Gene Therapy in Treating Patients With Human Immunodeficiency Virus-Related Lymphoma Receiving Stem Cell Transplant
NCT ID: NCT02797470
Last Updated: 2025-04-20
Study Results
Results available
Outcome measurements, participant flow, baseline characteristics, and adverse events have been published for this study.
View full resultsBasic Information
Get a concise snapshot of the trial, including recruitment status, study phase, enrollment targets, and key timeline milestones.
Recruitment Status
ACTIVE_NOT_RECRUITING
Clinical Phase
PHASE1/PHASE2
Total Enrollment
11 participants
Study Classification
INTERVENTIONAL
Study Start Date
2016-06-23
Study Completion Date
2036-03-31
Brief Summary
Review the sponsor-provided synopsis that highlights what the study is about and why it is being conducted.
This phase I/II trial studies the side effects and best dose of gene therapy in treating patients with human immunodeficiency virus (HIV)-related lymphoma that did not respond to therapy or came back after an original response receiving stem cell transplant. In gene therapy, small stretches of deoxyribonucleic acid (DNA) called "anti-HIV genes" are introduced into the stem cells in the laboratory to make the gene therapy product used in this study. The type of anti-HIV genes and therapy in this study may make the patient's immune cells more resistant to HIV-1 and prevent new immune cells from getting infected with HIV-1.
Related Clinical Trials
Explore similar clinical trials based on study characteristics and research focus.
Gene Therapy After Frontline Chemotherapy in Treating Patients With AIDS-Related Non-Hodgkin Lymphoma
NCT01961063
AIDS-related Non-Hodgkin Lymphoma
AIDS-related Plasmablastic Lymphoma
AIDS-related Primary Effusion Lymphoma
+1 more
ACTIVE_NOT_RECRUITING
PHASE1
Twins Study of Gene Therapy for HIV Infection
NCT00001535
Acquired Immunodeficiency Syndrome
HIV Infection
Kaposi's Sarcoma
COMPLETED
PHASE1
Immune Response After Stem Cell Transplant in HIV-Positive Patients With Hematologic Cancer
NCT00968630
Hematopoietic and Lymphoid Cell Neoplasm
HIV Infection
COMPLETED
PHASE2
Safety, Tolerability and Immunogenicity Study of Different Vaccine Regimens of Trivalent Ad26.Mos.HIV or Tetravalent Ad26.Mos4.HIV Along With Clade C Glycoprotein (gp)140 in Healthy Human Immunodeficiency Virus (HIV)-Uninfected Adults
NCT02788045
Healthy
COMPLETED
PHASE1/PHASE2
A Multicenter, Double-Blind, Phase III, Adjuvant-Controlled Study of the Effect of 10 Units of HIV-1 Immunogen (Remune) Compared to Incomplete Freund's Adjuvant (IFA) Alone Every 12 Weeks on AIDS-Free Survival in Subjects With HIV Infection and CD4 T-Lymphocytes Between 300 and 549 Cells/microL Rega
NCT00002359
HIV Infections
COMPLETED
PHASE3
Detailed Description
Dive into the extended narrative that explains the scientific background, objectives, and procedures in greater depth.
PRIMARY OBJECTIVE:
I. Safety, defined as timely engraftment (the collective establishment of a persistent absolute neutrophil count of at least 500 cells/mm\^3 and platelet count of 20,000 cells/mm\^3 without transfusion for 3 consecutive measurements of laboratory values obtained on different days) by one month post-transplant, in the absence of any grade 3 and 4 non-hematopoietic organ toxicity that can be attributed (possibly, probably, or definitely) to lentiviral transduced stem cell transplant, excluding alopecia, or any clonal expansion and excluding expected toxicities that are associated with the pre-transplant conditioning regimen.
SECONDARY OBJECTIVES:
I. To determine efficacy of the candidate product, defined as establishment of \> 5% mononuclear blood cells expressing anti-HIV genes in the peripheral blood at 3 months post-transplant.
II. To determine the presence, quantity, and duration of gene modified HIV-1 resistant peripheral blood cells and gut mucosal immune cells.
III. To study the integration sites of vector sequences in circulating cells. IV. To study progression-free survival. V. To study overall survival. VI. To study complete response rate and duration. VII. To study partial response rate and duration. VIII. To study time to neutrophil engraftment (first measurement of 3 consecutive laboratory values on different days) of absolute neutrophil count \[ANC\] \>= 500 cells/mm\^3).
IX. To study time to platelet engraftment (first measurement of 3 consecutive measurements laboratory values obtained on different days) of platelets \>= 20,000 cells/mm\^3 without platelet transfusions 7 days prior).
