Copy-of-Copy-of-DDS-LEC PDF Pharmaceutical Dosage Forms

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This document is lecture notes for a Pharmaceutical Dosage Forms course. It covers early drug history and early research on drug development and formulation.

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LEC NOTES-Phar 2104 | Pharmaceutical Dosage Forms, Drug Delivery systems and Medical
Services

FIRST SEMESTER | ACADEMIC YEAR 24-25 | RELLES
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citizenship, aimed to create a perfect system of
physiology, pathology, and treatment.He originated so
many preparations of vegetable drugs by mixing or
melting the individual ingredients that the field of
pharmaceutical preparations was once commonly
An agent intended for use in the diagnosis, referred to as “Galenic pharmacy”.
mitigate, treatment, cure, or prevention of
4.)Emperor Frederik II, 1240 AD
disease in humans or in other animals.
-regulated the practice of pharmacy within the part of
One of its most astounding qualities is the
his kingdom called the Two Sicilies.
diversity of their actions and effects on the
body. 5.)Paracelsus (1493 - 1541 AD)
The use of drugs predates recorded human -Swiss physician and chemist.
history in man's efforts to relieve pain and -He influenced the transformation of pharmacy from a
suffering, recover from injury, and extend life. profession based primarily on botanical science to one
based on chemical science.

Drugs have existed as long as humans. Their 1.) Karl Wilhelm Scheele
discovery was led by human disease and the -Discovered Lactic acid, citric acid, oxalic acid, tartaric
instinct to survive. acid, arsenic acid, glycerin, calomel, benzoic acid,
Disease was believed to be caused by demons oxygen
or evil spirits entering the body.
2.)Friedrich Serturner
-in 1805 isolated morphine from opium.-Quinine, cinchonine, and brucine.
1.) Ebers papyrus
3.) Joseph Caventou & Joseph Pelletier
-dominated by drug formulas, with more than 800
- solated quinine and cinchonine from cinchona and
formulas or prescriptions being described and more
strychnine and brucine from nux vomica.
than 700 drugs mentioned.
4.)Joseph Pelletier and Pierre Robiquet
2.) Botanical
- isolated quinine and cinchonine from cinchona and
3.) Mineral strychnine and brucine from nux vomica.
-isolated caffeine
4.)Animal
5.)Pierre Robiquet
5.) Vehicle use -separated codeine from opium.

6.)Philadelphia College of Pharmacy, 1821
-The nation's first school of pharmacy. In 1820
1.) Hippocrates (ca. 460 - 377 BC)
-a Greek physician, is credited with the introduction of 7.)United States Pharmacopeia, 1820 - was created
scientific pharmacy and medicine. to aid in establishing standards for drugs in the United
-Father of Medicine State.

-Pharmakon - drug

2.) Dioscorides (first century AD) 1.)Pharmakon- means drug
-a Greek physician and botanist, was the first to deal
with botany as an applied science of pharmacy. 2.) Poiein- means to make

Pharmacognosy- a term formed from two Greek words, 3.)Pharmacopeia- means to make drugs
pharmakon, drug, and gnosis, knowledge.
1580:drug standards book In Bergamo, Italy
3.) Galen (ca. 130-20 AD)
-a Greek pharmacist– physician who attained Roman
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Many city, state, and the national multinational pharmaceutical companies that develop
pharmacopeias were established (as it still and market products
today)
Great Britain, London, Edinburgh, and Dublin 4.)Canada generally uses the USP-NF.
pharmacopeias replaced by. British -does not have its own national pharmacopeia
Pharmacopoeia in 1864
Lititz Pharmacopoeia, 1778. 5.)USP-NF is the only "nongovernmental"
Lyman Spalding- Father of the USP pharmacopeia in the world.
1820, the United States Pharmacopeia (USP)
established by physicians
1830, pharmacists became involved.
The manufacturer must rigidly adhere to
USP under continuous revision
established initial drug and drug product
The National Formulary(NF) published in 1888
standards and assay methods.
by the APhA
These and future standards are adopted as
1975, the USP purchased NF
new monographs by the USP-NF
In 2006, a spanish edition of the USP NF was
introduced
Today, the USP-NF Is revised annually in
hardcopy and online International consortium to develop and
promote uniform or harmonized international
standards.
ISO 9000 t0 ISO 9004 - Among the various
-adopt standards for drug substances,
ISO standards used in the pharmaceutical
pharmaceutical ingredients, and dosage forms
industry are those in the series ISO 9000 to
reflecting the best in the current practices of medicine
ISO 9004.
and pharmacy and provide suitable tests and assay
procedures for demonstrating compliance with these
standards.
“The first federal law in the United States designed
1.) USP - includes detailed monograph of drug to regulate drug products manufactured
substances and their dosage forms domestically was the Food and Drug Act of 1906.”
2.) NF - includes detailed monograph of pharmaceutic The law required drugs marketed interstate to
ingredients. comply with their claimed standards for strength,
purity, and quality.

1.)Homeopathic pharmacopeia
-used by pharmacists and homeopathists as well as by The FDA created to enforce the Federal Food,
law enforcement agencies that must ensure the quality Drug, and Cosmetic Act of 1938.
of homeopathic drugs. The purpose of FDA was to enforce standards
for the pharmaceutical industry.
The term homeopathy was coined by Samuel
“New Drug Application"
Hahnemann (1755–1843)
"Safety."
★ homoios, meaning similar "Grandfathered drugs."
★ pathos, meaning disease Issue: Sulfanilamide mixed with diethylene
glycol - 100 persons died.
2.)International pharmacopeia The 1938 Act prohibits the distribution and use
-published by the World Health Organization (WHO) of of any new drug or drug product without the
the United Nations with the cooperation of member prior filing of a New Drug Application (NDA)
countries. and approval of the FDA.

