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NAcGM3/VSSP-aids-patients drug resistant to antiretroviral treatment-Phase I-II
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27 Enero 2017 - 4:38pm
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2 Agosto 2023 - 10:10am
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2014-10-27
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2014-10-27
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Date of first enrollment
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2015-01-28
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2015-01-28
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2017
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2023
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Next update date
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2018
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2024
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08
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02
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Source(s) of monetary or material support
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Center of Molecular Immunology (CIM)
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Center of Molecular Immunology (CIM)Tropical Medicine Institute Pedro Kouri (PK)
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Tropical Medicine Institute Pedro Kouri (PK)
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Revisión de 2 Agosto 2023 - 10:10am
NAcGM3/VSSP-aids-patients drug resistant to antiretroviral treatment-Phase I-II
General information
Section to complete general information about the trial: scientific and public title, protocol identifiers, sponsors and Source(s) of Monetary or Material Support.
Acronym of Public Title:
NacGM3/VSSP AIDS Phase I/II
Scientific title:
Evaluation of safety and effect of four doses level of NAcGM3/VSSP formulation as immunopotentiator by subcutaneous route in the treatment of aids patients drug resistant to antiretroviral treatment.
Acronym of Scientific Title:
Not applicable
Secondary indentifying numbers:
IICRD-EC-155
Issuing authority of the secondary identifying numbers:
Center of Molecular Immunology
Primary sponsor:
Center of Molecular Immunology (CIM)
Secondary sponsor:
Not applicable
Source(s) of monetary or material support:
Center of Molecular Immunology (CIM)Tropical Medicine Institute Pedro Kouri (PK)
Authorization for beginning
Section to complete information about the regulatory approval of clinical trial: regulatory agency name, approval date and reference number in the agency.
Regulatory instance to authorize the initiation of the study:
Center for State Control of Drugs, Medical Devices and Equipment (CECMED)
Authorization date :
27/10/2014
Reference number:
05-009-14BC
Principal investigator
Section to complete information about Email address, telephone number and postal address of the Principal Investigator.
First name:
Vianka
Last name:
Calas Hechavarria
Medical Specialty :
Second Degree in Internal Medicine
Affiliation:
Tropical Medicine Institute Pedro Kouri (IPK)
Postal address:
Autopista Novia del Mediodía km 6½ entre Autopista Nacional y Carretera Central
City:
Havana
País:
Cuba
Zip Code:
17100
Telephone:
+53-72553451
+53-72553236
Email address:
vianka@ipk.sld.cu
Clinical sites to participate
Section to complete the data related to the clinical sites involved in the trial: site and responsible investigator for every site.
Countries of recruitment:
Cuba
Clinical sites:
Not applicable
Research ethics committees:
Tropical Medicine Institute “Pedro Kouri”, March 18th, 2014
Recruitment status
Section to complete information about the recruitment status and the date of first enrolment subject
Recruitment status:
Complete
Date of first enrollment:
28/01/2015
Health condition and Intervention
Section to complete information about the primary medical condition(s) or problem(s) studied and, a characteristics of the intervention(s).
