Trial Title:
tTF-NGR Randomized Study - STS
NCT ID:
NCT05597917
Condition:
Soft Tissue Sarcoma
Conditions: Official terms:
Sarcoma
Trabectedin
Conditions: Keywords:
tTF-NGR
vascular targeting
CD13
aminopeptidase N
Trabectedin
Study type:
Interventional
Study phase:
Phase 3
Overall status:
Recruiting
Study design:
Allocation:
Randomized
Intervention model:
Parallel Assignment
Primary purpose:
Treatment
Masking:
None (Open Label)
Intervention:
Intervention type:
Drug
Intervention name:
Trabectedin
Description:
Patients will receive standard trabectedin 1.5 mg/m2 as a 24-hour central intravenous
(IV) infusion on day 1, q d 22 x until disease progression or contraindications against
further application.
Arm group label:
Arm 1: Standard chemotherapy with trabectidin (in-label)
Arm group label:
Arm 2: tTF-NGR added to standard trabectedin
Other name:
Yondelis
Intervention type:
Biological
Intervention name:
tTF-NGR
Description:
Patients will receive standard trabectedin according to arm 1 plus the safe dose
according to safety run-in part of tTF-NGR (1-hour ratecontrolled infusion, port central
venous access, 0.9 % NaCl ad 100 mL) per day for 4 or lower number of consecutive days
following each trabectedin cycle (within 1 hour interval between end of trabectedin
infusion and tTF-NGR: e.g.: trabectedin on monday 8 am to tuesday 8 am followed by
tTF-NGR on tuesday 9 am and on the following days, q d 22 x until disease progression or
contraindications against further application.
Arm group label:
Arm 2: tTF-NGR added to standard trabectedin
Summary:
In this phase III open label, controlled clinical trial patients with unresectable or
metastatic soft-tissue sarcoma after failure of anthracycline-containing first line
therapy or with contraindications to these drugs and CD13 positivity in central histology
(grade >/= 1+) are treated to evaluate whether tTF-NGR in combination with standard
trabectedin chemotherapy prolongs progression-free survival (according to iRECIST), as
compared with trabectedin alone. Further objectives are to evaluate the efficacy of
tTF-NGR in combination with standard trabectedin chemotherapy with respect to the
response rate and overall survival as well as to assess the safety profile of tTF-NGR
combined with trabectedin. Before the randomized phase III part of the study, there will
be a safety run-in part. The final dose of tTF-NGR established as safe in this safety
run-in part will be used for the randomized (parallel 1:1; Arm 1: standard trabectedin,
Arm 2: standard trabectedin plus tTF-NGR) phase III part of this trail.
Detailed description:
Rationale: tTF-NGR targets CD13 present in tumor-associated vasculature and on tumor
cells of the majority of STS tissue samples examined; preclinical data on combination of
tTF-NGR with anthracyclines and trabectedin; low competition of targeted or immune
therapy in soft tissue sarcoma (STS)
Investigational Medicinal Product: Patients will receive a dose of the Investigational
Medicinal Product (IMP) tTF-NGR determined to be safe within the safety run-in cohort of
the study as 1-hour rate-controlled infusion (port central venous access, 0.9 % NaCl ad
100 mL) per day for 4 or lower number of consecutive days following each trabectedin
cycle (within 1 hour interval between end of trabectedin infusion and tTF-NGR: e.g.:
trabectedin on monday 8 am to tuesday 8 am followed by tTF-NGR on tuesday latest 9 am and
on the following days, q d 22 x until disease progression or contraindications against
further application.
Indication: Unresectable or metastatic STS after failure of anthracycline-containing
first line treatment or with contraindications to these drugs; CD13 positivity in central
histology (grade >/= 1+)
Primary objective and endpoints: The primary objective of the trial is to evaluate
whether tTF-NGR in combination with standard trabectedin chemotherapy given for
unresectable or metastatic soft tissue sarcoma after failure of anthracycline-containing
first line therapy or with contraindications to these drugs prolongs progression-free
survival, as compared with trabectedin alone. The following efficacy endpoint (for the
randomized phase III part) will be considered:
- Progression-free survival (PFS) according to iRECIST (Seymour L, Lancet Oncol. 2017)
as judged by central radiology in a blinded fashion after end of trial.
