Clinical Trials Logo

Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT03764085
Other study ID # RheoSTAT-CP0620
Secondary ID
Status Completed
Phase Phase 4
First received
Last updated
Start date December 6, 2016
Est. completion date December 11, 2019

Study information

Verified date January 2020
Source Yuria-Pharm
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This study evaluates the efficacy and safety of Rheosorbilact®, solution for infusion ("Yuria-Pharm" LLC), in comparison with Ringer's Lactate, solution for infusion, in a complex therapy of sepsis. Half of participants will receive Rheosorbilact® in complex therapy, while the other half will receive Ringer's Lactate in complex therapy.


Description:

Rheosorbilact® has rheological, anti-shock, detoxification, and alkalizing effects. Sorbitol and sodium lactate are the major pharmacologically active ingredients. In the liver, sorbitol is first converted into fructose, which is then converted into glucose, and then into glycogen. Part of sorbitol is used for urgent energy needs, while the other part is kept as a reserve in the form of glycogen. Isotonic sorbitol solution has a disaggregating effect and, therefore, improves microcirculation and tissue perfusion.

The management of metabolic acidosis with sodium lactate goes more slowly compared to bicarbonate solution, as far as sodium lactate enters the metabolic process; however the latter does not cause swings in pH values. The effect of sodium lactate is typically seen 20 to 30 minutes after administration.

Sodium chloride is a plasma-substituting agent that exhibits a detoxification and rehydration effect. It replenishes the deficiency of sodium and chlorine ions in various pathological conditions.

Calcium chloride replenishes deficiency of calcium ions. Calcium ions are essential in the transmission of nerve impulses, contraction of skeletal and smooth muscles, myocardial activity, bone tissue formation, and blood clotting. It reduces the permeability of cells and vascular walls, prevents the development of inflammatory reactions, enhances the resistance of the body to infections and can significantly boost phagocytosis.

Potassium chloride restores the water-electrolyte balance. It exhibits a negative chrono- and bathmotropic action and, when administered in high doses, has a negative ino- and dromotropic and moderate diuretic effect. It is involved in the process of nerve impulse conduction, increases the content of acetylcholine and causes excitation of the sympathetic segment of the autonomic nervous system and improves the contraction of skeletal muscles in subjects with muscular dystrophy or myasthenia.

Rheosorbilact® is administered to improve capillary blood flow for the prevention and treatment of traumatic, surgical, hemolytic, toxic and burn shock, acute blood loss, and burn disease; infectious diseases accompanied by intoxication, exacerbation of chronic hepatitis; sepsis, pre- and postoperative period to improve arterial and venous circulation for the prevention and treatment of thrombosis, thrombophlebitis, endarteritis, and Raynaud's disease.

Ringer's Lactate, solution for infusion will be used as a comparator. As a rehydrating agent, Ringer's Lactate has a detoxification effect, replenishes the deficiency of circulating blood volume, and stabilizes the water and electrolyte composition of blood. Ringer's Lactate normalizes the acid-base balance. Lactate is metabolized in the body to bicarbonate, so the solution has an alkalizing effect. With osmolarity at 273 mOsm/l, Ringer's Lactate is close to isotonic solution and is indicated for hypovolemia, isotonic dehydration, and metabolic alkalosis.


Recruitment information / eligibility

Status Completed
Enrollment 180
Est. completion date December 11, 2019
Est. primary completion date December 11, 2019
Accepts healthy volunteers No
Gender All
Age group 18 Years to 60 Years
Eligibility Inclusion Criteria:

1. Male and female aged 18 to 60 years inclusive

2. Sepsis diagnosed according to ACCP / SCCM criteria (no later than 24 hours from the time of diagnosis of sepsis to screening visit) (Annex 1: Sequence Diagnostic Criteria for SCCM / ESICM / ACCP / ATS / SIS)

3. Informed consent for participation in the study signed by subject's own hand.

4. The baseline value of the SOFA scale = 2 points.

Non-inclusion Criteria:

1. The presence of any of the criteria for severe sepsis by ACCP / SCCM (presence of signs of organ failure - Annex 1: criteria for diagnosis of sepsis SCCM / ESICM / ACCP / ATS / SIS)

2. Individual intolerance of the components of the study drug and the comparator;

3. Hypersensitivity to sodium lactate;

4. Intravenous infusions of lactate- or sorbitol-containing products within 24 hours before enrollment;

5. Pregnancy or breast-feeding;

6. Severe renal dysfunction (creatinine is more than 300 µmol/l or estimated creatinine clearance is less than 30 ml/min);

7. Metabolic alkalosis;

8. Severe metabolic acidosis;

9. Intracerebral hemorrhage;

10. Any thromboembolism;

11. Decompensated cardiovascular failure;

12. Arterial hypertension III st;

13. Conditions associated with immunodeficiency (the use of cytostatics or system steroids, AIDS);

14. Extracellular hyperhydration or hypervolemia;

15. Severe renal insuffiency (with oliguria / anuria);

16. Hyperkalaemia;

17. Hypercalcemia;

18. Ascites associated with cirrhosis;

19. Conditions associated with increased lactate levels (hyperlactatemia > 2 mmol / l), including lactic acidosis, or impaired lactate uptake (including due severe hepatic insufficiency);

20. Concomitant therapy with cardiac glycosides;

Exclusion Criteria:

1. Infusion of the study drug or the comparator is started more than 12 hours after randomization;

2. Lack of data for sepsis (diagnosis not confirmed);

3. Withdrawal of the informed consent by the subject;

4. Investigator considers that the infusion therapy with either study drug or comparator may not be continued for safety reasons;

5. Development of conditions that prevent further use of the study drug/comparator before efficacy evaluation visit (Visit 3);

6. Subject needs concomitant therapy prohibited in the study before efficacy evaluation visit (Visit 3);

7. Development of conditions (including serious adverse events) which make it impossible to evaluate the primary endpoint;

8. Confirmation of pregnancy at any time of the study.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Rheosorbilact®
Administered intravenously (with speed 40-60 drip per minute) at a dose of 600 to 1,000 ml (10 to 15 ml/kg body weight per 24 hours) for 3 days.
Ringer lactate
Administered intravenously (with speed 40-60 drip per minute) at a dose of 1,000 to 2,500 ml (15 to 40 ml/kg body weight per 24 hours) for 3 days.

Locations

Country Name City State
Georgia "Unimedi Adjara" LLC Batumi
Georgia Kutaisi Referral Hospital Kutaisi
Kazakhstan Hospital of the Medical Center of the Administration of the President of the Republic of Kazakhstan Astana
Moldova, Republic of Institute of Ambulance Chisinau
Moldova, Republic of Municipal Clinical Hospital "Sfinta Treime" Chisinau
Moldova, Republic of Republican Clinical Hospital Chisinau
Ukraine Dnipro`s Medical Academy of Ministry of Health of Ukraine Dnipro
Ukraine Zaicev's Institute of general and urgent surgery NMA Ukraine Kharkiv
Ukraine Khmelnytskyi Regional Clinical Hospital Khmelnytskyi
Ukraine HSEE of Ukraine "Ukrainian Medical Stomatological Academy"; Poltava Central District Hospital Poltava
Ukraine Central District Clinical Hospital Vinnitsa
Ukraine Zaporizka Medical Academy of postgraduate education, Zaporizkyi Clinical Hospital N9 Zaporizhzhya
Uzbekistan Republic Centre of Ambulance Tashkent

Sponsors (1)