Health condition(s) or Problem(s) studied:
Acquired immunodeficiency syndrome (AIDS)
Health condition(s) code:
Acquired Immunodeficiency Syndrome
HIV Infections
Immunologic Deficiency Syndromes
Lentivirus Infections
Retroviridae Infections
RNA Virus Infections
Sexually Transmitted Diseases
Sexually Transmitted Diseases, Viral
Slow Virus Diseases
Immune System Diseases
Intervention(s):
Interventions in Phase I Four Doses Level Group I (experimental): NAcGM3/VSSP vaccine (dose 150 µg) will be administered by subcutaneous route. The first 5 doses will be administered each 14 days (± 7 days of tolerance), the next 10 doses will be administered each 28 days (± 15 days of tolerance), to complete a year of treatment. Group II (experimental): NAcGM3/VSSP vaccine (dose 300 µg) will be administered by subcutaneous route. The first 5 doses will be administered each 14 days (± 7 days of tolerance), the next 10 doses will be administered each 28 days (± 15 days of tolerance), to complete a year of treatment. Group III (experimental): NAcGM3/VSSP vaccine (doses 600 µg) will be administered by subcutaneous route. The first 5 doses will be administered each 14 days (± 7 days of tolerance), the next 10 doses will be administered each 28 days (± 15 days of tolerance), to complete a year of treatment. Group IV (experimental): NAcGM3/VSSP vaccine (doses 900 µg) will be administered by subcutaneous route. The first 5 doses will be administered each 14 days (± 7 days of tolerance), the next 10 doses will be administered each 28 days (± 15 days of tolerance), to complete a year of treatment. Patients who presented favorable response to the treatment, after 15 administration, will can continuous with the same administration of formulation every 28 days (± 15 days of tolerance, always remain with the performance status during the follow of protocol another year and after that under clinical consideration. Interventions in Phase II Group I ( study) : Depending on the selected dose Phase I is administered subcutaneously , the first 5 doses at intervals of 14 days ( ± 7 days tolerance), the following 10 doses at intervals of 28 days ( ± 15 days tolerance ) to complete one year of treatment . Group II (control) : Placebo to be received by the same route following the same frequency and duration of the study group After all patients receive the 15 administrations of the formulation or placebo, blinding opens for each patient individually. Patients in the study group to submit favorable response to treatment may also continue administrations at intervals of 28 days (tolerance +/- 15 days) during the follow-up protocol for another year and then to medical judgment.
Intervention code:
N-Acetylneuraminic Acid
G(M3) Ganglioside
Adjuvants, Immunologic
Gangliosides
Proteolipids
Vaccines
Injections, Subcutaneous
Placebos
Intervention keyword:
NAcGM3/VSSP
Outcomes and Timepoint
Section to complete information about primary and secondary outcomes including. It includes the metric or method of measurement used and, the time point for every outcome.
Primary outcome(s):
Phase I Optimal therapeutic dose (Level of dose in that they yield minor patients' number with new opportunistic diseases or deaths to the 12 months, once a minor toxicity was associated (adverse serious event, related to the formulation). Measuring time: 168, 336 days. Phase II Clinical response (Appearance of opportunistic bigger diseases or death in the period of treatment. The opportunistic diseases will be evaluated using the criteria of the Control Disease Center for AIDS patients of the United States). Measuring time: 168, 336 days. Adverse serious events related to with the formulation (The adverse events will be evaluated using the World Health Organization toxicity criteria). Measuring time: 168, 336 days.
Key secondary outcomes:
Immunopotenciator Effect (It will evaluate based on the decrease or no increase in CD4 levels in the course of treatment). Measuring time: 168, 336 days. Virologic response (It will evaluate based on no increase in viral load in at least one decimal log or decrease it, in the course of treatment). Measuring time: 168, 336 days. Immunologic response (Values of CD3, CD4, CD8, NK, CD4CD25FoxP3. The result will be collected by those units in the institution). Measuring time: 168, 336 days. Quality of life (It will evaluate through the Spanish version of the MOS-HIV (for its acronym in English Medical Outcomes Study -Human Immunodeficiency Virus), validated in the Cuban population by IPK. It is a questionnaire of Quality of life for aids Cuban patients). Measuring time: 0, 168, 336 days. Safety. Toxicity (Occurrence of any EA, description, duration, intensity, severity, outcome, attitude towards treatment and causation). This outcome will measure every 28 days. - Occurrence of any AE (Yes, No) - Description AE (name of the event) - Duration of AE (Difference between the start and end dates of the adverse event) - AE Intensity (It is classified according to the nomenclature and intensity criteria to assess the severity of adverse events in AIDS patients adult and pediatric version 1.0, December 2004; with clarification of August 2009. It includes the following categories: mild, moderate, severe, EA potentially life-threatening or EA that produces death. - Causality relationship (1. Final, 2. Very Likely, 3. Probable, 4.Possible. 5. Not related, 6.Unknown) - Seriousness / Gravity (Serious, Not serious. Are severe/serious adverse events those that 1. Produce death, 2. Threaten life, 3. Require / prolonged hospitalization, 4. Produce disability / persistent or significant disability or 5. Produce birth defect or congenital anomaly) Results of laboratory tests. Measuring time: every 28 days. Hematopoietic Laboratory (Hb (g/L), Leukocyte (109 cells/L), Granulocyte (109 cells/L), Platelets (109 cells/L). Measuring time: every 28 days. Liver Laboratotry (Bilirubin (µmol/L), ALAT (U/L), ASAT (U/L), Alkaline Phosphatase (U/L), LDH (U/L)). Measuring time: every 28 days. Renal Laboratory (Serum Creatinine (µmol/L)). Measuring time: every 28 days.
