What Physiologists Working in Industry Do

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What Physiologists Working in Industry Do

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Title: What Physiologists Working in Industry Do

1
What Physiologists Working in Industry Do

Liaison with Industry Committee (LWIC)
American Physiological Society

2
Objective
The purpose of this presentation is to 1) inform
you about the responsibilities and types of work
a Physiologist performs as a member of the
pharmaceutical, biotech, or nutritional industry
and 2) describe some of the primary personal
attributes necessary to succeed in this
environment.
3
Science and Drug Discovery

The drug discovery process requires concerted
efforts of scientists
across many disciplines (Biochemists,
Chemists, Molecular Biologists,
Pharmacologists, Physiologists, Technologists,
etc) to advance a
project from initial scientific principles (an
idea or hypothesis) to a
clinical candidate, and ultimately a drug to
treat human disease.
This extremely challenging undertaking is
pursued under strict
guidelines regulated by federal (i.e. FDA,
USDA) and international
(EMEA) agencies. Successful drug discovery
requires critical
thinking, organizational skills, creativity,
as well as flexibility and
resourcefulness.
In short, success in drug discovery requires
well-trained, disciplined,
and rigorous scientists. The process is one
in which Physiologists
can assume many critical roles. Do you fit
these criteria?

4
Scope of Scientific Activities of Physiologists
in Drug Discovery

Activities are listed from first discovery
principles (hypothesis generation and
testing) to clinical trials and submission of an
NDA (New Drug Application)
Target discovery and validation
Proof-of-concept studies
Development of in vitro efficacy models
Mechanism of compound action
Development of in vivo models (normal function
and disease)
Pharmacokinetic studies
Pharmacodynamic studies
Assay development
Ex vivo functional studies
Disease efficacy testing
Development and utilization of biomarkers
Safety pharmacology
Interpretation of clinical results
Exploration of additional indications
Regulatory submission for product and claim
approval

5
Description of Bench Science Activities of
Physiologists in Industry (Part I)

Target Discovery and Validation Studies of
disease mechanisms
using molecular and genomic approaches
including genetic
association studies in humans, knockout and
transgenic animals,
engineered tool compounds to identify or
confirm a biochemical
target

Proof-of-Concept Studies Studies are conducted
to address the
questions does the enzyme, receptor, channel,
etc play a role in
the physiological or disease process? Is the
target of interest be
activated/inactivated in this process?

In Vitro Efficacy Testing Develop and use
assays to test the
hypothesis in simple systems such as isolated
proteins and/or
cell-based systems. These assays may often
use high-throughput
or multiplexed (multiple readouts) platforms.

6
Examples of Bench Science Activities of
Physiologists in Industry (Part II)

Mechanism of Compound Action Studies are
designed to address
questions such as does the compound affect
enzyme, ion channel,
or receptor activity? Does the compound affect
a specific signaling
pathway? Does the compound affect genetic
regulation (expression)
of the target?

Development of Disease Models Studies are
designed to address
questions such as does the cell, tissue, or
animal model resemble
the human condition? Is the model valid?
(i.e. does the
pathophysiology respond to current
pharmacotherapies?)

7
Examples of Bench Science Activities of
Physiologists in Industry (Part III)

Pharmacokinetic (PK) Studies generally
considered in terms of what
the organism does to drug and studies are
designed to address
questions such as what is the maximal plasma
concentration of drug
after dosing and when does this occur? how
much drug gets to the
tissue of interest and how widely is the drug
distributed in the body?
how quickly is the drug cleared after dosing?
Pharmacodynamic (PD) Studies generally
considered in terms of
what the compound does to the organism and
studies are designed
to address questions such as is the
biochemical target affected by the
compound and to what extent? Is the tissue
of interest affected?

8
Examples of Bench Science Activities of
Physiologists in Industry (Part IV)

Ex vivo functional studies Evaluation of
integrated tissue or whole
organ function with ability to carefully
control dose, duration, and
exposure to compound (e.g. isolated working
heart, isolated perfused
kidney, isolated blood vessel, brain slice,
etc)

Disease efficacy testing Acute and/or chronic
studies are conducted
to address questions such as does the
compound modify disease
progression in vivo (i.e. prevention model)?
Can the compound
regress the disease (treatment model)? How
does the efficacy of
the compound compare to existing
pharmacotherapies or potential
co-therapies?

Development and utilization of biomarkers
Studies are conducted to investigate whether
there a quantifiable blood or urinary biochemical
marker that predicts severity or progression of
the disease? Can the marker serve as a surrogate
for long-term efficacy of the compound?

9
Examples of Bench Science Activities of
Physiologists in Industry (pt V)

Exploration of additional indications Evaluate
experimental results and literature to determine
whether additional scientific opportunities exist
(i.e. does the mechanism of action or signaling
pathway play a role in other conditions other
than the primary indication?)

