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The HT-RNAi-based Target Validation Program Efficient, Detailed Functional Analyses in Human Cells
The selection of candidate genes worthy of exploitation as
drug development targets requires a crucial but difficult
prioritization process, made all the more expensive
and complex nowadays by the plethora of targets candidates now on the
market. Indeed, the widespread application of first generation
functional genomics technologies in recent years has resulted in a
large increase in new targets discovered, creating a new bottleneck in
the process: the need for large-scale target validation.
The advent of RNAi technology has offered arguably the best tool
available to date for addressing this need. In particular, the
application of RNAi at high throughput (HT) in combination with high
content (HC) readouts in human cells allows the efficient yet detailed
validation of large collections of
target candidates. The resulting target prioritization processes
are inherently more meaningful, as they are based on the analysis of
loss-of-function phenotypes, i.e. the type of cell-based experimental
data that offers highest patho-physiological relevance and predictive
value for the development of antagonist-type therapeutics.
The RNAi-based Target Validation Program at Cenix has emerged from
the company's pioneering expertise in carrying out genome-scale HT-RNAi
studies, integrating a diverse range of HC readouts. This background
has ideally prepared the company for taking on virtually any scale and
scope of target validation project. Having applied HT/HC-RNAi in multiple disease areas
using a wide range
of human and rodent cells for industry clients and academic
partners
alike, Cenix scientists are uniquely experienced at combining their own
assays with those of our partners and clients to build-up target
validation programs that are fully-customized for their needs.
The extensive expertise available at Cenix for developing
multiplexed cell-based assays offers the particularly powerful ability
to efficiently carry out
comprehensive profiling of
RNAi-induced phenotypes. The value of this approach derives not
only from the need to characterize the desired loss-of-function
phenotype, but also, and perhaps even more importantly, to broaden the analysis window
so as to maximize the ability to detect undesirable aspects of a
target's associated phenotypes as early as possible.
Indeed, a key guiding principle of Cenix's philosophy in building
target validation and prioritization programs is the concept of Target Invalidation:
making all possible efforts to extract the most comprehensive and
predictive datasets that can be obtained from in vitro cell-based experimentation
not only to confirm "winners"
but also to eliminate false leads at this early stage when
investments
are still relatively modest, before much larger downstream expenses are
incurred. Such
- testing a target's possible involvement in other pathways known
to be beneficial or problematic;
- surveying broader range of cellular components and processes;
- surveying results from several
cell lines of different tissue derivations;
- monitoring more time points
to better understand the kinetics of a given phenotype;
The RNAi Profiling
approach therefore offers an ideal way of efficiently generating
broader, more predictive validation datasets that will not only
facilitate target prioritization in the short-term, but also greatly
strengthen the scientific basis for securing regulatory approvals in
the long-term.
Target validation projects at Cenix, especially the ones
starting from large collections of genes, are typically structured in
two
stages:
- Prioritization stage: a
primary, streamlined set of multiplexed assays is applied to eliminate
"false leads" and select those targets that warrant the more in-depth
analysis;
- Profiling stage: a more
comprehensive program of cell-based analyses, jointly designed with the
client, is applied to those targets selected above, making
maximal use
of multiplexed assays to generate the most complete yet most
cost-efficient profile possible.
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Typical Project Outline
for a Large-Scale HT-RNAi Target Validation Study:
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