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 The term “dendrimer” is derived from the Greek
 words   “dendron” means tree or branches and
 “meros” means part.

 It was introduced in 1984 by Donald A. Tomalia.
 Highly branched
    macromolecule
   Capable of encapsulating
   High loading capacity
   Backbone of Carbons or
    Nitrogens
   Monodisperse and
    controllable
   Highly stable
   Low immunogenicity and
    toxicity
 The structure is highly defined and organized.


 Dendrimers posses 3 distinguishing architectural
 components:
   1) Initiator core.
   2) Interior layers.
   3) Terminal functionalities.
 They start from a core molecule with at least 3
 chemically reactive arms.

 To these arms, branches are attached.
      - Repeated many time
•Branches extend from core to periphery.


•Large dendrimers adopt a globular shape, in
which all bonds converge to a focal point


•“Star Burst Effect”.
 Monodispersive.


 Exact same molecular weight and structure.


 Peculiar behaviour of intrinsic viscosity
 The terminal groups affect solubility and viscosity




 The outer surface area of the molecule increases with the number of
  generations


 There are void space within the molecule.



 These unique geometries give the molecule special properties such as ability to
  entrap foreign molecules (drugs).
       Two common delivery systems

    1.    Liposome                   2. Polymers


         Poor stability
         Difficulty in targeting
         Toxicity
         Reduces circulation time
ENTANG L EMENTS




     Dendrimers             Linear Polymers

    less entanglements            more entanglement
.
Architecture

Dendrimers                                Linear Polymers
Dendritic architecture              Linear architecture
has been shown as                     has not been shown
elegant, uniform,                    as elegant and can be
spherical and as                      visualized as
“green peas”                       “ cooked spaghetti”.
e.g.                                 e.g Polyether linear
Polyether dendrimer.                 polymer
Size / Polydispersity



Dendrimers                   L inear Polymers
Have certain size,      Does not have
monodisperse            certain size and are    , .
 usually poly disperse.
Solubility

Dendrimers                    Linear Polymers
More solubility in           Less soluble than
organic solvent in           analogous dendrimer
comparison to the             in organic solvent
analogous linear              e.g. phenylene linear
polymer e.g.                 analogue.
1, 3, 5 phenylene
based dendrimer.
SYMMETRY

Dendrimers                          Hyper branched Polymers
Monodispersible regular            P olydispersible , neither
and highly symmetrical.            regular nor symmetrical.
                   SYNTHESIS

Obtained by careful ,               Obtained in a single step
stepwise growth of                  by poly condensation of
successive                          an A2B monomer.
generations.
   There are two defined methods of dendrimer
    synthesis:
       -Divergent
       -Convergent growth approach.

   In the divergent method the molecule is
    assembled from the core to the periphery.
 In  the divergent method, the surface groups
 initially are non-reactive or protected species which
 are converted to reactive species for the next stage
 of the reaction.

 In the convergent approach the opposite holds, as
 the reactive species must be on the focal point of
 dendritic wedge.
This type of synthesis involves two steps:

( 1 ) The activation of functional surface groups.

( 2 ) Addition of branching monomer units.
ADVANTAGE

 The advantage of this method is the ability to modify the
 surface of the dendrimer molecule.
 In successive generation growth, side reactions and
  incomplete additions become more apparent.
   This is due to steric hindrance.


 The overall yield is considerably small


 The outer generation has only one kind of functional
  group.
•The difficulty of many reactions that have to be
performed on one molecule is overcome by
starting the synthesis at the periphery and ending
at the core.
•In this method, growth begins at what will
become the periphery of the final macromolecule
and proceed inward, the final reaction being
attachment to a polyfunctional core.
 It involves the attachment of the outermost functional group
  to an inner generation and the attachment of the inner
  generation to the core.
 The structural units before the final attachment to the core is
  called the wedge.
 Usually 3 to 4 wedges attach to the core.
 Each wedge can have different functional groups at periphery.
Advantage of this method over “divergent growth”
 approach :-

 control over surface functionality.


 Ease for purification.
 More susceptible to steric inhibition at the focal point
    group.

 This effectively limits the size of the macromolecules
    that may be prepared in conventional fashion.

.
 Convergent approach affords better control to obtain a better
 dendrites architecture than the divergent approach.

 Divergent approach is for large scale production.


