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1
Nanoparticles
• Size: 1 to 100 nm
• Organic and inorganic in nature
• Metalic, liposomes and dendrimers etc.
• Used as carrier molecules
• Problems- toxic, non-degradable and non-specific
2
Viral nanoparticles - a versatile nanomachine
Saurav Saha
(2014-11-106)
Centre for Plant Biotechnology and Molecular Biology
College of Horticulture
3
Outline
• Introduction to virus
• Virus as a nanomachine
• Development of viral nanoparticles
• Applications
• Challenges
• Recent achievements
• Summary
• Conclusion
4
Introduction to virus
 Naturally occurring biomolecule
 Size- 15 to 2000 nm
 Rod-like or spherical in shape
 Capsid- outer protein coat
 Genomic material- DNA or RNA
 Deliver genome in host cells
5
(Grasso and Santi, 2010 )
• High strength of capsid protein
• Polyvalent and self-assembly process
• Monodisperse structure
• Mass production of viruses
6
(Alexander et al., 2013)
Virus as a nanomachine
7
(Kristopher et al., 2015)
…virus as a nanomachine
Development of viral nanoparticle
8
Virus
Genetic
engineering
Bioconjugation Biomineralization Encapsulation
Modifications
• Epitope sequence
• Targeting sequence
• Unnatural amino acid
9
(Merzlyak et al., 2008)
Genetic engineering approach
 Coating of various substances within another material
 Assemble and de-assemble in-vitro
 Artificial polymer, enzyme, metallic nanoparticles
10
Encapsulation
(Carissa et al., 2010)
 pH > 6.5- swells and release RNA molecule
 pH decreases- PSS molecule assemble and entrapped
Polystyrene encapsulation
11
(Soto et al., 2010)
Biomineralization
Accumulation of minerals in cells and tissues
12
(Wang et al., 2012)
Contd…
13
BVSE- Biomineralized- based virus shell engineering
CAR- Coxsackie virus and adinovirus receptor
(Wang et al., 2012)
Bioconjugation
Two main strategies
 Standard bioconjugation chemistries
 Copper-catalyzed azide-alkyne cycloaddition
14
(Smith et al., 2013)
Standard bioconjugation chemistries
15(Smith et al., 2013)
 Azides and alkynes in the presence of copper
 Popularly known as click reaction
 Conjugation of protein building block
Copper-catalyzed azide-alkyne cycloaddition
16(Smith et al., 2013)
Application of viral nanoparticles
17
Viral nanoparticles
(VNP)
Targeted drug
delivery
Vaccines Imaging
Plant disease
management
Targeted drug delivery
 Reduce drug toxicity and degradation
 Target particular organ
 Increase bioavailability and circulation
18
( Nicholas et al., 2014)
 Anti-cancer drug
 Poor selectivity
 High cardio toxicity
Doxorubicin (DOX) delivery
19
(Zeng et al., 2013)
FA- Folic acid
Cytotoxicity of various DOX formulations at
different DOX concentration
20( Zeng et al., 2013)
0
10
20
30
40
50
60
70
80
90
Dox CMV-DOX CMV-FA-DOX
Apoptoticpercentage
 DOX concentration (5 µg/ml) incubate for 3 hr
Effect of DOX on cardiomyocytes cells
21
( Zeng et al., 2013 )
Vaccine Production
Virus like particles (VLPs)
Antigen stability
Potential to carry two or more different antigen (chimera)
22( Kristopher et al., 2015)
Flock house virus VLP production
23
( Destito et al., 2009 )
Universal influenza vaccine from VLP
 Globally 250,000–500,000 deaths annually
 Virus continually evolving
 H1, H2, H5, H6, H7, H10, and H11 hemagglutinin subtypes
 Universal vaccine are most effective
24
(Kang et al., 2009)
.…universal influenza vaccine from VLP
 Mice vaccinated with mixture of 1.5g each of H1, H3, H5, and
H7 VLPs
 Mice were boosted at 21 days post immunization
 After 35 days of immunization
 Mice are infected with different strains of virus
25
(Kang et al., 2009)
Effect of homologous challenge
26(Kang et al., 2009)
Bodyweight(%)
Survival(%)(Days)
H1N1
Effect of heterosubtypic challenge
27
Bodyweight(%)
Survival(%) Days
H6N1
(Kang et al., 2009)
Days
VLP type Antigen Indication Product
