Prothena Presents New Data for Alzheimer’s and Parkinson’s Disease
Programs at AD/PD 2022
Prothena Corporation plc (NASDAQ:PRTA), a late-stage clinical
biotechnology company with a robust pipeline of investigational
therapeutics built on protein dysregulation expertise, presented
new preclinical data from both its dual Aβ/tau vaccine for the
potential treatment and prevention of Alzheimer’s disease (AD) and
from its tandem C-terminal α-synuclein vaccine programs for the
potential treatment and prevention of Parkinson’s disease (PD) and
related synucleinopathies. The data were presented at the
International Conference on Alzheimer’s and Parkinson’s Diseases
(AD/PD 2022), taking place March 15-20, 2022, in Barcelona, Spain.
Additionally, the scientific legacy of Dr. Dale
Schenk, late Co-Founder and CEO of Prothena, was honored at the
AD/PD 2022 opening ceremony. During this memorial, Dr. Dennis
Selkoe, the Vincent and Stella Coates Professor of Neurologic
Diseases at Harvard Medical School, Co-Director of the Ann Romney
Center for Neurologic Diseases at Brigham and Women’s Hospital and
Director on Prothena’s Board of Directors, celebrated the impact of
Dr. Schenk’s pioneering research. Dr. Schenk’s work spans
fundamental discoveries elucidating the roles that amyloid, gamma
secretase and beta secretase contribute to AD, to research that has
paved the way for multiple scientific and therapeutic breakthroughs
for patients suffering from AD and PD.
“The need for vaccines to prevent Alzheimer’s
and Parkinson’s diseases from ever occurring is urgent. We are
making exciting progress in that direction by combining our
unbiased Biology-Directed Engine and our know-how with the many
learnings from the development of therapies in Alzheimer’s and
Parkinson’s over the last several decades,” said Wagner M. Zago,
Ph.D., Chief Scientific Officer of Prothena. “At AD/PD 2022, we are
excited to present a wealth of data highlighting potential advances
across the therapeutic spectrum, from active treatment to
prevention of these devastating neurodegenerative diseases.
Specifically in Alzheimer’s, our dual Aβ/tau vaccine demonstrated,
in a preclinical setting, simultaneous generation of antibodies
against Aβ and tau with the proper quantity and quality of
response, while avoiding engagement of cytotoxic immune responses.
We continue to build momentum toward our ultimate goal of
eradicating Alzheimer’s disease and plan for an IND for this AD
vaccine candidate in 2023.”
Dual Aβ/tau
vaccine for the treatment and prevention of Alzheimer’s
disease
Preclinical data on Prothena’s dual Aβ/tau
vaccine were presented in an oral presentation
titled: Development of a Dual Aβ/tau Vaccine for the Treatment
and Prevention of Alzheimer’s Disease (Oral Presentation SO007 /
#814).
Prothena’s dual Aβ/tau vaccines were described
as linear peptide conjugates designed to prevent the two key
processes associated with AD: 1) the formation of Aβ-plaque and 2)
the development of intraneuronal tau tangles. The incremental
results from preclinical studies support the continued development
of this dual-epitope vaccine for the treatment and prevention of
AD.
Specifically, the findings presented at AD/PD
2022 provide proof of concept in multiple preclinical species for
Prothena’s dual Aβ/tau vaccine to address the desirable attributes
of quantity, quality and safety that have prevented the advancement
of safe and effective vaccines for the treatment or prevention of
AD. From a quantity standpoint, results demonstrated both the
generation of robust and balanced immunogenic responses against
pathogenic Aβ and tau in multiple animal species, demonstrating the
ability to overcome immunodominance. For quality, sera from
immunized animals inhibited the binding of soluble Aβ aggregates to
cultured hippocampal neurons and bound to Aβ plaques and tau
tangles in human AD brain sections at titers expected to be
achieved in the central nervous system in vivo, potentially
demonstrating strong immunoreactivity to Aβ and tau pathology. The
antibodies generated by these vaccines also induced phagocytosis
and blocked binding of tau to heparin, an analog of heparan sulfate
(HS). Tau-HS interactions are believed to be involved in both the
secretion of tau and its subsequent internalization into neurons.
For safety, the sera from immunized non-human primates did not
generate measurable cytotoxic T-cell responses to endogenous Aβ or
tau proteins.
Tandem C-terminal α-synuclein vaccine for the treatment
and prevention of Parkinson’s disease and other
synucleinopathies
Prothena presented preclinical data from a study
of Prothena’s tandem C-terminal α-synuclein vaccine in a poster
presentation titled: Development of C-Terminal α-Synuclein Vaccine
for Treatment and Prevention of Parkinson’s Disease and Other
Synucleinopathies (Poster P563 / #156).
The findings demonstrate that the lead vaccine
candidate with tandem C-terminal α-synuclein peptides resulted in
titers, with robust binding to pathogenic α-synuclein and
inhibition of uptake of soluble α-synuclein aggregates into cells,
when compared to immunization with vaccines containing a single
peptide sequence. The robust and functional characteristics of the
immune response following vaccination support the further
development of this approach for the potential treatment and
prevention of PD and related synucleinopathies.
