Phase 1 N=40 Treatment

LMP-specific T-cells for Patients With Relapsed EBV-positive Lymphoma

Hodgkin Disease · Non Hodgkin Lymphoma · Lymphoepithelioma · Leiomyosarcoma

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View on ClinicalTrials.gov: NCT00062868 ↗

Enrolled (actual)

Serious AEs

18.9%

Results posted

Feb 2020

Primary outcome: Primary: Dose Limiting Toxicity (DLT) Rate by the NCI Common Toxicity Criteria (CTCAE) v2.0 and the Method of Przepiorka et al (Protocol Appendix I) — 0; 0; 0; 0 proportion of participants

Study Design & Population

Study type: Interventional
Phase: Phase 1
Interventions: LMP1/2 CTLs (ALCI - Group A) (Biological); LMP1/2 CTLs (ALCI - Group B) (Biological); LMP1/2 CTLs (ALCI - Group C) (Biological); LMP2 CTLs (ALSCER - Group A) (Biological); LMP2 CTLs (ALSCER - Group B) (Biological); LMP2 CTLs (ALSCER - Group C) (Biological); LMP1/2 CTLs (ALCI - Expansion - Group A) (Biological); LMP1/2 CTLs (ALCI - Expansion Group B) (Biological); LMP1/2 CTLs (ALCI - Expansion Group C) (Biological)
Age: Pediatric, Adult, Older Adult
Sex: All
Sponsor: Baylor College of Medicine
Primary completion: Apr 2014

Outcome Measures

Outcome	Result	p-value
PRIMARY Dose Limiting Toxicity (DLT) Rate by the NCI Common Toxicity Criteria (CTCAE) v2.0 and the Method of Przepiorka et al (Protocol Appendix I)	0; 0; 0; 0; 0; 0	—
SECONDARY Response Rate According to the Harmonization Project (Protocol 8.5.1) or RECIST Criteria.	0.667; 0.833; 0.667; 0.333; 0.667; 0.75	—
SECONDARY Grade III-IV Toxicity Rate in Participants Receiving an Extended Dosage Regimen According to the NCI Common Toxicity Criteria (CTCAE) Version 2.0 and the Method of Przepiorka et. al. (Protocol Appendix I).	0; 0; 0; 0; 0; 0	—

Summary

This protocol is broken up into 2 portions to determine the maximum tolerated dose for treating patients with a type of lymph gland disease. The 1st portion, called ALASCER are for people with a type of lymph gland cancer called Hodgkin or non-Hodgkin Lymphoma or Lymphoepithelioma which has returned or may return or has not gone away after treatment, including the best treatment we know for Lymphoma. While the 2nd portion (ALCI) also includes Lymphoepithelioma, severe chronic active EBV (SCAEBC), and leiomyosarcoma. Some patients with Lymphoma show evidence of infection with the virus that causes infectious mononucleosis Epstein Barr virus (EBV) before or at the time of their diagnosis. EBV is found in the cancer cells of up to half the patients with Hodgkin's and non-Hodgkin Lymphoma, suggesting that it may play a role in causing Lymphoma. The cancer cells (in lymphoma) and some B cells (in SCAEBV) infected by EBV are able to hide from the body's immune system and escape destruction. Investigators want to see if special white blood cells, called T cells, that have been trained to kill EBV infected cells can survive in your blood and affect the tumor. The investigators have used this sort of therapy to treat a different type of cancer that occurs after bone marrow or solid organ transplant called post transplant lymphoma. In this type of cancer the tumor cells have 9 proteins made by EBV on their surface. The investigators grew T cells in the laboratory that recognized all 9 proteins and were able to successfully prevent and treat post transplant lymphoma. However in Hodgkin disease and non-Hodgkin Lymphoma and SCAEBV, the tumor cells and B cells only express 2 EBV proteins. In a previous study we made T cells that recognized all 9 proteins and gave them to patients with Hodgkin disease. Some patients had a partial response to this therapy but no patients had a complete response. Investigators think one reason may be that many of the T cells reacted with proteins that were not on the tumor cells. In this present study we are trying to find out if we can improve this treatment by growing T cells that only recognize one of the proteins expressed on infected EBV Lymphoma cells called LMP-2a, and B cells called LMP1 and LMP2. These special T cells are called LMP specific cytotoxic T-lymphocytes (CTLs). The purpose of the study is to find the largest safe dose of LMP specific cytotoxic T cells, to learn what the side effects are and to see whether this therapy might help patients with Hodgkin disease, non-Hodgkin Lymphoma, Lymphoepithelioma, SCAEBV or leiomyosarcoma.

