Clinical Trial Details
— Status: Active, not recruiting
Administrative data
| NCT number |
NCT05105971 |
| Other study ID # |
BAT-6026-001-CR |
| Secondary ID |
|
| Status |
Active, not recruiting |
| Phase |
Phase 1
|
| First received |
|
| Last updated |
|
| Start date |
December 23, 2021 |
| Est. completion date |
November 14, 2024 |
Study information
| Verified date |
March 2024 |
| Source |
Bio-Thera Solutions |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
the main purpose:
- Evaluate the safety and resistance of BAT6026 injection as a single agent in the
treatment of patients with locally advanced or metastatic solid tumors Acceptability
- Explore maximum tolerated dose (MTD) or maximum administered dose (MAD) and be phase II
or follow-up clinical The study provides recommended doses and reasonable dosing
schedules.
Secondary purpose:
- Evaluate the single dose and multiple doses of BAT6026 injection in patients with
locally advanced or metastatic solid tumors Pharmacokinetic (PK) characteristics of the
drug;
- Evaluate the immunogenicity of BAT6026 injection;
- Evaluate the pharmacodynamic properties of BAT6026 injection;
- Preliminary evaluation of the anti-tumor efficacy of BAT6026 injection.
Description:
This study is designed as a phase I clinical trial of multi-center, open, dose escalation,
and extended research.
The study mainly evaluates the safety, tolerability and PK characteristics of BAT6026
injection in patients with advanced malignant solid tumors, explores the maximum tolerated
dose and preliminary anti-tumor efficacy, and provides a basis for the recommended dose of
subsequent clinical trials.
The research is divided into 2 phases:
The first stage: dose escalation study. The safety, tolerability and pharmacokinetic
characteristics of BAT6026 were explored using rapid titration and the "3+3" dose escalation
rule.
Because the clinical efficacy benefit of a single drug may be limited, from the ethical point
of view of exposing fewer subjects to invalid doses, this dose escalation study uses rapid
titration and the "3+3" dose escalation rule to explore the safe dose range . A total of 7
(or 8) dose groups are set up, namely the 0.01 mg/kg group, 0.03mg/kg group, 0.1mg/kg group,
0.3mg/kg group, 1mg/kg group, 3mg/kg group, 6mg/kg Group and 10mg/kg group (optional). Among
them, the 0.01mg/kg group and the 0.03mg/kg group use accelerated titration Method to
increase the dose; 0.1mg/kg group, 0.3mg/kg group, 1mg/kg group, 3mg/kg group, The 6mg/kg
group and the 10mg/kg group were studied in dose escalation according to the standard "3+3"
rule.
Group/Ascending Method Dose (mg/kg) Group Number of People A/single subject 0.01 1, or 3~6
B/single subject 0.03 1, or 3~6 C/"Standard 3+3" 0.1 3~6 D/"Standard 3+3" 0.3 3~6 E/"Standard
3+3" 1 3~6 F/"Standard 3+3" 3 3~6 G*/"Standard 3+3" 6 3~6 H*/"Standard 3+3" 10 3~6 *Remarks:
After the completion of the dose escalation study of groups A to G, after comprehensive
assessment of safety and other factors, it may be considered as appropriate whether to add a
10 mg/kg dose group for further tolerability exploration; it can also be discussed with the
investigator according to the specific situation. A new dose is selected between the dose
that stops climbing and the previous lower dose group, and the experiment is conducted
according to the above rules to determine the more accurate maximum tolerated dose.
The dose escalation rules are as follows:
The first two dose groups A and B adopt an accelerated titration dose escalation plan, that
is, cohort size=1. First, one case of group A is included. If no ≥ 2 grade toxic reaction
related to the study drug is observed, they can directly enter group B for dose escalation.
