Prestigious Nature Publication Highlights Novel PTEN Cancer Approach with Prescient’s PTX-100
June 18 2017 - 8:08PM
Business Wire
- PTX-100 effective in inhibiting
newly-identified cancer causing pathway
- The combination of PTX-100 and
photodynamic therapy is highly effective in cancers with defective
PTEN
- Potential to also combine PTX-100 with
PTX-200 in PTEN defective cancers
Clinical-stage oncology company Prescient Therapeutics Ltd
(ASX:PTX; Prescient) announced that a pre-clinical study published
in the scientific journal Nature this week indicates that
Prescient’s geranylgeranyl transferase inhibitor GGTI-2418, known
as PTX-100, plays a key role in mitigating a new cancer pathway
discovered by Professor Michele Pagano at New York University’s
Langone Medical Center, in New York. Nature is regarded as one of
the world’s most cited and prestigious scientific publications.
In the study, Professor Pagano’s group in collaboration with
Prescient’s Chief Scientific Officer Professor Said Sebti
demonstrated new details about the tumor suppressor gene, PTEN,
which is defective in 30-60% of certain breast, brain and uterine
cancers.
“When defective, PTEN cannot control a protein known as FBXL2,
which is thought to be responsible for cancer growth in many
patients,” said Professor Pagano.
Professor Pagano’s study also showed in mouse models that when
administered with Prescient’s drug candidate PTX-100, plus
photodynamic therapy, FBXL2 is “switched-off” allowing abnormal
cells to self-destruct. Therefore, patients whose tumors harbor
defective PTEN may also be more likely to respond to a combination
of PTEN and photodynamic therapy.
Professor Said Sebti said, “These findings have important
translational implications for Prescient as patients whose tumors
harbor defective PTEN may be more likely to respond to a
combination of PTX-100 and photodynamic therapy.”
“Furthermore, given that PTEN is known to also suppress the Akt
tumor survival pathway, patients with PTEN defective tumors could
respond to a combination of PTX-100 and an Akt inhibitor like
PTX-200.”
Prescient’s CEO and Managing Director, Steven Yatomi-Clarke
said, “This discovery of a new cancer-causing pathway targeted by
PTX-100 is an exciting development for Prescient. Our precision
medicine strategy uses targeted therapies to address specific
cancer mutations. Therefore, this discovery opens up a new frontier
of clinical possibilities for PTX-100.”
“PTEN has been the subject of cancer research for many years,
but this new study is very exciting in showing a novel way in which
defective PTEN adds to cancer risk, and more importantly,
demonstrates that it can be inhibited with PTX-100.”
PTX-100 was developed by Professor Sebti, Chair of the
Department of Drug Discovery at H. Lee Moffitt Cancer Center, and
Chief Scientific Officer at Prescient Therapeutics, and NYU
President Andrew Hamilton while he was at Yale University. PTX-100
has already been tested as a single agent in patients with advanced
solid tumors in a Phase 1 trial and will be the focus of studies in
rare hematological malignancies.
The Nature publication can be previewed at www.nature.com.
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Prescient Therapeutics LimitedSteven Yatomi-Clarke, +61 417 601
440CEO & Managing DirectororWE BuchanKyahn Williamson, +61 401
018 828kwilliamson@buchanwe.com.au
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