Tumor Targeting: Presented by M.Pharm 2 Semester (Pharmaceutics) Reg No. 121725101005
Tumor Targeting: Presented by M.Pharm 2 Semester (Pharmaceutics) Reg No. 121725101005
Tumor Targeting: Presented by M.Pharm 2 Semester (Pharmaceutics) Reg No. 121725101005
Presented By
K. TRIDEVA SASTRI
M.Pharm 2nd semester (Pharmaceutics)
Reg No. 121725101005
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Tumors classified as….
They can be classified in two forms. These are-
• Benign • Malignant
• Benign: They are- • Malignant: They are-
• Slow growing • Fast growing
• Capsulated • Non-capsulated
• Non- invasive • Invasive & infiltrate
• Do not metastasize • Metastasize
• Well differentiated • Poorly differtiated
• Suffix “oma” • Suffix “carcinoma” or
• Example : Fibroma, Adenoma, “sarcoma”
Emangioma, Ipoma, Eningioma 3
Key contributing factors of carcinogenesis
4
• Subsequently these changes lead to distinct tumor
microenvironment as compared to normal cells. This discriminatory
microenvironment and altered pathophysiological signaling pathways
have been classically used in the recent drug discovery approaches
and set the genesis of molecularly targeted therapies.
• Unfortunately, most of the anticancer drugs till time target the DNA
or other biologicals actively involved in cell division and thereby
control the rapidly diving cancer cells.
• However, in the course of that, the normal host tissues are also not
spared and nonspecific generalized toxicity is noted which may be
severely intense at times and may lead to either early termination of
therapy or other secondary complications
5
• Firstly, main targets include rapidly dividing lymphohematopoietic
cells, epithelial linings and other mucus secreting regions of gut, hair
follicular regions, etc. These complexities lead to low
chemotherapeutic index of the anticancer drugs.
• Secondly, rapid emergence of drug resistance also contributes majorly
to the poor cancer chemotherapeutics.
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TUMOR TARGETING
(a) preferentially localizing its pharmacological activities at the site of
action,
(b) recognition and interaction with target cells, and
(c) achieving cellular concentrations so as to exhibit therapeutic
response
• Very often a variety of homing devices are being employed to
direct the drug and/or carriers to the particular site of action.
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Normal Vs Tumor Vasculature
• Prominent homeostasis among the proangiogenic and antiangiogenic
molecules in the normal tissues which are responsible for balanced
organization of the blood vessels.
• This system works in tandem with lymphatics for clearance of the cellular by-
products.
• Carcinogenesis leads to imbalances in these systems leading to a variety of
alterations.
• Subsequently, compromised basal membrane, disorganized pericyte layer,
downregulation of the adhesion molecules and endothelial linings contribute to
high permeability of the tumor tissues.
• The principal barriers for the conventional chemotherapeutic agents to access
the tumor tissues are malformed tumor vasculature which leads to altered
vascular permeability, high interstitial pressure, extracellular acidosis, and
hypoxia (due to high mitochondrial oxygen consumption)
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• In case of tumors interstitial pressure shoots up to 100 mmHg owing
to three principal reasons. These include
(a) compromised functionalities of the blood vessel and lymphatics,
(b) osmotic pressure generated by drainage of solutes from tissues, and
(c) high contractile characteristics of tumor tissues
• The pH of the tumor microenvironment is usually dropped relatively
towards acidic, as evident from the direct measurement by placing
sensitive electrodes into the solid tumors
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Barriers to Tumor Targeting
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• Nonuniform distribution of blood vessels across the tumor,
• Uneven distribution of administered therapeutics often leading to
poor therapeutic response.
• Overexpression of efflux transporters, often referred to as ATP
binding cassette (ABC) transporters such as P-glycoprotein, multidrug
resistance proteins (MRP-1, -2), etc. Most of the anticancer drugs are
substrates of such efflux transporters.
• Subsequently, other factors such as diffusional barrier due to high
intercapillary distance, cell density, and extracellular matrix
components also pose potential barrier to tumor delivery of
therapeutics.
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A) Conventional Strategies for Tumor Targeting
• Selective accumulation of the drug at preferred site is also majorly affected by
its physicochemical properties.
• Most of the anticancer drugs fall in the category II/IV of Biopharmaceutical
Classification Systems (BCS), thereby posing pharmaceutical problems while
water soluble drugs pose problems related to permeability across various
biological barriers.
