introduction to rate controlled drug delivery system , feedback & types of feedback regulated drug delivery system, example of each type of feedback regulated drug delivery system.
2. CONTENT
1. Introduction of rate controlled drug delivery system
2. Rate controlled drug delivery system classification
3. What is feedback regulated drug delivery system & its types.
(3.1)Bioerosion & example
(3.2)Bioresponsive & example
(3.3)Self regulating & example
4. References
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3. 1. INTRODUCTION TO RATE CONTROLLED
DRUG DELIVERY SYSTEM
In conventional drug delivery system, there are many problems in maintaining
the dose in therapeutic window due to fluctuation in drug dose level.
To overcome such, researchers devolped a system called as controlled drug
delivery system .
Control release is one where drug release of drug is at predetermined rate to
maintain constant drug concentration for specific period of time.
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4. 2.RATE CONTROLLED DRUG DELIVERY SYSTEM
CLASSIFICATION
A. RATE PREPROGRAMMED DRUG DELIVERY
SYSTEM.
B. ACTIVATION MODULATED DRUG DELIVERY
SYSTEM
C. FEEDBACK REGULATED DRUG DELIVERY
SYSTEM
D. SITE TARGETTING DRUG DELIVERY STEM
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5. 3.FEEDBACK REGULATED DRUG DELIVERY
SYSTEM
In this system, release of drug molecuules from delivery system is activated by
the triggering agent, such as biochemical substance in body by its concentration
via some feed-back mechanism.
It feedback-regulated system also it majorily have three systems::
1. Bioerosion regulated dds
2. Bioresponsive dds
3. Self regulating dds
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6. (3.1) BIOEROSION-REGULATED DRUG
DELIVERY SYSTEM
Bioerosion-regulated dds was devolped
by heller & trescony by applying the
concept of feedback regulated dds.
In this, the system consist of drug
dispersed bioerodible matrix fabricated
from half ester such as poly (vinyl methyl
ether) which is coated with layer of
immobilised urease.
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7. (3.1) BIOEROSION-REGULATED DRUG
DELIVERY SYSTEM
In a neutral pH, polymer erosion is very
slow, while in presence of urea, urease at
surface of drug delivery system
metabolizes urea to ammonia, which
cause increase in pH.
Increase in pH, leads to rapid
degradation of polymer matrix as well as
release of drug molecules from matrix.
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8. (3.2) BIORESPONSIVE DRUG DELIVERY SYSTEM
Bioresponsive dds was devolped by horbett as a applied feedback
regulated dds.
In this system, the drug reservoir is contained in a device enclosed by
bioresponsive polymeric membrane whose drug permeability is totally
controlled by concentration of biochemical agent in tissue where the
system is located.
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9. (3.2) BIORESPONSIVE DRUG DELIVERY SYSTEM
Example:
Devolpment of glucose triggered insulin
delivery system in which insulin
reservoir is encapsulated with hydrogel
membrane having NR2 group ( as given
in figure )
INR2 groups are neutral in alkaline
solution thus membrane is unswollen
and impermeable to insulin.
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10. (3.2) BIORESPONSIVE DRUG DELIVERY SYSTEM
As glucose as triggering agent penetrates into the
membrane, it gets oxidized enzymetically by glucose
oxidase entrappd in membrane to form gluconic acid.
The NR2 groups are then protonated to gotm NR2-
H+ & membrane leads to swell thus permeablity of
insulin molecule is possible.
Here, the amount of insulin delivered is the
bioresponsive to concentration of glucose penetrating
insulin delivery system.
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11. (3.3) SELF REGULATING DRUG DELIVERY
SYSTEM
This system totally depends on reversible & competitve binding mechanism to
activate as well as release of drug.
Here, within a semipermeable membrane, drug reservoir is present, which gets
activated by membrane permeation of biochemical agent from thissue in which it
is located.
Kim was first to apply mechanism of reversible binding of sugar molecule by
lectin into design of self regulating drug delivery system.
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12. (3.3) SELF REGULATING DRUG DELIVERY
SYSTEM
Example:
It first involve preparation of biologically active insulin derivatives in which
insulin is coupled with sugar component & this into insulin-sugar-lectin complex,
which is then encapsulated in semepermeable membrane.
As blood glucose diffuse into device & bind at sugar binding sites in lectin
molecules, it activate release of insulin-sugar dvts .
This dvts then diffuse out of device, and the whole amount of release is depend
on glucose oncentration. Thus self regulating drug delivery is achieved.
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14. 1.SELF-REGULATED GLYCOSYLATED INSULIN
DELIVERY
A self-regulating insulin delivery system, based on the concept of competitive
binding between synthetic glycosylated insulin (g-insulin) and glucose to
concanavalin A (con A) ligand substrate, has been designed. The competitive
binding of the two ligands for the substrate regulates G- insulin release in relation
to the outside glucose concentration, while a polymeric membrane, serving as a
peritoneal implant pouch containing g-insulin and con A, is used to control the
permeability of glucose influx and g-insulin efflux. Mono-, di- and tri-sugar
substituted insulins have been characterized.
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EXAMPLES FROM
ARTICLES
15. 2.FEEDBACK REGULATED DRUG DELIVERY
VEHICLE: CARBONDIOXIDE RESPONSIVE
HYDROGEL FOR ANTIDOTE
A possible approach to handling the harmful side effects of an analgesic
overdose, without losing its therapeutic potential, involves feedback regulated
delivery of an antidote. For example, overdose of morphine causes
hypoventilation, an inadequate ventilation to perform gas exchanges in lungs
leading to increased CO2 concentration in the blood. Taking advantage of CO2
as a toxicity marker, a hydrogel-based delivery vehicle containing dimethylamino
groups [poly(n,n-dimethylaminoethyl methacrylate) cross-linked by
trimethylolpropane tri- methacrylate] was designed. 15
16. Stimulus controlled swelling of these hydrogels in naloxone delivery is done. A
remarkable control over naloxone release was achieved against the concentration
of the biomarker.
The overall stimuli response of the gel could be enhanced further by
encapsulating carbonic anhydrase, a metalloenzyme known to catalyze the
reversible hydration of CO2. Thus, a feedback regulated drug delivery vehicle
based on toxicity biomarker strategy was modeled successfully, which has the
potential to mitigate risks associated with drug overdose.
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17. 4. REFERENCES
Yie W. Chien “Novel Drug Delivery Systems”feedback-regulated Drug
Delivery System, PG NO.2, 33-37, 43, 44
Sung Wan Kim, Chaul Min Pai, Kimiko Makino, Leah A. Seminoff, David L.
Holmberg, Jeremy M. Gleeson, Dana E. Wilson And Eric J. Mack “Self-
regulated Glycosylated Insulin Delivery” Journal Of Controlled Release, 11
(1990) PGNO.193-201
Sunita S. Satav, Shreedhar Bhat, And S. Thayumanavan, “Feedback Regulated
Drug Delivery Vehicles: Carbon Dioxide Responsive Cationic Hydrogels For
Antidote Release” , Biomacromolecules ,11 (2010) PG NO.1735–1740
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