L-Annamycin for Injection in Combination With Cytarabine Injection as Second Line Therapy for Remission Induction in Adult Subjects With Refractory/Relapsed AML

This pivotal phase 2/3, multi-center, adaptive design study of L-Annamycin for Injection

in combination with Cytarabine Injection as second line therapy for remission induction

in adult subjects with refractory/relapsed AML is divided into two parts, Part A and Part

B.

Part A (Determination of Optimal Dosage Regimen) Part A of this study is a randomized,

double-blind, placebo-controlled (RDBPC), efficacy, safety, tolerability, and

pharmacokinetics study comparing two dose levels of L Annamycin for Injection (190 versus

230 mg/m2/day) in combination with Cytarabine Injection (2.0 g/m2/day) versus placebo in

combination with Cytarabine Injection to identify the optimal dosage regimen as second

line therapy for remission induction in adult subjects with refractory/relapsed AML.

Seventy-five to ninety subjects with a pathologically confirmed diagnosis of AML who have

refractory/relapsed AML after having received only one prior line of therapy will be

enrolled in Part A. A prior line of therapy will be defined as the planned therapy

consisting of one or more cycles of episodic treatment or a defined period of continuous

treatment. This may consist of single-agent or combination therapy as well as a planned

sequence of treatment phases. For example, first-line treatment of AML with induction,

consolidation, and allogeneic hematopoietic stem cell transplantation (alloHSCT) is

considered one line of therapy. A line of therapy ends when the patient fails to achieve

a response within a prespecified period (refractory) or relapses after achieving CR. For

the purpose of confirming refractory AML at screening, refractory disease will be defined

as CR not being achieved after first line therapy [i.e., after 1 cycle of intensive

therapy or 180 days after commencing less-intensive therapy (shorter durations of

less-intensive therapy may be considered for refractory disease on a case by case basis

after discussion between the PI and Medical Monitor)]. Subjects who meet all eligibility

criteria after the completion of both screening and baseline assessments will be

enrolled. Initially, 45 subjects will be randomized 1:1:1 to one of the three treatment

arms listed below (i.e.,approximately 15 per treatment arm). Randomization will be

stratified by continent. Depending on the outcome of the first interim analysis (see

further below), additional subjects will either be randomized 1:1:1 to one of the three

treatment arms listed below (for a total of approximately 30 per treatment arm in Part A)

randomized 1:1 to either placebo in combination with Cytarabine Injection (Treatment Arm

1) or the L-Annamycin for Injection in combination with Cytarabine Injection arm that was

selected to continue after the first interim analysis (i.e., Treatment Arm 2 or 3) (for a

total of approximately30 per treatment arm in Part A, except for the arm that is dropped

after the first interim analysis, which will have a total of approximately ≤15 and ≤30,

depending on how many subjects were enrolled at the point the decision to drop the arm

occurs).

- Treatment Arm 1: placebo (0.9% Sodium Chloride Injection, i.e., the diluent for

L-Annamycin for Injection) for three consecutive days in combination with 2.0

g/m2/day Cytarabine Injection for five consecutive days.

- Treatment Arm 2: 190 mg/m2/day L-Annamycin for Injection for three consecutive days

in combination with 2.0 g/m2/day Cytarabine Injection for five consecutive days.

- Treatment Arm 3: 230 mg/m2/day L-Annamycin for Injection for three consecutive days

in combination with 2.0 g/m2/day Cytarabine Injection for five consecutive days.

L-Annamycin for Injection will be administered as an intravenous (IV) infusion over 2

hours. The placebo will be administered the same (i.e., IV infusion over 2 hours).