• Major approaches could be employed which include
(a) subtle structural modifications for improving the physicochemical properties in
accordance with structure–activity relationships (SAR),
(b) conjugating homing ligands for predetermined bio-distribution patterns, and
(c) involvement of carrier based approaches
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Passive Targeting
• The natural biodistribution pattern of the drug delivery carrier is
exploited for its preferential localization in the vicinity of the tumors
such as enhanced permeation and retention effects, phagocytosis of
particulate carrier by mononuclear phagocytosis systems (MPS) and
preferential localization in the organs of reticuloendothelial system
(RES).
• In addition, other typical properties of the tumor microenvironment
such as low extracellular pH, relative micro-acidosis, mild
hyperthermia, etc. could also be employed for availing passive
targeting of therapeutics.
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Enhanced Permeation and Retention ( EPR ) Effect
• Classically, the cell proliferation leads to formation of solid mass and upon
reaching a specific size, cells in the interior starts getting deprived of the
nutrients. Release of growth mediators signaling the development of the blood
vessels within tumor.
• The formed blood vessels are often leaky owing to absence of basal membrane
leading to fenestrations within the size of 200–2,000 nm
• The principal factors affecting EPR effect includes vessel architecture, interstitial
fluid composition, extracellular matrix composition, phagocyte infiltration,
presence of necrotic domains, factors pertaining to the colloidal carriers such as
blood circulation time, particle size, particle shape, surface charge, and surface
functionalization, if any, (e.g., stealth characteristics by PEGylation )
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• The presence of fenestrations results in poor resistance to the
extravasation of macromolecules to the tumor microenvironment and
contributes to the enhanced permeation part of EPR.
• Simultaneously, it has also been found that tumor mass is associated
with nonuniform lymphatic drainage and experience a huge physical
stress owing to rapid growth in the dimensions of the tumor mass.
This leads to the severe compromise in the drainage functionality of
the vessels and contributes to the retention part of EPR effect
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Surface Engineering of Colloidal Carriers for Stealth
Characteristics
• Drastic reduction in RES uptake and significant appreciation in the EPR
effect of the colloidal carriers can be achieved by surface engineering.
• Usually, the opsonins interact with the colloidal carriers via forces such as
van der Waal’s forces, weak electrostatic forces, ionic forces, and
hydrophobic/hydrophilic forces.
• In purview of this, hydrophobic and charged particles are rapidly
processed by RES and significant prolongation in the circulation half-life
can be achieved by surface functionalizing PEG chains forming “stealth”
systems.
• Mechanistically, the stealth characteristics are imparted by steric barrier,
shielding of anionic charge, and binding with dysopsonins
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Active Targeting
• Active targeting refers to the attachment of marker component to the
colloidal carrier system which is specifically recognized by the target
in concern may it be either from organelle or organ.
• Usually molecular targets are employed such as overexpression of
surface receptors on tumor cells for site specific delivery of
therapeutics such as dietary ligands (carbohydrate based, folate ,
etc.), monoclonal antibodies and their fragments, non-antibody
ligands (peptidic ligands), etc.
• The active targeting could be divided into various levels depending
upon extent of penetration,
i.e., organ level, cellular level, and subcellular level.
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Albumin Based Targeting
• Albumin plays a critical role in maintaining the homeostasis by mobilizing key
endogenous hydrophobic molecules. It specially binds via non-covalent
interactions and executes the transport of molecules in concern by
transcytosis across the endothelial cells into interstitial space.
• Paclitaxel bound albumin nanoparticle represents the classical example for
establishing the potential of albumin based delivery of anticancer drugs.
• The principal advantages associated with albumin based targeting include
superior stability over a wide range of pH (4–9) and temperature (10–60 °C),
biodegradation, non-immunogenic, and nontoxic.
• A striking advantage includes its additional cryoprotectant effect which makes
the lyophilization of formulation in concern quite easier than other systems in
race.
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Vitamin Based Targeting
• The vitamins employed for targeting potential includes folate, vitamin
B 12 , thiamine, and biotin.
• The principal advantages associated with vitamins, particularly folic
acid, includes stability over shelf and physiological conditions,
relatively inexpensive, nontoxic, non-immunogenic, endogenous
homing ligand, wide flexibility for diverse chemical reactions, and
relatively higher overexpression of folate receptors on most of the
cancers.
• It has been noted that folate functionalized colloidal carrier systems
are preferably absorbed by receptor mediated endocytosis.
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Folate
conjugated
nanoparticles
for improved
tumor
delivery of
therapeutics
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Transferrin Based Targeting
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Transferrin conjugated nanoparticles for
improved tumor delivery of therapeutics
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Lectin Based Targeting
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Peptide Based Targeting
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Physical Targeting
• The physical stimuli for drug targeting may either be endogenous
such as pH, temperature, redox potentials, etc., or be exogenous, i.e.,
employment of external forces such as magnetic, ultrasound, etc.
