This is a phase I dose escalation and expansion study in patients with ER+, HER2- advanced breast cancer to explore the tolerance, PK/PD(pharmacokinetics/pharmacodynamics) profiles and preliminary anti-tumor activity of different doses of LX-039 tablets. The trial consists of two parts, dose escalation and dose expansion. Part 1 is the dose escalation phase with initial 6 dose groups, and "3 + 3" design is used to explore MTD of the drug; Part 2 is the dose expansion phase with 2 \~ 3 doses selected for expansion according to the escalation results of Part 1, and more subjects are enrolled to further observe the tolerance and preliminary anti-tumor activity of the drug. After the completion of dose expansion, the recommended phase II dose (RP2D) will be determined after discussion based on the obtained tolerance and PK/PD data.
Study Type
INTERVENTIONAL
Allocation
NON_RANDOMIZED
Purpose
TREATMENT
Masking
QUADRUPLE
Enrollment
44
orally once daily until disease progression, unacceptable toxicity, withdrawal of consent, or study termination
Fudan University Shanghai Cancer Center
Shanghai, Shanghai Municipality, China
To explore the tolerance of LX-039 in ER +, HER2 - patients with advanced breast cancer
Incidence of dose limiting toxicities (DLTs)
Time frame: DLT observation period(5 weeks for dose escalation, 4 weeks for dose expansion)
The safety of LX-039 in ER +, HER2 - patients with advanced breast cancer
Number of participants with treatment related. adverse events as assessed by CTCAE v5.0
Time frame: through study completion,an average of 1 year
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
Objective response rate (ORR)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
proportion of subjects with complete response (CR)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
proportion of subjects with partial response (PR)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
proportion of subjects with stable disease (SD)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
proportion of subjects with progressive disease (PD)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
duration of response (DoR)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
disease control rate (DCR)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
clinical benefit rate (CBR)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
time to progression (TTP)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
progression-free survival (PFS)
Time frame: through study completion,an average of 1 year.
To explore the efficacy of LX-039 in ER +, HER2 - patients with advanced breast cancer according to Recist 1.1.
overall survival (OS)
Time frame: through study completion,an average of 1 year.
Comparison of changes in maximum uptake ability of FES(progression free survival) in breast cancer lesions before and after treatment with LX-039 by PET(positron emission tomography) scan (performed in some subjects)
Decrease in SUVmax in comparison with that before treatment
Time frame: Up to the third day of Cycle 2(each cycle is 28 days)
PK profiles after a single dose of LX-039
Peak Concentration (Cmax)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Peak Time (Tmax)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Elimination Half-life (t1/2)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Eliminate Rate Constant (Kel)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Mean Residence Time (MRT)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Area under plasma Concentration-time curve from 0 time to 24 hours (AUC0-24h)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Area under plasma Concentration-time curve from 0 time to sampling time t of the last measurable concentration (AUC0-last)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Area under plasma Concentration-time curve from administration (0) to infinity (AUC0-inf)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Apparent Total Clearance (CL/F)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after a single dose of LX-039
Apparent Volume of Distribution (Vd/F)
Time frame: Up to the third day of Cycle 0(Cycle 0 is 7 days)
PK profiles after continuous administration of LX-039
Trough Concentration at Steady State (Css, min)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Peak Concentration at Steady State (Css, max)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Average Concentration at Steady State (Css, av)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Peak Time (Tss, max)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Apparent Volume of Distribution at steady state (Vss/F)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Steady-state Clearance Half-life (tss,1/2)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Total Body Clearance (CLss/F)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Coefficient of Fluctuation (DF)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Area under Plasma Concentration-time Curve at Steady State (AUCss)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
PK profiles after continuous administration of LX-039
Accumulation Coefficient (Rac)
Time frame: Up to the Second day of Cycle 2(each cycle is 28 days)
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