- It is intended as a recommendation to national
pharmacopeia revision committees to modify their
pharmacopeias according to international standards. Prescription status of drugs.
Rx only or Caution: Federal law prohibits
3.)European pharmacopeia dispensing without prescription.
-are used within their legal jurisdictions and by Refill authorization.
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Prescription drugs must bear the symbol “Rx
Only” or the legend “Caution: Federal Law
Prohibits Dispensing Without Prescription.”
According to the Durham-Humphrey
Amendment, prescriptions for legend drugs
may not be refilled (dispensed again after
the initial filling of the prescription) without
the express consent of the prescriber.

Issue: Thalidomide - causes phocomelia to the
baby
the purpose of the enactment was to ensure a
greater degree of safety for approved drugs,
and manufacturers were now required to prove
a drug both safe and effective before it would
be granted FDA approval for marketing. 1. Birth defect or mental retardation rate is 3% to
Investigational new drug application (IND) 5% in general population.
2. Two important factors to consider when
assessing the teratogenic potential of a
medication Stage of pregnancy and the
amount of medication taken
3. Evaluate each patient individually for an
accurate risk assessment.
4. Teratogens:
Radiation
-served to consolidate and codify control authority over Infections
drugs of abuse into a single statute. Maternal and metabolic imbalance
Drugs and environmental chemicals
1.Consolidates:

Drug Abuse Control Amendments of 1965
Harrison Narcotic Act of 1914 FDA's strongest labeling requirements for
Other laws high-risk medicines
Most serious warning placed in the labeling of
2.DEA-Drug Enforcement Administration a prescription medication
Chloramphenicol was the first
The Comprehensive Drug Abuse Prevention and Advertisements or "reminder ads" are not
Control Act of 1970 established five “schedules” allowed
for the classification and control of drug
substances that are subject to abuse.

Each firm must register with the FDA and
submit information.
Enacted to provide the FDA with the legislative
authority to compile a list of marketed drugs

Exemptions:

Compounded Preparations
Research products

National Drug Code number system
-appear on all manufacturers' drug labeling.
-Once a number is assigned to a drug product, it is a
permanent assignment.
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Changes to speed FDA approval of generic food additives, human drugs and biologicals,
drugs and the extension of patent life for radiologic and medical devices, animal d
innovative new drugs were the major and feeds, and cosmetics.
components of the Drug Price Competition and The Center for Drug Evaluation and Research
Patent Restoration Act of 1984. (CDER)
Hasten FDA approval The Center for Biologics Evaluation and
Extend patent life Research (CBER)
Abbreviated new drug application (ANDA) Streamline FDA policies and codify regulations
Guidelines and regulations

Sets policies, establishes standards, issues
To reduce the risks of adulterated, misbranded, guidelines, and promulgates and enforces rules and
repackaged, or mislabelled drugs regulations governing the affected industries and their
products
Reimportation-Prohibits the reimportation of drug
products manufactured in the United States except by Monitors for regulatory compliance through reporting
the manufacturer of the product. requirements, product sampling and testing, and
establishment inspections
Sales restrictions-Prohibits selling, trading,
purchasing, or the offer to sell, trade, or purchase a Establishes product labeling requirements,
drug sample. disseminates product use and safety information,
issues product warnings, and directs product recalls
Sample distribution-Samples may be distributed only
to (a) practitioners licensed to prescribe such drugs Acts as the government's gatekeeper in making safe
and (b) at the written request of the practitioner, to and effective new drugs, clinical laboratory tests, and
pharmacies of hospitals or other health care medical devices available through a carefully
institutions. conducted application and review process

Wholesale distributors- Manufacturers are required
to maintain a list of their authorized distributors.
Class I

- Reasonable probability of serious adverse
These products, which include vitamins, health consequences or death
minerals, amino acids, and botanicals, legally
are not considered drugs if they have not been Class II
submitted for review on NDAs and thus have
not been evaluated for safety and efficacy by -May cause temporary or medically reversible
the FDA consequences
Labeling claims regulations
Not legally considered drugs Class III
USP-NF standards
The act forbids manufacturers or distributors of - Not likely to cause adverse health
these products to make any advertising or consequences
labeling claims that indicate that the use of the
product can prevent or cure a specific disease.
A disclaimer must appear on the product: “This
product is not intended to diagnose, treat,
cure, or prevent any disease.”
RPh- Registered Pharmacist

The mission of the FDA is to protect the public PharmD- Doctor of Pharmacy
health against risks associated with the
DPh- Doctor of Pharmacy
production, distribution, and sale of food and

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Board of Pharmaceutical

To gain marketing approval:
-To serve society as the profession responsible
for the appropriate use of medications, devices, and The drug must be safe and effective for its
services to achieve optimal therapeutic outcomes. proposed use
All processes and controls used must meet
established quality standards
-Pharmaceutical care is that component of
pharmacy practice that entails the direct interaction of
the pharmacist with the patient for the purpose of
caring for that patient's drug-related needs.

1. State laws and regulations
2. American Society of Health-System
Pharmacists
3. United States Pharmacopeia
General Chapters
Pharmaceutical Compounding-
Nonsterile
Pharmaceutical Compounding-Sterile

1. Natural sources
-Established the requirement for each state to 2. Synthesized in laboratories
develop and mandate Drug Utilization Review (DUR)
programs to improve the quality of pharmaceutical care 3.Genetic engineering
provided to Medicaid patients.
○ Recombinant DNA
○ Monoclonal antibodies

4.Human gene therapy
-a medical intervention based on the modification of
the genetic material of living cells.
A pharmacist respects the covenantal
relationship between the patient and
pharmacist.
A pharmacist promotes the good of every Produces desired effects
patient in a caring, compassionate, and Convenient administration
confidential manner. Minimal dosage
A pharmacist respects the autonomy and Minimal dosing frequency
dignity of each patient. Optimal onset
A pharmacist acts with honesty and integrity in Optimal duration of activity
professional relationships. No side effects
Eliminated from body efficiently, completely,
and without residual effect

