- DREAMM-8 phase III trial showed statistically significant and
clinically meaningful improvement in primary endpoint of
progression-free survival (PFS)
- Median PFS not yet reached at 21.8 months median follow-up
versus 12.7 months in bortezomib combination
- Second trial to show robust efficacy for a belantamab mafodotin
combination versus a standard of care in second line and later
relapsed/refractory multiple myeloma
- Results simultaneously published in the New England Journal of
Medicine
GSK plc (LSE/NYSE: GSK) today announced positive results from an
interim analysis of the DREAMM-8 phase III head-to-head trial
evaluating belantamab mafodotin, in combination with pomalidomide
plus dexamethasone (PomDex), versus a standard of care, bortezomib
plus PomDex, as a second line and later treatment for relapsed or
refractory multiple myeloma. These late-breaking data, being
presented today at the 2024 American Society of Clinical Oncology
(ASCO) Annual Meeting (May 31 – June 4) in Chicago, IL, were
featured in the official ASCO press program and simultaneously
published in the New England Journal of Medicine.
On the primary endpoint of progression-free survival (PFS), a
statistically significant and clinically meaningful improvement
(hazard ratio [HR]: 0.52 [95% confidence interval (CI): 0.37-0.73],
p-value<0.001) was observed with the belantamab mafodotin
combination (n=155) compared to the bortezomib combination (n=147).
At a median follow-up of 21.8 months, the median PFS was not yet
reached (95% CI: 20.6-not yet reached [NR]) with the belantamab
mafodotin combination compared to 12.7 months (95% CI: 9.1-18.5) in
the bortezomib combination. At the end of one year, 71% (95% CI:
63-78) of patients in the belantamab mafodotin combination group
compared to 51% (95% CI: 42-60) in the bortezomib combination group
were alive and had not progressed. A benefit for belantamab
mafodotin plus PomDex was observed across all pre-specified
subgroups including those with poor prognostic features, such as
patients who were refractory to lenalidomide and patients with
high-risk cytogenetics.
Hesham Abdullah, Senior Vice President, Global Head Oncology,
R&D, GSK, said: “With the robust results from the DREAMM-8
phase III head-to-head trial, we now have consistent data from two
phase III trials supporting the potential for belantamab mafodotin
combinations to redefine the treatment of multiple myeloma at or
after first relapse. This is exciting news given the high unmet
need for new and efficacious combinations once patients relapse or
stop responding to initial treatments. We continue to share data
and discuss our path forward with regulators.”
A positive overall survival (OS) trend was observed but not
statistically significant (HR: 0.77 [95% CI: 0.53-1.14]) at the
interim analysis. OS follow-up continues and further analyses are
planned. At the end of one year, 83% (95% CI: 76-88) of patients
were alive in the belantamab mafodotin combination group versus 76%
(95% CI: 68-82) in the bortezomib combination group. The safety and
tolerability profile of the belantamab mafodotin combination was
broadly consistent with the known profile of the individual
agents.
Suzanne Trudel, MD, Department of Medical Oncology and
Hematology, Princess Margaret Cancer Centre, University Health
Network, Toronto, Canada, said: “The profound progression-free
survival benefit seen in DREAMM-8 highlights the potential for
belantamab mafodotin, when used with pomalidomide and
dexamethasone, to improve outcomes for patients with
relapsed/refractory multiple myeloma. This combination may have
potential to redefine treatment of multiple myeloma at or after
first relapse, a setting where patients may benefit from novel
therapies.”
Similar to the results seen in the DREAMM-7 phase III
head-to-head trial, in DREAMM-8 the belantamab mafodotin
combination also resulted in clinically meaningful improvements
consistently across secondary efficacy endpoints, showing that the
belantamab mafodotin combination resulted in deeper and more
durable responses compared to the bortezomib combination. Key
improvements included rate of complete response (CR) or better
(more than twofold improvement); minimal residual disease (MRD)
negativity rate (nearly fivefold improvement); and duration of
response (median not yet reached with the belantamab mafodotin
combination versus 17.5 months with the bortezomib
combination).
