DD- Future approaches Flashcards

1
Q

Issues in drug development

A

Sustainability (increasing costs)

Risk aversion

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2
Q

What is pharmacogenomics

A

Drug development for small groups of population

Based on individual genomic factors which contribute to drug response

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3
Q

HER-2 overexpression example of pharmacogenomics

A

O/E 20% breast, and in gastric ca patients

Clinical trials for Trastuzumab

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4
Q

Advantages of pharmacogenomics

A
Efficient, potent disease targetting
Improved safety profile
Better dosing ability
Earlier screening implementations
Reduced costs
-Less ADRs and failures, shorter duration treatment
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5
Q

Issues in pharmacogenomics

A

Target validation
Higher development costs (~30% higher)
Ethics of marking disorders

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6
Q

Target validation issues in pharmacogenomics

A

Are polymorphisms consistent
Does the gene product produce a functional protein
Is the gene expressed for the entirety of the disease progression

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7
Q

What is biopharmaceuticals- examples

A

Genetically modified proteins (large molecule drugs) used therapeutically

Vaccines, recombinant proteins, blood/tissue products, synthetic peptides, gene/cell therapy, monoclonal antibodies

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8
Q

Properties of biopharmaceuticals

A
Species-specific* (issues with dev?)
Long acting
Parenteral administration
Eliminated by degradation/ catabolism
Relatively unstable (heat-sensitive, contamination)
Cannot cross the BBB
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9
Q

Generations of biopharmaceuticals

A
1st gen (artificial human proteins prepped by transfection)
2nd gen (Proteins GM'd pre transfection to improve efficacy)
3rd gen (Novel proteins with specific target functions)
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10
Q

Monoclonal antibodies-features

A

Immunoglobulins used to recognise a specific antigen
Targetting immune, inflammatory, oncological disease

1st gen (murine antibodies; induced HAMA response- toxicity)

2nd gen (chimeric 67% or humanised 100%)
- have improved efficacy due to affinity maturation (b ell cloning w/reduced chance of immune response)

ADCs (mAbs bound to small molecule drugs via biodegradable covalent links to improve targetting)
- Increased tolerability and lower toxicity

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11
Q

Monoclonal antibody examples

A

Secukinumab for Ankylosing spondylitis
IL-17a mAb which is key inflammatory mediator in AS
RCT: reduced clinical/biological features of AS, well tolerated

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12
Q

Issue with preclinical mAb testing

A

Species specific effects- primates most effective
-Repro tox not feasible (abortions, long gestation)

Alternative: GM mice with surrogate antibodies
-Can support chronic/repro tox

Long time to generate; species cross reactivity may still not prove safety- cytokine storm

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13
Q

Advantages of biopharmaceuticals

A

Less unexpected toxicity
Quicker discovery process (no screening/lead optomisation)
Reduced infection risk
Less need for routine gentox

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14
Q

Disadvantages of biopharmaceuticals

A

Expensive (complex purification process)
Not orally active
Short plasma t1/2
Don’t cross BBB

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15
Q

Biotechnology example

A

Implantable Drug Delivery Devices for metastatic cancer pain
-Pain occurs in 67% patients
RCT of IDDD showed 20% reduction in pain score and QoL for treatment group
Issues with terminal patients

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16
Q

Pharmacogenomic example schizophrenia

A

Gene polymorphisms identified for variability in Dopamine D2/3 receptor response
-14 novel gene markers identified based on pharmacodynamic mouse assays of efficacy
PDE7B identified to be related to risperidone response

17
Q

Potential approaches for improving DD

A

Reducing cycle times
Enhance the hit rate
Increase links with academia