A pharmacist maintains professional a goal drug would produce the specifically desired
competence. effect, be administered by the most desired route
A pharmacist respects the values and abilities (generally orally) at minimal dosage and dosing
of colleagues and other health professionals. frequency, have optimal onset and duration of activity,
A pharmacist serves individual, community, exhibit no side effects, and following its desired effect
and societal needs. would be eliminated from the body efficiently,
A pharmacist seeks justice in the distribution of completely, and without residual effect.
health resource.
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Screening New Molecular Entity (NME) - s an active ingredient
that has never before been marketed in the United
Random or Untargeted Screening -Random or States in any form (26).
untargeted screening involves the testing of large
numbers of synthetic organic compounds or change in a previously approved drug
substances of natural origin for biologic activity. product’s formulation or method of
manufacture constitutes newness under the
High-throughput screening- are capable of law since such changes can alter the
examining 15,000 chemical compounds a week using therapeutic efficacy and/or safety of a product.
10 to 20 biologic assays (23). A combination of two or more old drugs or a
-To be effective, this change in the usual proportions of drugs
requires a sizable and chemically diverse collection of Proposed new use, new regimen, new route of
compounds to examine, which many pharmaceutical administration, or new dosage form
and chemical companies have in chemical libraries.

Molecular modification of known agents - a
chemical alteration of a known and previously A prototype chemical compound with desired
characterized organic compound (frequently a lead activity that may not possess all the desired
compound; see "A Lead Compound") for the purpose features
of enhancing its usefulness as a drug. Synthesis of derivatives which will ultimately
lead to successive generations of the same
Mechanism-based drug design - is molecular pharmacologic type
modification to design a drug that interferes specifically
with the known or suspected biochemical pathway or
mechanism of a disease process.
When first synthesized or identified from a natural
source, an organic compound is represented by an
empirical formula, for example, C16H19N3 O5 S·3H2
A compound that requires metabolic O for amoxicillin, which indicates the number and
biotransformation after administration to relationship of the atoms in the molecule.
produce the desired pharmacologically active
compound As knowledge of the relative locations of these atoms
increases, the compound receives a systematic
Solubility - A prodrug may be designed to possess chemical name
solubility advantages over the active drug, enabling the use
of specifically desired dosage forms and routes of Nonproprietary (Generic) Name- U.S. Adopted
administration Names (USAN) Council
- A nonproprietary name of a drug serves numerous
Absorption - A drug may be made more water or lipid and varied purposes, its principal function being to
soluble, as desired, to facilitate absorption via the identify the substance to which it applies by means of a
intended route of administration. designation that may be used by the professional and
lay public free from the restrictions associated with
Biostability - If an active drug is prematurely registered trademarks.
destroyed by biochemical or enzymatic processes, the
design of a prodrug may protect the drug during its
transport in the body.
-Prospective drug substances must undergo preclinical
Prolonged release - Depending on a prodrug’s rate of testing for biologic activity to assess their potential as
metabolic conversion to an active drug, it may provide useful therapeutic agents.
prolonged drug release and extended therapeutic
activity
The science concerned with drugs, their
sources, appearance, chemistry, actions, and
uses
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It can include properties, biochemical and mammalian reproduction. Included in these
physiologic bioran, romation, a of extie, studies are fertility and mating behavior; early
absorption, distribution, embryonic, prenatal, and postnatal
development; multigenerational effects; and
Pharmacodynamics - the study of the biochemical teratology.
and physiologic effects of drugs and their mechanisms Genotoxicity or mutagenicity studies -
of action; performed to determine whether the test
compound can affect gene mutation or cause
Pharmacokinetics - which deals with the absorption, chromosome or DNA damage.
distribution, metabolism or biotransformation, and
excretion (ADME) of drugs

Clinical Pharmacology - which applies pharmacologic
principles to the study of the effects and actions of
drugs in humans.

-each drug substance has intrinsic chemical and
physical characteristics that must be considered before
ADME studies the development of a pharmaceutical formulation
a. the extent and rate of drug absorption from
various routes of administration, including the Drug solubility
one intended for human use
b. the rate of distribution of the drug through the -A drug substance administered by any route must
body and the site or sites and duration of the possess some aqueous solubility for systemic
drug’s residence absorption and therapeutic response. Poorly soluble
c. Rate, primary and secondary sites, and compounds (e.g., less than 10 mg/mL aqueous
mechanism of the drug's metabolism in the solubility) may exhibit incomplete, erratic, and/or slow
body absorption and thus produce a minimal response at
d. the proportion of administered doses desired dosage.
eliminated from the body and its rate and route
of elimination. Necessary for absorption/transport
Biochemical transformation into If less than about 10 mg/mL, may exhibit either
readily-eliminated polar compounds incomplete or erratic absorption and produce a
minimal response
Can be increased by modifying the structure,
form, complexation, or particle size reduction
-Adverse or undesired effects of drugs
Partition coefficient
Toxicity Studies:
-a drug molecule must first cross a biologic membrane
Acute or short-term toxicity studies - of protein and lipid, which acts as a lipophilic barrier to
determine the toxic effects of a test compound many drugs.
when administered in a single dose and/or in
multiple doses over a short period, usually a The drug must pass the biological membrane
single day. of protein/lipid, which acts as a lipophilic
Subacute or subchronic studies - In barrier to many drugs.
designing an animal toxicology program, Preference of drug for lipid:water.
relationships to projected human clinical Indicative of ability to penetrate biologic
studies for safety must be considered. multiphase systems.

Dissolution rate

-The speed at which a drug substance dissolves in a
medium is called its dissolution rate.
Carcinogenicity studies - a component of
chronic testing and is undertaken when the Speed/rate at which a substance dissolves
compound has shown sufficient promise as a Indicates a drug's absorption potential
drug to enter human clinical trials.
Reproduction studies - are undertaken to
reveal any effect of an active ingredient on
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Physical form

-The crystal or amorphous forms and/or the particle
size of a powdered drug can affect the dissolution rate,
and thus the rate and extent of absorption, for a
number of drugs.

