This document discusses targeted drug delivery systems. It defines targeted drug delivery as selectively delivering a pharmacologically active agent only to its site of action, not non-target tissues. Targeted delivery implies selectively localizing the drug at a pre-identified target site in a therapeutic concentration while restricting access to normal cells. This minimizes side effects and maximizes efficacy. Common approaches to targeted delivery include incorporating drugs into carrier systems, altering drug structure, or controlling drug release. Ideal targeted systems are non-toxic, biodegradable, stable, and controllably release drug at the target site.
Topic 9- General Principles of International Law.pptx
Targeted Drug Delivery: An Overview of Systems and Approaches
1. TARGETED DRUG DELIVERY
SYSTEM
• A special form of drug delivery system where
the pharmacologically active agent or
medicament is selectively targeted or delivered
only to its site of action or absorption and not
to the non-target organs or tissues or cells.
2. • Targeted drug delivery implies for selective and
effective localization of pharmacologically
active moiety at pre identified (preselected)
target in therapeutic concentration, while
restricting its access to non-target normal
cellular linings, thus minimizing toxic effects
and maximizing therapeutic index.
3.
4. ADVANTAGES OF DRUG
TARGETING
• Drug quantity may be greatly reduced as
well as the cost of therapy;
• Drug concentration in the required sites
can be sharply increased without negative
effects on non-target compartments.
5. Disadvantages of drug targeting:
Rapid clearance of targeted systems.
Immune reactions against intravenous administered
carrier systems.
Insufficient localization of targeted systems into
tumour cells.
Requires sophisticated technology for the formulation.
Requires skill for manufacturing storage,
administration.
6. Common Approaches of Targeted Drug Delivery
The basic approaches for targeting the drug to specific site
based on different research outcomes
I. Controlling the distribution of drug by incorporating it in a
carrier system
II. Altering the structure of the drug at molecular level
III. Controlling the input of the drug into bioenvironment to
ensure a programmed and desirable biodistribution
7. Properties of ideal targeted drug delivery:
• Nontoxic,biodegradable,biocompatibleand physicochemical
stable invivo and in-vitro
• Capable to deliver the drug to target cells or tissue or organ
and should have uniform capillary distribution.
• Release the dug in a controlled and predictable manner for
a suitable period of time.
• Efficiently maintain the drug concentration at the targeted
site within the therapeutic window for prolong period of
time
8. • Carrier used should be biodegradable or and
get readily eliminated from the body without
showing any toxic interaction.
• Its preparation should be easy or reasonably
simple, reproductive and cost effective.
• Minimal drug losses due to leakage of the
carrier system should be ensured.
9. CARRIERS:-
• Most important entity required for successful
transportation of the loaded drug.
• Drug vectors which, retain and transport
drug; deliver it within or in the vicinity of
target.
• Do so through an inherent characteristic or
acquired through structural modification.
10. PROPERTIES OF AN IDEAL DRUG
CARRIER:
• It must be able to cross anatomical barriers and in
case of tumour chemotherapy tumour vasculature.
• It must be recognized specifically and selectively by
the target cells and must maintain the specificity of
the surface ligands (anything that binds with
specificity can be considered a ligand).
11. • The linkage of the drug and the directing unit
(ligand) should be stable in plasma, interstitial and
other biofluids.
• Carrier should be non-toxic, non-immunogenic and
biodegradable particulate or macromolecule
•After recognition and internalization, the carrier
system should release the drug moiety inside the
target organs, tissues or cells.
12. LEVELS OF DRUG TARGETING:
1. Passive targeting
2. Inverse targeting
3. Active targeting
(a) Ligand mediated targeting
(b) Physical targeting
4. Dual targeting
5. Double targeting
6. Combination targeting
13. 1.Passive targeting:
• Systems that target the systemic circulation.
• Devices include- drug bearing bilayer
vesicular systems as well as cellular carriers
of micron or submicron size range.
15. Phagocytosis: by phagocytes of MPS/RES
• Monocytes / macrophages
• Mediated by adsorption of specific blood
components called opsonins
16.
17. 2.Inverse targeting:
• Drug targeting attempts made to
evade the passive uptake of the
colloidal carrier by reticuloendothelial
systems are referred to as inverse
targeting.
18. Strategy:
• The function of RES is suppressed by a pre-injection
of colloidal carriers or macromolecules like dextran
sulphate leading to RES blockade and resulting in
impairment of host defense system.
• Alternative strategies include: modification of the
size, surface charge, composition, surface
rigidity & hydrophilicity of carriers for
desirable bio fate.
19. 3.Active targeting:
• The facilitation of the binding of the drug
carrier to target cells by the use of ligands
to increase receptor mediated localization
of the drug and target specific delivery of
drug is referred to as active targeting.
20. 3 types
• First order targeting(organ compartmentalization).
• Second order targeting (cellular targeting).
• Third order targeting (intracellular targeting).
21. First
order
targeting
• Discrete organ or
tissue
Second
order
targeting
• Specific cell type
with in a tissue or
organ
• Tumour cells,
kupffer cells
Third
order
targeting
• Specific
intracellular
compartment
• lysosomes
classification
22. First order targeting:
• Restricted distribution of the drug carrier
system to the capillary bed of the
predetermined target site, organ or tissue.
• Compartmental targeting in lymphatics,
peritoneal cavity, plural cavity, cerebral
ventricles, lungs, joints, eyes, etc.
23. Second order targeting:
• The selective delivery of drugs to a
specific cell type such as tumour cells
(and not to the normal cells) is
referred to as second order targeting.
24. Third order targeting:
• Drug delivery specifically to the
intracellular site of target cells.
• e.g., receptor based ligand-mediated entry
of a drug complex into a cell by
endocytosis,lysosomal degradation of
carrier followed by release of drug
intracellularly or gene delivery to nucleolus.
25. Ligand mediated targeting:
• ligands are used as carrier surface
group(s), which can selectively direct the
carrier to the pre-specified site(s) housing
the appropriate receptor units to serve as
‘homing device’ to the carrier/drug
• Anti bodies, polypeptides
26. Examples of Ligands
Ligands Tumour target
Folate Overexpression of folate receptor
Transferrin Overexpression of transferrin receptor
Galactosamine --- Galactosamine receptors on
hepatocytes---- Hepatoma
27.
28. Physical targeting (Triggered Release)
• The drug delivery programmed and
monitored at the external level (ex vivo)
with the help of physical means.
• Temperature sensitive liposomes.
• Characteristics of environment changes
like pH, temperature, light intensity,
electric field, and ionic strength
29. 4.Dual targeting
• In this targeting approach carrier molecule itself
have their own therapeutic activity and thus
increase the therapeutic effect of drug.
• For example, a carrier molecule having its own
antiviral activity can be loaded with antiviral drug
and the net synergistic effect of drug conjugate
was observed.
30. Advantage
• The virus replication process can be
attacked at multiple points, excluding
the possibilities of resistant viral
strain development.
31. 5.Double targeting:
• When temporal and spatial methodologies are
combined to target a carrier system, then
targeting may be called double targeting.
• Spatial placement relates to targeting drugs to
specific organs tissues, cells or even subs
cellular compartment
• whereas temporal delivery refers to controlling
the rate of drug delivery to target site.
37. TYPES
• Based on the nature of their origin:
• Endogenous - LDL ,HDL
Chylomicrons, Serum albumin,
Erythrocytes.
• Exogenous - Microparticulates,
Soluble polymeric and
Biodegradable polymeric drug
carriers.
38. 1. Colloidal carriers
2. Cellular carriers
3. Supramolecular delivery systems
4. Polymer based systems
5. Macromolecular carriers