X. To study hematologic function at day 100 (ANC \> 1500, hemoglobin \[Hb\] \> 10 g/dl without transfusion and platelets \> 100,000) XI. To study CD4 recovery at the conclusion of the trial. XII. To study safety in terms of toxicities, infections, transfusions, and infusion-related reactions.
XIII. To study HIV-1 viral load over time. XIV. To study persistence of vector-transduced cells over time.
EXPLORATORY OBJECTIVE:
I. To evaluate the presence and the magnitude of expansion of HIV-1 resistant immune cells in the peripheral blood and gut mucosa of transplanted participants, subsequent to withholding anti-retroviral therapy (ART).
OUTLINE: This is a dose-escalation study of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells.
Patients receive BEAM or BEAM-R regimen administered as standard of care comprising carmustine on day -6, cytarabine twice daily (BID) on days -5 to -2, etoposide BID on days -5 to -2, and melphalan on day -1. Patients with B-cell lymphoma also receive rituximab on day -6 before chemotherapy and on days 21 and 28 post-transplant as standard of care. Patients undergo intravenous (IV) infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells over 1 hour.
After completion of study treatment, patients are followed up at days 7, 14, 21, 28, 42, 60, 90, 120, 180, 240, 300, 360, 420, 480, 520, 600, 660, and 720, and then yearly for at least 15 years.
I. Safety, defined as timely engraftment (the collective establishment of a persistent absolute neutrophil count of at least 500 cells/mm\^3 and platelet count of 20,000 cells/mm\^3 without transfusion for 3 consecutive measurements of laboratory values obtained on different days) by one month post-transplant, in the absence of any grade 3 and 4 non-hematopoietic organ toxicity that can be attributed (possibly, probably, or definitely) to lentiviral transduced stem cell transplant, excluding alopecia, or any clonal expansion and excluding expected toxicities that are associated with the pre-transplant conditioning regimen.
SECONDARY OBJECTIVES:
I. To determine efficacy of the candidate product, defined as establishment of \> 5% mononuclear blood cells expressing anti-HIV genes in the peripheral blood at 3 months post-transplant.
II. To determine the presence, quantity, and duration of gene modified HIV-1 resistant peripheral blood cells and gut mucosal immune cells.
III. To study the integration sites of vector sequences in circulating cells. IV. To study progression-free survival. V. To study overall survival. VI. To study complete response rate and duration. VII. To study partial response rate and duration. VIII. To study time to neutrophil engraftment (first measurement of 3 consecutive laboratory values on different days) of absolute neutrophil count \[ANC\] \>= 500 cells/mm\^3).
IX. To study time to platelet engraftment (first measurement of 3 consecutive measurements laboratory values obtained on different days) of platelets \>= 20,000 cells/mm\^3 without platelet transfusions 7 days prior).
X. To study hematologic function at day 100 (ANC \> 1500, hemoglobin \[Hb\] \> 10 g/dl without transfusion and platelets \> 100,000) XI. To study CD4 recovery at the conclusion of the trial. XII. To study safety in terms of toxicities, infections, transfusions, and infusion-related reactions.
XIII. To study HIV-1 viral load over time. XIV. To study persistence of vector-transduced cells over time.
EXPLORATORY OBJECTIVE:
I. To evaluate the presence and the magnitude of expansion of HIV-1 resistant immune cells in the peripheral blood and gut mucosa of transplanted participants, subsequent to withholding anti-retroviral therapy (ART).
OUTLINE: This is a dose-escalation study of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells.
Patients receive BEAM or BEAM-R regimen administered as standard of care comprising carmustine on day -6, cytarabine twice daily (BID) on days -5 to -2, etoposide BID on days -5 to -2, and melphalan on day -1. Patients with B-cell lymphoma also receive rituximab on day -6 before chemotherapy and on days 21 and 28 post-transplant as standard of care. Patients undergo intravenous (IV) infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells over 1 hour.
After completion of study treatment, patients are followed up at days 7, 14, 21, 28, 42, 60, 90, 120, 180, 240, 300, 360, 420, 480, 520, 600, 660, and 720, and then yearly for at least 15 years.
Conditions
See the medical conditions and disease areas that this research is targeting or investigating.
HIV Infection
Mature T-Cell and NK-Cell Non-Hodgkin Lymphoma
Plasmablastic Lymphoma
Recurrent Adult Hodgkin Lymphoma
Recurrent Adult Non-Hodgkin Lymphoma
Recurrent Burkitt Lymphoma
Recurrent Follicular Lymphoma
Stage III Follicular Lymphoma
Stage III Mantle Cell Lymphoma
Stage IV Follicular Lymphoma
Stage IV Mantle Cell Lymphoma
Study Design
Understand how the trial is structured, including allocation methods, masking strategies, primary purpose, and other design elements.