• The tumor microenvironment is slightly acidic and exhibits mild
hyperthermia which could be specifically exploited as a stimulus for
physical targeting.
• Magnet assisted tumor targeting approaches have also widely been
explored considering its immense potential. The drug in concern is
immobilized on ferromagnetic colloidal carriers and allowed to
circulate in body.
• Similarly, the circulating colloidal carrier may be accumulated at the
desired site of action using ultrasound energy.
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B) Recent Advances in Tumor Targeting Approaches
• Molecular Targeted Therapies
• Inhibition of the CDKs is an important target.
• Strategic inhibitors could be designed to compete via inhibition of the ATP
binding sites or upregulation of the native CDK inhibitors.
• Molecular targeted therapies, the available bioactives could be crudely
categorized among three broad generations
• First generation comprising ones that act predominantly via DNA damage,
synthesis and/or other linked processes such as tubulins,
• Second generation comprising agents that target cancer growth signaling
mechanisms such as kinases, etc., and
• Third generation, comprising agents which act on cellular pathways indirectly
related to cancer growth such as chromatin modifiers, protein chaperones,
proteasome inhibitors, etc.
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Agents Acting on Protein Folding and Proteotoxic Stresses
• Considering the typical microenvironment in the vicinity of tumor,
cancer cells constantly experience a variety of stresses, especially
permanent proteotoxic stress which is generally caused by the
misfolding and aggregation of proteins.
• The latter effect is predominantly observed in cancer cells owing to
molecular crowding of the cellular milieu.
• Usually such stresses are counterfeited by a group of molecules
inclusive of chaperones and protein remodeling factors
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Tumor Angiogenesis
• In routine physiological conditions, the vascular network develops in
three phases, viz., vasculogenesis, angiogenesis, and vascular
remodelling.
• Angiogenesis is initiated in tumor upon reaching the size 1–2 mm and
is typically coordinated by the hypoxic microenvironment of the
tumor. Hypoxia inducible factors (HIFs), heterodimeric transcription
factors, direct the expression of VEGF -A for angiogenic sequences
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Targeting tumor vasculature to inhibit angiogenesis. ( a ) Inhibition of binding to proangiogenic
receptors and/or altering the interaction of angiogenic factors with co-receptors. ( b ) Penetration
into the cells followed by binding with tyrosine kinase receptors ( c ) Direct activation of
receptors, e.g., thrombospondin peptide mimetics ( d ) Extracellular matrix receptors, e.g., αvβ3
integrins. ( e ) Nonspecific inhibitors of proliferation 30
Cancer Immunotherapy
• Principally, these act through
antibody dependent cellular
cytotoxicity (ADCC) and
complement-activation-
dependent cytotoxicity (CDC)
for imparting cytotoxicity and
play a crucial role in efficient
management of a variety of
cancers
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Radioimmunotherapy (RAIT)
• RAIT or Radioimmunoconjugates refer to the macromolecular entities
where monoclonal antibodies (mAbs) are covalently attached to high
linear energy transfer (LET) radionuclides.
• The radionuclides could either be alpha emitters such as
• 213 bismuth, 211 astatine, 223 radium, 149 terbium, 225 actinium, 227
thorium, 230 uranium or beta emitters such as 131 iodine, 90 yttrium, 60
cobalt, 99m technetium capable of damaging DNA either by strand
breakage or by other effects ultimately resulting in cell death.
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General architecture of multifunctional
nanoparticles and associated principal advantages.
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Immunotoxins
• Immunotoxins represents a group of macromolecular species
essentially comprising toxin conjugates and targeting antibodies
linked via gene fusions, peptide bonds, disulfide bonds, thioether
bonds, etc.
• Upon successful internalization within target cells, the immunotoxins
releases toxin by a variety of mechanisms such as degradation by
proteases, reduction of disulfide bonds, or acid hydrolysis.
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Antibody Directed Enzyme Prodrug Therapy ADEPT
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Immunoliposomes
• Internalization of liposomal drug delivery systems. (A) Plain liposomes are entitled for either specific adsorption ( a ),
nonspecificc adsorption at cell surface ( b ) fusion with cell membrane ( c ), destabilized of liposomes upon adsorption at
cell surface by internal components ( d ), direct or transfer-protein-mediated exchange of lipid component ( e ) and
endocytosis ( f ). The endocytosed liposomes either fuses with lysosomes ( g ) or leads to endosomal escape and drug
delivery to cytoplasm ( h ). (B) Surface functionalization of the liposomes with appropriate ligands can be performed ( a ) to
interact with target receptors ( b ), followed by endocytosis ( c ), and drug release ( d )
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