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INTRODUCTION
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Marketing is the process of communicating the value of a product or service to customers, for the
purpose of selling the product or service. It is a critical business function for attracting customers.
From a societal point of view, marketing is the link between a society’s material requirements and its
economic patterns of response. Marketing satisfies these needs and wants through exchange processes
and building long term relationships. It is the process of communicating the value of a product or service
through positioning to customers. Marketing can be looked at as an organizational function and a set of
processes for creating, delivering and communicating value to customers, and managing customer
relationships in ways that also benefit the organisation and its shareholders. Marketing is the science of
choosing target markets through market analysis and market segmentation, as well as understanding
consumer buying behavior and providing superior customer value.
There are five competing concepts under which organizations can choose to operate their business; the
production concept, the product concept, the selling concept, the marketing concept, and the holistic
marketing concept. The four components of holistic marketing are relationship marketing, internal
marketing, integrated marketing, and socially responsive marketing. The set of engagements necessary
for successful marketing management includes, capturing marketing insights, connecting with customers,
building strong brands, shaping the market offerings, delivering and communicating value, creating long-
term growth, and developing marketing strategies and plans.
Pharmaceutical marketing, sometimes called medico-marketing or pharma marketing in some
countries, is the business of advertising or otherwise promoting the sale of pharmaceuticals or drugs.
There is some evidence that marketing practices can negatively affect both patients and the health care
profession. Many countries have measures in place to limit advertising by pharmaceutical companies.
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Pharmaceutical company spending on marketing far exceeds that spent on research. In Canada, $1.7
billion was spent in 2004 to market drugs to physicians; in the United States, $21 billion was spent in
2002. In 2005 money spent on pharmaceutical marketing in the US was estimated at $29.9 billion with
one estimate as high as $57 billion. When the US numbers are broken down, 56% was free samples, 25%
was detailing of physicians, 12.5% was direct to user advertising, 4% on hospital detailing, and 2% on
journal ads.
The marketing of medication has a long history. The sale of miracle cures, many with little real
potency, has always been common. Marketing of legitimate non-prescription medications, such as pain
relievers or allergy medicine, has also long been practiced, although, until recently, mass marketing of
prescription medications has been rare. It was long believed that since doctors made the selection of
drugs, mass marketing was a waste of resources; specific ads targeting the medical profession were
thought to be cheaper and just as effective. This would involve ads in professional journals and visits by
sales staff to doctor’s offices and hospitals. An important part of these efforts was marketing to medical
students
To health care providers
Marketing to health care providers takes four main forms: gifting, detailing, drug samples, and
sponsoring continuing medical education (CME).Of the 237,000 medical sites representing 680,000
physicians surveyed in SK&A's 2010 Physician Access survey, half said they prefer or require an
appointment to see a rep (up from 38.5% preferring or requiring an appointment in 2008), while 23%
won't see reps at all, according to the survey data. Practices owned by hospitals or health systems are
tougher to get into than private practices, since appointments have to go through headquarters, the survey
found. 13.3% of offices with just one or two doctors won't see reps, compared with a no-see rate of 42%
at offices with 10 or more docs The most accessible physicians for promotional purposes are
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allergists/immunologists – only 4.2% won't see reps at all – followed by orthopedic specialists (5.1%)
and diabetes specialists (7.6%). Diagnostic radiologists are the most rigid about allowing details – 92.1%
won't see reps – followed by pathologists and neuroradiologists, at 92.1% and 91.8%, respectively.
Edetailing is widely used to reach "no see physicians"; approximately 23% of primary care physicians
and 28% of specialists prefer computer-based edetailing, according to survey findings reported in the
April 25, 2011, edition of American Medical News (AMNews), published by the American Medical
Association (AMA).
New pharma code & guidelines
The Pharmaceutical Research and Manufacturers of America (PhRMA) released updates to its voluntary
Code on Interactions with Healthcare Professionals on July 10. The new guidelines take effect January
2009."