Lead Sponsor Collaborator
Yuria-Pharm

Countries where clinical trial is conducted

Georgia,  Kazakhstan,  Moldova, Republic of,  Ukraine,  Uzbekistan, 

Outcome

Type Measure Description Time frame Safety issue
Other Incidence of Treatment-Emergent Adverse events All types of adverse events Patients will be followed during 14 days.
Other Incidence of multiple organ failure Incidence of multiple organ failure Patients will be followed during 14 days.
Other Overall survival (%) at follow-up visit. Overall survival (%) at follow-up visit. Follow-up visit (Day 14±1)
Primary A change in the total SOFA score vs. baseline score upon admission; Sequential Organ Failure Assessment (SOFA) score is composed of scores of six organ systems: R-respiratory, C-cardiovascular, H-hepatic, Co-coagulation, Re-renal, and N-neurological graded from 0 to 4 according to the degree of dysfunction or failure.
The SOFA score ranges from 0 to 24 points. We evaluate initial SOFA score and differences between subsequent scores (?-SOFA scores).
Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary A change in the total APACHE II score vs. baseline score upon admission; Acute physiology and chronic health evaluation(APACHE) II score is calculated from a patient's age (0-6 points) and 12 physiological parameters (each item 0-4 points): AaDO2 or PaO2 (depending on FiO2), Temperature (rectal), Mean arterial pressure, pH arterial, Heart rate, Respiratory rate, Sodium (serum), Potassium (serum), Creatinine, Hematocrit, White blood cell count, Glasgow Coma Scale and chronic disease health status (0-5 points).
The APACHE II score ranges from 0 to 71 points. We evaluate initial APACHE II score and differences between subsequent scores (?-APACHE II scores).
Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary A change in the total SAPS II score vs. baseline score upon admission The SAPS II score is made of 17 variables: 12 physiology variables, age, type of admission (scheduled surgical, unscheduled surgical, or medical), and three underlying disease variables (acquired immunodeficiency syndrome, metastatic cancer, and hematologic malignancy).
The SAPS II score ranges from 0 to 160 points. We evaluate initial SAPS II score and differences between subsequent scores (?-SAPS II scores).
Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary A change in the total MODS score vs. baseline score upon admission MODS (Multiple Organ Dysfunction Score) is composed of scores of six organ systems: R-respiratory, C-cardiovascular, H-hepatic, Co-coagulation, Re-renal, and N-neurological graded from 0 to 4 according to the degree of dysfunction or failure.
The MODS score ranges from 0 to 24 points. We evaluate initial MODS score and differences between subsequent scores (MODS scores).
Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of glucose Concentration of glucose (mmol/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of sodium Concentration of sodium (mmol/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of potassium Concentration of potassium (mmol/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of lactate Concentration of lactate (mmol/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of pyruvate Concentration of pyruvate (mmol/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of urea Concentration of urea (mmol/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of creatinine Concentration of creatinine (µmol/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of bilirubin Concentration of bilirubin (µmol/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of alanine aminotransferase Concentration of alanine aminotransferase (U/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of aspartate aminotransferase Concentration of aspartate aminotransferase (U/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of lactate dehydrogenase Concentration of lactate dehydrogenase (U/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of alkaline phosphatase Concentration of alkaline phosphatase (U/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of creatine kinase Concentration of creatine kinase (U/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of ?-Glutamyltransferase Concentration of ?-Glutamyltransferase (U/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of low-molecular-weight adiponectin (LMW) Concentration of low-molecular-weight adiponectin (U/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of middle-molecular-weight adiponectin (MMW) Concentration of middle-molecular-weight adiponectin (U/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of albumin Concentration of albumin in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Procalcitonin level Concentration of procalcitonin level (µg/L) in blood serum after 8-hour fasting. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary White blood cells (WBC) count level White blood cells (billion/L) count level in blood serum after 8-hour fasting Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Lymphocyte count level Lymphocyte count (%) level in blood serum after 8-hour fasting Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Platelet count level Platelet count level (billion/L) in blood serum after 8-hour fasting Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Calculation of Nuclear index of intoxication (NII) Calculated by dividing the number of myelocytes, young and stab neutrophils by number of segmented neutrophils. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Calculation of Leukocyte index of intoxication (LII) Calculated by the formula of Kalf-Kalifa: correlation between the level of neutrophils and the content of other cells in the blood leukocytic composition. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of C-reactive protein (CRP) Concentration of C-reactive protein (CRP) in blood serum after 8-hour fasting Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Level of circulating immune complexes (CIC) Level of Circulating immune complexes (CIC) in blood serum after 8-hour fasting Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of Interleukin-1 and 2 Concentration of Interleukin-1 (pg/ml) and Interleukin-2 (pg/ml) in blood serum after 8-hour fasting Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Calculation of neutrophil-to-lymphocyte ratio (NLR) Calculated by dividing the number of neutrophils (%) by number of lymphocytes (%). Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of immunoglobulins Concentration of Ig A, Ig M and Ig G in blood serum after 8-hour fasting Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Concentration of complements Concentration of complements (C3, C4) in blood sample after 8-hour fasting Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Assessment of central hemodynamics Measurement of central venous pressure (mmh2o) in the central vein Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary A change in the total Glasgow Coma Scale (GCS) score vs. baseline score upon admission The GCS is composed of 3 components: ocular response (assessment 1-4 points), motor response (assessment 1-6 points) verbal response (evaluation of 1-5 points). Scores for each component are added together to get the total that will range between a minimum of 3 points (which corresponds to a patient who does not open his eyes and no motor response to stimulation or verbal response) and a maximum value of 15 points (corresponding to a patient with open eyes, obeying orders and maintaining a consistent language). Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Assessment of electrocardiogram (ECG) Presence of clinically significant changes on ECG is evaluated. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
Secondary Clinical signs Presence of clinical signs (adynamia, weakness, memory impairment, sleep disorder, irritability) is based on patient's subjective complaints. Will be evaluated for the duration of Intensive Care Unit (ICU) stay, at screening (Day 0) and Visit 3 (Day 3) of ICU stay.
See also
  Status Clinical Trial Phase
Active, not recruiting NCT05095324 - The Biomarker Prediction Model of Septic Risk in Infected Patients
Completed NCT02714595 - Study of Cefiderocol (S-649266) or Best Available Therapy for the Treatment of Severe Infections Caused by Carbapenem-resistant Gram-negative Pathogens Phase 3
Completed NCT03644030 - Phase Angle, Lean Body Mass Index and Tissue Edema and Immediate Outcome of Cardiac Surgery Patients
Completed NCT02867267 - The Efficacy and Safety of Ta1 for Sepsis Phase 3
Completed NCT04804306 - Sepsis Post Market Clinical Utility Simple Endpoint Study - HUMC
Recruiting NCT05578196 - Fecal Microbial Transplantation in Critically Ill Patients With Severe Infections. N/A
Terminated NCT04117568 - The Role of Emergency Neutrophils and Glycans in Postoperative and Septic Patients
Completed NCT03550794 - Thiamine as a Renal Protective Agent in Septic Shock Phase 2
Completed NCT04332861 - Evaluation of Infection in Obstructing Urolithiasis
Completed NCT04227652 - Control of Fever in Septic Patients N/A
Enrolling by invitation NCT05052203 - Researching the Effects of Sepsis on Quality Of Life, Vitality, Epigenome and Gene Expression During RecoverY From Sepsis
Terminated NCT03335124 - The Effect of Vitamin C, Thiamine and Hydrocortisone on Clinical Course and Outcome in Patients With Severe Sepsis and Septic Shock Phase 4
Recruiting NCT04005001 - Machine Learning Sepsis Alert Notification Using Clinical Data Phase 2
Completed NCT03258684 - Hydrocortisone, Vitamin C, and Thiamine for the Treatment of Sepsis and Septic Shock N/A
Recruiting NCT05217836 - Iron Metabolism Disorders in Patients With Sepsis or Septic Shock.
Completed NCT05018546 - Safety and Efficacy of Different Irrigation System in Retrograde Intrarenal Surgery N/A
Completed NCT03295825 - Heparin Binding Protein in Early Sepsis Diagnosis N/A
Not yet recruiting NCT06045130 - PUFAs in Preterm Infants
Not yet recruiting NCT05361135 - 18-fluorodeoxyglucose Positron Emission Tomography/Computed Tomography in S. Aureus Bacteraemia N/A
Not yet recruiting NCT05443854 - Impact of Aminoglycosides-based Antibiotics Combination and Protective Isolation on Outcomes in Critically-ill Neutropenic Patients With Sepsis: (Combination-Lock01) Phase 3