This is a prospective, multi-centric, randomized, double-blind, parallel, controlled phase-III efficacy clinical study of PMZ-2010 therapy in patients with hypovolemic shock. Centhaquine (previously used names, centhaquin and PMZ-2010; International Non-proprietary Name (INN) recently approved by WHO is centhaquine) has been found to be an effective resuscitative agent in rat, rabbit and swine models of hemorrhagic shock, it decreased blood lactate, increased mean arterial pressure, cardiac output, and decreased mortality. An increase in cardiac output during resuscitation is mainly attributed to an increase in stroke volume. Centhaquine acts on the venous α2B-adrenergic receptors and enhances venous return to the heart, in addition, it produces arterial dilatation by acting on central α2A-adrenergic receptors to reduce sympathetic activity and systemic vascular resistance.
Approximately 105 patients will be randomized 2:1 into 2 treatment groups after meeting the eligibility criteria. Total 70 patients will be enrolled in PMZ-2010 group (Group 1) and in Normal Saline group (Group 2) total 35 patients will be enrolled. * Group 1: PMZ-2010 (Dose: 0.01 mg/kg) + Standard of care * Group 2: Normal Saline (Dose: Equal volume) + Standard of care In both treatment groups, patients will be provided the standard of care. PMZ-2010 or Normal Saline will be administered intravenously after randomization to hypovolemic shock patients with systolic arterial blood pressure ≤ 90 mmHg at presentation and continue to receive standard Shock Treatment. In PMZ-2010 group, dose of PMZ-2010 (0.01 mg/kg) will be administered as an intravenous (IV) infusion over 1 hour in 100 mL of normal saline. Second dose of PMZ-2010 will be administered if SBP falls below or remains below or equal to 90 mmHg but not before 4 hours of previous dose and total doses per day (in 24 hours) will not exceed 3 doses. PMZ-2010 administration if needed will continue for two days post randomization. Minimum 1 dose or maximum 6 doses of PMZ-2010 will be administered within first 48 hours. post randomization. In Control group, single dose of equal volume of Normal Saline will be administered as intravenous (IV) infusion over 1 hour in 100 mL of normal saline post randomization. Condition of administration will remain same as for PMZ-2010 group. Each patient will be monitored closely throughout his/her hospitalization and will be followed until discharge from randomization. Each patient will be assessed for efficacy parameters over 28 days from randomization to a clinic visit.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
QUADRUPLE
Enrollment
105
Normal Saline to be Used as Vehicle in the Phase-III Study to Assess Efficacy of PMZ-2010 as a Resuscitative Agent for Hypovolemic Shock
Phase-III Study to Assess Efficacy of PMZ-2010 as a Resuscitative Agent for Hypovolemic Shock
Seven Star Hospital
Nagpur, Maha, India
Jawahar Lal Nehru Medical College & Attached Hospitals
Ajmer, India
Radiant Superspeciality Hospital
Amravati, India
People Tree Hospitals
Bangalore, India
KLE's Dr. Prabhakar Kore Hospital & Medical Research Centre
Belagavi, India
Shri Guru Ram Rai Institute of Medical & Health Sciences
Dehradun, India
Department of Surgery, GSVM Medical College
Kanpur, India
Institute of Postgraduate Medical Education & Research and SSKM Hospital
Kolkata, India
King George's Medical University
Lucknow, India
Christian Medical College & Hospital
Ludhiana, India
...and 8 more locations
Change in systolic and diastolic blood pressure
Change in systolic and diastolic blood pressure - Mean through 48 hours
Time frame: 48 hours
Change in blood lactate level
Change in blood lactate level - Mean through 48 hours
Time frame: 48 hours
Change in base-deficit
Change in Base-deficit - Mean through 48 hours
Time frame: 48 hours
Total Urine Output
Total volume of urine output - Mean through 48 hours
Time frame: 48 hours
Vasopressor(s) infused
Amount of total vasopressor(s) infused - Mean through 48 hours
Time frame: 48 hours
Volume of fluid administered
Total volume of fluid administered - Mean through 48 hours
Time frame: 48 hours
Doses of study drug
Number of doses of study drug administered in first 48 hours post randomization
Time frame: 48 hours
Incidence of mortality
Proportion of patients with all-cause mortality at 48 hours and 28 days
Time frame: 28 days
Stay in hospital, in ICU and/or on Ventilator
Days in hospital, in ICU and/or on Ventilator - Mean through 28 days
Time frame: 28 days
Change in Multiple Organ Dysfunction Syndrome Score
Change in Multiple Organ Dysfunction Syndrome Score (MODS) - Mean through 28 days. MODS is a 5 grade scale from 0 to 4, where 0 is the best and 4 is the worst outcome.
Time frame: 28 days
Change in Acute Respiratory Distress Syndrome
Change in Acute Respiratory Distress Syndrome (ARDS) - Mean through 28 days. ARDS will be determined using Murray Score for Acute Lung Injury which is based upon radiological findings, oxygenation status, ventilation status of the patient. A lower score of 0 is the best and about 2.5 is the worst outcome.
Time frame: 28 days
Change in Glasgow coma score
Change in Glasgow coma score (GCS) - Mean through 28 days. GCS is a 15 point scale to assess the level of consciousness of patients where less than 3 is comatose state and 15 is fully awake.
Time frame: 28 days
Incidence of adverse events
Proportion of patients with drug related adverse events during 28 days
Time frame: 28 days
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