Allocation Method
NA
Intervention Model
SINGLE_GROUP
Primary Study Purpose
TREATMENT
Blinding Strategy
NONE
Study Groups
Review each arm or cohort in the study, along with the interventions and objectives associated with them.
Treatment (anti-HIV gene transduced CD34+ cells)
Patients receive BEAM regimen administered as standard of care comprising carmustine on day -6, cytarabine BID on days -5 to -2, etoposide BID on days -5 to -2, and melphalan on day -1. Patients undergo infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells over 1 hour.
Group Type
EXPERIMENTAL
Autologous Hematopoietic Stem Cell Transplantation
Intervention Type
PROCEDURE
Undergo infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells
Carmustine
Intervention Type
DRUG
300 mg/m2 on Day -6, as part of BEAM and R-BEAM regimens.
Cytarabine
Intervention Type
DRUG
100 mg/m2 BID on Days -5 through -2, as part of BEAM and R-BEAM regimens.
Etoposide
Intervention Type
DRUG
VP-16: 100 mg/m2 BID on Days -5 through -2, as part of BEAM and R-BEAM regimens.
Laboratory Biomarker Analysis
Intervention Type
OTHER
Correlative studies
Lentivirus Vector CCR5 shRNA/TRIM5alpha/TAR Decoy-transduced Autologous CD34-positive Hematopoietic Progenitor Cells
Intervention Type
BIOLOGICAL
Undergo infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells
Melphalan
Intervention Type
DRUG
140 mg/m2 on Day -1, as part of BEAM and R-BEAM regimens.
Peripheral Blood Stem Cell Transplantation
Intervention Type
PROCEDURE
Undergo infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells
Interventions
Learn about the drugs, procedures, or behavioral strategies being tested and how they are applied within this trial.
Autologous Hematopoietic Stem Cell Transplantation
Undergo infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells
Intervention Type
PROCEDURE
Carmustine
300 mg/m2 on Day -6, as part of BEAM and R-BEAM regimens.
Intervention Type
DRUG
Cytarabine
100 mg/m2 BID on Days -5 through -2, as part of BEAM and R-BEAM regimens.
Intervention Type
DRUG
Etoposide
VP-16: 100 mg/m2 BID on Days -5 through -2, as part of BEAM and R-BEAM regimens.
Intervention Type
DRUG
Laboratory Biomarker Analysis
Correlative studies
Intervention Type
OTHER
Lentivirus Vector CCR5 shRNA/TRIM5alpha/TAR Decoy-transduced Autologous CD34-positive Hematopoietic Progenitor Cells
Undergo infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells
Intervention Type
BIOLOGICAL
Melphalan
140 mg/m2 on Day -1, as part of BEAM and R-BEAM regimens.
Intervention Type
DRUG
Peripheral Blood Stem Cell Transplantation
Undergo infusion of lentivirus vector CCR5 shRNA/TRIM5alpha/TAR decoy-transduced autologous CD34-positive hematopoietic progenitor cells
Intervention Type
PROCEDURE
Other Intervention Names
Discover alternative or legacy names that may be used to describe the listed interventions across different sources.
Autologous Stem Cell Transplantation
BCNU
Becenum
Becenun
BiCNU
Bis(chloroethyl) Nitrosourea
Bis-Chloronitrosourea
Carmubris
Carmustin
Carmustinum
FDA 0345
Gliadel
N,N'-Bis(2-chloroethyl)-N-nitrosourea
Nitrourean
Nitrumon
SK 27702
SRI 1720
WR-139021
.beta.-Cytosine arabinoside
1-.beta.-D-Arabinofuranosyl-4-amino-2(1H)pyrimidinone
1-.beta.-D-Arabinofuranosylcytosine
1-Beta-D-arabinofuranosyl-4-amino-2(1H)pyrimidinone
1-Beta-D-arabinofuranosylcytosine
1.beta.-D-Arabinofuranosylcytosine
2(1H)-Pyrimidinone, 4-Amino-1-beta-D-arabinofuranosyl-
2(1H)-Pyrimidinone, 4-amino-1.beta.-D-arabinofuranosyl-
Alexan
Ara-C
ARA-cell
Arabine
Arabinofuranosylcytosine
Arabinosylcytosine
Aracytidine
Aracytin
Aracytine
Beta-Cytosine Arabinoside
CHX-3311
Cytarabinum
Cytarbel
Cytosar
Cytosar-U
Cytosine Arabinoside
Cytosine-.beta.-arabinoside
Cytosine-beta-arabinoside
Erpalfa
Starasid
Tarabine PFS
U 19920
U-19920
Udicil
WR-28453
Demethyl Epipodophyllotoxin Ethylidine Glucoside
EPEG
Lastet
Toposar
Vepesid
VP 16-213
VP-16
VP-16-213
Lentivirus Vector CCR5 shRNA/TRIM5alpha/TAR Decoy-transduced Autologous CD34-positive HPCs
Alanine Nitrogen Mustard
CB-3025
L-PAM
L-Phenylalanine Mustard
L-Sarcolysin
L-Sarcolysin Phenylalanine mustard
L-Sarcolysine
Melphalanum
Phenylalanine Mustard
Phenylalanine Nitrogen Mustard
Sarcoclorin
Sarkolysin
WR-19813
PBPC transplantation
Peripheral Blood Progenitor Cell Transplantation
Peripheral Stem Cell Support
Peripheral Stem Cell Transplantation
Eligibility Criteria
Check the participation requirements, including inclusion and exclusion rules, age limits, and whether healthy volunteers are accepted.
