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Drug discovery > Ion channel drug screening steps > Flashcards

Ion channel drug screening steps Flashcards

1
Q

Drug discovery screening steps

A 
Target selection and validationi
primary screen
secondary screen
lead optimisation
safety + toxicity 
efficacy 
clinical trials
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2
Q

What is primary screening?

A
  • Determining molecular targets
  • How they correlate to disease
  • Where are they found in the body?
  • Pathways and roles
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3
Q

How to do primary/pre-screening

A
  • Genetics – sequencing, family traits
  • In vitro – cellular models
  • Manual patch clamp
  • In vivo – animals e.g., mouse
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4
Q

Primary screen steps

A
  • Large amounts of compound (100k)
  • High throughput screening
  • Identify active compounds against specified targets
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5
Q

How to do primary screening details

A
  • Radio-flux assays - Use radioisotopes of key ions – track where they go - sodium, calcium etc
  • Voltage/ion sensitive dyes/fluorophores which detect voltage and ion changes
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6
Q

Pros of radio flux and dyes

A
  • Can do large screening
  • High throughput – tests millions of samples rapidly
  • Quite cheap
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7
Q

CONS of radio-flux and dyes

A
  • Radioactive – so careful with handling and waste
  • Indirect measure for ion channel activity which can lead to false positives/negatives
  • Provide limited qualitative data
  • No real-time data/mechanism of action
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8
Q

What is secondary screening?

A

About 1-20k compounds
• Put through medium/high throughput screening
• Identify most active compounds against target
• Selectivity screens against similar channels

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9
Q

How to do secondary screening?

A

• Automated patch clamp e.g., Qpatch

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10
Q

Pros of automated patch clamp

A
  • Data rich
  • High quality
  • Mechanism of action can be determined
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11
Q

New changes to screening methods?

A
  • Scientists want to do just one big APC screening rather than 1 and 2
  • Save time and resources
  • Better than doing the whole radioactive bla
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12
Q

What is lead optimisation?

A
  • Chemically improve the secondary screen approved compounds
  • Look at Absorption, distribution, metabolism and excretion
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13
Q

What is the Lipinski rule of 5?

A
  • Found that most successful drug-like compounds share physical properties
  • The best drugs have:
  • MWt < 500
  • Solubility < 5
  • <5 H-bond donors
  • < 10 H-bond acceptors
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14
Q

Safety and toxicity

A
  • Target selectivity over other ion channels
  • Ion channel cardiac safety pharmacology
  • Therapeutic index – measure safety of drug
  • TI = Toxic dose/effective dose
  • High TI = bigger window of drug effect
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15
Q

Efficacy

A
  • Animal models
  • Show the efficacy In mouse for example
  • Animal to human translation?
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Drug discovery (8 decks)

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