Secondary objectives and endpoints: The secondary objective of the trial is to evaluate
the efficacy of tTF-NGR in combination with standard trabectedin chemotherapy given for
unresectable or metastatic STS after failure of anthracycline-containing first line
therapy or with contraindications to these drugs with respect to the response rate and
overall survival as well as to assess the safety profile of tTF-NGR combined with
trabectedin.
To assess the efficacy, the following measurements will be considered:
- Overall response rate (ORR, consisting of CR and PR)
- Disease control rate (DCR, consisting of CR, PR, and stable disease (SD) for >18
weeks)
- Median progression-free survival (mPFS)
- Median overall survival (mOS)
- Overall survival (OS) rate at 12 and 18 months
To assess the safety profile of tTF-NGR combined with trabectedin (for the phase II and
the phase III parts), the following safety endpoints will be considered:
- Adverse Events (AEs) assessment based on CTCAE v.5.0.
- Standard laboratory parameters and pharmacokinetics
- Physical examination findings including assessment of vital signs
- Patient reported outcomes (PRO)
Study design: Open label, randomized, controlled study in subjects with metastatic or
refractory soft tissue sarcoma. Approx. 150 patients will be screened, 126 evaluable
patients are enrolled and parallel assigned in a 1:1 fashion to one of two different
arms, as outlined below. Randomization will be stratified into CD13+ grades 1 and 2
versus CD13+ grade 3 and number of chemotherapy regimen before entry on trial: 1 versus
>1.
Safety run-in part:
Before the randomized phase III part of the study, there will be a safety cohort of a
minimum of 6 patients obtaining at least 2 cycles each of the combination outlined in arm
2 (see below) to confirm safety of this combination (1.5 mg/m2 trabectedin plus a
starting dose of 3 mg/m2 tTF-NGR). The patients will be treated in-house and in sequence.
In case of dose-limiting toxicity (DLT) in one patient of this cohort, a dosemodification
protocol for tTF-NGR to 2 mg/m2 is planned, and in case of further tolerability problems
in one patient further deescalations in 0.5 mg/m2 steps of tTF-NGR and/or by a reduction
of application days are planned. The safe dose is then transferred to the randomized
phase III part of the study. The final dose and the final number of application days of
tTF-NGR in this combination has to be applied to 6 patients with 2 cycles each without
DLT to be established as safe. The randomized part of the study will be opened after
judgement of the safety in the safety cohort by the DSMB, Ethics Committee and National
Competenent Authority (PEI).
Randaomzied Phase III part:
ARM 1:
Trabectedin 1.5 mg/m2 as a 24-hour central intravenous (IV) infusion on day 1, q d 22 x
until disease progression or contraindications against further application.
ARM 2:
Patients will receive standard trabectedin according to arm 1 plus the safe dose
according to safety run-in part of tTF-NGR (1-hour ratecontrolled infusion, port central
venous access, 0.9 % NaCl ad 100 mL) per day for 4 or lower number of consecutive days
following each trabectedin cycle (within 1 hour interval between end of trabectedin
infusion and tTF-NGR: e.g.: trabectedin on monday 8 am to tuesday 8 am followed by
tTF-NGR on tuesday 9 am and on the following days, q d 22 x until disease progression or
contraindications against further application.
As the evaluation of the study results is based on an intention-to-treat analysis, all
patients after randomization will be part of the efficacy population as evaluated by
central iRECIST evaluation after end of study.
Therapy in both arms can be given on an out-patient basis. All patients receive best
supportive care (BSC) according to institutional guidelines. Anti-cancer activity
(iRECIST modification) will be assessed (clinically and imaging) at week 9 and then every
9 weeks (adjusted to cycle length of 3 weeks) until confirmed progression by iRECIST
(iCPD). Decision on application of next cycle at week 9 will be clinical. Imaging and
clinical based decision will follow. Transfer of pseudonymized imaging pictures (CD, DVD)
and imaging results of a patient to the study center has to be performed after each
imaging time point.