name
Status Reference
Non-
enveloped
Virus structural
protein
HBV GenHevac B® Licensed Soulie et al.,
1991
Non-
enveloped
Virus structural
protein
HPV Cervarix® Licensed Agnandji et
al., 2012
Non-
enveloped
(chimeric)
Parasite protein Malaria RTS,S Phase 1 El-Attar et
al.,
2009
Enveloped
(virosome )
Parasite protein Malaria PEV3 Phase 1/2 Cech et al.,
2011
HBV-Hepatitis B virus
HPV-Human papilloma virus
Other types of VLP based vaccine
28
Vaccine for tumor/ cancer
29
 Tn glycan over expressed
 Low immunogenicity of carbohydrates (Tn)
 Induce a strong T cell-dependent immune
 Cowpea mosaic virus (CMV) conjugate with Tn glycoprotein
( Miermont et al., 2008 )
0
2000
4000
6000
8000
10000
12000
14000
16000
day 0 day35 day 35+
GAlNac
day 35
comtrol
Titre
ELISA titres of anti-Tn conjugate with CMV
30
(GAINac- Tn antigen) ( Miermont et al., 2008 )
control IgG control IgM
Series1 10000 5000
0
2000
4000
6000
8000
10000
12000Titre
Titre of different types antibodies
31( Miermont et al., 2008 )
 Visual representation of internal structures
 Synthetic dye ,quantum dot and green fluorescent protein
 Low sensitive and photo stability
 VNP used as carrier for imaging dye
32
Imaging
( Yoo et al., 2012)
Intravital vascular imaging
Fd- Florescine dextran
A4d- A488 dextran
Rhl- Rhadomine-leveled
33
(Lewis et al., 2006)
Effect of injection of viral nanoparticle based
fluorescence dye on mouse
34(Lewis et al., 2006)
In -vivo stability of fluorescent viral
nanoparticles
35
( Yoo et al., 2012)
 Worldwide crop damage - 157 million dollar
 Highly toxic contact and fumigant nematicides
 Abamectin (Abm)- biologically active compound
 Immobile in soil and photo-oxidative in nature
 VNPs used as carrier for abamectin
Plant parasitic nematode control
36
Red clover necrotic mosaic virus (RCNMV) as VNP
37( Richard et al., 2015)
Performance of VNP loaded abamectin
Time (Hour)
pH 5.2
A- Within 5 hours 95% of the chemical diffuse out
B- Within 5 hours 25% of the chemical diffuse out
38( Richard et al., 2015)
pH 5.2
A B
Effect of VNP loaded abamectin on tomato
seedling
39Gall No gall ( Richard et al., 2015)
Recent achievements
40
• Herpes virus- genetically modified
• BioVex company in USA
• FDA approval for treating cancer
• Brand name imlygic
Cancer-hunting virus
41
(Bell et al., 2015)
Carbon-free hydrogen fuel
 Hydrogenase enzyme
 Protons (H+) and electrons (e-) into molecules of H2
 P22 bacteriophage coat protein to encapsulate
 Mixed with Protons and electrons-ferrying molecules
 Hydrogen produced inside a virus
42
( Robert et al., 2015 )
Challenges
• Purity in compound
• Encapsulate contaminants
• Manufacturing- not scalable or cost-effective
• Structural complexity
• Baculovirus as a vector
43
(Crisci et al., 2012 )
Summary
 Viral nanoparticles
 Features of viral nanoparticles
 Modification strategies
 Targeted drug delivery, vaccination and imaging
 Plant disease control
 Major Challenges
44
• VNPs used as biological nanocarrier
• Enormous application in biomedical and agriculture
• Modification- chemical and genetic
• Drug, toxin and targeted sequence
1/17/2016 45
Conclusion
46
“Where Nature finishes producing its own species, man
begins, using natural things and with the help of this
nature, to create an infinity of species”
Leonardo-Da-Vinci
1/17/2016 47
Thank you

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viral nanoparticles

  • 1. 1
  • 2. Nanoparticles • Size: 1 to 100 nm • Organic and inorganic in nature • Metalic, liposomes and dendrimers etc. • Used as carrier molecules • Problems- toxic, non-degradable and non-specific 2
  • 3. Viral nanoparticles - a versatile nanomachine Saurav Saha (2014-11-106) Centre for Plant Biotechnology and Molecular Biology College of Horticulture 3
