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A Phase 3 study of NPC-06 in Patients With Pain Associated with acute Herpes Zoster

Basic Information

Recruitment status	Not Recruiting
Health condition(s) or Problem(s) studied	Pain Associated with acute Herpes Zoster
Date of first enrollment	21/09/2022
Target sample size	50
Countries of recruitment
Study type	Interventional
Intervention(s)	(NPC-06) (Placebo) (1) Initial dose (Day 1) <Dose> An 18 mg/kg of the test drug or placebo will be injected by intravenous drip infusion once daily. The maximum dose of the test drug should not exceed 1,200 mg as fosphenytoin sodium. <Administration method> Dilute the study drug 3 to 4-fold using physiological saline for intravenous infusion and then administer the solution over 18 minutes. (2) Maintenance dose(Day 2-7) Maintenance dose on the next day (Day 2) after the initial dose will be mandatory, and will be dosed up to 6 days. Maintenance dose on Day 3 and thereafter will follow the transition criteria for maintenance dose. <Dose> A 7.5 mg/kg of the test drug or placebo will be injected as needed by intravenous drip infusion once daily. The maximum dose of the test drug should not exceed 500 mg as fosphenytoin sodium. <Administration method> Dilute the study drug 3-to 4-fold using physiological saline for intravenous infusion and then administer the solution over 7 minutes and 30 seconds.

Outcome(s)

Primary Outcome

Change in the NRS pain score from baseline at 120 minutes after the study drug administration.

Secondary Outcome

1. Change in the NRS pain score from baseline at each assessment time point up to 120 minutes after the first maintenance dose. 2. Change in the NRS pain score from baseline at each assessment time point after the study drug administration. 3. Taking the time point immediately before the first maintenance dose as the tentative baseline, changes in the pain NRS score from the tentative baseline at each assessment time point after the first maintenance dose to immediately before the second maintenance dose. 4. Time to the first occurrence of the following event (Time to event) during the period from immediately before the study drug administration to immediately before the second maintenance dose. -Event that change in the NRS pain score remained unchanged or increased (increase of 1 point or more) 5. The period of time during which the NRS pain score has been maintained to improve by 2 points or more from baseline. 6. Proportion of subjects whose NRS pain score has improved by 2 points or more at 120 minutes after the study drug administration from immediately before the study drug administration. 7. Change in the SF-8 (24-hour version) score for QOL from baseline. 8. Change in the NPSI score (as assessed by type of pain and total score) from baseline. 9. Number of times non-opioid analgesics used before and after the study drug administration. 10. Proportion of subjects who have continued the maintenance dose.

Key inclusion & exclusion criteria

Age minimum	>= 18age old
Age maximum	Not applicable
Gender	Both
Include criteria	(1) Patients aged 18 years or older at the time of informed consent. (2) Patients who are male or female. (3) Patients who are inpatient or outpatient. (4) Patients who are diagnosed with herpes zoster and have acute pain. (5) Patients who are within 28 days after the onset of herpes zoster. (6) Patients whose mean NRS pain score is 4 or higher despite the use of the following drugs during the period between 24 hours and 120 minutes before the study drug administration. During this period, one or two of the following drugs should have been used, and the same drug should have been used at least twice. -Non-opioid analgesics (excluding its sustained release formulations and topical drugs used for other sites than the target site for efficacy) -Ca2+ channels alpha2delta ligands (excluding gabapentin) -Tramadol (excluding its sustained release formulations) -An extract from inflammatory rabbit skin inoculated by vaccinia virus (7) Patients whose NRS pain score immediately before the study drug administration is 4 or higher. (8) Patients who are able to perform NRS self-assessment appropriately. (9) Patients who gave written informed consent based on their own free will after receiving adequate explanation and fully understanding the details of the explanation in participating in the study.
Exclude criteria	(1) Patients who are suspected to be increased intracranial pressure. (2) Patients who are complicated with epilepsy, serious mental or neuropsychiatric disorders (including dementia, Parkinson's disease, or schizophrenia) or consciousness disturbance. (3) Patients who are being treated for malignancy. However, those who do not interfere with daily life and have good general condition may be included in the study. (4) Patients who are being treated for HIV infection or those who are receiving immunosuppressant (including biologics). However, those who do not interfere with daily life and have good general condition may be included in the study. (5) Patients who are being treated for idiopathic trigeminal neuralgia. (6) Patients who have other severe pain that may affect the assessment of pain associated with acute herpes zoster. (7) Patients who have received non-opioid analgesics (excluding its sustained release formulations and topical drugs used for other sites than the target site for efficacy), Ca2+ channel alpha2delta ligands (excluding gabapentin), tramadol (excluding its sustained release formulations), or an extract from inflammatory rabbit skin inoculated by vaccinia virus during the period from 120 minutes before the study drug administration to the start of study drug administration. (8) Patients who have received the following drugs during the period from 24 hours before the study drug administration to immediately before the study drug administration. -Non-opioid analgesics (its sustained release formulations) -Gabapentin -Tramadol (its sustained release formulations) -Opioid analgesics -Steroidal anti-inflammatory drugs (systemic) for treatment of herpes zoster and pain associated with acute herpes zoster -Antidepressants, antiarrhythmics (excluding those in Vaughan Williams class 2), NMDA receptor antagonists, centrally acting muscle relaxants, and anesthetics (excluding topical drugs used for other sites than the target site for efficacy). (9) Patients who have sinus bradycardia or advanced conduction disturbance. (10)Patients who have a history of hypersensitivity to hydantoin. (11)Patients who are receiving drugs that are contraindicated in the package insert for fosphenytoin. (12)Patients who have received amenamevir during the period from 24 hours before the study drug administration to immediately before the study drug administration. (13)Patients who are complicated with meningitis or have symptoms of meningeal irritation. (14)Patients who have serious cardiac disease, respiratory disorder, or hepatic or renal dysfunction (as a guide, seriousness corresponding to Grade 3 of Standards for Classification of Seriousness of Adverse Drug Reactions [Notification No.80 of the Pharmaceutical Safety Notificatio]). (15)Patients who are receiving fosphenytoin, phenytoin, ethotoin, or a combination of these drugs or have received these drugs as adjuvant analgesics. (16)Patients who have participated in other clinical study within 3 months of the date of the screening test. (17)Pregnant women, lactating women or patients of childbearing potential during the study period. (18)Patients who are unable to give appropriate contraception in accordance with the instructions of the investigator or sub-investigator (hereafter, the investigators) during the period from after obtaining informed consent to the end of the follow-up period. (19)Other patients who are deemed inappropriate for participation in the study by the investigators.