Selection criterias
Section to complete information about the inclusion and exclusion criteria for participant selection, including age and gender.
Gender:
Male/Female
Minimum age:
18 years
Maximum age:
50 years
Inclusion criteria:
1. Patients who have signed informed consent. 2. AIDS patients with antiretroviral treatment and evidence of multidrug resistance or with CD4 counts below 200 cells / uL for more than 2 consecutive assessments in the last 6 months with controlled viral load (not detectable or with values below the range 1 000 copies). 3. Patients aged between 18 and 50 years (including both). 4. Patients with overall according to WHO between 0 and 1. 5. Patients who have functioning of organs and bone marrow as defined by the following parameters (a) Hematopoietic: Hb>=100 g / L, Leukocytes>= 3 x 109 cells / L, granulocytes>= 1 x 109 cells / L, Platelets >= 150 x 109 cells / L; b) Liver (No more than five times the upper limit of normal (ULN) *), Bilirubin: 17 pmol / L (LSN *), ALAT: 40 U / L (LSN *) ASAT: 40 U / L (LSN *), Alkaline Phosphatase: 279 U / L *, LDH within normal levels: 214 U / L (LSN); c) Renal: Serum creatinine<= 132 pmol / L) 6. Life expectancy of 6 months or more.
Exclusion criteria:
1. Patients who have previously received the investigational product . 2. Patients receiving other investigational product . 3. Patients with known hypersensitivity to any component of the formulation. 4. pregnant or lactating patients 5. Patients of childbearing age who are not using an appropriate method of contraception ( intrauterine devices, hormonal contraceptives , barrier methods or tubal ligation) . If male (vasectomy , condom use ) during treatment . 6. Patients with acute allergic conditions or history of severe allergic reactions. 7. Patients suffering from uncontrolled intercurrent illness including, but not limited to : active infections , symptomatic congestive heart failure, unstable angina , cardiac arrhythmia and psychiatric diseases involving the incompetence of the subject. 8. Patients with other malignant disease treated correctly in the previous 5 years , except in situ cancer. 9. Virus infection Hepatitis B or C. 10. Opportunistic at the time of inclusion in the study infection
Type of population:
Adults
Type of participant:
Patients
Study design
Section to complete information about the characteristics of the study design.
Type study:
Interventional
Purpose:
Treatment
Allocation:
Randomized controlled trial
Masking:
Double Blind
Control group:
Placebo
Study design:
Parallel
Phase:
1-2
Target sample size:
25
Contact for public queries
Section to complete information about Email address, telephone number and postal address of the contact who will respond to general queries, including information about current recruitment status
First Name:
Vianka
Last Name:
Calas Hechevarria
Specialty:
Second Degree Specialist in Internal Medicine
Affiliation:
Tropical Medicine Institute Pedro Kouri (IPK)
Postal Address:
Autopista Novia del Mediodia km 6½ entre Autopista Nacional y Carretera Central
City:
Havana
País:
Cuba
Zip Code:
17100
Telephone:
+537 255 3451
Email :
vianka@ipk.sld.cu
Contact for scientific queries
Section to complete information about Email address, telephone number and postal address of the contact who will respond to scientific queries.
First Name:
Adriana
Last Name:
Carr Perez
Specialty:
Biochemist. PhD in Health Sciences Biochemist
Affiliation:
Center of Molecular Immunology (CIM)
Postal Address:
216 y 15 , Atabey; Playa
City:
Havana
País:
Cuba
Zip Code:
11300
Telephone:
+53 7 214 3168
Email :
adriana@cim.sld.cu
Registration and Update
Section to complete information about the name of Primary Registry, date of registration and the unique ID number assigned by the registry (RPCEC).
Primary registry:
RPCEC
Unique ID number:
RPCEC00000213
Date of Registration in Primary Registry:
22/04/2016
Record Verification Date:
2023/08/02
Next update date:
2024/08/02
Link to the spanish version:
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