In addition to prohibiting small gifts and reminder items such as pens, notepads, staplers, clipboards, pill
boxes, etc., the revised Code:
1. Prohibits company sales representatives from providing restaurant meals to healthcare
professionals, but allows them to provide occasional meals in healthcare professionals’ offices in
conjunction with informational presentations"
2. Includes new provisions requiring companies to ensure their representatives are sufficiently
trained about applicable laws, regulations, and industry codes of practice and ethics.
3. Provides that each company will state its intentions to abide by the Code and that company CEOs
and compliance officers will certify each year that they have processes in place to comply
4. Includes more detailed standards regarding the independence of continuing medical education.
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5. Provides additional guidance and restrictions for speaking and consulting arrangements with
healthcare professionals.
However, the Good Works Health government-approved platform offers physicians and other health care
professionals the opportunity to direct donations to charities of their choice in exchange for participation
in pharmaceutical promotional/educational programs.
Free samples
Free samples have been shown to affect physician prescribing behaviour. Physicians with access to free
samples are more likely to prescribe brand name medication over equivalent generic medications. Other
studies found that free samples decreased the likelihood that physicians would follow standard of care
practices.
Receiving pharmaceutical samples does not reduce prescription costs. Even after receiving samples,
sample recipients remain disproportionately burdened by prescription costs.
It is argued that a benefit to free samples is the “try it before you buy it” approach. Free Samples give
immediate access to the medication and the patient can begin treatment right away. Also, it saves time
from going to a pharmacy to get it filled before treatment begins. Since not all medications work for
everyone, and many do not work the same way for each person, free samples allow patients to find which
dose and brand of medication works best before having to spend money on a filled prescription at a
pharmacy.
Sale and techniques of sales
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To become a successful sales representative you need to have a solid understanding of selling concepts.
These concepts give you the foundation to understand why customers act the way they do and provide a
guide as to how to use your selling skills to overcome obstacles and increase sales.
Successful Selling Steps
If we consider the steps most successful sales representatives go through to increase their effectiveness
on sales calls, we will see there are three general areas for consideration:
1. Business Planning
2. The Sales Call (pre-call, sales call, post-call)
3. Follow-Up
Business planning is a critical step in ensuring your selling skills are most effective. Sales representatives
in the healthcare industry manage their territories as if they were running their own business. To be
successful in your sales territory you need to fully understand it before you attempt to call on customers.
This includes knowing which customers drive your business, what their “buying” style is so you can
match your selling style to it, managing an investment budget, managing your daily and weekly schedule,
and working with your team to implement the territory business plans. You can view the business
planning process as creating a blueprint for success. Most healthcare companies will give you a territory,
a list of target customers, the sales tools needed to influence your target customers and a budget. It is up
to you and your territory team to come up with a plan that will most effectively make use of these
resources to increase sales.
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Following the business planning process, there are three main steps to consider to improve your sales call
effectiveness:
1. Pre-call planning (before you meet the customer)
2. The sales call (face to face with the customer)
3. Post-call analysis and follow-up (after your sales call)
Pre-call planning done prior to meeting your customer involves several steps such as reviewing past
customer call notes, setting call objectives and preparing sales tools to be most effective in the short time
with your customer. This will be covered in more detail shortly.
During the actual sales call itself, there are several steps to be aware of: opening, presenting features and
benefits, probing, objection handling, etc. Making an effective sales call involves excellent skills within
each of these areas and we will cover them more in-depth in the coming chapters.
After leaving each and every sales call, post-call analysis needs to be completed, and any follow-up
required accurately recorded and completed. These notes which you make post-call are what you will be
reviewing prior to your next appointment with your customers. Without having these notes, your
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effectiveness on the next call will not be as high.
One major goal of a healthcare sales representative is to be seen as a valued consultant by customers.
Once you are viewed by your target customers as an excellent and credible resource (and not just another
sales representative) you will have increased access and time with them – and increased face-to-face
selling time is a key ingredient for success in healthcare sales. Ensuring timely follow-up to customer
requests in a professional manner will go a long way in ensuring you become that value added consultant
in their practices.
The Sales Cycle
A sales cycle is the stages that a typical customer goes through before agreeing to purchase or use your
product. Although the ultimate goal is a sale, there are several stages which you must take the customer
through before you can ask for the business.