Crystalline versus amorphous
Particle size -

Stability

-The chemical and physical stability of a drug Phase I
substance alone, and when combined with formulation
components, is critical to preparing a successful - Determine human pharmacology of the drug,
pharmaceutical product. structure-activity relationships, side effects with
increasing doses, possible early evidence of
Both physical and chemical properties effectiveness
Addition of formulation components to create a
successful pharmaceutical product Phase II
Absorption
Hydrolysis: moisture in packaging - Controlled clinical studies for effectiveness in
Heat and Humidity patients with the condition

Phase III

-An initial product is formulated using the information -Several hundred to several thousand patients
gained during the preformulation studies and with the in controlled and uncontrolled trials.
consideration of the dose or doses, dosage form, and
route of administration desired for the clinical studies
and for the proposed marketed product.
placebo (placebo control) or an active drug
Dosage form, Dosage strength, Route of (positive control), a standard or comparator drug
administration product.
Initial formulations
Clinical supplies Both a placebo and an active drug may be used as
controls in the same study

Study designs
-Filed when adequate safety and usefulness
as a new drug has been demonstrated through
preclinical studies
Usual dose
Contents: Dosage regimen
Initial/Priming/Loading dose
Code of Federal Regulations Maintenance dose
Form FDA-1571 Prophylactic dose
Therapeutic dose
Minimum Effective Concentration
Minimum Toxic Concentration
Protects the safety and rights of the human Median Effective Dose (ED50)
subjects Median Toxic Dose (TD50)
Ensures that the study allows the evaluation of
the drug's safety and effectiveness

Age
Pharmacogenetics
Body weight
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Body surface area May reveal additional:
Sex
Pathologic state Side effects
Tolerance Serious and unexpected adverse effects
Concomitant drug therapy Drug interactions
Time and conditions of administration
Dosage form and route of administration 2.)Continued clinical investigations

Better understand the drug's MOA
Indicate possible new therapeutic uses
Permits the use of an investigational drug in Demonstrate need for new formulations
patients not enrolled in a clinical study. Additional side effects, adverse effects and/or
Patients have serious or immediately drug
life-threatening disease.
No satisfactory alternative is available.
-adverse drug experience that is both serious (life
threatening or fatal) and unexpected (not contained in
-Orphan disease is a rare disease or condition the approved drug product labeling), regardless of the
affecting fewer than 200,000 people in the United source of the information, within 15 working days of
States and of which there is no reasonable expectation receipt of the information.
that R&D costs will be recovered by product sales.
Adverse drug experiences must be reported to
Examples: the FDA within 15 working days of receipt of
information.
Chronic lymphocytic leukemia The FDA may require to revise product
Cystic fibrosis labeling or other actions.
Gaucher disease Annual Reports

-A sponsor may withdraw an IND at any time, ending
all clinical investigations. All stock of clinical supplies
must be returned to the sponsor or otherwise
destroyed.
-nonclinical laboratory studies and clinical
The sponsor can withdraw at any time. investigations may be omitted, except those pertaining
Inactive status to the drug’s bioavailability.
FDA termination for reasons of safety, efficacy,
or regulatory compliance. Nonclinical laboratory studies and clinical
investigations may be omitted, except for
studies pertaining to drug's bioavailability.
Generic drug products (based upon innovator's
NDA).

-Must meet specific labeling requirements in the CFR
and approved for each product by the FDA
-BLAs are submitted to the FDA’s CBER for the
Labeling includes: manufacture of biologics such as blood products,
vaccines, and toxins.
Labels on immediate container
Package insert For the manufacture of Biologics:
Company literature
Advertising Blood products
Promotional materials Vaccines
Toxins

1.)Continued data collection for drugs after they are
marketed -The Federal Food, Drug, and Cosmetic Act, as
amended, contains specific regulations pertaining to
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the approval for the marketing and labeling of drugs 2.)Employees- must be educated, trained and have
intended for animal use (6). the experience needed

1. Specific regulations involved 3.)Consultants- should possess the required
2. The Animal Medicinal Drug Use qualifications
Clarification Act of 1994 (AMDUCA)

-Allows veterinarians to prescribe extralabel
uses of approved animal drugs and approved Structure, space, design, and placement of
human drugs for animals. equipment must enable thorough cleaning,
inspection, and safe and effective use of the
designated operations.
All work must be logged in, inspected by a
supervisor, and signed off.

-harmonizing, or bringing together, the regulatory -Each piece of equipment must be of appropriate
requirements with the long-range goal of establishing a design and size and suitably located to facilitate
uniform set of standards for drug registration within operations for its intended use, cleaning, and
these geographic areas. maintenance.

International marketplace 1.)Appropriate:
US FDA, EU, Japan, and geographic
representatives Design
To establish a uniform set of standards for drug Size
registration
2.)Suitably located to facilitate:
KAYA PA NE?? WATER BREAK DANAY DW UHAW
KANAGID OH! Intended use
Cleaning
Maintenance

Written procedures

Established by the FDA -That describe the receipt, identification,
Ensure that minimum standards are met for storage, handling, sampling, testing, and approval or
drug product quality rejection of all drug product components, product
First cGMP regulations were promulgated in containers, and closures must be maintained and
1963 under the Kefauver-Harris Drug followed

Written procedures.
Ensure correct identity, strength, quality, and
21 CFR, Part 211 contains minimum good purity.
manufacturing practice requirements for Any deviation must be recorded and justified.
preparation of finished pharmaceutical All product ingredients, equipment, and drums
products for administration to humans or or other containers must be distinctively
animals. identified.

deals with the responsibilities of the quality control unit, 1.)Written procedures - Written procedures must be
employees, and consultants established and followed for the holding and
distribution of products.
Responsibilities of the:
Holding
1.)Quality control unit- authority and responsibility Distribution
Quarantined
for all functions affecting product quality.
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2.)Stored and shipped under appropriate
conditions - Products must be stored and shipped
under conditions that do not affect product quality.

