Lecture #13 - Biotech 1 Flashcards

1
Q

Therapeutic proteins - non-human sources:

What problem? (2)

A

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2
Q

Therapeutic proteins - human sources:

What problems could this cause? (3)

A

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3
Q

Therapeutic proteins - recombinant human proteins:

What does this allow?

A

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4
Q

Recombinant insulin - how is it done?

A

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5
Q

List 3 advantages and 2 disadvantages of using prokaryotic systems

A

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6
Q

Erythropoitein (EPO):

  1. When was this gene cloned?
  2. What kind of PTM does this go through?
  3. What is this PTM important for?
  4. What is this protein made in?
  5. How many aa’ is this protein and is that big/small?
  6. How many and what kind of secondary structure?
  7. What kind of protein is it (enzyme, transporter etc)
  8. Produced mainly by what?
A

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7
Q

Expression vector for EPO - what does it look like?

A

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8
Q

EPO regulated haematopoeiesis:

  1. Its synthesis and release is regulated (in part) by what? What does this mean if you are in a low oxygen environment?
  2. Epo stimulates what two things?
A

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9
Q

What two things can affect EPO levels (leading to what?)

How can you restore red blood cell levels?

A

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10
Q

Why is EPO used as a performance enhancing drug? (3)

A

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11
Q

Detecting EPO - how? What’s the problem with that nowadays?

A

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12
Q

Recombinant antibodies:

  1. Why are they increasingly being used?
  2. Most therapeutic AB target what?
A

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13
Q

Making an AB to TNF-alpha:

  1. Why target this? (2)
  2. What was developed to bind and neutralise TNF-alpha?
  3. What is a monoclonal AB?
  4. How do you make a mAB?
  5. What problems could this cause?
A

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14
Q

Infliximab:

What is it?

A

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15
Q

Since cells can’t perform all PTM equally well (e.g. gla which is needed for blood clotting processes), what do they do now? What example did she use?

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16
Q

What two next big things?

A

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17
Q

What is pharming?

A

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