Inclusion Criteria
* Biopsy-proven intermediate or high-grade non-Hodgkin's lymphoma, meeting one of the following criteria (timeline 8 months prior to enrollment in the screening segment):
\- In partial remission,
\- Relapsed after initial complete remission,
\- Failed induction therapy, but responds to salvage therapy (i.e., chemosensitive disease),
\- In complete remission with high-risk features as specified by the International Prognostic Index.
* Biopsy-proven advanced stage follicular lymphoma, that have failed at least two lines of therapy multi-agent chemotherapy, but responds to salvage therapy i.e.,chemosensitive disease) (timeline 8 months prior to enrollment in the screening segment).
* Biopsy-proven advanced stage Mantle cell lymphoma with Ki-67 \> 10% in first complete remission (timeline 8 months prior to enrollment in the screening segment).
* Biopsy-proven Hodgkin's lymphoma, meeting one of the following criteria (timeline 8 months prior to enrollment).
\- In first, or greater relapse after initial complete remission,
\- In partial remission,
\- Failed induction therapy, but responds to salvage therapy (i.e., chemosensitive disease).
* Biopsy-proven Burkitt's lymphoma, meeting one of the following criteria (timeline 8 months prior to enrollment):
\- In second complete remission after relapse following initial complete remission,
\- Failed induction therapy, but responds (very good partial remission, complete remission, or near complete remission) to salvage therapy (i.e., chemosensitive disease).
* Biopsy proven plasmablastic lymphomas, or peripheral T cell lymphoma (with the exception of ALK+ type in first or second complete remission) \*NOTE: Patients meeting the following criteria are exempt from the 8-month timeline and do not require additional biopsy:
* Patients who have never achieved a complete remission on the last biopsy-proven site of disease and went on to the next therapy then achieved a complete remission.
* Patients who relapsed quickly (within 3 months of their last chemotherapy) and now have achieved a complete remission with salvage therapy.
* HIV-1 infection, as documented by any federally approved, licensed HIV rapid test performed in conjunction with screening (or ELISA, test kit, and confirmed by Western blot or other approved test). Alternatively, this documentation may include a record demonstrating that another physician has documented the participant's HIV status based on either: 1) approved diagnostic tests, or 2) the referring physician's written record that HIV infection was documented, with supporting information on the participant's relevant medical history and/or current management of HIV infection.
* Must be on a multi-drug anti-HIV regimen (excluding zidovudine \[AZT, ZDV, Retrovir®, or agents containing zidovudine (e.g., Combivir® and Trizivir®)\], and efavirenz \[Sustiva®, or agents containing efavirenz (e.g., Atripla®)\]).
Participants on zidovudine \[AZT, ZDV, Retrovir®; including Combivir® and Trizivir®\] and efavirenz \[Sustiva®; including Atripla®\] must switch to an alternative regimen without anticipated drug-drug interactions or myelosuppressive properties based on known viral resistance patterns and/or ART history, such as raltegravir and Truvada (emtricitabine and tenofovir) at least two weeks prior to the transplant.
o Participant taking ARTs must satisfy one of the following:
* Undetectable HIV viral load (\< 50 copies/mL). For patients who have had negative viral loads in the past 6 months and no known HIV viral load \>500 copies/mL within the last 6 months, minor fluctuations of viral load (isolated escalations up to 500 copies/mL) are acceptable. The participant's history of negative viral loads may be documented with recent laboratory results and/or a record from the participant's HIV care provider.
* If viral load is detectable at \< 2000 copies/mL a review of previous antiretroviral regimens or previous genotypic or phenotypic testing which indicate the ability to fully suppress virus by addition of sensitive drugs must be performed. This review will be carried out by the protocol ID team or the ID specialist caring for the patient.