Interpretation of clinical results mechanistic
and/or theoretical
evaluation of unexpected clinical events
(utilization and identification of
appropriate biomarkers to track mechanistic
or pathophysiological
responses to agent).

Preclinical safety pharmacology Studies are
designed to address
questions such as what is the therapeutic
index of the compound?
What is the incidence of adverse events in
major organ systems (e.g.
cardiovascular, renal, gastrointestinal,
respiratory, CNS) at multiples
(3x, 10x, 30x) of therapeutic plasma
concentrations of the compound?

10
Non-Bench Science Activities of Physiologists in
Industry

Industry scientists have many
responsibilities beyond benchwork
Training and supervision of technical staff
Generation of novel scientific and technical
hypotheses
Rigorous design, analysis, and interpretation of
experiments
Presentation of scientific concepts and business
applications of
research to various professionals to enable
business and scientific
decisions
Participation in project team and strategic
planning meetings
Writing of technical reports and scientific
manuscripts
Documentation of all scientific observations and
submitting patents
Planning facility development and resource
(people, space, equipment)
deployment
Participation in the preparation and submission
of documents (IND
Investigational New Drug NDA New Drug
Application) to the Food
Drug Administration (FDA)

11
Personal Attributes of Successful Industry
Scientists(Part I)

To be successful in discovering and developing a
new drug, you must
participate in a process that requires concerted
efforts by many people
across many departments and disciplines.
Specific attributes are required
to succeed in this fast-paced environment
Critical Thinking Industry scientists identify
key issues and deliver
timely scientific responses to discovery
projects and business
development opportunities
Team and Collaborative Behavior Industry
scientists network with
internal/external scientists to assure access
to current and innovative
technologies and scientific advances.
Interpersonal Skills The drug discovery and
development process is a
huge undertaking, successful industry
scientists foster a cooperative
spirit, and work well with other scientific,
regulatory, clinical, and
business professionals.

12
Personal Attributes of Successful Industry
Scientists (Part II)

Strong Communication Skills Effective
communication of ideas
whether one on one, in small groups, or
through formal presentations.
Writing is clear, well-organized and
logically developed the audience
is taken into consideration.
Efficiency The demands on an industry scientist
are many (various
experimental models to run and multiple
compounds to test). Thus,
industry scientists are constantly challenged
to implement new processes
to streamline procedures while maintaining
rigorous standards.
Flexibility Effectively initiates change as
needed and adapts to
necessary changes in operations or
strategies also initiates new ways
of accomplishing work.
Leadership Industry scientists drive
operational plans and develop
and implement tactics to deliver results by
set timelines. Leads by
appropriate actions and behaviors inspires
and guides others to
achieve corporate and personal goals.

13
Physiologists in IndustryTarget Discovery and
Validation
Target discovery studies investigate disease
mechanisms using molecular and genomic approaches
in knockout and transgenic animals.
Physiologists use these approaches to identify or
confirm a role for biochemical targets in organ
and organism function and dysfunction. Below
gene knockout of PKCa improves cardiac
performance following pressure overload (TAC),
while transgenic overexpression of PKCa impairs
cardiac performance.
Overexpression of PKC? (Prkca) in transgenic mice
reduces cardiac ventricular performance
PKC? knockout (Prkca -/-) mice have enhanced
cardiac ventricular performance
Reprinted with permission from Braz et al. Nature
Med 10(3), 2004
14
Physiologists in IndustryProof-of Concept
Studies
Proof-of-concept studies address whether a
biochemical target plays a role in a disease
process (i.e. is the target of interest
activated, inhibited or differentially expressed
in disease?) Physiologists use various approaches
to learn whether a biochemical target is involved
in disease. Lower left panel over-expression of
the cardiac enzyme, calcineurin (CN) transgenic
mouse, induces cardiac hypertrophy lower right
panel aortic-banding increases cardiac CN
expression (A) and activity (B), treatment with
CsA, a CN, inhibitor prevents aortic-banding
induced cardiac hypertrophy (C).
C
Reprinted with permission from Molkentin Circ Res
87, 2000
Reprinted with permission from Lim et al.
Circulation 101, 2000
15
Physiologists in IndustryIn Vitro Efficacy
Testing
In vitro efficacy studies employ assays utilizing
simple systems (e.g. isolated proteins and/or
cell-based systems). These preparations allow
Physiologists to carefully control experimental
conditions and compound concentrations while
measuring and comparing responses and behaviors
of large numbers of compounds. Below a
classical competition curve utilizes radioligand
binding techniques to evaluate the ability of
compound Y to compete for receptor subtype
binding, in turn generating affinity and potency
data.
16
Physiologists in IndustryMechanism(s) of
Compound Action
Enalapril blocks the blood pressure response
to Angiotensin I The mechanism of action is the
antagonism of angiotensin converting enzyme
100
80
60
inhibition of the mean arterial pressure
response to Angiotensin I bolus
40
20
0
-120
-60
0
60
120
180
240
300
360
Time (min)
Angiotensin I
Enalapril
(300 ng/kg, IV)
(10 mg/kg)
17
Physiologists in IndustryDevelopment of Disease
Models
Ultimately, drugs developed through the discovery
process must be able to modify disease
progression and outcome. Physiologists develop
models of disease for drug discovery, and must
have an thorough understanding of normal and
pathologic ranges of functional parameters. A
valid disease model must involve many of the
critical biochemical pathways and display many
clinical findings of the human disease state.
Below Surgical instrumentation and induction of
chronic pacing-induced heart failure.
Surgical Instrumentation
Pacing-Induced HF and Recovery