By analogy with this rule ("1+1"), the increase will be accelerated to Group C. If during the
accelerated escalation process, once a group has observed a ≥2 level toxic reaction related
to the study drug, the accelerated titration dose escalation should be stopped, and two more
subjects need to be included in the dose group to be converted to the standard "3+ 3" dose
escalation (ie, cohort size=3) mode until MTD or MAD is reached. Starting from Group C, it is
adjusted to the standard "3+3" rule of dose increasing mode, the increasing mode is shown in
the following table:
Number of people with DLT/number of people in current dose group Decision of dose increase or
decrease 0/3 3 new subjects receive the next high-dose group trial 1/3 The current dose group
was added to the group with 3 new subjects 1/3 and 0/3 (ie 1/6) 3 new subjects receive the
next high-dose group trial
≥2/3 or ≥2/6 indicates that the dose has exceeded the MTD, and the dose escalation should be
stopped. If there are 6 people in the previous dose group, use the previous lower dose group
as MTD. If there are only 3 people in the previous dose group, 3 people will be added to the
previous dose group. After 3 additional people, if there are ≥ 2 DLTs in the previous dose
group, the MTD will continue to decrease. If MTD is explored, the sponsor can discuss with
the investigator according to the specific situation and select MTD or a dose lower than MTD
as the phase II clinical study Recommended dosage. If the MTD is not reached, the sponsor may
also discuss with the investigator based on the specific situation, and select a dose of MAD
or a dose group below MAD as the recommended dose for the phase II clinical study as
appropriate. As the research progresses, the DLT definition can be revised as appropriate
based on new clinical findings. Although the adverse events that meet the DLT criteria or
other adverse safety information deemed by the researcher to be meaningful outside the DLT
evaluation period do not directly affect the dose escalation decision, they need to be taken
into account in the final decision on RP2D. The sponsor and investigator will Before the dose
is increased, the existing safety, PK (if any), effectiveness and other information should be
used to discuss and comprehensively evaluate the decision-making of dose increase or
decrease. When tolerability is explored according to the standard "3+3" dose escalation rule,
all subjects in the previous dose group must complete a 21-day DLT observation before the
next dose group is enrolled in the cohort. In the dose escalation study, a maximum of 2
subjects in each group are allowed to be in the DLT observation period at the same time.
Within each dose group, There must be a time interval of at least 24 hours between the
administration of the first enrolled subject and the subsequent enrolled subject.
Adjustments for dose reduction are not allowed. The dose is allowed to be increased as
appropriate, but extreme caution is required, and at least it needs to be met at the same
time: ①The subject has received at least 4 cycles of study drug treatment; ②After discussion
between the sponsor and the investigator, it is deemed that the subject has received a higher
first-level dose The treatment of the current dose group will bring more clinical benefits;
③The higher-level dose group has passed the follow-up dose escalation study and proved to
have not reached the MTD.
The second stage: Dose extension study. Based on the preliminary safety and effectiveness
results of the dose escalation study, the investigator and the sponsor decide whether to
choose an appropriate dose group for the extended study, further study the safety and
clinical effectiveness of BAT6026, and provide a basis for subsequent clinical studies. A
study of 2 dose cohorts is planned, and each cohort has no less than 6 subjects for PK study.
The overall research cycle is roughly divided into the screening period, the treatment
period, and the follow-up period:
Screening period: -28d~0d, that is, after signing the informed consent form, the screening
evaluation can be completed within 28 days; Treatment period: every 3 weeks is a dosing
cycle. The study drug is given on the first day of each cycle. Starting from the second
cycle, the dosing time window can be ±3 days, but within 72 hours before each dosing, except
In addition to imaging examinations, subjects must complete various examinations including
vital signs, laboratory examinations, and physical status scoring. The test subjects also
need to complete the clinical tumor imaging evaluation (evaluation The method is consistent,
CT or MRI). Study drug treatment should continue until emergence: disease progression/death,
or withdrawal due to intolerable toxicity, or acceptance of new anti-tumor therapy due to no
therapeutic benefit, or withdrawal of informed consent and voluntary withdrawal for other
reasons, or up to 17 Cycles (approximately 1 year), whichever comes first.
The DLT evaluation period is defined as the first treatment cycle, that is, from the first
administration to 21 days after the administration.
Follow-up period: If the subject stops using study medication, the treatment period will be
deemed to be over(End of Therapy, EOT). All subjects, including those who discontinued
treatment for any reason (except for loss of follow-up, death,withdrawal of informed
consent), will arrange an EOT visit in a timely manner within 21 + 7 days after receiving the
last study drug or before receiving subsequent new anti-tumor treatments . The EOT visit
should include vital signs, physical examination, laboratory examination, clinical tumor
imaging evaluation (CT or MRI) and other examinations.
Safety follow-up: After receiving the last dose of study drug, the subjects are required to
be at 21 + 7 days,A safety visit was conducted on days and 90 days (±7 days), including
immune-related adverse events (irAE), until 90 days or the subject received new anti-tumor
therapy. Safety visits must be conducted at the research center, and various examinations
such as vital signs, physical examinations, and laboratory examinations should be performed
to evaluate AEs, concomitant medications, and concomitant treatments. Until the adverse event
related to the study drug disappears (or drops to ≤1 level), if the adverse event still
exists after the subject stops treatment, the investigator has the discretion to determine
the frequency of follow-up according to the actual clinical situation until the investigator
considers it undesirable The outcome of the event is returning to normal, stable at an
acceptable level, or no further improvement. Survival follow-up: After the safety follow-up,
the subjects were followed up for survival every 12 weeks (±14 days), followed by telephone
until death, loss of follow-up, withdrawal of informed consent, observation for 1 year or
termination of the study.
Subjects will be informed that the sponsor will not provide additional study drugs after
completion/discontinuation of study drugs. If necessary, the subjects are recommended to
return to the research center, and the investigator and the sponsor will discuss and
formulate a new study medication treatment plan for the subjects.
