(a) Structure of Mass Spectrometer - PowerPoint PPT Presentation

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(a) Structure of Mass Spectrometer

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(a) Structure of Mass Spectrometer A=Vaporization Chamber B=Ionization Chamber C=Accelerating Chamber D=Deflection Chamber E=Ions detector (a) Functions for each ... – PowerPoint PPT presentation

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Title: (a) Structure of Mass Spectrometer


1
(a) Structure of Mass Spectrometer
  • AVaporization Chamber
  • BIonization Chamber
  • CAccelerating Chamber
  • DDeflection Chamber
  • EIons detector

2
(a) Functions for each parts of Mass
Spectrometer
  • AVaporization Chamber
  • BIonization Chamber
  • CAccelerating Chamber
  • DDeflection Chamber
  • EIons detector
  • to vaporize the sample to be tested by heat
  • molecules are bombarded by alpha/beta rays to
    form cations
  • cations are accelerated by a strong electric
    field
  • cations are deflected by strong magnetic field
    according to their mass/charge ratio
  • amounts of ions are proportional to the electric
    current detected

3
(b) Give two reasons why such kind of mass
spectrometer cannot be used to determine the
molecular mass of biomolecules.
  • (1) Because biomolecules are thermal labile,
    they would decompose in the evaporation chamber
    under strong heating
  • (2) The biomolecules would be cracked by the
    bombardment with alpha/beta rays in the
    ionisation chamber

4
(b) Name the two parts in the traditional
mass spectrometer which were replaced by
electrospray ionization (ESI) technique.
Explain why such a technique can be used to
study biological macromolecules.
  • ESI technique can replace the vaporization
    chamber and ionization chamber.
  • As no heating and bombardment with high energy
    particles to the bio-macromolecules are required
    by using electrospray ionization technique, the
    bio-molecules would not decompose.

5
(d) Name the two parts in the traditional mass
spectrometer which were replaced by soft laser
desorption (SLD) technique. Explain why such a
technique can be used to study biological
macromolecules.
  • SLD technique can replace the vaporization
    chamber and ionization chamber.
  • As no heating and bombardment with high energy
    particles to the bio-macromolecules are required
    by using soft laser desorption technique, the
    bio-molecules would not decompose.

6
(e) State two advantages of applying ESI and SLD
techniques in Mass Spectrometer to study
biological macromolecules.
  • The method is superior to other methods in the
    rapidity, sensitivity and identification of the
    actual interaction.
  • This analytical methods are relatively cheap,
    enabling them to spread quickly to laboratories
    all around the world.
  • By having a surface that cancer cells adhere to
    and then analysing this with soft laser
    desorption chemists can discover cancer faster
    than doctors can.
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