Cardiac function and coronary flow are measured
in the conscious state by chronic
instrumentation.
Heart failure (elevated end diastolic pressure,
reduced ejection fraction and cardiac reserve) is
induced by right ventricular pacing for 3-4
weeks.
Recovery from heart failure is allowed by the
termination of pacing for 5-6 weeks after
developed heart failure.

18
Physiologists in IndustryPharmacokinetic Studies
Pharmacokinetic studies characterize how the body
handles a compound. Physiologists work
alongside Medicinal and Bioanalytical Chemists to
determine if a compound is orally bioavailable
and will achieve adequate plasma and tissue
exposure and duration prior to undertaking an
efficacy or chronic disease modification study.
Below Oral administration of Compound X (10 mpk)
exhibited good fractional bioavailability (F
54) and plasma half-life (t1/2 6 hours).
19
Physiologists in IndustryPharmacodynamic Studies
Pharmacodynamic studies characterize the effects
of a compound on the body. Certain enzymes are
activated (e.g. phosphorylated) or modified (e.g.
glycosylated) in disease processes. For example,
to determine if a compound will inhibit an enzyme
of interest, Physiologists determine whether
enzyme phosphorylation and kinase activity are
suitable pharmacodynamic indices for compound
activity. Below intraperitoneal administration
of a physiological stimulus dose-dependently
increased enzyme phosphorylation and kinase
activity, providing a model to assay compound
activity against this enzymes activity.
Western Blot Phosphorylated Enzyme
Immunoprecipitation Kinase Assay
vehicle
3 mpk
10 mpk
p-TXXX
p lt 0.01 vs. vehicle

Total Enzyme

p lt 0.01 vs. vehicle
0.12
0.10

0.08
p-TXXX / Total enzyme
0.06
0.04
0.02
0.00
vehicle
3 mpk
10 mpk
20
Physiologists in IndustryEx Vivo Functional
Studies
Ex vivo studies evaluate integrated organs and
organ systems from normal and diseased organisms.
These preparations allow Physiologists to
carefully control experimental conditions and
organ compound exposures while measuring and
comparing functional responses in normal and
diseased organs. Below an isolated working
heart preparation allows careful control of
preload, afterload, heart rate, and compound
exposure.
Cardiac Systolic Performance Endpoints LV
Systolic Pressure mmHg LV End Diastolic
Pressure mmHg Left Atrial Pressure mmHg
Aortic Mean Pressure mmHg Max
/-dP/dt mmHg/sec Peak Pressure mmHg Time
to Peak Press (TPP) msec TPP/PP msec/mmHg Dias
tolic Function Endpoints tau msec 1/2
Relaxation Press (1/2 RP) mmHg 1/2 Relaxation
Time (RT1/2) msec (RT1/2) / (1/2 RP) msec/mmHg
21
Physiologists in IndustryDisease Efficacy
Studies
Drugs developed through the discovery process
must show efficacy in modifying disease
progression and outcome. Physiologists develop
models of disease for drug discovery, and are
required to have a thorough understanding of
normal function as well as the pathology of
disease states. Last, models of human diseases
for drug discovery must be amenable to standard
pharmacotherapies. Below Effects of varying
delay (7 day vs. 30 days post-MI) of ACE
inhibitor treatment on a) survival, b) cardiac
hemodynamics, and c) morphology after myocardial
infarction (MI).
b
a
c
untreated
ACEi 30d post-MI
ACEi 7d post-MI
Reprinted with permission from Mulder et al.
Circulation 95, 1997
22
Physiologists in IndustryDevelopment and
Utilization of Biomarkers
Blood and/or urinary biochemical markers that are
correlated to disease severity allow tracking of
disease progression and regression following drug
therapy. Physiologists a) develop disease models
that have biomarker profiles similar to those
observed in human disease, b) evaluate biomarker
responses to standard and novel therapeutic
agents, and c) develop assays to quantify
biomarkers. Below Kaplan-Meier survival curve
for mortality and morbidity in human heart
failure patients based on plasma brain
natriuretic peptide (BNP) concentrations. Thus,
plasma BNP is associated with disease severity
and may be used in place of more expensive and
time-consuming assays.
Reprinted with permission from Anand et al.
Circulation 107, 2003
23
Physiologists in IndustryPreclinical Safety
Pharmacology