 Both involve stepwise processes that are tedious and time
 consuming.
 The well-defined structure, compact globular shape, size monodispersity
  and controllable „surface‟ functionalities of dendrimer makes them excellent
  candidates for evaluation as drug carriers.

 They can be used as drug delivery agents in 2 ways


  (1) Drugs molecules can be physically entrapped inside
      the dentritic structure.

  (2) Drug molecules can be covalently attached onto
      surface or other functionalities to afford dendrimer
      drug conjugates.
 The internal „cavity‟ of the dendritic structure can be
  used for the entrapment drugs.

( I ) FIRST STRATEGY: -
   First strategy for the encapsulation of the guest
   molecules in dendrimers is physical encapsulation.
 Held by Van der
  Waals or dipole
  moments
 Carrier compounds
  do not have to be
  solublized
1.   Targeted delivery would be difficult to achieve   because
     drug release occurred by dialysis.


2.    Difficult to make universal for all drugs, because
     encapsulation by the dendrimer varied significantly
     depending on drug and the dendrimer structure.
 The second strategy for the encapsulation of guest
  molecules in dendrimers is based on multiple non-
  covalent chemical interactions, such as hydrogen bonding
  between guest molecules and dendritic structure.

 Sustained release is possible.
 The third and the most easily implemented startegy
 for the encapsulation of drug molecules in
 dendrimers is making use of hydrophobic
 interactions

 Newkome et al. prepared dendritic macromolecules
 with a hydrophobic interiors and hydrophilic chain
 ends.

 These molecules were said to behave as unimolecular
 micelles capable of solubilizing various hydrophobic
 e.g.:- Poly (aryl ether) dendrimers bearing
 carboxylic groups as chain ends are able to
 enhance the water solubility of the
 hydrophobic compound such as pyrene and
 anthracene.
 Higher generation dendrimers
  have a greater number of end
  groups that can be functionalized
 Longer retention time in blood –
  PEG
 Targeting – ability to attach to
  certain tissues or active sites
 Imaging – Fluorescence, MRI, or
  X-ray
Applications in gene delivery
Dendrimers as Cancer Therapy

Therapeutic                   Cancer
      agent                   detector




  Reporter                    Cell death
                              monitor




       Water     Nanodevces
      molecule
A single dendrimer can carry a molecule
that recognizes cancer cells,