Key and other secondary endpoint summaries are listed below.
Key and Other Secondary
Endpoints
Endpoint
belantamab mafodotin +
pomalidomide and dexamethasone (BPd) (n= 155)
pomalidomide + bortezomib and
dexamethasone (PVd) (n=147)
ORR (overall response rate), % (95%
CI)
77% (70.0-83.7)
72% (64.1-79.2)
sCR (stringent complete response), %
9%
3%
CR (complete response), %
31%
14%
VGPR (very good partial response), %
24%
22%
PR (partial response), %
14%
34%
CR or better rate (sCR+CR), % (95% CI)
40% (32.2-48.2)
16% (10.7-23.3)
VGPR or better rate (sCR+CR+VGPR), % (95%
CI)
64% (55.8-71.4)
38% (30.2-46.5)
MRD negativity rate* % (95% CI)
23.9% (17.4-31.4)
4.8% (1.9-9.6)
Duration of response (months), median (95%
CI)
NR (24.9-NR)
17.5 months (12.1-26.4)
Overall Survival**
HR (95% CI)
0.77 (0.53-1.14)
* Measured in patients with a sCR or
CR.
** Follow-up for OS is ongoing.
NR: Not yet reached.
Grade 3 or higher non-ocular adverse events (AEs) of clinical
interest in the belantamab mafodotin combination versus bortezomib
combination arms, respectively, included neutropenia (57% vs 39%;
42 patients/100 person-years in both arms); thrombocytopenia (38%
vs 29%; 28 vs 31 patients/100 person-years); and pneumonia (17% vs
8%; 13 vs 8 patients/100 person-years).
Eye-related side effects, a known risk of treatment with
belantamab mafodotin, were generally reversible, manageable with
dose modifications, and led to low (9%) treatment discontinuation
rates. Grade 3 or higher ocular adverse events occurred in 43% of
patients receiving the belantamab mafodotin combination (Grade 3:
42%; Grade 4: 1%). Most commonly reported grade 3 or higher ocular
symptoms included blurred vision (Grade 3: 17%; Grade 4: 0), dry
eye (Grade 3: 8%: Grade 4: 0), and foreign body sensation in the
eyes (Grade 3: 6%; Grade 4: 0). Fifty-one patients (34%) with a
best corrected visual acuity (BCVA) of 20/25 or better in at least
one eye at baseline had a worsening in both eyes to 20/50 or worse.
At the time of this analysis, the first occurrence of such events
had improved in 92% of these patients, and resolved in 85%, with a
median time to resolution of 57 days (range: 14-451 days).
Global health status quality of life (QOL), as measured by the
EORTC-QLQ-C30 remained stable in both treatment arms over time,
suggesting that treatment did not lead to any decline in overall
health related QOL.
The DREAMM (DRiving Excellence in Approaches to Multiple
Myeloma) clinical development program continues to evaluate the
potential of belantamab mafodotin in early lines of treatment and
in combination with novel therapies and standard of care
treatments. DREAMM-8 is the second phase III head-to-head
belantamab mafodotin combination trial in second line and later
treatment for multiple myeloma to report positive results. Positive
findings from DREAMM-7, a phase III head-to-head trial evaluating
belantamab mafodotin in combination with bortezomib and
dexamethasone (BorDex) versus daratumumab plus BorDex in the same
treatment setting, were presented1 at the ASCO Plenary Series on
February 6, 2024, shared in an encore presentation at the 2024 ASCO
Annual Meeting, and published in the New England Journal of
Medicine.