Prothena leadership will participate in two AD/PD 2022
Forum Discussions
Anti-Tau Approaches In Clinical Trials Co-Moderators: Luc Buee
(France), William Jagust (USA)Wagner M. Zago, Ph.D., Chief
Scientific OfficerWednesday, March 16, 2022 - 17:30–18:30 CET
Amyloid-Removing Therapies: The Beginning Of The End Or The End
Of The Beginning?Co-Moderators: Al Sandrock (USA), Philip Scheltens
(The Netherlands)Gene Kinney, Ph.D., President and Chief Executive
OfficerSaturday, March 19, 2022 - 15:50–16:50 CET
Roche (partner) Presentations on
Prasinezumab
Results from the delayed-start analysis of Phase 2
PASADENA study of prasinezumab for the treatment of Parkinson’s
disease
Data from Phase 2 PASADENA study of
prasinezumab, first-in-class anti-α-synuclein antibody and the
focus of a worldwide collaboration with Roche, were presented in an
oral presentation titled: A 104-Week Delayed-Start Analysis of
PASADENA (Phase 2 Study Evaluating the Safety and Efficacy of
Prasinezumab in Early Parkinson’s Disease (Oral Presentation SO309
/ #408).
Results presented by Roche showed that
participants with PD who were treated with prasinezumab for two
years (early-start group) showed slower decline of Movement
Disorder Society-Unified Parkinson’s Disease Rating Scale
(MDS-UPDRS) Part 3 scores relative to participants treated with
prasinezumab for one year (delayed-start group).
Additional Roche (partner) presentations on prasinezumab
include:
Oral - Delayed Start Analysis of Roche PD Mobile
Application V2 In Pasadena Shows Persistent Positive Effects of
Prasinezumab on Bradykinesia Progression (Oral Presentation SO307 /
#123)
Poster - Estimating the Meaningful
Within-Patient Change Threshold for the MDS-UPDRS PART III (Poster
P595 / #407)
Poster - Non-motor Symptoms In Parkinson’s
Disease: A Systematic Review and Meta-analysis of Prevalence
(Poster OO229 / #418)
About Alzheimer’s Disease
Alzheimer’s disease is the most common form of
dementia causing increasingly serious symptoms, including
confusion, disorientation, mood and behavioral changes, difficulty
speaking, swallowing, and walking. Approximately 50 million people
worldwide are estimated to be living with Alzheimer’s disease or
other dementias. Alzheimer’s disease is the most common
neurodegenerative disorder. There is an urgent need for therapies
that slow the progression and ultimately prevent Alzheimer’s
disease to address this global healthcare crisis. Prothena’s
Alzheimer’s disease portfolio spans next generation antibody
immunotherapy, small molecule, and vaccine approaches, geared
toward building upon first generation treatments to advance the
treatment paradigm.
About Parkinson's Disease
Parkinson's disease is a progressive
degenerative disorder of the entire nervous system that affects one
in 100 people over age 60. An estimated 10 million people are
living with Parkinson's disease worldwide. It is the second most
common neurodegenerative disorder after Alzheimer's disease. The
disease is characterized by the neuronal accumulation of aggregated
alpha-synuclein in the CNS and peripheral nervous system that
results in a wide spectrum of worsening progressive motor and
non-motor symptoms. While diagnosis relies on motor symptoms
classically associated with Parkinson's disease, non-motor symptoms
may present many years earlier. Current treatments for Parkinson's
disease are symptomatic and only address a subset of symptoms such
as motor impairment, dementia, or psychosis. There are currently no
treatments available that target the underlying cause of the
disease and can slow its progression.
About Prothena
Prothena Corporation plc is a late-stage
clinical company with a robust pipeline of novel investigational
therapeutics built on protein dysregulation expertise with the
potential to change the course of devastating neurodegenerative and
rare peripheral amyloid diseases. Fueled by its deep scientific
expertise built over decades of research, Prothena is advancing a
pipeline of therapeutic candidates for a number of indications and
novel targets for which its ability to integrate scientific
insights around neurological dysfunction and the biology of
misfolded proteins can be leveraged. Prothena’s pipeline includes
both wholly-owned and partnered programs being developed for the
potential treatment of diseases including AL amyloidosis, ATTR
amyloidosis, Alzheimer’s disease, Parkinson’s disease and a number
of other neurodegenerative diseases. For more information, please
visit the Company’s website at www.prothena.com and
follow the Company on Twitter @ProthenaCorp.
Forward-looking Statements
This press release contains forward-looking
statements. These statements relate to, among other things, the
treatment potentials, designs, and proposed mechanisms of action of
our dual Aβ/tau vaccine, our α-synuclein vaccine, and prasinezumab;
plans for future clinical studies of our dual Aβ/tau vaccine; and
the continued advancement of our discovery, preclinical, and
clinical pipeline. These statements are based on estimates,
projections and assumptions that may prove not to be accurate, and
actual results could differ materially from those anticipated due
to known and unknown risks, uncertainties and other factors,
including but not limited to those described in the “Risk Factors”
sections of our Annual Report on Form 10-K filed with the
Securities and Exchange Commission (SEC) on February 25, 2022, and
discussions of potential risks, uncertainties, and other important
factors in our subsequent filings with the SEC. We undertake no
obligation to update publicly any forward-looking statements
contained in this press release as a result of new information,
future events, or changes in our expectations.
Contacts:MediaEric Endicott,
Senior Vice President, Corporate
Affairs650-448-3670, eric.endicott@prothena.com
InvestorsJennifer Zibuda, Director, Investor
Relations &
Communications650-837-8535, jennifer.zibuda@prothena.com
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