Trial Title:
A First-In-Human Trial of pTTL in Advanced Colorectal Cancer
NCT ID:
NCT05908643
Condition:
Colorectal Cancer
Conditions: Official terms:
Colorectal Neoplasms
Conditions: Keywords:
Immunotherapy
Adoptive cell therapy
T cell therapy
Neoantigens
Autologous cell therapy
Study type:
Interventional
Study phase:
Phase 1/Phase 2
Overall status:
Recruiting
Study design:
Allocation:
N/A
Intervention model:
Single Group Assignment
Primary purpose:
Treatment
Masking:
None (Open Label)
Intervention:
Intervention type:
Drug
Intervention name:
pTTL
Description:
pTTL is an autologous cell product for adoptive cancer immunotherapy containing in vitro
expanded T cells stimulated with patient-specific tumour neoantigens derived from
tumour-draining lymph nodes.
Arm group label:
Treatment with pTTL
Other name:
personal tumour-trained lymphocytes
Summary:
This is an open-label, non-randomised FIH trial investigating the safety and tolerability
of a novel ATMP, pTTL, composed of autologous tumour-draining lymph node-derived T cells
stimulated in vitro with personalised cancer neoantigens.
The neoantigens are selected through a process starting with next generation sequencing
(NGS) of tumour material from the patient followed by selection of neoantigenic mutations
using an in-house software, PIOR®. Selected neoantigen epitopes are expressed as
recombinant proteins, NAG, and used to stimulate T cells to promote neoantigen-specific T
cell expansion in vitro in pTTL production.
pTTL is thus based on autologous cells stimulated with patient-specific neoantigens. In
consequence, every pTTL product is unique and designated for use in one single
individual.
pTTL will be administered to patients with stage IV colorectal cancer (CRC) as a single
intravenous dose.
Detailed description:
STUDY RATIONALE The present trial is an open-label, non-randomised FIH trial
investigating the safety and tolerability of pTTL, an immunotherapy consisting of
autologous T cells activated and expanded in vitro using tumour-specific personalised
neoantigens. The scientific rationale for pTTL relies on the fact that somatic mutations
in tumour cells arising during malignant transformation result in altered proteins or
peptides, so called neoantigens. Each individual tumour harbours multiple mutations that
form a unique mutation profile, which enables personalisation of each therapeutic
product. The neoantigens distinguish tumour cells from normal cells and make the tumour
cells targetable by the immune system, and also allows targeting of several targets in
the tumour simultaneously. In the present trial, up to 36 neoantigens will be targeted.
The starting material for pTTL is derived from tumour-draining regional lymph nodes
(RLNs). The choice of this source of T cells is based on several advantages: The exposure
to tumour antigens and, in the case of metastasis, tumour cells causes an enrichment of
tumour- specific T cells. These T cells also have the potential to be superior to
tumour-infiltrating T cells due to less exposure to tumour-mediated immunosuppression.
The production process for pTTL includes in vitro expansion, which increases the
neoantigen-reactive T cell population. The selective T cell expansion is achieved by
stimulation with protein constructs containing neoantigen epitopes, based on sequencing
data from each patient's own tumour. This improves the chance of effective cancer cell
eradication by both increasing the number of cells able to recognise and respond to the
tumour, and by breaking immunological tolerance created in vivo by immunosuppressive
mechanisms through activation in a non-suppressive environment.
PATIENTS The selected target group of the trial is adults with stage IV CRC. Patients may
be considered eligible for inclusion if they have received treatments according to
standard of care or if further standard of care treatment options are judged not to be in
the patients' best interest (e.g. due to toxicity issues). Patients could also be
eligible for inclusion in the trial during a scheduled pause in ongoing palliative
therapy, at the discretion of the treating Investigator. Eligible patients must have a
primary or metastatic lesion that is accessible to biopsy or surgery to obtain tumour
material for NGS analysis. In addition, it is a requirement that the patient can undergo
surgical excision of RLNs for use in pTTL production. Eligible patients should also have
a good performance status (ECOG 0-1) and organ function, and no pre-existing
conditionings deemed to increase their risk for severe side effects of pTTL therapy.
Materials for Part I of the trial can be collected, while non-curative therapeutic
options remain, and cryopreserved for later use if the patient should become eligible for
inclusion in Part II.
METHODOLOGY The trial is composed of 3 parts, referred to as Part I, Part II and Part
III.
Patients will be consented separately for Part I and for Part II/III: a first consent is
given for tissue collection and pTTL production, and a second consent is given for pTTL
treatment, including pre-conditioning chemotherapy and follow-up.
Part I of the trial entails patient identification, recruitment and screening of trial
patients. It also comprises production of pTTL, which is performed in 3 steps:
1. Collection of tumour samples and normal samples for NGS and neoantigen selection.
Production of stimulatory NAG-coupled beads raw material TC0301.
2. Collection of starting material for pTTL manufacturing from RLN.
3. pTTL manufacturing.
The time required from collection of tumour material and RLNs up until pTTL production
and administration to the patient is approximately 8 to 12 weeks. The RLN starting
material is cryopreserved after initial processing, enabling flexibility in the timing of
pTTL administration.