3.)FIFO - Ordinarily, the oldest approved stock is
distributed first.
The quality of all components affects the
quality of the finished pharmaceutical product
APIs and excipients must comply to GMP
-Written procedures are required for the receipt, standards since it is critical in the FDA's
identification, storage, handling, sampling, and testing preapproval inspection program for NDAs and
of drug product and issuance of labeling and ANDAs.
packaging materials

Expiration dating- to ensure that the drug product
meets applicable standards at the time of use Must be produced under cGMP standards
Flexibility in the regulations is applicable during
Tamper-evident packaging - On November 5, 1982, the preclinical testing and in the earlier part of
the FDA published initial regulations on the clinical tests.
tamper-resistant packaging in the Federal Register

These regulations were promulgated after criminal
tampering with over-the-counter (OTC) drug products Additional mandates specific for blood,
earlier in that year resulted in illness and deaths. bacterial, and viral products are found in the
regulations due to their nature.
-Have one or more indicators or barriers to entry which,
if breached or missing, can reasonably be expected to
provide visible evidence to consumers that tampering
has occurred. Approval process similar to pharmaceuticals.
Similar standards in place.
Thousands of medical devices are covered.
Intraocular lenses, hearing aids, intrauterine
Complete production, control, and distribution devices, cardiac pacemakers, clinical
records: chemistry analyzers, catheters, bypass
machines, dental x-ray equipment, surgical
Maintained for not less than 1 year after gloves, condoms, prosthetic hip joints, traction
expiration date of the batch. equipment, and powered wheelchairs.

must be identified by lot number and product Result to FDA Regulatory actions
quality must be determined through
appropriate testing -Noncompliance determined during a premarket
Salvaging or reprocessing are allowed if approval inspection of facilities as part of an NDA or
specifications are met ANDA application likely would result in a delay of
Complete records must be maintained approval of an otherwise approvable application.
Noncompliance with cGMP regulations during a
regularly scheduled FDA inspection can lead to various
actions, depending on the severity of the offenses.
Not part of the GMP requirements, but when
used effectively they can enhance process
developments, production efficiency, product
quality and compliance,

Good Compounding Practices Applicable to
State-Licensed Pharmacies-Model Act
Eight recommendations
Compounding vs Manufacturing
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8.)Multiple-unit:

-Contain more than a single unit/dose

9.)Tamper-resistant

10.)Light-resistant:

USP: that which holds the article and is or may -Protects the contents from the effects of light
be in direct contact with the article by virtue of the specific properties of the material of
Immediate container - that which is in direct which it is composed, including any coating applied to
contact with the article at all times it. Alternatively, a clear and colorless or a translucent
Must be clean and dry before it is filled, and container may be made light resistant by means of an
must not physically or chemically interact with opaque covering, in which case the label of the
the drug container bears a statement that the opaque covering
is needed until the contents are to be used or
administered.

1.)Well-closed:

-Minimally acceptable container; Protects the
contents from extraneous solids and from loss of the
article under the ordinary or customary conditions of
handling, shipment, storage, and distribution

2.)Tight:

-Protects the contents from contamination by
extraneous liquids, solids, or vapors, from loss of the
article, and from efflorescence, deliquescence, or
evaporation under the ordinary or customary conditions
of handling, shipment, storage and distribution, and is
capable of tight reclosure

3.)Hermetic: Plastic- most widely used

-Impervious to air or any other gas under Advantages:
ordinary conditions
Lighter and more resistant to impact vs glass
4.)Sterile Hermetic: Versatility
Consumer preference (plastic squeeze bottles)
-For parenteral preparations Popularity of blister packaging and unit-dose
dispensing
5.)Single-dose:
Problems encountered:
-Holds a quantity intended for a single dose
and cannot be resealed once opened Permeability - ability of moisture vapor or gas
to enter the plastic
6.)Multiple-dose: Leaching - movement of container
components into the contents
-Hermetic container that allows successive Sorption - binding of molecules to polymer
withdrawals of portions without changing the strength materials
of the contents or endangering the remaining portion's Physical changes (deformation, softening or
quality or purity. hardening) due to contents or external factors.

7.)Single-unit: Types of Plastics:

-Unit-dose Package; Holds a quantity intended 1.)Polyethylene
to be administered as a single dose immediately after
opening Widely used
Good water barrier
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Poor oxygen barrier
Not too clear
Odors, flavors, gases permeate
Cannot be autoclaved

2.)Polypropylene

Very popular
Excellent barrier to water, gases
Not too clear
Can be autoclaved

3.)Polyvinyl Chloride

Clear, rigid To ensure the stability of a pharmaceutical
Good oxygen barrier preparation for the period of its intended shelf life,
Permeable to water the product must be stored in proper conditions.
Yellows when exposed to heat or UV light; The labeling of each product includes the desired
Unsuitable for gamma sterilization conditions of storage.
Used for parenteral solutions and in blister
-Increases the rate of chemical reactions
packaging
1.)High temperatures:
4.)Polystyrene
Sublimation (solid)
Rigid
Solvent loss (liquid)
Crystal clear
Chemical decomposition of dyes (color fading)
Used for solid dosage forms
Phase separation (emulsions)
5.)Polycarbonate Increased sedimentation (suspensions)
Increased disintegration times (tablets)
Clear, transparent
Rigid 2.)Low temperatures
Possible replacement for glass
Crystal formation in solutions
Expensive
Phase separation (emulsions)
6.)Polyethylene terephthalate Increased sedimentation (suspensions)
Cracking of sugar-coated tablets
Excellent transparency and luster
Can be sterilized with gamma radiation 3.)Humidity

4.)Gases

Reduce accidental poisonings. 5.)Light
It is significantly difficult for children under 5
years of age to open or to obtain a harmful
amount of its contents within a reasonable time Risk of container breakage
and that is not difficult for "normal adults" to Loss of strength or potency
use properly. Destructive alteration of dosage form

“When no specific instructions are given, it is
understood to include protection from moisture,
To assist patients in taking their medications
freezing, and excess heat.”
on schedule
Oral contraceptive pills

Stability considerations
Packing considerations
"Drug Facts"
Temperature
Label format and design should be easily read
Humidity
and understood, especially by the elderly
Time
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Shipping schedules

Drug substances are mostly given as a part of a Liquids: many are volatile; those intended PO cannot
formulation. be made into tablets without modification.

