BeyondSpring Delivers Oral Presentation at ISLAC 2024 World Conference on Lung Cancer of its Lead Anti-Cancer Asset Plinabulin Showcasing Positive Final Phase 3 Data in 2L/3L NSCLC EGFR Wild-Type with Concurrent Publication in the Lancet Respiratory Medici
10 Septiembre 2024 - 6:00AM
BeyondSpring Inc. (NASDAQ: BYSI) (“BeyondSpring”
or the “Company”), a clinical-stage global biopharmaceutical
company focused on developing innovative cancer therapies, today
announces Dublin-3 final phase 3 efficacy data of its late
clinical-stage agent Plinabulin in combination with docetaxel in
second/third line (2L/3L) advanced and metastatic non-small cell
lung cancer (NSCLC) with epidermal growth factor receptor (EGFR)
wild-type. The lead principal investigator, Dr. Trevor Feinstein
from Piedmont Cancer Institute, presented the data in an oral
presentation (OA08.04) at ISLAC 2024 World Conference on Lung
Cancer on September 9th 2024 in San Diego, CA. Concurrently,
Dublin-3 study was published in the Lancet Respiratory Medicine
(https://doi.org/10.1016/S2213-2600(24)00178-4).
Docetaxel remains the standard of care for patients with 2L/3L
NSCLC without targetable alterations despite severe neutropenia
(>40%) that greatly impair patients’ quality of life. Six recent
phase 3 studies in patients with EGFR wild-type NSCLC who were
previously treated with immune checkpoint inhibitors failed to show
overall survival (OS) benefit compared with docetaxel (SAPPHIRE,
LEAP-008, CONTACT01, EVOKE-01, CARMEN-LC03, and CANOPY-2). Two
phase 3 studies (LUNAR and TROPION-Lung01) showed positive but
mixed outcomes compared with docetaxel.
The DUBLIN-3 study was a multicenter, randomized, single-blind,
placebo-controlled trial that enrolled patients from 58 medical
centers internationally. For the intention-to-treat (ITT)
population, 559 patients received either docetaxel plus plinabulin
(n=278 [male 199, female 79]) or docetaxel plus placebo (n=281
[male 207, female 74]).
Key findings of Dublin-3 study are summarized below:
- Favorable benefit/risk ratio: Significant
improvement in OS (Hazard ratio or HR=0.82; same HR in the Western
vs. Asian patients), PFS (HR=0.79) and ORR (nearly doubled).
Durable anti-cancer benefits in doubling 24-months and 36-months OS
rates. And 82% relative reduction in Grade 4 neutropenia in Cycle 1
Day 8 (p<0.0001).
- Consistent OS benefit in 24-month follow up after the
database lock: OS HR=0.81 in the ITT population, with
better OS benefit in the non-squamous subset (OS HR=0.72,
p=0.0078). For the non-squamous subset patients, median OS (mOS) in
plinabulin/docetaxel arm was 11.4 months vs. 8.8 months in the
docetaxel arm, with a mOS benefit of 2.6 months.
- Improved OS benefit with more cycles of
treatment (≥ 4, 6, 8, 10, or 12 cycles): for patients who
used at least 4 cycles of treatment, OS HR=0.64, p=0.0027, with a
mOS benefit of 4.8 months (plinabulin/docetaxel arm n=133;
docetaxel arm n=127).
- Plinabulin/docetaxel combination is
well-tolerated: Treatment-emergent adverse-events occurred
in 273/274 (99·6%) of patients in the plinabulin group and 276/278
(99·3%) in the control group. Higher incidences of Grade 3/4
gastrointestinal disorders (46 patients [16·8%] vs. 8 [2·9%]) and
transient Grade 3 hypertension (50 patients [18·2%] vs. 8 [2·9%])
occurred in the plinabulin vs. control group.
“There is a poor prognosis for NSCLC patients without targetable
alterations whose disease has progressed on platinum-based
therapies. Unfortunately, multiple high-profile phase 3 studies
failed to show overall survival benefit in this hard-to-treat
population compared to standard of care docetaxel, a drug approved
over 20 years ago. The data from DUBLIN-3 study demonstrates that
the addition and proper sequencing of plinabulin to docetaxel has a
favorable benefit/risk ratio compared with docetaxel alone and may
have broad utility. This combination could be considered as a new
treatment option for this population with high unmet medical
needs,” said Dr. Feinstein, a lead principal investigator of the
DUBLIN-3 study at Piedmont Cancer Center, Atlanta.
Citation:Han B., et al. Plinabulin plus
docetaxel versus docetaxel in patients with non-small-cell lung
cancer after disease progression on platinum-based regimen
(DUBLIN-3): a phase 3, international, multicentre, single-blind,
parallel group, randomised controlled trial. Lancet Respir Med.
2024 Sep 09: S2213-2600(24)00178-4.
About PlinabulinPlinabulin is a novel
first-in-class dendritic cell maturation agent with durable
anti-cancer benefit observed across multiple clinical studies. As a
reversible binder at a distinct tubulin pocket, plinabulin does not
change tubulin dynamics or antagonize tubulin stabilizing agents,
such as docetaxel, which contributes to its differentiated activity
and tolerability compared to other tubulin binders. In addition,
plinabulin significantly reduces chemotherapy induced neutropenia
and could thereby increase docetaxel tolerability. Over 700
patients have been treated with plinabulin with good
tolerability.
About Dublin-3 StudyDUBLIN-3 is a multicenter,
single-blinded (patient) and randomized, phase 3 trial in 58
medical centers (US, China, and Australia). Only patients with EGFR
wild-type NSCLC who had progressed after first-line platinum-based
therapy were enrolled. Patients were randomized (1:1) to receive
docetaxel (75 mg/m2) on Day 1 and either plinabulin (30 mg/m2) or
placebo on Days 1 and 8 in 21-day cycles until progression,
unacceptable toxicity, withdrawal, or death. Treated patients were
included in the safety analysis and ITT population in the primary
efficacy analyses (NCT02504489). The primary endpoint for the study
was OS, and secondary endpoints were PFS, ORR, Duration of Response
(DoR), Grade 4 neutropenia and Quality of Life.
About BeyondSpringBeyondSpring is a global
clinical-stage biopharmaceutical company focused on developing
innovative therapies to improve clinical outcomes for patients with
high unmet medical needs. The Company is advancing its
first-in-class lead asset, Plinabulin, a potent inducer of
dendritic cell maturation, in late-stage clinical development as a
direct anti-cancer agent in NSCLC and a variety of cancer
indications. BeyondSpring’s pipeline also includes three
preclinical immuno-oncology assets. Additionally, BeyondSpring is
an equity owner of SEED Therapeutics, Inc which is a pioneer in
Target Protein Degradation technology and its application in
innovative drug development. Learn more by visiting
https://beyondspringpharma.com.
Investor Contact:IR@beyondspringpharma.com
Media Contact:PR@beyondspringpharma.com
A photo accompanying this announcement is available
at:https://www.globenewswire.com/NewsRoom/AttachmentNg/66242c15-b61a-48be-a69d-8cf334951a84
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