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Incyte Corporation
today announced that eleven abstracts
detailing its emerging development pipeline will be presented at the 2015
American Association for Cancer Research (AACR) Annual Meeting in
Philadelphia, PA. These abstracts include characterizations of Incyte's FGFR,
BRD and PIM inhibitors as potential targeted therapies for cancer, as well as
data supporting the potential immuno-therapeutic activity of the company's
portfolio of JAK and PI3Kδ inhibitors alone and in combination, including with
epacadostat, Incyte's leading IDO1 inhibitor.
"We are excited to be able to present such a deep and broad portfolio of
emerging therapeutics from our own discovery research," stated Reid Huber,
PhD, Incyte's Chief Scientific Officer. "Incyte is a company founded on the
premise that investment in good science and the rigorous pursuit of R&D
excellence can translate into new medicines which can improve patients' lives.
The presentations we are making at AACR this week provide compelling evidence
that our teams are fulfilling this vision."
The Company also provided an updated presentation of its clinical portfolio,
which now includes INCB54828, a potent and selective FGFR inhibitor and
INCB50465, a PI3Kδ inhibitor, which entered clinical trials in Q1 2015 for
solid tumors and B-lymphoid malignancies. INCB54329, a bromodomain inhibitor,
is expected to enter clinical trials in Q2 2015 in hematology oncology.
Additional first-line pancreatic cancer patients are being recruited into the
expansion cohort of JAK1-selective inhibitor INCB39110 in combination with
gemcitabine and nab-paclitaxel to continue the dose optimization phase of this
proof-of-concept trial. Incyte therefore no longer expects to initiate a
pivotal trial of INCB39110 in first-line pancreatic cancer during 2015.
Abstracts
691: Stubbs et al., Activity of the BET inhibitor INCB054329 in models of
multiple myeloma. Sunday, Apr 19, 2015, 1:00 PM - 5:00 PM.
692: Stubbs et al., The BET inhibitor INCB054329 is synergistic with JAK1
inhibition in models of multiple myeloma. Sunday, Apr 19, 2015, 1:00 PM - 5:00
PM.
771: Liu et al., Preclinical characterization of the selective FGFR inhibitor
INCB054828. Sunday, Apr 19, 2015, 1:00 PM - 5:00 PM.
779: Li et al., Blockade of the IL-6/JAK/STAT3 signaling pathway inhibits
pancreatic tumor cell growth in 3D spheroid cultures and in xenograft models.
Sunday, Apr 19, 2015, 1:00 PM - 5:00 PM.
1336: Koblish et al., Novel immunotherapeutic activity of JAK and PI3Kδ
inhibitors in a model of pancreatic cancer. Monday, Apr 20, 2015, 8:00 AM
-12:00 PM.
2671: Shin et al., INCB050465, a novel PI3Kδ inhibitor, synergizes with PIM
protein kinase inhibition to cause tumor regression in a model of DLBCL.
Monday, Apr 20, 2015, 1:00 PM - 5:00 PM.
3523: Liu et al., Discovery of a novel BET inhibitor INCB054329. Tuesday, Apr
21, 2015, 8:00 AM -12:00 PM.
3525: Liu et al., The BET inhibitor INCB054329 is efficacious as a single
agent or in combination with targeted agents in colorectal cancer models.
Tuesday, Apr 21, 2015, 8:00 AM -12:00 PM.
5397: Shin et al., Characterization of INCB053914, a novel pan-PIM kinase
inhibitor. Wednesday, Apr 22, 2015, 8:00 AM -12:00 PM
5414: Koblish et al., Activity of the pan-PIM kinase inhibitor INCB053914 in
models of multiple myeloma. Wednesday, Apr 22, 2015, 8:00 AM -12:00 PM.
5416: Koblish et al., Activity of the pan-PIM kinase inhibitor INCB053914 in
models of acute myelogenous leukemia. Wednesday, Apr 22, 2015, 8:00 AM -12:00
PM.
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