  • 4. Outline • Introduction to virus • Virus as a nanomachine • Development of viral nanoparticles • Applications • Challenges • Recent achievements • Summary • Conclusion 4
  • 5. Introduction to virus  Naturally occurring biomolecule  Size- 15 to 2000 nm  Rod-like or spherical in shape  Capsid- outer protein coat  Genomic material- DNA or RNA  Deliver genome in host cells 5 (Grasso and Santi, 2010 )
  • 6. • High strength of capsid protein • Polyvalent and self-assembly process • Monodisperse structure • Mass production of viruses 6 (Alexander et al., 2013) Virus as a nanomachine
  • 7. 7 (Kristopher et al., 2015) …virus as a nanomachine
  • 8. Development of viral nanoparticle 8 Virus Genetic engineering Bioconjugation Biomineralization Encapsulation Modifications
  • 9. • Epitope sequence • Targeting sequence • Unnatural amino acid 9 (Merzlyak et al., 2008) Genetic engineering approach
  • 10.  Coating of various substances within another material  Assemble and de-assemble in-vitro  Artificial polymer, enzyme, metallic nanoparticles 10 Encapsulation (Carissa et al., 2010)
  • 11.  pH > 6.5- swells and release RNA molecule  pH decreases- PSS molecule assemble and entrapped Polystyrene encapsulation 11 (Soto et al., 2010)
  • 12. Biomineralization Accumulation of minerals in cells and tissues 12 (Wang et al., 2012)
  • 13. Contd… 13 BVSE- Biomineralized- based virus shell engineering CAR- Coxsackie virus and adinovirus receptor (Wang et al., 2012)
  • 14. Bioconjugation Two main strategies  Standard bioconjugation chemistries  Copper-catalyzed azide-alkyne cycloaddition 14 (Smith et al., 2013)
  • 16.  Azides and alkynes in the presence of copper  Popularly known as click reaction  Conjugation of protein building block Copper-catalyzed azide-alkyne cycloaddition 16(Smith et al., 2013)
  • 17. Application of viral nanoparticles 17 Viral nanoparticles (VNP) Targeted drug delivery Vaccines Imaging Plant disease management
  • 18. Targeted drug delivery  Reduce drug toxicity and degradation  Target particular organ  Increase bioavailability and circulation 18 ( Nicholas et al., 2014)
  • 19.  Anti-cancer drug  Poor selectivity  High cardio toxicity Doxorubicin (DOX) delivery 19 (Zeng et al., 2013) FA- Folic acid
  • 20. Cytotoxicity of various DOX formulations at different DOX concentration 20( Zeng et al., 2013)
  • 21. 0 10 20 30 40 50 60 70 80 90 Dox CMV-DOX CMV-FA-DOX Apoptoticpercentage  DOX concentration (5 µg/ml) incubate for 3 hr Effect of DOX on cardiomyocytes cells 21 ( Zeng et al., 2013 )
  • 22. Vaccine Production Virus like particles (VLPs) Antigen stability Potential to carry two or more different antigen (chimera) 22( Kristopher et al., 2015)
  • 23. Flock house virus VLP production 23 ( Destito et al., 2009 )
  • 24. Universal influenza vaccine from VLP  Globally 250,000–500,000 deaths annually  Virus continually evolving  H1, H2, H5, H6, H7, H10, and H11 hemagglutinin subtypes  Universal vaccine are most effective 24 (Kang et al., 2009)
  • 25. .…universal influenza vaccine from VLP  Mice vaccinated with mixture of 1.5g each of H1, H3, H5, and H7 VLPs  Mice were boosted at 21 days post immunization  After 35 days of immunization  Mice are infected with different strains of virus 25 (Kang et al., 2009)
  • 26. Effect of homologous challenge 26(Kang et al., 2009) Bodyweight(%) Survival(%)(Days) H1N1
  • 27. Effect of heterosubtypic challenge 27 Bodyweight(%) Survival(%) Days H6N1 (Kang et al., 2009) Days
  • 28. VLP type Antigen Indication Product name Status Reference Non- enveloped Virus structural protein HBV GenHevac B® Licensed Soulie et al., 1991 Non- enveloped Virus structural protein HPV Cervarix® Licensed Agnandji et al., 2012 Non- enveloped (chimeric) Parasite protein Malaria RTS,S Phase 1 El-Attar et al., 2009 Enveloped (virosome ) Parasite protein Malaria PEV3 Phase 1/2 Cech et al., 2011 HBV-Hepatitis B virus HPV-Human papilloma virus Other types of VLP based vaccine 28