Excipients - Pharmaceutical Ingredients;
Nonmedicinal agents combined with the API in a
formulation Particle size
Particle size range
Pharmaceutics - area of study concerned with the Crystal structure
formulation, manufacture, stability, and effectiveness of Particle shape
pharmaceutical dosage forms

Physical, chemical and biologic characteristics must be
considered in the design and formulation of a dosage Vapor pressure.
form. Important in the operation of implantable
pumps delivering medications and also in
aerosol dosage forms; nasal inhalants
Volatile drugs can migrate within a solid
Dosage Forms provide the mechanism for the dosage form.
safe and convenient delivery of accurate Personnel exposure.
dosage
Protection from: Destruction due to oxygen
and humidity, and gastric acid (for drugs given
PO) A defined melting point or range is a
Conceal the unpleasant taste and odor characteristic of a pure substance.
Determination of Purity and Identity
Provide:

Liquid preparations (dispersions or clear
preparations) Dissolution rate
Rate-controlled drug action Bioavailability
Optimal drug action for drugs given topically Content uniformity
For insertion into body orifices; Direct Taste
placement into the bloodstream or tissues; Texture
Optimal drug action when inhaled Color
Stability
Flow characteristics
Sedimentation rates
Physicochemical Properties of the drug Particle size significantly influences the oral
substance absorption profiles of some drugs.
Therapeutic considerations
Age

Crystalline or Amorphous
Different Physicochemical properties such as
-Solids, liquids, gases Melting point and Solubility.
Amorphous form is always more soluble than
1.)Chemical properties the crystal form.
Changes in crystal characteristics would
-Structure, form, reactivity influence bioavailability and stability
2.)Physical properties

-Description, particle size, crystalline structure, Some aqueous solubility for to be
melting point, solubility therapeutically effective
A drug must be in solution for it to enter the
3.)Biological properties
systemic circulation and elicit a response
-Ability to get to the site of action and elicit a To increase solubility, chemical modification
response into salt or ester form
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Equilibrium solubility method 1.)Hygroscopic

- Tend to absorb moisture from the air

Small increases in solubility can be achieved 2.)Deliquescent
by
- Absorb moisture from the air and liquefy
particle size reduction.
Decreases in particle size may enhance 3.)Efflorescent
dissolution rates.
- Give up its water of crystallization and may
become damp and pasty

Adjusting the pH of the solvent can enhance
solubility of the drug.
Electrolytes
Base form or Ester form
Esters are the most important acid derivatives
Dissolution may be the rate-limiting step in the used in pharmacy after salts.
absorption of poorly soluble drugs, especially Important means of preparing prodrugs.
those administered PO or IM.
Can affect onset, intensity, and duration of
response and control overall bioavailability of
API is not 100% active
the drug from the dosage form.
Activity: "Units of activity"; "mcg/mg"
Decrease in particle size, increasing the
Biological potency: IU
solubility in the diffusion layer, use a highly
water-soluble salt of a parent substance

Proteins are the most complex molecules and
biotechnology products
Drug must pass through the biologic
Unstable and have a complicated degradation
membrane (lipid barrier) to elicit a biologic
profiles
response.
Stabilization, formulation, and delivery to the
pKa, solubility, and dissolution rate data can
site
provide an indication of absorption.

evaluation of the physical and chemical
Octanol: water partition coefficient
stability of the pure drug substance.
Shelf life of 2 to 3 years is generally desired
The presence of impurities can lead to
erroneous conclusions in such evaluations.

Extent of dissociation or ionization
Dependent on pH of the medium
Can affect absorption, distribution, and 1.)Hydrolysis
elimination
solvolysis process where water breaks down
molecules
Most important single cause of drug
Most drugs are either Weak acids or Weak decomposition
bases
Used as Salts to increase their aqueous 2.)Oxidation
solubility
destroys many drug types, including
Albuterol sulfate (dosed as the base)
aldehydes, alcohols, phenols, sugars,
Diphenhydramine HCI (dosed as the salt)
alkaloids, and unsaturated fats and oils.
Chemically, oxidation is loss of electrons from
an atom or a molecule.
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1.)Chemical stability- Each active ingredient retains
its chemical integrity and labeled potency within the
specified limits. temperature, humidity, and where appropriate,
oxidation, light and microbial exposure.
2.)Physical stability- Sterility or resistance to
microbial growth is retained according to the specified Active pharmaceutical ingredients
requirements. Antimicrobial agents retain effectiveness Pharmaceutical ingredients added to prepare a
within specified limits dosage form.

3.)Microbiological stability-

4.)Therapeutic stability- The therapeutic effect Drug
remains unchanged. Route of administration
Suitable physical dosage form
5.)Toxicologic stability- No significant increase in Use of chemical derivatives of the drug
toxicity occurs. Control of certain physicochemical and/or
biochemical processes that alter the rate and
extent of response

-Change of drug concentration with respect to time.

Coloring agents
Sweetening agents
- lets the pharmacist estimate shelf life for a product Flavoring agents
that has been stored or is going to be stored under a Surfactants
different set of conditions. Solubilizing agents
Antioxidants
Shelf life estimation Preservatives
Q10 = ef(Ea/R)[(1/T + 10) - (1/7)] Thickening agents
Suspending agents
Binding agents
Done at each stage of product development. Solvents
Product containers and closures must be Lubricants
considered. Perfumes
Temperature and humidity studies. Fats and oils
Light studies.
Changes in physical appearance, color, odor,
taste, texture. Monographs on more than 300 excipients used
Chemical changes of drug degradation. in dosage form preparation
The pharmacist is the last professional to Additional excipients listed in the Food
check for quality and stability prior to Chemicals Codes and National Formulary.
dispensing.