Safety assessment will be performed on an ongoing basis during study participation,
including standard laboratory assessments. The incidence of AEs will be summarized by
severity in all patients with at least one study drug intake
Number of sites, countries and patients: Multicenter, up to 11 active study sites in
Germany. At least 6 patients are treated in the phase II safety part, 126 patients will
be randomized in a 1:1 ratio to receive open label Trabectedin (Arm 1) or Trabectedin
plus tTF-NGR (Arm 2) in the phase III part.
Target population: Patients (18-75 years) with advanced or metastatic soft-tissue sarcoma
after failure of anthracycline-containing first line therapy or with contraindications to
these drugs.
ARM 1: Standard chemotherapy with Trabectidin (in-label)
ARM 2: Test product tTF-NGR added to standard Trabectedin
Severity grading: Hematological and chemical laboratory tests, and AEs will be graded
based on CTCAE v. 5.0.
Duration of Treatment: Patients will be treated in repeated cycles until definite disease
progression (iRECIST; Seymour L, Lancet Oncol. 2017) in the absence of other withdrawal
criteria, and as long as neither patient nor investigator requests treatment
discontinuation.
Tumor assessments: Detailed tumor assessment visits (clinical and laboratory
examinations) after start of therapy are performed before treatment start, at week 9 (+/-
1 week), followed by every 9 weeks (+/- 1 week, independent from cycle length of 3 weeks)
thereafter. Post-study treatment (treatment with another anti-cancer agent) is according
to investigator´s choice, but is recorded in the eCRF. At iCPD (confirmed at next tumor
assessment after iUPD) tumor assessments will end, but time of death will be recorded for
estimation of OS. In case EOT is not determined by iCPD, tumor assessments will go on
after EOT until iCPD. Survival status will be collected also for patients withdrawn from
the study until death. Transfer of pseudonymized imaging pictures (CD, DVD) and imaging
results of a patient to the study center has to be performed after each imaging time
point.
Statistical analysis: Safety data of the safety run-in part of the study will be
evaluated using descriptive statistical methods.
In the primary statistical analysis of the randomized phase III part, the primary
endpoint progression-free survival (PFS) according to iRECIST as judged by central
blinded radiology will be compared between the two randomized treatment groups (Arm 1
versus Arm 2). The primary statistical analysis will include all randomized patients
(full analysis set) and will be performed according to the intention-to-treat principle.
A stratified log-rank test with stratification according to the randomization will be
applied (two-sided significance level 5%, power 80%) that provides confirmatory
statistical evidence.
The timing of the study will be event-driven. The primary statistical analysis will be
performed at the time when 106 events in terms of PFS have been observed in total across
both treatment groups. This required number of events results from the following sample
size calculation. Based on the observed PFS in previous trials, PFS is expected to be
exponential, and the expected median PFS is 4.6 months in the control arm (Arm 1) and 8
months in the experimental arm (Arm 2). The corresponding expected hazard ratio is
HR=0.575. In a 36 months enrolment period with a rate of 3-4 patients per month, 126
patients will be recruited and randomized. The drop-out process after randomization is
expected to be exponential with an up to 25% cumulative drop-out rate at month 24
(competing with the survival process). Follow-up after the last randomized patient is
planned to be 12 months, after which it is expected that the required number of 106
events in terms of PFS will have occurred.
The statistical analysis of pre-specified secondary endpoints will be performed with
descriptive and inferential statistical methods. Prespecified subgroup analyses will be
performed with respect to stratification, L-sarcoma vs. others, FNCLCC grade (2 vs. 3),
and ECOG performance status (ECOG PS 0 vs. PS 1). Further exploratory analyses will be
performed for other relevant treatment variables (e.g. sex, age, number of treatment
cycles).
Safety data will be evaluated and summarized descriptively.
Withdrawal and patient replacement criteria: The patient can withdraw consent for
participation in the study at any time without disadvantages for further treatment or
prejudice by the therapeutic team. The investigator can withdraw a patient if, in his or
her clinical judgment, it is in the best interest of the patient or if the patient cannot
comply with the protocol.