About DREAMM-8
The DREAMM-8 phase III clinical trial is a multi-center,
open-label, randomized trial evaluating the efficacy and safety of
belantamab mafodotin in combination with PomDex compared to a
combination of bortezomib and PomDex in patients with
relapsed/refractory multiple myeloma previously treated with at
least one prior line of multiple myeloma therapy, including a
lenalidomide-containing regimen, and who have documented disease
progression during or after their most recent therapy. Compared to
the patient population studied in the DREAMM-7 trial, patients in
DREAMM-8 were more heavily pre-treated in that all had prior
exposure to lenalidomide, 75% were refractory to lenalidomide, 25%
had prior daratumumab exposure and of those most were daratumumab
refractory.
A total of 302 participants were randomized at a 1:1 ratio to
receive either belantamab mafodotin plus PomDex, or bortezomib plus
PomDex.
The primary endpoint is PFS as per an independent review
committee. Key secondary endpoints include OS, minimal residual
disease negativity as assessed by next-generation sequencing, and
duration of response. Other secondary endpoints include ORR,
patient-reported quality of life outcomes, adverse events, eye exam
findings, and laboratory investigations.
About multiple myeloma
Multiple myeloma is the third most common blood cancer globally
and is generally considered treatable but not curable.2,3 There are
approximately 176,000 new cases of multiple myeloma diagnosed
globally each year.4 Research into new therapies is needed as
multiple myeloma commonly becomes refractory to available
treatments.5
About belantamab mafodotin
Belantamab mafodotin is an investigational antibody-drug
conjugate comprising a humanized B-cell maturation antigen
monoclonal antibody conjugated to the cytotoxic agent auristatin F
via a non-cleavable linker. The drug linker technology is licensed
from Seagen Inc.; the monoclonal antibody is produced using
POTELLIGENT Technology licensed from BioWa Inc., a member of the
Kyowa Kirin Group.
GSK in oncology
Oncology is an emerging therapeutic area for GSK where we are
committed to maximizing patient survival with a current focus on
hematologic malignancies, gynecologic cancers, and other solid
tumors through breakthroughs in immuno-oncology and tumor-cell
targeting therapies.
About GSK
GSK is a global biopharma company with a purpose to unite
science, technology, and talent to get ahead of disease together.
Find out more at us.gsk.com.
Cautionary statement regarding forward-looking
statements
GSK cautions investors that any forward-looking statements or
projections made by GSK, including those made in this announcement,
are subject to risks and uncertainties that may cause actual
results to differ materially from those projected. Such factors
include, but are not limited to, those described under Item 3.D
“Risk factors” in GSK’s Annual Report on Form 20-F for 2023, and
GSK’s Q1 Results for 2024.
Registered in England & Wales:
No. 3888792
Registered Office:
980 Great West Road
Brentford, Middlesex
TW8 9GS
References
1 GSK press release issued 05 February 2024. DREAMM-7 phase III
trial shows Blenrep combination nearly tripled median
progression-free survival versus standard of care combination in
patients with relapsed/refractory multiple myeloma. Available at:
https://www.gsk.com/en-gb/media/press-releases/dreamm-7-phase-iii-trial-shows-pfs-improvement-and-strong-os-trend-for-blenrep-combo-versus-soc-combo-in-multiple-myeloma/.
2 Sung H, Ferlay J, Siegel R, et al. Global Cancer Statistics 2020:
GLOBOCAN Estimates of Incidence and Mortality Worldwide for 36
Cancers in 185 Countries. CA Cancer J Clin. 2021;71(3):209-249.
doi:10.3322/caac.21660. 3 Kazandjian D. Multiple myeloma
epidemiology and survival: A unique malignancy. Semin Oncol.
2016;43(6):676–681.doi:10.1053/j.seminoncol.2016.11.004. 4 Multiple
Myeloma: Statistics. Cancer.net. Published February 2022.
https://www.cancer.net/cancer-types/multiple-myeloma/statistics.
Accessed 19 October 2023. 5 Nooka AK, Kastritis E, Dimopoulos MA.
Treatment options for relapsed and refractory multiple myeloma.
Blood. 2015;125(20).
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