Part II of the trial entails pre-conditioning and supportive care therapy, treatment with
pTTL, and 26 weeks safety follow-up.
Pre-conditioning contains cyclophosphamide and fludarabine, and will be administered
between Day -7 and Day -5 before scheduled pTTL administration. Supportive care treatment
will start on Day -9 or Day -8. pTTL administration will normally be administered on Day
1, with the option of administration on Day -3 if cell expansion kinetics during pTTL
production indicates this would be preferable. Part II will end when the last treated
patient has been followed for 26 weeks or earlier in case of death or patient withdrawal.
Part III of the trial is a long-term follow-up initiated after completion of the initial
26 weeks safety follow-up period. Patients will participate in Part III for up to 4.5
years after end of Part II or until death, whichever comes first.
pTTL DOSAGE AND ADMINISTRATION The drug product (DP), i.e. pTTL, is composed of in vitro
expanded RLN cells, enriched for neoantigen-specific T cells. It is formulated as a cell
suspension with the excipients NaCl (9 mg/mL) and human serum albumin (25 mg/mL) in a
transfusion bag intended for intravenous transfusion. The product is administered fresh.
Each patient will receive a single administration of pTTL.The cell dose obtained during
the manufacturing process will vary depending on the size of the neoantigen-reactive
clones present in the starting material and their proliferative capacity. The minimum
dose of a pTTL unit is 20 million viable cells and the maximum dose is 1 billion viable
cells.
Criteria for eligibility:
Criteria:
Inclusion Criteria:
1. Signed informed consent.
2. Adult (age ≥18 years).
3. Histological or cytological confirmation of CRC.
4. Verified metastatic disease (stage IV classification) and have received all possible
standard of care therapies, OR further standard of care therapies are currently not
considered to be in the patient's best interest, OR toxicity from previous therapy
limits the choice of suitable standard of care therapy OR scheduled pause in
palliative standard of care therapy as judged by the Investigator.
5. Measurable disease according to RECIST1.1.
6. Minimum life expectancy of 6 months at primary inclusion and 3 months at pTTL
administration.
7. Minimum life expectancy of 3 months from the time that the individual pTTL DP is
estimated to be available (as per Investigators clinical assessment). 7. ECOG
performance status 0 to 1
8. Adequate hematopoietic, hepatic and renal function defined as:
1. Haemoglobin≥ 95 g/L (blood transfusion not less than 21 days prior to
screening),
2. Absolute neutrophil count ≥ 1.0x 109/L, platelets ≥100 x 109/L
3. Total bilirubin < 1.5 x ULN (does not apply to patients with Gilberts Syndrome)
4. AST and ALT ≤ 1.5 x ULN (or ≤ 5 x ULN in the presence of liver metastases)
5. Serum creatinine ≤ ULN (if serum creatinine is between 1 and 1.5 x ULN,
patients may be eligible provided that the calculated GFR is at least 35 mL/min
using Cockcroft- Gault method).
6. Albumin ≥24 g/L
9. Patients of childbearing potential or their partners of childbearing potential must
be willing to take the appropriate precaution to avoid pregnancy or fathering a
child for the duration of Part I and Part II and practice an approved, highly
effective method of birth control during treatment and for 6months after receiving
pTTL.
Approved methods of birth control include:
- Combined (oestrogen and progesterone containing) hormonal birth control
associated with inhibition of ovulation: oral, intravaginal, transdermal
- Progesterone-only hormonal birth control associated with inhibition
ofovulation: oral, injectable, implantable
- Intrauterine device (IUD)or intrauterine hormone-releasing system
(IUS)•Bilateral tubal occlusion
- Vasectomised partner
- True sexual abstinence when this is in line with the preferred and
usuallifestyle of the patient. Periodic abstinence (e.g., calendar
ovulation,symptothermal, post-ovulation methods) is not acceptable
10. Able to undergo surgery or biopsy to obtain tumour tissue for neoantigen evaluation
and to retrieve RLNs as starting material for pTTL manufacturing
11. The area from which the RLNs will be obtained shall not have been exposed to
radiotherapy.
Exclusion Criteria:
1. Less than 4 months at primary inclusion and 6 months at pTTL administration since a
clinically significant cardiovascular event such as myocardial infarction, unstable
angina, angioplasty, bypass surgery, stroke or transient ischemic attack (TIA).
Atrial fibrillation if treated and well controlled is not considered a bar to
inclusion even if diagnosed less than 6 months ago.
2. Congestive heart failure New York Heart Association (NYHA)class III or IV.
3. Significantly reduced lung function with clinical implications. If such is
suspected, spirometry should be performed. Spirometry should also be considered in
patients who have been hospitalised due to Covid-19 infection during the last 6
months, and in patients with any other lung affectation judged significant by the
Principal Investigators, in discussion withSponsor's Medical Representative, such as
treatment-related pneumonitis or severe lung infection. Spirometry results of less
than 65% of the expected value regarding forced expiratory volume in 1 second(FEV1)
and/or diffusion capacity (diffusing capacity of the lung for carbon monoxide,
DLCO,corrected for haemoglobinvalue, DLCOco) is regarded as a criterium for
exclusion.
