Prospective registration

Human bioequivalence study of fentanyl citrate oral mucosal patch (pre-trial)

Human bioequivalence study of fentanyl citrate oral mucosal patch (pre-trial)

Human bioequivalence study of fentanyl citrate oral mucosal patch (pre-trial)

Shegting Zhang 

Guoping Yang/Wen Ouyang 

172 Tongzipo Road, Yuelu District, Changsha, Hu'nan

138 Tongzipo Road, Yuelu District, Changsha, Hu'nan

Clinical Trial Center of the Third Xiangya Hospital of Central South University

Clinical Trial Center of the Third Xiangya Hospital of Central South University

Yes

Institutional Review Board of theThird Xiangya Hospital of Central South University

Xiaomin WANG

Institutional Review Board of theThird Xiangya Hospital of Central South University, 138 Tongzipo Road, Yuelu District, Changsha, Hu'nan

Clinical Trial Center of the Third Xiangya Hospital of Central South University

138 Tongzipo Road, Yuelu District, Changsha, Hu'nan

Jiangsu Enhua Pharmaceutical Co., Ltd

pain

Interventional study

1

Cross-sectional 

Main purpose: To use fentanyl citrate oral mucosal patch (0.1 mg/piece or 0.2 mg/tablet) developed and produced by Jiangsu Sihua Pharmaceutical Co., Ltd. as the test preparation, and fentanyl citrate oral mucosal patch (0.1 mg/piece or 0.2 mg/tablet, trade name: Effentora) produced by TEVA PHARMACEUTICALS EUROPE B.V. as the reference preparation, The pharmacokinetic characteristics of the test preparation and the reference preparation when administered in a single dose under fasting conditions in Chinese subjects with mild chronic pain were studied, and the human bioequivalence of the two preparations under fasting conditions was preliminarily evaluated, which provided a basis for the design of blood collection points for the later formal bioequivalence test protocol. Secondary objective: To observe the safety of a single buccal test preparation and a reference preparation in Chinese subjects with mild chronic pain.

Subjects must meet all of the following criteria to be selected: 1. Aged 18-55 years (including boundary value), male or female; 2. The weight of male subjects >= 50.0 kg, the weight of female subjects >= 45.0kg, and the body mass index (BMI) is between 19~26 kg/㎡, including critical values; 3. Average pain scores over the past 24 hours assessed using the Digital Pain Scale (NRS) should be < 4 when a history of chronic pain is not receiving analgesics, and pain disorders remain stable in the near term and are predicted to remain stable throughout the study period; 4. Agree that no unprotected sexual activity will occur from the date of screening to 3 months after the test, and non-drug contraceptive measures must be used during the trial (pharmacological contraception includes oral contraceptives, contraceptive injections, subcutaneous embedded contraceptives, local contraceptives such as spermicides, etc.) and the results of female blood pregnancy (β-HCG) examination are not clinically significant; 5. The subject voluntarily signs a written informed consent form.

Subjects who meet one or more of the following criteria will be excluded: 1. Those who have suffered or are currently suffering from any serious clinical diseases such as circulatory system, endocrine system, nervous system, digestive system, respiratory system, genitourinary system, hematology, immunology, psychiatry and metabolism or any other diseases that can interfere with the test results; 2. Have a history of dysphagia or gastrointestinal diseases (such as gastric or small bowel resection, atrophic gastritis, gastrointestinal ulcer and/or gastrointestinal bleeding, obstruction, etc., except appendicitis appendectomy), or suffer from paralytic intestinal obstruction, gastrointestinal stricture, acute abdomen, and now feel digestive tract discomfort; 3. Patients with biliary tract disease, cholecystitis, pancreatitis, prostatic hypertrophy, thyroid dysfunction, adrenal insufficiency or urethral stricture; 4. Those with a history of seizures or increased intracranial pressure, brain swelling and pain, head injury or impaired consciousness; 5. Have a history of frequent or extensive bilateral oral ulcers, oral herpes or Sjogren's syndrome, or currently need oral pathological examination, or have dentures or braces that interfere with tablet placement; 6. Frequent heart or vomiting history caused by any cause; 7. Have a history of allergies to drugs (including fentanyl citrate and naltrexone), food or other substances; 8. Those who have undergone surgery within 4 weeks prior to the trial, or who plan to undergo surgery during the study; 9. Those who receive active or attenuated vaccines within 1 month before the test or during the planned trial; 10. Those who have taken any drug or health supplement (including Chinese herbal medicine) within 14 days prior to the use of the study drug; 11. Those who have used any drug that induces liver metabolism of the drug (such as: inducers-barbiturates, carbamazepine, phenytoin, glucocorticoids, omeprazole) within 30 days before the use of the study drug; 12. Those who have participated in any clinical trial and taken any clinical trial drug within 3 months before the trial; 13. Those who donated blood or lost a large amount of blood (>= 200 mL, except for women's menstrual blood loss), received blood transfusions or used blood products within 3 months before selection; 14. Pregnant or lactating women; 15. Those who have special requirements for diet and cannot comply with the uniform diet; 16. Those who have difficulty in venous blood collection or have needle sickness or blood sickness; 17. Excessive consumption of tea, coffee and/or caffeinated beverages (more than 8 cups, 1 cup = 250 mL) per day; 18. There is no guarantee that from 48 hours before the use of the study drug to the end of the study, any beverage or food rich in xanthine (such as animal liver), caffeine, theophylline (such as chocolate, tea, coffee and cola, etc.), or grapefruit fruit (grapefruit) or products containing grapefruit ingredients are prohibited; 19. Those who smoked more than 5 cigarettes per day in the 3 months before the test or could not stop using any tobacco products during the trial; 20. Positive alcohol breath test result or regular drinker in the 6 months before the test, that is, drinking more than 14 units of alcohol per week (1 unit = 360 mL of beer or 45 mL of spirits or 150 mL of wine with 40% alcohol content) or who cannot stop using any alcoholic products during the test; 21. Those who have positive drug abuse screening or have used soft drugs (such as marijuana) in the 3 months before the test or hard drugs (such as cocaine, phencyclic hexylpiperidine, etc.) in 1 year before the test; 22. Abnormal vital signs (systolic blood pressure < 90 mmHg or > 140 mmHg, diastolic blood pressure < 50 mmHg or > 90 mmHg; pulse < 50 bpm or > 100 bpm; Respiratory < 12 minutes or > 20 minutes) or blood oxygen saturation (Sp02) < 95%, or abnormal physical examination, electrocardiogram, laboratory examination have clinical significance (subject to the judgment of clinical research doctors); 23. Improved Markov score > grade II.; 24. Subjects may not be able to complete the study for other reasons or who the investigator believes should not be included.

The random table is randomly generated by the statistical unit using SAS (9.4 or later) in blocks with a 1:1 ratio between groups, and each subject is randomly placed in either the (T-R) group or the (R-T) group. This random data is reproducible, and the set random initial value seed parameter n

NO

Data Management Plan (DMP): The DMP is written by the Data Steward (DM) as a guidance document for data management and approved by the sponsor, and the data management will be carried out according to the time, content and methodology defined by the DMP. Electronic Medical Case Report Form (eCRF): The data manager builds according to the trial protocol design and sets up logical checks according to the Logic Review Plan (DVP), which is tested and approved by the sponsor before being released for use. Data entry: The eCRF data is derived from the original record, and the data entry personnel enter the subject event data into the EDC in a timely manner according to the cCRF filling instructions. Source Data On-Site Audit (SDV): Auditors check the consistency of cCRF data with source data, and ask questions if you have questions.