Aptose Biosciences Announces Results of Annual Meeting of Shareholders
06 Junio 2017 - 3:05PM
Aptose Biosciences Inc. (“Aptose” or the “Company”) (NASDAQ:APTO)
(TSX:APS), a clinical-stage company developing highly
differentiated therapeutics that target the underlying mechanisms
of cancer, today announced the voting results from the Company’s
annual meeting of shareholders held today, June 6, 2017 (the
“Meeting”).
The Company is pleased to announce that all of
the nominees listed in the management proxy circular dated April
18, 2017 were elected as directors. Each of the directors was
elected with greater than 94% of the votes cast by shareholders
present at the Meeting or represented by proxy. The results of the
vote are detailed below:
Nominee |
|
Votes For |
|
% Votes For |
|
Votes Withheld |
|
% Votes |
|
|
|
|
|
|
|
|
Withheld |
Dr.
Denis Burger |
|
4,942,137 |
|
94.88 |
|
266,640 |
|
5.12 |
Dr.
Erich Platzer |
|
4,942,126 |
|
94.88 |
|
266,651 |
|
5.12 |
Dr.
William G. Rice |
|
4,939,458 |
|
94.83 |
|
269,319 |
|
5.17 |
Dr.
Bradley Thompson |
|
4,931,745 |
|
94.68 |
|
277,032 |
|
5.32 |
Dr.
Mark D. Vincent |
|
4,943,710 |
|
94.91 |
|
265,067 |
|
5.09 |
Warren Whitehead |
|
4,944,586 |
|
94.93 |
|
264,191 |
|
5.07 |
Aptose shareholders also voted to re-appoint
KPMG LLP as auditor of the Company.
A total of 26.2% of the issued and outstanding
common shares of the Company were represented in person and by
proxy at the Meeting.
During the Annual Meeting of Shareholders, the
Company also provided a corporate update on CG’806 and APTO-253.
Data for CG’806 as a first-in-class pan-FLT3/BTK inhibitor were
presented in two poster presentations last month at the 2017 AACR
Hematologic Malignancies meeting held in Boston. In a study
conducted at The University of Texas MD Anderson Cancer Center,
CG’806 demonstrated superior potency against AML cells driven by
various mutant forms of FLT3 relative to competitive agents, and
achieved complete elimination of AML FLT3-ITD tumors in the absence
of toxicity in a murine model. A second poster highlighted studies
conducted at Oregon Health & Science University (OHSU) that
demonstrated the ability of CG’806 to potently kill primary
malignant cells in samples from patients with various hematologic
malignancies including AML, CLL and others. The posters can be
viewed at the Publications & Presentations section of the
Aptose website here. As noted previously, Aptose has
continued formal studies on APTO-253 in an effort to define the
root cause of recent manufacturing setbacks related to the
intravenous formulation, and to restore the molecule to a state
supporting clinical development and potential partnering. APTO-253
inhibits expression of the c-Myc oncogene, which highlights the
rationale to develop the molecule as a potential treatment for
AML.
Please refer to the Company’s management proxy
circular available on SEDAR at www.sedar.com or EDGAR
https://www.sec.gov/edgar.shtml for more details on the matters
covered at the Meeting. Final voting results on all matters
voted on at the Meeting will also be filed on SEDAR and EDGAR.
About Aptose
Aptose Biosciences is a clinical-stage
biotechnology company committed to developing personalized
therapies addressing unmet medical needs in oncology. Aptose is
advancing new therapeutics focused on novel cellular targets on the
leading edge of cancer. The Company's small molecule cancer
therapeutics pipeline includes products designed to provide single
agent efficacy and to enhance the efficacy of other anti-cancer
therapies and regimens without overlapping toxicities. For further
information, please visit www.aptose.com.
For further information, please contact:
Aptose Biosciences
Greg Chow, CFO
647-479-9828
gchow@aptose.com
SMP Communications
Susan Pietropaolo
201-923-2049
susan@smpcommunications.com
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