Compliance issues
-To establish the shelf life and storage conditions. Odor, color, and taste
Important for all age groups, especially
-increase the rate of chemical degradation or physical
pediatrics and geriatrics
change of a drug substance or drug product by using
“Electronic tongue” is used to aid in providing
exaggerated storage conditions as part of long-term,
a global “taste fingerprint” during formulation
intermediate, and accelerated studies.
development
The purpose of stability testing is to provide
evidence on how the quality of a drug substance or
drug product varies with time under the influence
of a variety of environmental factors, such as
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Saccharin
Sorbitol
Sucrose

The flavoring of pharmaceuticals applies
primarily to liquids intended for oral
administration -are used in pharmaceutical preparations for esthetics..Complex area.
Important for compliance. A distinction should be made between agents
Color, taste, and odor should generally match that have inherent color and those that are
employed as colorants
Lighter shades preferred

1. Dyes: FD&C, D&C, external D&C
Sour taste H+
2. Lakes: Calcium and aluminum salts
3. Liquids: 0.0005% to 0.001%
Saltiness Anions and cations
4. Powders: 0.1%
5. Caramel
Bitter High MW salts
6. Ferric oxide: Red/yellow
Sweet Polyhydroxyl
compounds,
polyhalogenated Sterilization and preservation
compounds,and alpha Preservative selection
amino acids General preservative considerations
Mode of action
Sharp,biting Unsaturation Preservative utilization
Camphoraceous odor Tertiary "C" atom -to the stabilization of pharmaceutical preparations
against chemical and physical degradation due to
changed environmental conditions within a formulation,
certain liquid and semisolid preparations must be
preserved against microbial contamination.

Dosage form
1.)Pleasant odor Ketones Route of administration
Compatibility with excipients
2.)Methylparaben Floral, gauze pad Container and closure compatibility

3.)Propyl/buty| paraben Numbing mouthfeel From book

prevents the growth of the type of
microorganisms considered the most likely
Immediate flavor identity contaminants of the preparation.
Rapid full flavor development s soluble enough in water to achieve adequate
Acceptable mouthfeel concentrations in the aqueous phase of a
Short aftertaste system with two or more phases.
No undesirable sensations The proportion of preservative remaining
undissociated at the pH of the preparation
makes it capable of penetrating the
microorganism and destroying its integrity.
-Natural versus synthetic
The required concentration of the preservative
does not affect the safety or comfort of the
patient when the pharmaceutical preparation is
Dextrose administered by the usual or intended route;
Mannitol
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that is, it is nonirritating, non sensitizing, and
nontoxic.
has adequate stability and will not be reduced
in concentration by chemical decomposition or
volatilization during the desired shelf life of the 1.)Passive diffusion - passage through a membrane
preparation. driven by the concentration gradient
completely compatible with all other
formulative ingredients and does not interfere 2.)Specialized transport mechanisms - involves
with them nor do they interfere with the membrane components capable of forming a complex
effectiveness of the preservative agent with the drug, which will then move across the
e does not adversely affect the preparation’s membrane, release the drug, and would return to its
container or closure. original surface.

- Active transport
- Facilitated diffusion
Range of activity
Concentration required
pH requirements
1.)Active transport
Compatibility
- A process using a "carrier" with the additional
feature of the drug being moved across the membrane
Modification of cell membrane permeability against a concentration gradient; from lower
Lysis and cytoplasmic leakage concentration to higher concentration
Irreversible coagulation of cytoplasmic
2.)Facilitated diffusion
constituents
Inhibition of cellular metabolism -A specialized transport using the "carrier," but
Oxidation of cellular constituents the drug is not moved against a concentration gradient.
Hydrolysis

It must first be dissolved in the fluid at the
Benzoic acid/sodium benzoate absorption site.
Alcohol Dissolution - process by which drug particles
Phenylmercuric nitrate/acetate dissolve
Phenol Surface Area
Cresol Crystal or Amorphous
Chlorobutanol Salt Form
Benzalkonium chloride Other Factors
Methylparaben/propylparaben
Others

-Particle size has an effect on dissolution rate and
solubility. As shown in the Noyes-Whitney equation,

-When a drug particle is broken up, the total surface
Principles of drug absorption area is increased.
Dissolution and drug absorption
Bioavailability and bioequivalence dC
Routes of drug administration
Fate of drug after absorption dT
Pharmacokinetic principles
= KS(Cs - Ct)

where
-Area of study dealing with the relationship between
physical, chemical, and biological sciences applied to dC/dT is the rate of dissolution (concentration
drugs, dosage forms, and drug action. with respect to time).
K is the dissolution rate constant.
S is the surface area of the particles.
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C. is the concentration of the drug in the - Area under the serum concentration-time
immediate Ere imity of the dissolving particle, curve
that is, the solubility of - represents the total amount of drug absorbed
G is the concentration of the drug in the bulk into the circulation after a single dose
fluid. Bioequivalence of drug products

Blood, Serum, or Plasma Concentration Time curve

1.)Crystalline

Lowest energy state
Ordered

2.)Amorphous

Metastable state
Gradually revert back to crystalline state over
time
Stable and unstable polymorphs
Serum concentration-time curve showing peak
height concentration, time of peak
1.)Solubility- Salts are generally more soluble. concentration, snd AUC.

2.)Dissolution- Salts generally dissolve faster. A Generic Drug Must:

3.)Sodium and potassium salts of weak organic Contain the same active ingredient(s)
acids Be identical in strength, dosage form, and
route of administration
4.)Hydrochloride salts of weak organic bases Have the same indications and precautions for
use and other labeling instructions
Be bioequivalent
Meet the same batch-to-batch requirements for
State of hydration identity, strength, purity, and quality.
Complex formation
Adsorption of drug

1.)Pharmaceutical equivalents

--Describes the rate and extent to which an active drug - Drug products that contain identical amounts
ingredient or therapeutic moiety is absorbed from a of the identical active drug ingredient.
drug product and becomes available at the site of
action 2.)Pharmaceutical alternatives

- Drug products that contain the identical
therapeutic moiety or its precursor but not necessarily
-comparison of bioavailabilities. in the same amount or dosage form or as the same
salt or ester.