* If viral load is detectable at ≥ 2000 copies/mL, a current HIV genotype and/or phenotype must be obtained. If a HAART regimen to which the patient's virus is sensitive can be determined based on genotype and previous antiretroviral experience, then the patient will be considered eligible in this regard. This review will be carried out by the protocol ID team or the ID specialist caring for the patient.
* Karnofsky performance status of 70-100%. ECOG performance status \<2
* SGOT and SGPT ≤ 2.5 times upper limit of normal (ULN). Serum bilirubin ≤ 2.5 times ULN except for participants who are on atazanavir or indinavir, or with elevated indirect bilirubin related to bilirubin conjugation issues such as Gilbert's disease, provided that the participant's direct bilirubin is within normal institutional limits.
* Participants who are hepatitis C virus antibody positive, or hepatitis B virus surface antigen positive must be free of clinical evidence of cirrhosis as determined by the principal investigator in consultation with the institutional Gastroenterology Service.
* Participants with Hepatitis B should be on appropriate anti-viral therapy at the time of the transplant, and their viral load should be negative.
* Serum creatinine ≤ 2 times ULN.
* Creatinine clearance ≥ 60 mL/min by the modified Cockcroft-Gault Formula.
* PT/PTT ≤ 2 times upper limit of normal (ULN), or international normalized ratio (INR)/PTT ≤ 2 times the ULN.
* FEV-1 or DLCO (corrected for hemoglobin) ≥ 50% predicted.
* LVEF ≥ 50% by 2D ECHO or MUGA scan.
* Not pregnant or nursing, with negative serum pregnancy test. Pregnant women are excluded from this study because the conditioning regimen has the potential for teratogenic or abortifacient effects. Because there is an unknown but potential risk for adverse events in nursing infants secondary to treatment of the mother with BEAM, breastfeeding should be discontinued. These potential risks may also apply to other agents used in this study.
* Participants should agree to practice effective contraceptive precautions and to use at least one method of contraception for the duration of the study and for 3 months post-transplant.
* Age ≥18 years. Because only adult transplant centers are participating as study sites.
* Life expectancy of greater than 3 months.
* Ability to understand and the willingness to sign a written informed consent document.
* Receipt of a stable ART regimen for at least 3 weeks prior to enrollment.
\- In partial remission,
\- Relapsed after initial complete remission,
\- Failed induction therapy, but responds to salvage therapy (i.e., chemosensitive disease),
\- In complete remission with high-risk features as specified by the International Prognostic Index.
* Biopsy-proven advanced stage follicular lymphoma, that have failed at least two lines of therapy multi-agent chemotherapy, but responds to salvage therapy i.e.,chemosensitive disease) (timeline 8 months prior to enrollment in the screening segment).
* Biopsy-proven advanced stage Mantle cell lymphoma with Ki-67 \> 10% in first complete remission (timeline 8 months prior to enrollment in the screening segment).
* Biopsy-proven Hodgkin's lymphoma, meeting one of the following criteria (timeline 8 months prior to enrollment).
\- In first, or greater relapse after initial complete remission,
\- In partial remission,
\- Failed induction therapy, but responds to salvage therapy (i.e., chemosensitive disease).
* Biopsy-proven Burkitt's lymphoma, meeting one of the following criteria (timeline 8 months prior to enrollment):
\- In second complete remission after relapse following initial complete remission,
\- Failed induction therapy, but responds (very good partial remission, complete remission, or near complete remission) to salvage therapy (i.e., chemosensitive disease).
* Biopsy proven plasmablastic lymphomas, or peripheral T cell lymphoma (with the exception of ALK+ type in first or second complete remission) \*NOTE: Patients meeting the following criteria are exempt from the 8-month timeline and do not require additional biopsy:
* Patients who have never achieved a complete remission on the last biopsy-proven site of disease and went on to the next therapy then achieved a complete remission.
* Patients who relapsed quickly (within 3 months of their last chemotherapy) and now have achieved a complete remission with salvage therapy.
* HIV-1 infection, as documented by any federally approved, licensed HIV rapid test performed in conjunction with screening (or ELISA, test kit, and confirmed by Western blot or other approved test). Alternatively, this documentation may include a record demonstrating that another physician has documented the participant's HIV status based on either: 1) approved diagnostic tests, or 2) the referring physician's written record that HIV infection was documented, with supporting information on the participant's relevant medical history and/or current management of HIV infection.
* Must be on a multi-drug anti-HIV regimen (excluding zidovudine \[AZT, ZDV, Retrovir®, or agents containing zidovudine (e.g., Combivir® and Trizivir®)\], and efavirenz \[Sustiva®, or agents containing efavirenz (e.g., Atripla®)\]).