A therapeutic agent to kill those cells,

A molecule that recognizes the signals
of cell death
YOU

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Dendrimer

  • 1.
  • 2.  The term “dendrimer” is derived from the Greek words “dendron” means tree or branches and “meros” means part.  It was introduced in 1984 by Donald A. Tomalia.
  • 3.  Highly branched macromolecule  Capable of encapsulating  High loading capacity  Backbone of Carbons or Nitrogens  Monodisperse and controllable  Highly stable  Low immunogenicity and toxicity
  • 4.  The structure is highly defined and organized.  Dendrimers posses 3 distinguishing architectural components: 1) Initiator core. 2) Interior layers. 3) Terminal functionalities.
  • 5.  They start from a core molecule with at least 3 chemically reactive arms.  To these arms, branches are attached. - Repeated many time
  • 6. •Branches extend from core to periphery. •Large dendrimers adopt a globular shape, in which all bonds converge to a focal point •“Star Burst Effect”.
  • 7.  Monodispersive.  Exact same molecular weight and structure.  Peculiar behaviour of intrinsic viscosity
  • 8.  The terminal groups affect solubility and viscosity  The outer surface area of the molecule increases with the number of generations  There are void space within the molecule.  These unique geometries give the molecule special properties such as ability to entrap foreign molecules (drugs).
  • 9. Two common delivery systems 1. Liposome 2. Polymers  Poor stability  Difficulty in targeting  Toxicity  Reduces circulation time
  • 10. ENTANG L EMENTS Dendrimers Linear Polymers less entanglements more entanglement .
  • 11. Architecture Dendrimers Linear Polymers Dendritic architecture Linear architecture has been shown as has not been shown elegant, uniform, as elegant and can be spherical and as visualized as “green peas” “ cooked spaghetti”. e.g. e.g Polyether linear Polyether dendrimer. polymer
  • 12. Size / Polydispersity Dendrimers L inear Polymers Have certain size, Does not have monodisperse certain size and are , . usually poly disperse.
  • 13. Solubility Dendrimers Linear Polymers More solubility in Less soluble than organic solvent in analogous dendrimer comparison to the in organic solvent analogous linear e.g. phenylene linear polymer e.g. analogue. 1, 3, 5 phenylene based dendrimer.
  • 14. SYMMETRY Dendrimers Hyper branched Polymers Monodispersible regular P olydispersible , neither and highly symmetrical. regular nor symmetrical. SYNTHESIS Obtained by careful , Obtained in a single step stepwise growth of by poly condensation of successive an A2B monomer. generations.
  • 15. There are two defined methods of dendrimer synthesis: -Divergent -Convergent growth approach.  In the divergent method the molecule is assembled from the core to the periphery.
  • 16.  In the divergent method, the surface groups initially are non-reactive or protected species which are converted to reactive species for the next stage of the reaction.  In the convergent approach the opposite holds, as the reactive species must be on the focal point of dendritic wedge.
  • 17.
  • 18. This type of synthesis involves two steps: ( 1 ) The activation of functional surface groups. ( 2 ) Addition of branching monomer units.
  • 19.
  • 20. ADVANTAGE  The advantage of this method is the ability to modify the surface of the dendrimer molecule.
  • 21.  In successive generation growth, side reactions and incomplete additions become more apparent.  This is due to steric hindrance.  The overall yield is considerably small  The outer generation has only one kind of functional group.
  • 22. •The difficulty of many reactions that have to be performed on one molecule is overcome by starting the synthesis at the periphery and ending at the core. •In this method, growth begins at what will become the periphery of the final macromolecule and proceed inward, the final reaction being attachment to a polyfunctional core.
  • 23.  It involves the attachment of the outermost functional group to an inner generation and the attachment of the inner generation to the core.  The structural units before the final attachment to the core is called the wedge.  Usually 3 to 4 wedges attach to the core.  Each wedge can have different functional groups at periphery.
  • 24.
  • 25. Advantage of this method over “divergent growth” approach :-  control over surface functionality.  Ease for purification.
  • 26.  More susceptible to steric inhibition at the focal point group.  This effectively limits the size of the macromolecules that may be prepared in conventional fashion. .
  • 27.
  • 28.  Convergent approach affords better control to obtain a better dendrites architecture than the divergent approach.  Divergent approach is for large scale production.  Both involve stepwise processes that are tedious and time consuming.
  • 29.  The well-defined structure, compact globular shape, size monodispersity and controllable „surface‟ functionalities of dendrimer makes them excellent candidates for evaluation as drug carriers.  They can be used as drug delivery agents in 2 ways (1) Drugs molecules can be physically entrapped inside the dentritic structure. (2) Drug molecules can be covalently attached onto surface or other functionalities to afford dendrimer drug conjugates.
  • 30.  The internal „cavity‟ of the dendritic structure can be used for the entrapment drugs. ( I ) FIRST STRATEGY: - First strategy for the encapsulation of the guest molecules in dendrimers is physical encapsulation.
  • 31.  Held by Van der Waals or dipole moments  Carrier compounds do not have to be solublized
  • 32. 1. Targeted delivery would be difficult to achieve because drug release occurred by dialysis. 2. Difficult to make universal for all drugs, because encapsulation by the dendrimer varied significantly depending on drug and the dendrimer structure.
  • 33.  The second strategy for the encapsulation of guest molecules in dendrimers is based on multiple non- covalent chemical interactions, such as hydrogen bonding between guest molecules and dendritic structure.  Sustained release is possible.
  • 34.  The third and the most easily implemented startegy for the encapsulation of drug molecules in dendrimers is making use of hydrophobic interactions  Newkome et al. prepared dendritic macromolecules with a hydrophobic interiors and hydrophilic chain ends.  These molecules were said to behave as unimolecular micelles capable of solubilizing various hydrophobic
  • 35.  e.g.:- Poly (aryl ether) dendrimers bearing carboxylic groups as chain ends are able to enhance the water solubility of the hydrophobic compound such as pyrene and anthracene.
  • 36.  Higher generation dendrimers have a greater number of end groups that can be functionalized  Longer retention time in blood – PEG  Targeting – ability to attach to certain tissues or active sites  Imaging – Fluorescence, MRI, or X-ray
  • 37.
  • 39. Dendrimers as Cancer Therapy Therapeutic Cancer agent detector Reporter Cell death monitor Water Nanodevces molecule
  • 40. A single dendrimer can carry a molecule that recognizes cancer cells, A therapeutic agent to kill those cells, A molecule that recognizes the signals of cell death
  • 41. YOU