  • 29. Vaccine for tumor/ cancer 29  Tn glycan over expressed  Low immunogenicity of carbohydrates (Tn)  Induce a strong T cell-dependent immune  Cowpea mosaic virus (CMV) conjugate with Tn glycoprotein ( Miermont et al., 2008 )
  • 30. 0 2000 4000 6000 8000 10000 12000 14000 16000 day 0 day35 day 35+ GAlNac day 35 comtrol Titre ELISA titres of anti-Tn conjugate with CMV 30 (GAINac- Tn antigen) ( Miermont et al., 2008 )
  • 31. control IgG control IgM Series1 10000 5000 0 2000 4000 6000 8000 10000 12000Titre Titre of different types antibodies 31( Miermont et al., 2008 )
  • 32.  Visual representation of internal structures  Synthetic dye ,quantum dot and green fluorescent protein  Low sensitive and photo stability  VNP used as carrier for imaging dye 32 Imaging ( Yoo et al., 2012)
  • 33. Intravital vascular imaging Fd- Florescine dextran A4d- A488 dextran Rhl- Rhadomine-leveled 33 (Lewis et al., 2006)
  • 34. Effect of injection of viral nanoparticle based fluorescence dye on mouse 34(Lewis et al., 2006)
  • 35. In -vivo stability of fluorescent viral nanoparticles 35 ( Yoo et al., 2012)
  • 36.  Worldwide crop damage - 157 million dollar  Highly toxic contact and fumigant nematicides  Abamectin (Abm)- biologically active compound  Immobile in soil and photo-oxidative in nature  VNPs used as carrier for abamectin Plant parasitic nematode control 36
  • 37. Red clover necrotic mosaic virus (RCNMV) as VNP 37( Richard et al., 2015)
  • 38. Performance of VNP loaded abamectin Time (Hour) pH 5.2 A- Within 5 hours 95% of the chemical diffuse out B- Within 5 hours 25% of the chemical diffuse out 38( Richard et al., 2015) pH 5.2 A B
  • 39. Effect of VNP loaded abamectin on tomato seedling 39Gall No gall ( Richard et al., 2015)
  • 41. • Herpes virus- genetically modified • BioVex company in USA • FDA approval for treating cancer • Brand name imlygic Cancer-hunting virus 41 (Bell et al., 2015)
  • 42. Carbon-free hydrogen fuel  Hydrogenase enzyme  Protons (H+) and electrons (e-) into molecules of H2  P22 bacteriophage coat protein to encapsulate  Mixed with Protons and electrons-ferrying molecules  Hydrogen produced inside a virus 42 ( Robert et al., 2015 )
  • 43. Challenges • Purity in compound • Encapsulate contaminants • Manufacturing- not scalable or cost-effective • Structural complexity • Baculovirus as a vector 43 (Crisci et al., 2012 )
  • 44. Summary  Viral nanoparticles  Features of viral nanoparticles  Modification strategies  Targeted drug delivery, vaccination and imaging  Plant disease control  Major Challenges 44
  • 45. • VNPs used as biological nanocarrier • Enormous application in biomedical and agriculture • Modification- chemical and genetic • Drug, toxin and targeted sequence 1/17/2016 45 Conclusion
  • 46. 46 “Where Nature finishes producing its own species, man begins, using natural things and with the help of this nature, to create an infinity of species” Leonardo-Da-Vinci

Notas do Editor

  1. and a defined identical protein subunits
  2. Nanoscale structure and dimensions(15 nm -2 μm)
  3. Nanoencapsulation is the coating of various substances within another material at sizes on the nano scale. This technique is already commonplace within a range of industries but it is accepted that only around 10% of potential applications are being exploited.
  4. multiprotein structure Mimic- organization and structure
  5. result numerous distinct strain of virus
  6. Streptomyces avermitilis Macrocyclic lactone metabolites Broad spectrum of nematodes Inability to pass the blood brain barrier Immobile in soil and photo-oxidative in nature