Participants on zidovudine \[AZT, ZDV, Retrovir®; including Combivir® and Trizivir®\] and efavirenz \[Sustiva®; including Atripla®\] must switch to an alternative regimen without anticipated drug-drug interactions or myelosuppressive properties based on known viral resistance patterns and/or ART history, such as raltegravir and Truvada (emtricitabine and tenofovir) at least two weeks prior to the transplant.
o Participant taking ARTs must satisfy one of the following:
* Undetectable HIV viral load (\< 50 copies/mL). For patients who have had negative viral loads in the past 6 months and no known HIV viral load \>500 copies/mL within the last 6 months, minor fluctuations of viral load (isolated escalations up to 500 copies/mL) are acceptable. The participant's history of negative viral loads may be documented with recent laboratory results and/or a record from the participant's HIV care provider.
* If viral load is detectable at \< 2000 copies/mL a review of previous antiretroviral regimens or previous genotypic or phenotypic testing which indicate the ability to fully suppress virus by addition of sensitive drugs must be performed. This review will be carried out by the protocol ID team or the ID specialist caring for the patient.
* If viral load is detectable at ≥ 2000 copies/mL, a current HIV genotype and/or phenotype must be obtained. If a HAART regimen to which the patient's virus is sensitive can be determined based on genotype and previous antiretroviral experience, then the patient will be considered eligible in this regard. This review will be carried out by the protocol ID team or the ID specialist caring for the patient.
* Karnofsky performance status of 70-100%. ECOG performance status \<2
* SGOT and SGPT ≤ 2.5 times upper limit of normal (ULN). Serum bilirubin ≤ 2.5 times ULN except for participants who are on atazanavir or indinavir, or with elevated indirect bilirubin related to bilirubin conjugation issues such as Gilbert's disease, provided that the participant's direct bilirubin is within normal institutional limits.
* Participants who are hepatitis C virus antibody positive, or hepatitis B virus surface antigen positive must be free of clinical evidence of cirrhosis as determined by the principal investigator in consultation with the institutional Gastroenterology Service.
* Participants with Hepatitis B should be on appropriate anti-viral therapy at the time of the transplant, and their viral load should be negative.
* Serum creatinine ≤ 2 times ULN.
* Creatinine clearance ≥ 60 mL/min by the modified Cockcroft-Gault Formula.
* PT/PTT ≤ 2 times upper limit of normal (ULN), or international normalized ratio (INR)/PTT ≤ 2 times the ULN.
* FEV-1 or DLCO (corrected for hemoglobin) ≥ 50% predicted.
* LVEF ≥ 50% by 2D ECHO or MUGA scan.
* Not pregnant or nursing, with negative serum pregnancy test. Pregnant women are excluded from this study because the conditioning regimen has the potential for teratogenic or abortifacient effects. Because there is an unknown but potential risk for adverse events in nursing infants secondary to treatment of the mother with BEAM, breastfeeding should be discontinued. These potential risks may also apply to other agents used in this study.
* Participants should agree to practice effective contraceptive precautions and to use at least one method of contraception for the duration of the study and for 3 months post-transplant.
* Age ≥18 years. Because only adult transplant centers are participating as study sites.
* Life expectancy of greater than 3 months.
* Ability to understand and the willingness to sign a written informed consent document.
* Receipt of a stable ART regimen for at least 3 weeks prior to enrollment.
Exclusion Criteria
* Participants with \> 5% involvement of bone marrow by malignant cells (either by manual count or flow cytometry) prior to stem cell collection.
* Participants with any abnormal cytogenetics in the bone marrow not related to the lymphoma, and not deemed to be constitutional.
* Participants with unexplained anemia and/or thrombocytopenia.
* Participants with clear evidence of myeloproliferative disorders, or myelodysplastic disorders in the marrow.
* Presence of any active CNS disease at the time of evaluation (parenchymal or leptomeningeal).
* Any history of HIV-1 associated encephalopathy.
* Participants with persistently low CD4 counts less than 200 and a history of any AIDS-defining infection in the last 6 months before screening are excluded from the study.
* Symptomatic/active bacterial, or fungal, or any other opportunistic infection.
* Active CMV retinitis, or other active CMV-related organ dysfunction.
* Relapse of pneumocystis carinii pneumonia within the past year before enrollment.
* Intractable, severe diarrhea, defined as \> 1.500 cc diarrheal fluid per day, or diarrhea causing persistent severe electrolyte abnormalities, or hypoalbuminemia.
* History of active myocardial ischemia, cardiomyopathy, uncontrolled dysrhythmia, or congestive heart failure within the last 6 months before enrollment.