Criteria for eligibility:
Criteria:
Inclusion Criteria:
1. Patients of all genders (female, male, diverse), with no restriction regarding
ethnic or religious background age 18 - 75 years.
2. Patients with advanced or metastatic soft-tissue sarcoma after failure of
anthracycline-containing first line therapy (or anthracycline-containing adjuvant
therapy within 12 months before entry on study) or with contraindications to these
drugs
3. Patients must have histological evidence of high-grade advanced unresectable or
metastatic soft tissue sarcoma (grade 2 - 3) according to the FNCLCC grading system.
The following tumor types are included:
- Dedifferentiated liposarcoma
- Myxoid liposarcoma (high grade)
- Pleomorphic liposarcoma
- Adult fibrosarcoma
- Myxofibrosarcoma (high-grade)
- Leiomyosarcoma
- Rhabdomyosarcoma (alveolar, pleomorphic)
- Angiosarcoma
- Synovial sarcoma
- Undifferentiated sarcoma
Tumor types not listed above may be included upon communication with Coordinating
Investigator.
The following tumor types will not be included:
- Gastrointestinal stromal tumors (GIST)
- Epitheloid sarcoma
- Alveolar soft part sarcoma
- Desmoplastic small round cell tumor
- Chondrosarcoma
- Osteosarcoma
- Ewing sarcoma (including CIC-rearranged sarcoma and Sarcoma with BCOR
alterations)
4. CD13 positivity with a score of ≥ 1 (20) by central pathology (GDI Münster)
5. Patients must have at least one unidimensionally measurable lesion by computed
tomography as defined by RECIST criteria 1.1. This lesion should not have been
irradiated during previous treatments
6. Life expectancy of at least 3 months
7. Eastern Cooperative Oncology Group (ECOG) Performance Status ≤ 2
8. No contraindications for trabectedin (see attachment)
9. Negative serum pregnancy test for females of childbearing potential* within 14 days
of starting treatment
10. Informed consent signed and dated to participate in the study
11. Willingness and ability to comply with the scheduled visits, treatment plan,
laboratory tests and other study procedures
- Women of childbearing potential (WOCBP) must be using, from the screening to 3
months following the last trabectedin (Arm 1) or the last last study drug (Arm
2) administration, highly effective contraception methods, as defined by the
"Recommendations for contraception and pregnancy testing in clinical trials"
issued by the Head of Medicine Agencies' Clinical Trial Facilitation Group
(www.hma.eu/ctfg.html) and which include, for instance, progesteron-only or
combined (estrogen- and progesteron-containing) hormonal contraception
associated with inhibition of ovulation, intrauterine devices, intrauterine
hormone-releasing systems, bilateral tubal occlusion, vasectomized partner or
sexual abstinence. Pregnancy test will be repeated monthly. For men
contraception methods should be performed for 5 months after the last
application of trabectedin (Arm1) or study drug (Arm 2).Women of childbearing
potential are defined as females who have experienced menarche, are not
postmenopausal (12 months with no menses without an alternative medical cause)
and are not permanently sterilized (e.g., tubal occlusion, hysterectomy,
bilateral oophorectomy or bilateral salpingectomy)
Exclusion Criteria:
1. curative therapy available
2. clinically significant unrelated illness, which in the judgement of the
investigators could compromise the patient's ability to tolerate the IMP or be
likely to interfere with the study procedures or results
3. immobilized tumor patients (wheel chair etc.) with increased risk for DVT
4. known hypersensitivity reactions to prior application of E. coli-derived material
5. history of coronary heart disease, stroke, transitent ischemic attacks, pulmonary
embolism, or deep vein thrombosis. For reason of mechanism of action of tTF-NGR,
exclusion of patients with a history of any of the vascular conditions mentioned is
important. Clinical suspicion of coronary heart disease must be further checked e.g.
by cardiac MRI or myocardial scintigraphy to exclude coronary heart disease.
6. known hereditary syndromes with elevated thromboembolic risk (FV Leiden and
prothrombin mutations (G20210A), hereditary antithrombin, protein C and S
deficiency, and antiphospholipid syndrome) after one or more clinical thromboembolic
events
7. patients with hereditary vascular disorders (such as Klippel-Trenauny-Weber
syndrome) with increased thromboembolic risk.
