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THE PROBLEM

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sialic acid on cell surface (cell receptor) Release of Influenza Virus. Virus trapped on cell surface since haemagglutinin binds sialic acid. Neuraminidase aids ... – PowerPoint PPT presentation

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Title: THE PROBLEM


1
THE PROBLEM
  • Antiviral drugs must inhibit virus replication
  • BUT
  • viruses depend on host metabolic pathways

2
THE SOLUTION
  • Inhibit virus encoded proteins
  • with essential functions
  • BUT
  • must be specific

3
  • THERAPEUTIC INDEX
  • Minimum virus inhibitory dose
  • Minimum cell toxic dose
  • Should be at least 10 preferably 102-103

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5
THERAPEUTIC STRATEGIES
  • Inhibit virus replication at-
  • Attachment
  • Penetration/Uncoating
  • Nucleic acid synthesis
  • Assembly
  • Maturation
  • Release

6
NUCLEIC ACID SYNTHESIS
  • Viral DNA polymerase
  • Viral Reverse Transcriptase (RT)
  • Inhibited by nucleoside analogues

7
INHIBITION of VIRAL DNA POLYMERASE
  • ACYCLOVIR/ACICLOVIR for
  • Herpes simplex virus (HSV)
  • Varicella zoster virus (VZV)

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  • ACYCLOVIR (ACV) - MODE of ACTION
  • HSV VZV thymidine kinase? ACV-P
  • ACV-P ? ACV-PPP by cell
  • ACV-PPP inhibits viral DNA polymerase
  • Herpes simplex virus
  • Varicella zoster virus

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11
Acyclovir mechanism of action
nucleosides
Nuc-P
Nuc-P
Nuc-3P
Nuc-3P
HSV DNA polymerase
Herpesvirus-infected cell
Uninfected cell
12
  • RESISTANCE TO ACYCLOVIR
  • Common Virus TK absent
  • or
  • altered substrate specificity
  • Rarely Virus DNA polymerase
  • altered substrate specificity
  • Thymidine kinase

13
Drugs to bypass phosphorylation
  • ACV
  • ? Viral thymidine kinase
  • ACV-P
  • ? cellular kinases
  • ACV- PPP
  • ? viral DNA polymerase ? Foscarnet
  • Viral DNA

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16
RETROVIRUSES eg HIV
  • RT synthesises DNA from HIV RNA genome
  • RT inhibitors
  • Nucleoside
  • e.g. AZT (azidothymidine aka zidovudine)
  • Non-nucleoside
  • e.g. nevirapine
  • Reverse transcriptase

17
AZT
ACV
18
Acyclovir v Zidovudine (AZT)
  • AZT
  • ? Cellular kinases
  • AZT-P
  • ? cellular kinases
  • AZT- PPP
  • ? viral RT
  • Viral DNA
  • ?
  • Chain termination
  • ACV
  • ? Viral thymidine kinase
  • ACV-P
  • ? cellular kinases
  • ACV- PPP
  • ? viral DNA polymerase
  • Viral DNA
  • ?
  • Chain termination

19
NON-NUCLEOSIDE RT INHIBITORS
  • Act by allosteric inhibition
  • eg nevirapine

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22
THERAPEUTIC STRATEGIES
  • Inhibit virus replication at-
  • Attachment
  • Penetration/Uncoating
  • Nucleic acid synthesis
  • Assembly
  • Maturation
  • Release

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26
INHIBIT VIRUS PROTEASE TO INHIBIT VIRUS MATURATION
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34
  • DETERMINANTS of VIRAL RESISTANCE
  • Increased mutation rate
  • high virus replication
  • immunosuppression
  • RNA v DNA virus
  • Selection pressure
  • potent drug
  • lengthy treatment
  • BUT
  • No resistance if virus fully suppressed

35
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36
  • HIV - PROBLEMS WITH HAART
  • Expensive
  • Compliance
  • Cant eradicate latent virus
  • Viral load rebounds if stopped
  • Drug resistance
  • (RT no proof reading)

37
THERAPEUTIC STRATEGIES
  • Inhibit virus replication at-
  • Attachment
  • Penetration or fusion/Uncoating
  • Nucleic acid synthesis
  • Assembly
  • Maturation
  • Release

38
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39
T20 Binds to GP41 and Inhibits HIV Entry
40
THERAPEUTIC STRATEGIES
  • Inhibit virus replication at-
  • Attachment
  • Penetration or fusion/Uncoating
  • Nucleic acid synthesis
  • Assembly
  • Maturation
  • Release

41
6.2.13
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43
In endosome low pH activates M2 ion
channel Protons enter virus Uncoating of viral
nucleic acid proceeds
44
Amantadine blocks M2 prevents uncoating
Amantadine
Influenza virus envelope
M2 ion channel protein
45
6.2.17
46
THERAPEUTIC STRATEGIES
  • Inhibit virus replication at-
  • Attachment
  • Penetration/Uncoating
  • Nucleic acid synthesis
  • Assembly
  • Maturation
  • Release

47
NA inhibitor
6.2.19
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49
Influenza virus attachment
  • Haemagglutinin (virus attachment protein)
  • binds to
  • sialic acid on cell surface
  • (cell receptor)

50
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51
Release of Influenza Virus
  • Virus trapped on cell surface since
    haemagglutinin binds sialic acid
  • Neuraminidase aids release
  • Neuraminidase inhibitors block release

52
  • ANTIVIRAL THERAPY
  • Difficult since viruses are intracellular
  • Latent viruses cannot be eradicated

53
INHIBIT VIRUS REPLICATION AT
  • Fusion - HIV about to be licensed
  • Uncoating amantadine for influenza
  • Nucleic acid synthesis
  • - nucleoside analogues
  • - other e.g. foscarnet nevirapine
  • Maturation - HIV protease inhibitors
  • Release - Neuraminidase inhibitors
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