* Dementia of any kind.
* Seizures within the past 12 months before enrollment.
* History of Grade III hemorrhagic cystitis due to prior cyclophosphamide chemotherapy.
* History of other prior malignancy, except squamous cell carcinoma of the cervix or anus, superficial basal cell or squamous cell skin cancer, or other malignancy curatively treated more than 5 years ago before enrollment.
* Active psychosocial condition that would hinder study compliance and follow-up.
* Any perceived inability to directly (and without the means of a legal guardian) provide informed consent.
* Any medical or physical contraindication, or other inability to undergo HPC collection.
* Participants who are receiving any other investigational agents.
* Uncontrolled intercurrent illness including, but not limited to, ongoing or active infection, symptomatic congestive heart failure, unstable angina pectoris, cardiac arrhythmia, or psychiatric illness/social situations that would limit compliance with study requirements.
* Participants with any abnormal cytogenetics in the bone marrow not related to the lymphoma, and not deemed to be constitutional.
* Participants with unexplained anemia and/or thrombocytopenia.
* Participants with clear evidence of myeloproliferative disorders, or myelodysplastic disorders in the marrow.
* Presence of any active CNS disease at the time of evaluation (parenchymal or leptomeningeal).
* Any history of HIV-1 associated encephalopathy.
* Participants with persistently low CD4 counts less than 200 and a history of any AIDS-defining infection in the last 6 months before screening are excluded from the study.
* Symptomatic/active bacterial, or fungal, or any other opportunistic infection.
* Active CMV retinitis, or other active CMV-related organ dysfunction.
* Relapse of pneumocystis carinii pneumonia within the past year before enrollment.
* Intractable, severe diarrhea, defined as \> 1.500 cc diarrheal fluid per day, or diarrhea causing persistent severe electrolyte abnormalities, or hypoalbuminemia.
* History of active myocardial ischemia, cardiomyopathy, uncontrolled dysrhythmia, or congestive heart failure within the last 6 months before enrollment.
* Dementia of any kind.
* Seizures within the past 12 months before enrollment.
* History of Grade III hemorrhagic cystitis due to prior cyclophosphamide chemotherapy.
* History of other prior malignancy, except squamous cell carcinoma of the cervix or anus, superficial basal cell or squamous cell skin cancer, or other malignancy curatively treated more than 5 years ago before enrollment.
* Active psychosocial condition that would hinder study compliance and follow-up.
* Any perceived inability to directly (and without the means of a legal guardian) provide informed consent.
* Any medical or physical contraindication, or other inability to undergo HPC collection.
* Participants who are receiving any other investigational agents.
* Uncontrolled intercurrent illness including, but not limited to, ongoing or active infection, symptomatic congestive heart failure, unstable angina pectoris, cardiac arrhythmia, or psychiatric illness/social situations that would limit compliance with study requirements.
Minimum Eligible Age
18 Years
Eligible Sex
ALL
Accepts Healthy Volunteers
No
Sponsors
Meet the organizations funding or collaborating on the study and learn about their roles.
National Cancer Institute (NCI)
NIH
Sponsor Role
collaborator
California Institute for Regenerative Medicine (CIRM)
OTHER
Sponsor Role
collaborator
AIDS Malignancy Consortium
NETWORK
Sponsor Role
lead
Responsible Party
Identify the individual or organization who holds primary responsibility for the study information submitted to regulators.
Responsibility Role
SPONSOR
Principal Investigators
Learn about the lead researchers overseeing the trial and their institutional affiliations.
Mehrdad Abedi
Role: PRINCIPAL_INVESTIGATOR
AIDS Malignancy Consortium
Locations
Explore where the study is taking place and check the recruitment status at each participating site.
UC San Diego Moores Cancer Center
La Jolla, California, United States
Site Status
University of California Davis Comprehensive Cancer Center
Sacramento, California, United States
Site Status
UCSF Medical Center-Parnassus
San Francisco, California, United States
Site Status
Memorial Sloan Kettering Cancer Center
New York, New York, United States
Site Status
Countries
Review the countries where the study has at least one active or historical site.
United States
Provided Documents
Download supplemental materials such as informed consent forms, study protocols, or participant manuals.
Document Type: Study Protocol and Statistical Analysis Plan
Document Type: Informed Consent Form
Other Identifiers
Review additional registry numbers or institutional identifiers associated with this trial.
NCI-2015-01745
Identifier Type: REGISTRY
Identifier Source: secondary_id
9933
Identifier Type: OTHER
Identifier Source: secondary_id
AMC 097
Identifier Type: OTHER
Identifier Source: secondary_id
097
Identifier Type: OTHER
Identifier Source: secondary_id
AMC-097
Identifier Type: OTHER
Identifier Source: secondary_id
AMC-097
Identifier Type: -
Identifier Source: org_study_id
More Related Trials
Additional clinical trials that may be relevant based on similarity analysis.