Cytarabine Injection will be administered as an IV infusion over 4 hours. The first day

of Cytarabine Injection treatment will start on the first day of L-Annamycin for

Injection or placebo treatment (Day 1). On the days where both Cytarabine Injection and

L-Annamycin for Injection or placebo are administered, the Cytarabine Injection infusion

will be initiated after the L-Annamycin for Injection or placebo infusion is

completed.The recommended time between infusions is 15 minutes (± 5 minutes). Part A of

this study will include two interim analyses as follows:

First Interim Analysis: After the 45 subjects enrolled in Part A of this study have

completed their first treatment cycle response assessment at Day 35 ± 14 days, the data

for those subjects will be verified/cleaned and locked, and the data will be unblinded

and analyzed (n = approximately 15 per treatment arm). Enrollment in the study will not

be halted while the first interim analysis is performed. Comparisons will be made between

the three treatment arms to determine if continuation of the study should be halted due

to a lack of efficacy difference between the placebo in combination with Cytarabine

Injection arm (Treatment Arm 1) and the L-Annamycin for Injection in combination with

Cytarabine Injection arms (Treatment Arms 2 and 3; i.e., futility analysis) or too

excessive of a risk of serious adverse events (SAEs) with Treatment Arms 2 and/or 3

relative to Treatment Arm 1. An unblinded independent data monitoring committee (iDMC)

will review the available efficacy, safety, and pharmacokinetic (PK) data and make

recommendations to the Sponsor on how to proceed with the remainder of Part A of the

study. The primary options will be to recommend that the study be halted for futility

reasons, for safety reasons, or that the study continue. If the iDMC recommends that the

study continues, they will recommend if one or both L-Annamycin for Injection dosage

regimens (i.e., 190 mg/m2/day or 230 mg/m2/day) continue for Part A.

In the European Union (EU), the iDMC recommendations from the first interim analysis will

be provided to the Competent Authorities of EU Member States concerned, and if a protocol

amendment is needed, it will be submitted within a Substantial Modification.

Second Interim Analysis: After all subjects enrolled in Part A of this study (total of 75

to 90 subjects; see above for explanation of variable total subject number) have

completed their first treatment cycle response assessment at Day 35 ± 14 days, enrollment

in the study will be temporarily halted, the data will be verified/cleaned and locked,

the data for the second group of subjects (i.e., who were not part of the first interim

analysis) will be unblinded, and the pooled Part A data will be analyzed. If all three

arms were continued after the first interim analysis, three treatment arms will be

compared (n = approximately 30 per treatment arm) to determine which of the L Annamycin

for Injection dosage regimens (190 mg/m2/day versus 230 mg/m2/day) is the optimal dosage

regimen for continuing with for the remainder of the study (Part B) and which dosage

regimen will be dropped from further enrollment. If one of the two L Annamycin for

Injection in combination with Cytarabine Injection dosage regimens (Treatment Arm 2 or 3)

was dropped after the first interim analysis, the remaining arm will be compared against

placebo in combination with Cytarabine Injection (Treatment Arm 1) (n = approximately 30

per treatment arm) to confirm that the study should continue with that regimen to Part B.

Part B (Expansion at Optimal Dosage Regimen) Part B of this study is a RDBPC, efficacy,

safety, tolerability, and pharmacokinetics study of the optimal dosage regimen of

L-Annamycin for Injection in combination with Cytarabine Injection (as determined in Part

A) versus placebo in combination with Cytarabine Injection as second line therapy for

remission induction in adult subjects with refractory/relapsed AML.

Once the optimal dosage regimen is determined (see Part A above), enrollment will resume

under Part B of the study. Approximately 222 additional subjects with a pathologically

confirmed diagnosis of AML who have refractory/relapsed AML after having received only

one prior line of therapy (i.e., the same patient population as for Part A) will be

enrolled in Part B.

Subjects who meet all eligibility criteria after the completion of both screening and

baseline assessments will be enrolled and randomized 1:1 to one of the two treatment arms

listed below (i.e., 111 per treatment arm). Randomization will be stratified by

continent.

- Treatment Arm 1: placebo (0.9% Sodium Chloride Injection) for three consecutive days

in combination with 2.0 g/m2/day Cytarabine Injection for five consecutive days

(i.e., the same as Treatment Arm 1 of Part A).

- Treatment Arm X: optimal dosage regimen (as determined in Part A) of L Annamycin for

Injection (190 mg/m2/day or 230 mg/m2/day) for three consecutive days in combination

with 2.0 g/m2/day Cytarabine Injection for five consecutive days (i.e., the same as

Treatment Arm 2 or 3, respectively, of Part A).