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Practical Applications in Virology

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T.Klimkait. 22.1.2004. Practical Applications. in Virology. Thomas Klimkait ... applications for virology. diagnostic need of real time PCR for quantification ... – PowerPoint PPT presentation

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Title: Practical Applications in Virology


1
Practical Applications in Virology
  • Thomas Klimkait
  • Institut für medizinische Mikrobiologie
  • Jan. 22, 2004

2
Viruses
  • are harmless Bystanders
  • cause economical Damage
  • cause Disease
  • have utility in Research

3
Where do we find them?
  • ... everywhere!
  • As phages in bacteria
  • (T-series, Lambda, ?X,..)
  • As pests or ornamenting tools in plants
  • (various mosaic viruses)
  • In vertebrates
  • (multiple forms of DNA- und RNA-viruses)

4
attractive Simplicity!
  • simple nucleid Acid
  • - DNA or RNA, ss or ds

5
Variation is broad (everything is possible)
Classification is tricky(no natural systematic)
6
what is practical?
  • genetic material can be exchanged
  • Genes/proteins can be highly amplified
  • (information can become inheritable)

7
Viruses as vectors
  • for laboratory cloning, expression
  • for therapy
  • delivery system for antigens (vaccine)
  • delivery system for lost genetic information
    (gene therapy)
  • delivery system for new genes/active intervention

8
Conzepts of vectors
retrovirus
9
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10
Gene Therapy
  • Adenoviruses
  • Adeno-associated Virus
  • Retroviruses
  • Caveats
  • immunogenicity
  • prior immunity
  • lacking integration into host genome
  • chromosomal integration

11
properties of persisting Viruses
12
  • Diagnositics employing Nucleic Acids
  • qualitative determination
  • after signal amplification by
  • PCR/LCR/b-DNA
  • gt is an RNA/DNA detectable? pos/neg
  • quantitative determination
  • competitive PCR/real-time PCR
  • gt how much RNA/DNA is present in sample

13
DNA-detection via Agarose Gel
14
real-time PCR
Q
15
applications for virology
  • diagnostic need of real time PCR for
    quantification
  • need for new tools for higher sensitivity
  • test systems for novel pathogens
  • systems for new properties (therapy escape)

16
break
17
US - AIDS Tote seit 1980
18
properties of retroviruses
  • envelope (gp120, gp41 trimer)
  • retrotranscription in the cell
  • genome integration (gt Provirus)
  • gene activation
  • separate expression for Gag and glycoproteins
  • RNA and Env transport to viral buds
  • viral protease mediates maturation
  • intracellular recombination!
  • high mutability, high error rate of RT

19
HIV-life cycle
host genome
20
Primoinfection with HIV
read- out
CD4-cells
Virus
time
21
A patient under HAART-therapy
22
drug-dosing
dosing suboptimal
23
  • per cycle

? 1 Virus gt gt103 particle/cell
  • sloppy copying

? 1 mutation / 1 genome
24
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25
HAART (Highly Active Anti-Retroviral Therapy)
26
Escape-Mutations - HIV Protease
saquinavir
27
1. Problem assignment of complex mutations
28
Genotyping
mutations need to be translated into Resistances!
29
2. Problem ambiguities in the interpretation
different algorithms use different rules
30
3. Problem mixed virus populations, viral
minorities (lt10)
  • single sequences will not exhaustively evaluate
    complex virus populations.
  • mixtures can be analyzed in parallel by the
    employment of culture systems.

31
from patient
rev
5LTR
gag
vpu
tat
nef
pol
env
3LTR
32
Phenotyping
33
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34
PhenoTect
35
4. Problem HIV subtypes
HIV is regionally quite different - different
sequence different response to therapy! -
resistances and metabolic parameters have to
be clarified regionally!
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