CRISPR/Cas9-modified Human T Cell ( PD-1and ACE2 Knockout Engineered T Cells ) for Inducing Long-term Immunity in COVID-19 Patients
NCT ID: NCT04990557
Last Updated: 2021-08-16
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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UNKNOWN
PHASE1/PHASE2
16 participants
INTERVENTIONAL
2021-08-31
2022-11-30
Brief Summary
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Detailed Description
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Conditions
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Study Design
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NON_RANDOMIZED
PARALLEL
TREATMENT
NONE
Study Groups
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A - Two cycles
Peripheral blood lymphocytes will be collected and Programmed cell death protein 1(PDCD1) and ACE2 gene will be knocked out by CRISPR Cas9 in the laboratory (PD-1/ACE2 Knockout T cells). The lymphocytes will be selected and expanded ex vivo and infused back into patients.
A total of 1 x 10\^7/kg PD-1and ACE2 Knockout T cells will be infused in one cycle. Each cycle is divided into three administrations, with 20% infused in the first administration, 30% in the second, and the remaining 50% in the third. Patients will receive a total of two cycles of treatment.
PD-1 and ACE2 Knockout T Cells
Autologous lymphocytes are collected and both PDCD1 and ACE2 gene knocked out in the laboratory. Cells are selected and expanded ex vivo. Cells are infused back to the patients for treatment
B- Two cycles
Peripheral blood lymphocytes will be collected and Programmed cell death protein 1(PDCD1) and ACE2 gene will be knocked out by CRISPR Cas9 in the laboratory (PD-1/ACE2 Knockout T cells). The lymphocytes will be selected and expanded ex vivo and infused back into patients.
A total of 1 x 10\^7/kg PD-1 and ACE2 Knockout T cells will be infused in one cycle. Each cycle is divided into three administrations, with 20% infused in the first administration, 30% in the second, and the remaining 50% in the third. Patients will receive a total of two cycles of treatment.
A total of 2 x 10\^7/kg PD-1and ACE2 Knockout T cells will be infused in one cycle. Each cycle is divided into three administrations, with 20% infused in the first administration, 30% in the second, and the remaining 50% in the third. Patients will receive a total of two cycles of treatment.
PD-1 and ACE2 Knockout T Cells
Autologous lymphocytes are collected and both PDCD1 and ACE2 gene knocked out in the laboratory. Cells are selected and expanded ex vivo. Cells are infused back to the patients for treatment
C- Two cycles
Peripheral blood lymphocytes will be collected and Programmed cell death protein 1(PDCD1) and ACE2 gene will be knocked out by CRISPR Cas9 in the laboratory (PD-1/ACE2 Knockout T cells). The lymphocytes will be selected and expanded ex vivo and infused back into patients.
A total of 4 x 10\^7/kg PD-1 and ACE2 Knockout T cells will be infused in one cycle. Each cycle is divided into three administrations, with 20% infused in the first administration, 30% in the second, and the remaining 50% in the third. Patients will receive a total of two cycles of treatment.
PD-1 and ACE2 Knockout T Cells
Autologous lymphocytes are collected and both PDCD1 and ACE2 gene knocked out in the laboratory. Cells are selected and expanded ex vivo. Cells are infused back to the patients for treatment
Interventions
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PD-1 and ACE2 Knockout T Cells
Autologous lymphocytes are collected and both PDCD1 and ACE2 gene knocked out in the laboratory. Cells are selected and expanded ex vivo. Cells are infused back to the patients for treatment
PD-1 and ACE2 Knockout T Cells
Autologous lymphocytes are collected and both PDCD1 and ACE2 gene knocked out in the laboratory. Cells are selected and expanded ex vivo. Cells are infused back to the patients for treatment
PD-1 and ACE2 Knockout T Cells
Autologous lymphocytes are collected and both PDCD1 and ACE2 gene knocked out in the laboratory. Cells are selected and expanded ex vivo. Cells are infused back to the patients for treatment
Eligibility Criteria
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Inclusion Criteria
* Major organs function normally.
* Women at pregnant ages should be under contraception..
* Willing and able to provide informed consent
Exclusion Criteria
* History of mandatory custody because of psychosis or other psychological disease inappropriate for treatment deemed by treating physician.
* With other immune diseases, or chronic use of immunosuppressants or steroids.
* Compliance cannot be expected.
* Other conditions requiring exclusion deemed by physician
18 Years
70 Years
ALL
No
Sponsors
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Mahmoud Ramadan mohamed Elkazzaz
OTHER
Responsible Party
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Mahmoud Ramadan mohamed Elkazzaz
Clinical Researcher
Principal Investigators
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Mahmoud R Elkazzaz, M.Sc of Biochemistry
Role: PRINCIPAL_INVESTIGATOR
Faculty of science Damietta university
Central Contacts
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Other Identifiers
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Novel Treatment for Covid-19
Identifier Type: -
Identifier Source: org_study_id
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