Gene Therapy Flashcards

1
Q

Definition of gene therapy

A

Use of recombinant genetic material (DNA, RNA, hybrid molecules) under different forms or pharmaceutical preparations as a therapeutic agent

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2
Q

Definition of non integrating

A

Transgene not inserted into host DNA so it is not constantly expressed

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3
Q

Definition of integrating

A

Transgene inserted into host DNA so it is constantly expressed

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4
Q

What is gene therapy

What is legal

A

Recombinant genetic material (DNA, RNA, hybrid molecules) under different forms or pharmaceutical preparations as a therapeutic agent

Only somatic gene therapy is legal
Germline gene manipulation is illegal => designer babies

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5
Q

What are the 2 gene therapy delivery protocols

A

In vivo
-viruses containing recombinant genetic material is injected into the body part affected

Ex vivo

  • haematopoietic target cells isolated and infected with RGM
  • recombinant SC expanded and reinfused
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6
Q

What are the 3 components of gene therapy protocol

What is the most ideal cell target

A

Target tissue

  • Accessible
  • Manipulable

Efficient gene delivery

  • Viral vector
  • Non viral vector

Transcriptional control

  • Sufficiently high
  • Sustained

Pluripotent
Self regenerating stem cells from patient being treated

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7
Q

What are the 4 main viral gene therapy vectors

What are their fates post delivery

A

Adenovirus, non integrating
Adeno associated, non integrating
Retrovirus, integrating
Lentivirus, integrating

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8
Q

Describe the use of retro and lentiviruses

A
  1. Remove disease causing gene
  2. Insert plasmids that encode for the gene and proteins that can make the virus
    Does not have genes for further replication
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9
Q

How is transcription regulated

  • transient
  • long term
A

Transient

  • for acquired diseases
  • use non replicating viruses
  • repeated administration
  • target tissue specific promotors/enhancers

Long term

  • for inherited and acquired diseases
  • stable integration of transgenic material
  • negate chromatin interference of expression with LCRs
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10
Q

What should you watch out for when using retroviruses

A

Only transduce dividing cells

Preferential integration near/in genes being actively transcribed in targeted cells at time of transduction
-if uncontrolled => insertion into genes that control cell

Need to stabilise promoter for transgene
-if not done => promoter methylated and silenced

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11
Q

Describe current gene therapy

A

Viral vectors can successfully used but must be designed to be more reliable

Gene therapy medicines are currently being used

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12
Q

What are the potential developments in gene therapy

A

In vivo targeted gene delivery systems
Efficient non viral vectors
Minimise risks such as insertional mutagenics

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