3.)Bioequivalent drug products
Drug products whose rate and extents of
absorption do not show a significant difference - Pharmaceutical equivalents or
when administered at the same molar dose pharmaceutical alternatives whose rate and extent of
under similar conditions are bioequivalent. absorption do not show a significant difference.
Blood, serum, or plasma concentration-time
curve 4.)Therapeutic equivalents
Parameters for assessment and comparison of
bioavailability -used to indicate pharmaceutical equivalents
- Peak height (Cmax) that provide essentially the same therapeutic effect
- Time of peak (Tmax) when administered to the same individuals in the same
dosage regimens.
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Intramuscular injections

- are performed deep into the skeletal muscles,
generally the gluteal or lumbar muscles. The
-Drugs are most frequently taken by oral selected site is where the danger of hitting a
administration. nerve or blood vessel is minimal.
1.)Dosage forms applicable Intravenous injections
Tablets, capsules - intravenous administration of drugs, an
Suspensions, solutions, emulsions aqueous solution is injected directly into the
Others vein at a rate

2.)Absorption

Absorption of drugs after oral administration commensurate with efficiency, safety, comfort
may occur at the various body sites between to the patient, and the desired duration of drug
the mouth and rectum response.
he higher up a drug is absorbed along the
alimentary tract, the more rapid will be its Intradermal injections
action, a desirable feature in most instances.
-Intradermal injections are administered into
the corium of the skin, usually in volumes of
about 0.1 mL. Common sites for the injection
Suppositories are the arm and the back. The injections are
frequently performed as diagnostic measures,
-are solid bodies of various weights and as in tuberculin and allergy testing
shapes intended for introduction into a body
orifice (usually rectal, vaginal, or urethral)
where they soften, melt, or dissolve; release
their medication; and exert their drug effects -Drugs are frequently applied topically to the eye, ear,
and mucous membranes of the nose, usually as
Enemas ointments, suspensions, and solutions.

1.)Ocular
-parenteral is derived from the Greek words para, Solutions, suspensions
meaning beside, and enteron, meaning intestine,
which together indicate something done outside of the 2.)Otic
intestine and not by way of the alimentary tract.
Solutions, suspensions, powders
Dosage forms applicable
3.)Nasal
- Solutions, suspensions, emulsions, pellets
Solutions, suspensions, sprays, drops.
-most injectable preparations are either a
sterile suspension or solution of a drug
substance in water or in a suitable vegetable
oil Oral inhalation
Vaginal
-Drugs in solution act more rapidly than drugs Urethral
in suspension, with an aqueous vehicle
providing faster action in each instance than
an oleaginous vehicle.
-After absorption into the general circulation from any
Subcutaneous injections route of administration, a drug may become bound to
blood proteins and delayed in its passage into the
-subcutaneous (hypodermic) administration of surrounding tissues.
drugs entails injection through the skin into the
loose subcutaneous tissue. Drug metabolism, or biotransformation
Excretion of drugs
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Kinetic approach - This approach is based on
the assumption that the therapeutic and toxic
effects of a drug are related to the amount of
drug in the body or to the plasma (or serum)
Metabolism or biotransformation involves concentration of drug at the receptor site.
chemical changes to drugs within the body. Frequency of administration
Results in one or more compounds that are Activity/Toxicity, Pharmacokinetics, Clinical
more water soluble, more ionized, less capable Factors,Others
of binding to proteins of the plasma and
tissues, less capable of being stored in fat
tissue, and less able to penetrate cell
membranes
Consequently, more easily excreted
Also called detoxification or inactivation
Composition -Properly prepared, powders have a
uniform, small particle size that has an elegant
-The excretion of drugs and their metabolites appearance. In general, powders are more stable than
terminates their activity and presence in the body. are liquid dosage forms and are rapidly soluble,
enabling the drug to be absorbed quickly.
Kidney (urine)
Feces Application - Powders have qualities that make them
Lungs an attractive dosage form for certain situations. Unlike
Sweat a standardized capsule or tablet,powders enable a
Saliva primary care provider to easily alter the quantity of
Milk medication for each dose.
Reabsorption of some drugs

The particles of pharmaceutical powders and granules
Half-life may range from being extremely coarse, about 10 mm
(1 cm) in diameter, to extremely fine, approaching
-The half-life (t½) of a drug describes the time colloidal dimensions of 1 μm or less
required for a drug’s blood or plasma
concentration to decrease by half. This fall in
drug concentration is a reflection of metabolic
processes and/or excretion.

Concept of clearance (CIB = Cln + Cl + Clb)
Dosage regimen considerations

-Particle size determinations are complicated by the
fact that particles are not uniform in shape

Dissolution
Suspendability of suspensions
Uniformity of mixtures in liquids
Penetrability of particles for inhalation
Empirical approach - which entails Non grittiness for ointments, creams, gels
administration of a drug in a certain quantity,
noting the therapeutic response and modifying
the amount and interval of dosage accordingly
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If uniform, it will aid in mixing and distribution. 1.)Ball mills
Finer particles may migrate to the bottom.
Larger particles may migrate to the top. - Closed
Differences may change the color intensity of a
powder. - Continuous
Especially important in dermatologicals.

The process of reducing the particle size of a
solid substance to a finer state of subdivision. 2.)Roller mills
Stone mills were the original implement for
3.)Cutter mills
grinding.
Mortars and pestles are the symbol of 4.)Hammer mills
pharmacy.
5.)Colloid mills

Reduce particle size until uniform with other
Facilitate crude drug extraction ingredients.
Increase the dissolution rates of drugs Start with the substance present in the
Aid in the formulation process smallest amount and add ingredient with next
Enhance absorption larger quantity (if practical) using geometric
dilution technique. Also "tracer" method.
Continue adding substances until all are added
Manual and uniformly mixed.
Mechanical

-A process that tends to result in a randomization of
Trituration (to rub to pieces) dissimilar particles within a system
Pill tile and spatulaMortar and pestle
1. Small-scale blending equipment
Porcelain
Wedgewood - Compounding
Glass
2. Large-scale blending equipment

- Manufacturing
1.)Levigation to make smooth

Triturating while moistened with a liquid in
which the powder is insoluble Pill tile and spatula
Mortar and pestle
2.)Pulverization by intervention Bottle/container
Plastic baggie
Comminution by utilizing a solvent that can be
Easily cleanable
easily removed.
Dust tight
Provide complete discharge/recovery

Convective mixing