8. patients with a Khorana score of (Khorana AA, et al. J.Clin. Oncol. 2009, 27,
4839-4847, attached to this protocol) of > 3
9. elevated Troponin T hs (> 50 ng/L) before entry on study
10. presence of active central nervous system (CNS) disease and/or CNS vascular
abnormalities detected by MRI
11. no adequate bone marrow function, absolute neutrophil count (ANC) < 1.0 x 109/L,
platelets < 50 x 109/L (for trabectedin actually < 100 x 109/L - to be decided by
the investigator on an individual patient basis) and haemoglobin (Hb) < 8.0 g/dl.
12. chronically impaired renal function or creatinine ≥ 2.0 x upper limit of normal
(ULN).
13. inadequate liver function (alanine aminotranserase (ALT), aspartate aminotranserase
(AST), alkaline phosphatase (ALP) or total bilirubin ≥ 2.5 x ULN) unless due to
liver metastasis (decision by the investigator)
14. fibrinogen < 150 mg/dL, and/or International Normalized Ratio (INR) > 1,5 (global
coagulation parameters can be discussed with the Coordinating Investigator prior to
entry on study)
15. female patients with child-bearing who do not agree to exclusion of potential
pregnancy by adequate testing within 48 hours prior to entry on study
16. females of childbearing potential as well as fertile males who do not agree to use a
highly effective form of contraception (Pearl Index < 1) during the study and for 3
months (females) following the last trabectedin (Arm 1) or last study drug (Arm 2)
administration and 5 months (males) following the last dose of trabectedin (Arm 1)
or study drug (Arm 2)
17. women with breast-feeding activity
18. concomitant use of any other investigational agent (agent for which there is
currently no approved indication from regulatory authorities) or any other
anti-cancer drug
19. concomitant enrolment in another clinical trial interfering with the endpoints of
this study.
20. any medical condition which could compromise participation in the study according to
the investigator's assessment.
21. prophylactic or therapeutic anticoagulation within the last 3 days (see 11)
22. presence of active and uncontrolled infections or other severe concurrent disease,
which, in the opinion of the investigator, would place the patient at undue risk or
interfere with the study
23. concurrent malignancies other than STS, unless the patient has been disease-free for
at least 2 years
24. serious, non-healing wound, ulcer or bone fracture; not completed wound healing from
previous wounds and/or surgery
25. no central venous port system in place (prerequisite for ARM 2; valid exceptions
have to be discussed with the Coordinating Investigator).
NOTE: Outliers of laboratory values can be disregarded and set aside as exclusion
criteria by a Coordinating Investigator´s decision. The conditions for the use of
trabectedin as specified in the Summary of Product Characteristics are to be followed
according to institutional guidelines for standard of care.
Gender:
All
Minimum age:
18 Years
Maximum age:
75 Years
Healthy volunteers:
No
Locations:
Facility:
Name:
Medizinische Universität Graz
Address:
City:
Graz
Zip:
8010
Country:
Austria
Status:
Recruiting
Contact:
Last name:
Joanna Skandera, PD
Phone:
0043 316 38513115
Email:
joanna.szkandera@medunigraz.at
Investigator:
Last name:
Joanna Skandera, PD
Email:
Principal Investigator
Facility:
Name:
HELIOS Klinikum Bad Saarow
Address:
City:
Bad Saarow
Zip:
15529
Country:
Germany
Status:
Recruiting
Contact:
Last name:
Daniel Pink, Dr.
Phone:
+49 33631 73527
Email:
daniel.pink@helios-gesundheit.de
Investigator:
Last name:
Daniel Pink, Dr.
Email:
Principal Investigator
Investigator:
Last name:
Daniel Schöndube, Dr.
Email:
Sub-Investigator
Investigator:
Last name:
Antja West, Dr.
Email:
Sub-Investigator
Facility:
Name:
HELIOS Klinikum Berlin-Buch
Address:
City:
Berlin
Zip:
13125
Country:
Germany
Status:
Recruiting
Contact:
Last name:
Peter Reihardt, PD Dr.