4. Any severe acute or chronic medical condition that places the patient at increased
risk or interferes with the interpretationof trial results (as judged by the
Principal Investigators, in agreement with Sponsor's Medical Representative).
5. Immunodeficiency disorders which may pose a risk for patients treated with pTTL,
and/or affect the outcome of the pTTL treatment, as judged by Investigator at the
Treatment Site and/or the Investigator at the Recruitment and Follow-Up Site
Immunodeficiency disorders are here defined as including inborn and acquired
disorders reducing immunity but excluding human immunodeficiency virus (HIV), which
is discussed below. Examples include common variable immunodeficiency and status
post transplantation of a solid organ or stem cells. Immunodeficiency caused by the
cancer disorder to be treated within the trial or such cancer treatments as have
already been administered is considered a separate entity. This, if severe, might
impact the production of pTTL and potentially also the treatment outcome, and needs
to be carefully assessed as regards patient and pTTL production risks before
inclusion.
6. Autoimmunity disorders which may pose a risk for patients treated with pTTL, and/or
affect the outcome of the pTTL treatment, as judged by Investigator at the Treatment
Site and/or the Investigator at the Recruitment and Follow-Up Site.
7. Leptomeningeal metastases (patient with previously treated brain metastases are
eligible if there is no evidence of disease progression for a minimum of 8 weeks
prior to inclusion
- in these cases a CNS MRI is required within the screening period. These
patients must not have symptoms from their brain metastases or treatment
thereof and must not be taking steroid medications for treatment of CNS
symptoms).
8. Patients are not allowed to have ongoing systemic immunosuppressive concomitant
medications. Systemic immunosuppressive treatments should be completed 2 weeks prior
to surgery and/or 2 weeks prior to dose. Steroid medications are allowed if they are
used as substitution or are administrated topically or as inhalation steroids for
asthma.
9. Previous Grade 3 or greater immune-related toxicity from checkpoint modulation or
other immunotherapy (unless the toxicity has resolved and the patient rechallenged
with the therapy without recurrence of toxicity, in which situation the patient can
be considered).
10. Acute or chronic infection with hepatitis B or C or syphilis.
11. HIV infection.
12. Pregnancy or breast-feeding.
13. Investigator considers the patient unlikely to comply with trial procedures,
restrictions and requirements.
14. For patients required to undergo trial-specific surgery to obtain starting material:
1. Less than 3 identifiable enlarged lymph nodes on pre-surgery radiology
accessible for surgical excision.
2. Previous surgical removal of the primary CRC tumour (would entail a high risk
surgery)
3. Unable to withstand the planned surgery (including ineligibility for general
anaesthesia)
At decision to proceed to pTTL administration:
15. Less than 4 weeks since stopping previous systemic cancer treatment.
16. Less than 2 weeks since stopping radiotherapy.
17. Less than 4 weeks after major surgery and less than 3 weeks after minor surgery.
18. Participation in any other clinical cancer therapy trial, and planned treatment or
treatment with another investigational drug, within the previous 4 weeks.
19. Less than 4 weeks since administration of live attenuated vaccines.
Gender:
All
Minimum age:
18 Years
Maximum age:
N/A
Healthy volunteers:
No
Locations:
Facility:
Name:
Medical Unit Cell therapy and Allogeneic Stem cell Transplantation (ME CAST), and the Center for Clinical Cancer studies - Phase 1 unit, Karolinska University Hospital
Address:
City:
Stockholm
Zip:
17176
Country:
Sweden
Status:
Recruiting
Contact:
Last name:
Maximilian Kordes, MD, PhD
Email:
maximilian.kordes@regionstockholm.se
Contact backup:
Last name:
Mattias Carlsten, MD, PhD
Email:
mattias.carlsten@regionstockholm.se
Facility:
Name:
Unit for Colorectal Surgery, Dept. of Surgery, Västmanlands Sjukhus Västerås
Address:
City:
Västerås
Zip:
723 35
Country:
Sweden
Status:
Recruiting
Contact:
Last name:
Abbas Chabok, MD, PhD
Email:
abbas.chabok@regionvastmanland.se
Contact backup:
Last name:
Maziar Nikberg, MD, PhD
Email:
maziar.nikberg@regionvastmanland.se
Start date:
March 15, 2023
Completion date:
December 2029
Lead sponsor:
Agency:
Neogap Therapeutics AB
Agency class:
Industry
Collaborator:
Agency:
CTC Clinical Trial Consultants AB
Agency class:
Industry
Collaborator:
Agency:
Karolinska University Hospital
Agency class:
Other
Collaborator:
Agency:
Region Västmanland
Agency class:
Other
Collaborator:
Agency:
Vecura
Agency class:
Other
Source:
Neogap Therapeutics AB
Record processing date:
ClinicalTrials.gov processed this data on November 12, 2024
Source: ClinicalTrials.gov page:
https://clinicaltrials.gov/ct2/show/NCT05908643