Eligibility Criteria

ALASCER (Part 1 of Study)

INCLUSION CRITERIA

Any patient, regardless of age or sex, with EBV-positive Lymphoma, or lymphoepithelioma regardless of the histological subtype or EBV (associated)-T/NK-LPD.

In second or subsequent relapse (or first relapse or with active disease if immunosuppressive chemotherapy contraindicated or multiply relapsed patients in remission who have a high risk of relapse) OR any patient with primary disease or in first remission if immunosuppressive chemotherapy is contraindicated, e.g. patients who develop Hodgkin disease after solid organ transplantation or if the Lymphoma is a second malignancy e.g. a Richters transformation of CLL. (Group A) OR In remission or with minimal residual disease status after autologous or syngeneic SCT for Hodgkin's or non-Hodgkin's Lymphoma or lymphoepithelioma. (Group B) OR In remission or with detectable disease after allogeneic SCT. (Group C)

Patients with life expectancy > 6 weeks.
Patients with a Karnofsky/Lansky score of > 50
No severe intercurrent infection.
Donor HIV negative (if autologous product - patient must be HIV negative)
No evidence of GVHD > Grade II at time of enrollment.
If post allogeneic SCT must not have less than 50% donor chimerism in either peripheral blood or bone marrow
Patient, parent/guardian able to give informed consent.
Patients with bilirubin 8.0 (see Section 7.2).
Patients with a creatinine 3x normal. AST >5x normal or abnormal prothrombin time.
Patients with a creatinine >2x normal for age
Donors who are HIV positive (Patients who are HIV positive - if autologous product)
Patients with GVHD Grades III-IV
Due to unknown effects of this therapy on a fetus, pregnant women are excluded from this research. The male partner should use a condom.

Note: Patients who would be excluded from the protocol strictly for laboratory abnormalities can be included at the investigator's discretion after approval by the CCGT Protocol Review Committee and the FDA reviewer.

ALCI and ALCI Expansion (Part 2 of Study)

INCLUSION CRITERIA

Any patient, regardless of age or sex, with EBV-positive Hodgkin's or non-Hodgkin's Lymphoma, or lymphoepithelioma or leiomyosarcoma regardless of the histological subtype or EBV (associated)-T/NK-lymphoproliferative disease or Severe Chronic EBV#

(#SCAEBV is defined as patients with high EBV viral load in plasma or PBMC (>4000 genomes per ug PBMC DNA) and/or biopsy tissue positive for EBV)

a - In second or subsequent relapse (or first relapse or with active disease if immunosuppressive chemotherapy contraindicated or multiply relapsed patients currently in remission who have a high risk of relapse) OR with primary disease or in first or subsequent remission if immunosuppressive chemotherapy is contraindicated, e.g. patients who develop Hodgkin disease after solid organ transplantation or if the Lymphoma is a second malignancy e.g. a Richters transformation of CLL.(Group A)

b - In remission or with minimal residual disease status after autologous or syngeneic SCT for Hodgkin's or non-Hodgkin's Lymphoma/Lymphoepithelioma/SCAEBV. (Group B)

c - Patients in remission or with detectable disease after allogeneic SCT. (Group C)

Patients with life expectancy 6 weeks or greater.
Tumor tissue EBV positive
Patients with a Karnofsky/Lansky score of 50 or greater
Donor HIV negative (if autologous product - patient must be HIV negative)
If post allogeneic SCT must not have less than 50% donor chimerism in either peripheral blood or bone marrow
Patients with bilirubin 3x normal or less, AST 5x normal or less, and Hgb greater than 8.0
Patients with a creatinine 2x normal or less for age
Patients should have been off other investigational therapy for one month prior to entry in this study.
Patient, parent/guardian able to give informed consent.

EXCLUSION CRITERIA

Patients with a severe intercurrent infection.
Donors who are HIV positive or Pa

View full record on ClinicalTrials.gov →

Data sourced from ClinicalTrials.gov (NCT00062868). Outcome figures and adverse-event rates are extracted automatically from the registry's posted results and are provided for clinician reference, not as a substitute for the primary publication.