Phone:
+49 30 940114888
Email:
peter.reichardt@helios-gesundheit.de
Investigator:
Last name:
Peter Reihardt, PD Dr.
Email:
Principal Investigator
Investigator:
Last name:
Nicolas Ziegenhagen
Email:
Sub-Investigator
Investigator:
Last name:
Benjamin Unger
Email:
Sub-Investigator
Facility:
Name:
TU Dresden Medizinische Fakultät Carl Gustav Carus
Address:
City:
Dresden
Zip:
01307
Country:
Germany
Status:
Recruiting
Contact:
Last name:
Stephan Richter, Dr.
Phone:
+49 351 458 7108
Email:
Stephan.Richter@uniklinikum-dresden.de
Investigator:
Last name:
Stephan Richter, Dr.
Email:
Principal Investigator
Investigator:
Last name:
Martin Wermke, Dr.
Email:
Sub-Investigator
Facility:
Name:
Universitätsklinikum Frankfurt
Address:
City:
Frankfurt am Main
Zip:
60590
Country:
Germany
Status:
Recruiting
Contact:
Last name:
Marit Ahrens, Dr.
Phone:
+49 69 6301 83359
Email:
Marit.Ahrens@kgu.de
Investigator:
Last name:
Marit Ahrens, Dr.
Email:
Principal Investigator
Investigator:
Last name:
Björn Steffen, Dr.
Email:
Sub-Investigator
Facility:
Name:
Universitätsklinikum Heidelberg
Address:
City:
Heidelberg
Zip:
69120
Country:
Germany
Status:
Recruiting
Contact:
Last name:
Gerlinde Egerer, Prof. Dr.
Phone:
+49 6221 568029
Email:
Gerlinde.Egerer@med.uni-heidelberg.de
Investigator:
Last name:
Gerlinde Egerer, Prof. Dr.
Email:
Principal Investigator
Investigator:
Last name:
Susanne Hofmann, Dr.
Email:
Sub-Investigator
Facility:
Name:
Universitätsmedizin Mainz
Address:
City:
Mainz
Zip:
55131
Country:
Germany
Status:
Recruiting
Contact:
Last name:
Marius Fried, Dr.
Phone:
+49 6131 175952
Email:
Marius.Fried@unimedizin-mainz.de
Investigator:
Last name:
Marius Fried, Dr. med.
Email:
Principal Investigator
Investigator:
Last name:
Thomas Kindler, Prof. Dr.
Email:
Sub-Investigator
Facility:
Name:
LMU Klinikum
Address:
City:
Münich
Zip:
81377
Country:
Germany
Status:
Recruiting
Contact:
Last name:
Lars Lindner, Prof. Dr.
Phone:
+49 89 4400 77773
Email:
Lars.Lindner@med.uni-muenchen.de
Investigator:
Last name:
Lars Lindner, Prof. Dr.
Email:
Principal Investigator
Investigator:
Last name:
Dorit Di Gioia, PD Dr.
Email:
Sub-Investigator
Facility:
Name:
University Hospital Muenster, Germany
Address:
City:
Münster
Zip:
48149
Country:
Germany
Status:
Recruiting
Contact:
Last name:
Christoph Schliemann, Prof. Dr.
Phone:
+49 251 83 45363
Email:
Christoph.Schliemann@ukmuenster.de
Contact backup:
Last name:
Torsten Kessler, PD Dr.
Phone:
+49 251 83 45363
Email:
Torsten.Kessler@ukmuenster.de
Investigator:
Last name:
Christoph Schliemann, Prof. Dr.
Email:
Principal Investigator
Investigator:
Last name:
Torsten Kessler, PD Dr.
Email:
Sub-Investigator
Start date:
October 26, 2021
Completion date:
December 2026
Lead sponsor:
Agency:
Universität Münster
Agency class:
Other
Collaborator:
Agency:
Anturec Pharmaceuticals GmbH
Agency class:
Other
Source:
Universität Münster
Record processing date:
ClinicalTrials.gov processed this data on November 12, 2024
Source: ClinicalTrials.gov page:
https://clinicaltrials.gov/ct2/show/NCT05597917