CAR-T Cells for HIV Infection
NCT04648046
RECRUITING
PHASE1/PHASE2
Evaluation of Specific Infection-Fighting Cells For Prediction of Immune Response to Anti-HIV and Immune-Boosting Medication
NCT00006578
WITHDRAWN
NA
Phase I Study to Evaluate the Safety and Immunogenicity of HIV-1 Immunogen in Children With HIV-1 Infection
NCT00001445
COMPLETED
PHASE1
Evaluating the Safety, Tolerability, and Pharmacokinetics of Monoclonal Antibodies in Healthy Participants
NCT05959707
SUSPENDED
PHASE1
A Clinical Trial of PGDM1400 and PGT121 and VRC07-523LS Monoclonal Antibodies in HIV-infected and HIV-uninfected Adults
NCT03205917
COMPLETED
PHASE1
An Efficacy and Safety Study of Autologous Cluster of Differentiation 34 (CD34+) Hematopoietic Progenitor Cells Transduced With Placebo or an Anti- Human Immunodeficiency Virus Type 1 (HIV-1) Ribozyme (OZ1) in Participants With HIV-1 Infection
NCT00074997
COMPLETED
PHASE2
Safety, PK and Antiviral Activity of PGT121 Monoclonal Antibody in HIV-uninfected and HIV-infected Adults
NCT02960581
COMPLETED
PHASE1
Evaluating the Safety, Tolerability, and Pharmacokinetics of an Investigational, Injectable HIV Medicine (GSK1265744) in HIV-Uninfected Adults
NCT02178800
COMPLETED
PHASE2
Safety and Efficacy of T Cell Genetic Immunotherapy for HIV
NCT00131560
UNKNOWN
PHASE2
Safety of Transplantation of CRISPR CCR5 Modified CD34+ Cells in HIV-infected Subjects With Hematological Malignances
NCT03164135
UNKNOWN
NA
A Clinical Trial to Evaluate the Safety and Immunogenicity of BG505 MD39.3, BG505 MD39.3 gp151, and BG505 MD39.3 gp151 CD4KO HIV Trimer mRNA Vaccines in Healthy, HIV-uninfected Adult Participants
NCT05217641
ACTIVE_NOT_RECRUITING
PHASE1
Effectiveness of Giving an HIV Vaccine (Remune) to HIV-Positive Patients Receiving an Anti-HIV Drug Combination
NCT00005758
COMPLETED
PHASE3
Study to Evaluate the Safety of a Gene and Cell Therapy Product in Participants With HIV That is Well-Controlled on Antiretroviral Therapy
NCT04561258
COMPLETED
PHASE1
Safety and Immunotherapeutic Activity of an Anti-PD-1 Antibody (Cemiplimab) in Participants With HIV-1 on Suppressive cART
NCT03787095
TERMINATED
PHASE1/PHASE2
Safety and Effectiveness of Treating HIV-Positive Patients With an HIV Vaccine (Remune)
NCT00005001
COMPLETED
PHASE2
Phase 1 Dose Escalation Study of Autologous T-cells Genetically Modified at the CCR5 Gene by Zinc Finger Nucleases in HIV-Infected Patients
NCT01044654
COMPLETED
PHASE1
A Clinical Trial in Healthy, HIV-1-Uninfected Adult Participants to Compare the Safety, Tolerability and Immunogenicity of CH505TF gp120 Produced From Stably Transfected Cells to CH505TF gp120 Produced From Transiently Transfected Cells
NCT03856996
COMPLETED
PHASE1
Dose-Response Study of Ibalizumab (Monoclonal Antibody) Plus Optimized Background Regimen in Patients With HIV-1
NCT00784147
COMPLETED
PHASE2
Safety, Tolerability and Immunogenicity Study of 2 Dose Levels of Trimeric Glycoprotein140 (gp140) in Healthy Adult Volunteers
NCT02304185
COMPLETED
PHASE1
A Clinical Trial to Evaluate the Safety and Immunogenicity of CH505M5 N197D mRNA-gp160 Followed by CH505 TF mRNA-gp160 in Adults in Overall Good Health Without HIV
NCT06557785
ACTIVE_NOT_RECRUITING
PHASE1
GW873140 to Treat HIV-1 Infected Adults
NCT00076284
COMPLETED
PHASE2
Lymphocyte Infusions for the Treatment of HIV-Infected Patients Failing Anti-HIV Therapy
NCT00559416
TERMINATED
PHASE1