scores on day 10 and day 90 were <, respectively; Proportion of patients with scores of 7, =7, and =14.The scale used a 5-level scoring method, and the criteria for each level were: 0-asymptomatic; 1- Light; 2- Medium; 3- heavy; 4- Extremely heavy. The total score of Hamilton anxiety Scale is a very important basis to reflect the severity of patients' anxiety, that is, the less severe the disease, the lower the total score; The more severe the condition, the higher the total score. A total score of less than 7 is considered to have no symptoms of anxiety; A score of 7-13 is considered to be likely to have anxiety; A score of 14 to 20 is considered to be definitely anxious; 21 to 28 points, is considered to have significant anxiety; A score greater than 29 is considered likely to be severe anxiety.	On the 10th and 90th day of treatment
Other	Incidence of adverse events (AE) in each group;	Incidence of adverse events (AE) in each group;	From the time the subject receives medication to the end of the 90th day of the treatment
Other	The incidence of treatment-related adverse events (TEAEs) in each group;	The incidence of treatment-related adverse events (TEAEs) in each group;	From the time the subject receives medication to the end of the 90th day of the treatment
Other	The occurrence of important adverse events in each group;	The occurrence of important adverse events in each group;	From the time the subject receives medication to the end of the 90th day of the treatment
Other	The occurrence of serious adverse events (SAEs) in each group;	The occurrence of serious adverse events (SAEs) in each group;	From the time the subject receives medication to the end of the 90th day of the treatment
Other	The occurrence of suspicious and unexpected serious adverse reactions (SUSAR) in each group;	The occurrence of suspicious and unexpected serious adverse reactions (SUSAR) in each group;	From the time the subject receives medication to the end of the 90th day of the treatment
Other	Laboratory examination indicators: blood routine, urine routine, blood biochemistry, Laboratory examination indicators: blood routine, urine routine, blood biochemistry, coagulation function	Detect blood routine through a blood cell analyzer, including white blood cell count, neutrophil count, lymphocyte count, hemoglobin, and platelet count.Use a biochemical analyzer to detect blood biochemistry, including alanine aminotransferase, aspartate aminotransferase, alkaline phosphatase, total bilirubin, direct bilirubin, creatinine, urea/urea nitrogen, uric acid, and so on. Detect coagulation function through a coagulation analyzer, including prothrombin time (PT), partially activated prothrombin time (APTT), international standardized ratio (INR), fibrinogen (FIB).Detect urine routine through a urine analyzer.These indicators are measured during the baseline period and post administration visit period to observe the impact of the drug on this indicator, whether the drug will cause AE and SAE,the occurrence of AE and SAE, the type and severity of AE and SAE, and ultimately to determine the safety of the drug.	Baseline period, on the 10th , 30th and 90th day
Other	Vital signs: heart rate, blood pressure, body temperature, respiration	Detecting parameters such as heart rate, electrocardiogram, and QT interval through an electrocardiogram monitor.Detecting blood pressure through a blood pressure monitor.Detecting body temperature through a thermometer.Detect respiratory rate by observing changes in chest contour count of the subject.These indicators are measured during the baseline period and post administration visit period to observe the impact of the drug on this indicator, whether the drug will cause AE and SAE,the occurrence of AE and SAE, the type and severity of AE and SAE, and ultimately to determine the safety of the drug.	Baseline period, on the 10th , 30th and 90th day
Other	Physical examination of the whole body: lungs, gastrointestinal tract, urinary system, musculoskeletal system, skin, lymph nodes, and other systems.	Detect systems such as lungs, gastrointestinal tract, urinary system, musculoskeletal, skin, lymph nodes, etc. through observation, auscultation, percussion, palpation, and other examination methods. These indicators are measured during the baseline period and post administration visit period to observe the impact of the drug on this indicator, whether the drug will cause AE and SAE,the occurrence of AE and SAE, the type and severity of AE and SAE, and ultimately to determine the safety of the drug.	Baseline period, on the 10th , 30th and 90th day
Other	Clinical laboratory examination	Laboratory evaluation not specified in the protocol, including parameters such as hematology, biochemical tests, urine analysis, etc. These indicators are measured during the baseline period and post administration visit period to observe the impact of the drug on this indicator, whether the drug will cause AE and SAE,the occurrence of AE and SAE, the type and severity of AE and SAE, and ultimately to determine the safety of the drug.	From the baseline period to the end of the 90th day of the treatment
Other	Discontinuation due to adverse events;	Discontinuation due to adverse events?AE includes abnormal laboratory test results (haematological, clinical biochemical, or urinalysis) or other safety assessments (e.g. electrocardiograms, radiological scans, vital signs measurements), including deterioration relative to baseline and deemed clinically significant in the medical and scientific judgment of the investigator; Exacerbation of pre-existing diseases; A new condition detected or diagnosed after the initiation of the investigational drug.?	From the beginning to the end caused by adverse events
Other	Discontinuation due to any other non-adverse event.	Discontinuation due to any other non-adverse event(Any discontinuation other than an adverse event)	From the beginning to the end due to unexpected circumstances except for adverse events
Primary	The proportion of subjects with mRS score = 1 on the 90th day of treatment .	The proportion of subjects with mRS score = 1 on the 90th day of treatment .	90th day of treatment
Secondary	Grade analysis of mRS Score on the 90th day of treatment;	Grade analysis of mRS Score on the 90th day of treatment;	90th day of treatment
Secondary	The proportion of subjects with mRS Score =2 on the 90th day of treatment;	The proportion of subjects with mRS Score =2 on the 90th day of treatment;	90th day of treatment
Secondary	Changes in NIH Stroke Scale from baseline on day 10 of treatment;	Changes in NIH Stroke Scale from baseline on day 10 of treatment;	10th day of treatment
Secondary	Proportion of NIH Stroke of 0-1 or =4 reduction from baseline on day 10 and day 30 of treatment.	Proportion of NIH Stroke of 0-1 or =4 reduction from baseline on day 10 and day 30 of treatment.The content of NIHSS score included: consciousness level (consciousness level, consciousness level questioning, consciousness level command), gaze, visual field, facial paralysis, upper limb movement, lower limb movement, body aid movement, sensation, language, dysarthria, neglect. The score ranges from 0 to 42, with higher scores indicating more severe nerve damage.Score 0 to 1: normal or nearly normal Scores 1-4: mild stroke/minor stroke .5 to 15 points: moderate stroke .15-20 points: moderate to severe stroke Scores 21-42: severe stroke	On the 10th and 30th day of treatment