Personalis Presents Data from New Platform Features at the Society for Immunotherapy of Cancer (SITC) 37th Annual Meeting
November 07 2022 - 04:05PM
Business Wire
Personalis, Inc. (Nasdaq: PSNL) today announced that the company
will share data resulting from expanded features of its NeXT
Platform® at the Society for Immunotherapy of Cancer (SITC) Annual
Meeting, November 8-12 in Boston, with three abstracts that
highlight advanced R&D applications of next-generation
sequencing (NGS) in immuno-oncology.
"To understand the complex dynamics of cancer and ultimately
better predict response to therapy, we need to advance the tools
we're using to characterize the tumor microenvironment. We continue
to build upon the suite of technologies in our ImmunoID NeXT
Platform® to enable the high-resolution study of immuno-oncology
targets in an array of contexts, including improved neoantigen
prediction, immune-composition profiling, and composite biomarker
signatures,” said Sean Boyle, PhD, Executive Director of
Bioinformatics Science at Personalis.
The company will present the following posters at SITC2022, as
well as with customers including the Parker Institute for Cancer
Immunotherapy (Abstracts 559 and 587) and Geneos Therapeutics
(Abstracts 691 and 692).
Title: A combination of antigen presentation and T-cell
recognition features improves neoantigen immunogenicity predictions
(Abstract 51)
Overview: Tumor neoantigen burden outperformed tumor
mutational burden in prediction of patient response to checkpoint
inhibitor immunotherapy by better capturing the biological
mechanism underlying response. However, immune recognition of
neoantigens by T-cells requires more than antigen presentation,
which has been the focus of tumor neoantigen burden thus far. To
address this need, we extend the existing SHERPA® MHC-presentation
framework to predict neoantigen immunogenicity. By combining
antigen presentation and T-cell recognition features in a
two-tiered model, we can better predict immunogenic neoantigens and
make progress towards using neoantigens as biomarkers to assess
checkpoint inhibitor efficacy.
Title: Sensitive prediction of immunotherapy response by
integrating immune infiltration and neoantigen presentation score
in late-stage melanoma (Abstract 119)
Overview: Single-modality biomarkers such as tumor
mutational burden (TMB) often fail to reliably predict response to
immune checkpoint blockade (ICB), likely due to incomplete
characterization of the complex tumor-immune interactions that
influence treatment efficacy. We previously developed the composite
biomarker, neoantigen presentation score (NEOPS™), which integrates
neoantigen processing and presentation potency, and showed it
outperformed TMB and other single-modality biomarkers in predicting
ICB response in melanoma. Here, we combined NEOPS with the
assessment of tumor immune infiltration and demonstrated more
accurate patient stratification for ICB response.
Title: Transcriptome augmentation provides accurate and
sensitive quantification of genes associated with the tumor
microenvironment (Abstract 146)
Overview: While malignant cells dictate much of the tumor
biology, there is evidence that the tumor microenvironment (TME)
also plays a significant role in disease progression and response
to therapy. The role of the immune cells is particularly relevant
in immunotherapy, and multiple transcriptome-based biomarkers have
shown utility in predicting the efficacy of immune checkpoint
blockade. However, little is known about the benefits of enhancing
the depth and uniformity of transcriptome sequencing coverage for
quantifying the TME cell type composition. Using the ImmunoID NeXT
Platform®, which combines high-quality exome and transcriptome
sequencing with advanced informatics to comprehensively
characterize the tumor and TME from a single FFPE tumor sample,
applying augmented transcriptome coverage to the assessment of TME
benefited the identification of marker genes for cell type
enrichment analysis without introducing bias.
About Personalis
Personalis, Inc. is a leader in advanced cancer genomics,
enabling the next generation of precision cancer therapies and
diagnostics. The Personalis NeXT Platform® is designed to adapt to
the complex and evolving understanding of cancer, providing its
biopharmaceutical customers and clinicians with information on all
of the approximately 20,000 human genes, together with the immune
system, from a single sample. To enable cancer sequencing,
Personalis' Clinical Laboratory was built with a focus on clinical
accuracy, quality, big data, scale and efficiency. The laboratory
is GxP-aligned as well as Clinical Laboratory Improvement
Amendments of 1988-certified and College of American
Pathologists-accredited. For more information, visit the Personalis
website and News Center and follow Personalis on LinkedIn and
Twitter.
Forward-Looking Statements
All statements in this press release that are not historical are
“forward-looking statements” within the meaning of U.S. securities
laws, including statements relating to attributes or advantages of
the NeXT Platform, Personalis’ business opportunities, leadership,
plans or expectations, or other future events. Such forward-looking
statements involve risks and uncertainties that could cause actual
results to differ materially from any anticipated results or
expectations expressed or implied by such statements. Factors that
could materially affect actual results can be found in Personalis’
filings with the U.S. Securities and Exchange Commission, including
Personalis’ most recent reports on Forms 8-K, 10-K and 10-Q, and
include those listed under the caption “Risk Factors.” Personalis
disclaims any obligation to update such forward-looking
statements.
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version on businesswire.com: https://www.businesswire.com/news/home/20221107006051/en/
Investor Relations Contact for Personalis: Caroline
Corner investors@personalis.com 415-202-5678
Media Contact for Personalis: Jennifer Temple
pr@personalis.com 650-752-1300
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