CAMBRIDGE, Mass. -- (Business Wire)
Acceleron Pharma Inc. (NASDAQ:XLRN), a clinical stage biopharmaceutical
company focused on the discovery, development and commercialization of
novel therapeutic candidates that regulate cellular growth and repair,
today reported new preliminary data from the DART study, an ongoing
phase 2 clinical trial of dalantercept in patients with advanced renal
cell carcinoma (RCC). The preliminary data from part 1 of the DART study
were presented in an oral session at the American Society of Clinical
Oncology (ASCO) 2015 Genitourinary Cancers Symposium held in Orlando,
Florida on February 28, 2015.
“These promising response rates and progression-free survival data
suggest that the dual angiogenesis blockade of ALK1 and VEGFR signaling
with dalantercept and axitinib may provide additive efficacy compared to
VEGFR inhibitor therapy alone,” said Matthew Sherman, M.D., Chief
Medical Officer of Acceleron.
“The results from part 1 of this study provide encouraging evidence of
the safety and activity of this combination of two distinct
anti-angiogenic agents in previously treated patients with advanced
RCC,” said Martin H. Voss, M.D., medical oncologist at Memorial Sloan
Kettering Cancer Center and lead investigator for the trial. “We look
forward to building on these results in the randomized part 2 of the
ongoing DART trial.”
In the DART trial, dalantercept, an activin receptor-like kinase 1
(ALK1) inhibitor, is being evaluated in combination with Inlyta®
(axitinib), a VEGFR tyrosine kinase inhibitor, in patients with advanced
RCC who have progressed on one prior VEGFR tyrosine kinase inhibitor and
no more than three prior treatments.
Key preliminary data from part 1 of the DART study (open-label, dose
escalation and expansion cohorts):
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Three cohorts each received dalantercept (0.6, 0.9, or 1.2 mg/kg)
subcutaneously once every three weeks and axitinib 5 mg orally twice a
day for each 21 day cycle. The 0.9 and 1.2 mg/kg dose levels were
expanded.
-
Response rates (RECIST v1.1) of the combination of dalantercept and
axitinib:
-
Objective response rate of 25.0% (7 partial responses of 28
patients)
-
Stable disease rate of 60.7% (17 of 28 patients)
-
Disease control rate at 6 months of 57.1% (16 of 28 patients)
-
The preliminary median progression-free survival (PFS) of dalantercept
plus axitinib is 8.3 months across all dose levels tested in part 1.
-
The median PFS of the 0.9 mg/kg cohort has not yet been reached.
-
The most common treatment emergent adverse events were fatigue,
diarrhea, dysphonia and peripheral edema. There were no grade 4 or 5
related adverse events.
-
Common adverse reactions expected with axitinib such as diarrhea,
hypertension, palmar-plantar erythrodysesthesia, and proteinuria did
not increase in incidence or severity when combined with dalantercept.
For reference, in the axitinib AXIS phase 3 study, in the large subgroup
of sunitinib-refractory patients treated with single-agent axitinib, the
objective response rate was 11.3% and the median progression-free
survival was 4.8 months.
Key details for the ongoing part 2 of the DART study (randomized,
double-blind):
-
Part 2 of the DART study is open for enrollment of patients who have
received one VEGFR TKI and may have also received 1 prior mTOR
inhibitor and/or any number of prior immune therapies.
-
Based on the results from Part 1, dalantercept 0.9 mg/kg was selected
as the dose level in Part 2 of the DART study.
The poster and presentation slides are available on Acceleron’s website (www.acceleronpharma.com)
under the Publications section.
About the DART Phase 2 Clinical Trial in RCC
The phase 2 DART clinical trial is a two-part study in patients with
advanced renal cell carcinoma. Part 1 is a dose-escalation study of
dalantercept in combination with axitinib to evaluate the safety and
tolerability of the combination in patients whose disease has progressed
following one to three lines of prior therapy. Part 2 is a randomized,
double-blind study of 130 patients with advanced renal cell carcinoma
who have progressed following treatment with a VEGF receptor tyrosine
kinase inhibitor. Patients may have also received prior mTOR therapy
and/or immunotherapy. The objective of the study is to determine whether
treatment with dalantercept in combination with axitinib prolongs
progression-free survival compared to treatment with placebo plus
axitinib. For additional information on this clinical trial, please
visit www.clinicaltrials.gov,
identifier NCT01727336.
About Dalantercept
Dalantercept (ACE-041) is an investigational protein therapeutic that
inhibits angiogenesis by preventing BMP9, a protein in the TGF-β
superfamily, from interacting with activin receptor-like kinase 1
(ALK1), a cell-surface receptor found on proliferating vascular
endothelial cells. Dalantercept inhibits ALK1 signaling, which is
required for the development of mature, functional vasculature.
About Acceleron
Acceleron is a clinical stage biopharmaceutical company focused on the
discovery, development and commercialization of novel protein
therapeutics for cancer and rare diseases. The company is a leader in
understanding the biology of the Transforming Growth Factor-Beta (TGF-β)
protein superfamily, a large and diverse group of molecules that are key
regulators in the growth and repair of tissues throughout the human
body, and in targeting these pathways to develop important new
medicines. Acceleron has built a highly productive R&D platform that has
generated innovative clinical and preclinical protein therapeutic
candidates with novel mechanisms of action. These protein therapeutic
candidates have the potential to significantly improve clinical outcomes
for patients with cancer and rare diseases.
For more information, please visit www.acceleronpharma.com.
Contacts:
Acceleron Pharma
Steven Ertel, 617-649-9234
Senior Vice
President and Chief Business Officer
or
Media:
Suda
Communications LLC
Maureen L. Suda, 585-387-9248
Source: Acceleron Pharma
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