In the first stage, called Introduction and Awareness, the customer is not yet aware that you or your
products exist. They may not even know about any problems they are currently facing because they have
not taken the time to consider them. Your goal with a customer at this stage is to introduce your products
and services and try to identify any problem areas which your product can solve for them, their patients
or the healthcare system. Moving a customer through this stage is sometimes not easy and requires
certain sales techniques. Techniques used to move a customer from this stage to the next one are rapport
building, probing, objection handling, and gaining feedback. Throughout this book you will learn how to
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improve each of these skills to be successful in a healthcare sales role.
The second stage is Identification. At this stage you need to convince the customer that a problem does
indeed exist. This is sometimes the hardest stage to get through as many customers will tell you that they
are happy with their current product. To move the customer through this stage, sales skills such as
presenting features and benefits, probing, gaining feedback, and the ability to handle objections will be
needed.
In the third stage, the Knowledge stage, you must educate the customer on what your company and
products offer using the features and benefits of your products and or services. Without the proper
knowledge of what you and your company can offer (to the customer, the patient or the healthcare
system), the customer will not be able to evaluate his options properly. Excellent use of features and
benefits, probing, and objection handling will help you to move the customer through this stage to the
evaluation stage.
The Evaluation stage is where the customer takes the time to compare your product to that which he is
currently using. It is sometimes extremely difficult to change the habits of a customer, so persuasion and
persistence is needed. Realizing where the customer is at within this sales cycle will help you to maintain
perspective and use the appropriate sales skills to move him along the sales cycle. This is where your
needs analysis is critical, as you want to ensure you are reinforcing, on a frequent basis, the benefits your
product or service offers versus your competition in addressing THAT particular customer’s needs. To
move the customer through this stage you need to present strong features and benefits, use excellent
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competitive selling techniques in addition to probing and strong skills.
In the final stage, the customer makes a Decision to use your product or service or your competitors. If
he has chosen your product, you can feel good about taking your customer through the sales cycle and
convincing him of the benefits of your product versus the competition. If the customer does not choose
your product or service, then your job will be to take him back to the evaluation stage so he can re-
evaluate the options and reconsider your product. Sometimes this is very difficult to do, as they may be
very happy with what they are currently using. You may have to take them all the way back to the
identification stage to find new opportunities or problems which your product can address and your
competitor cannot. This is a very dynamic model, and each customer you deal with will be at a different
stage in this cycle. It is your job to identify where that customer is and try to get him to the next stage
using effective selling techniques.
Think of the sales cycle as a series of steps that you are climbing. Before you reach the top step (the
sale), you have to walk the customer up each of the lower steps first. It is very rare that you will meet a
customer for the first time and walk away with a sale. You need to complete the steps in the cycle and
earn the right to ask for the business.
Another concept to keep in mind is that the time needed to move a customer through the sales cycle
varies based on several factors:
1. Type of product – Healthcare sales products which are more expensive (such as capital equipment
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for use in hospitals) often requires consensus from a committee before the contract is signed. As a result,
to get all members of the committee to agree takes quite a bit longer than a sale where only one customer
needs to say “yes”.
2. Frequency of sales calls – The more frequently you are able to get face to face selling time with a
customer, the quicker you will be able to move them through the sales cycle…IF you have developed
excellent selling skills.
3. Representative selling skills – Without effective selling skills, you will not be able to move
customers through the sales cycle. To move them more quickly through the sales cycle, you must
continually develop and improve on all of the sales skills listed in this book.
Of the three listed here, representative selling skills is by far the most important one which affects the
time needed to move a customer through the sales cycle.
The Customer Environment
Before we discuss each stage and the selling skills needed, we will consider the customer environment.
The healthcare customer environment and selling into it requires a significant amount of planning,
preparation, persistence and versatility to be effective. As you will learn, time is a very valuable
commodity in the healthcare office or clinic, and making effective use of your time is critical to move
that customer along the sales cycle to a decision which is favorable for your product or service. The key
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to success in this environment is ensuring you are calling on the right customer, the right number of
times using the right message!
Why is it getting more difficult to get time with our customers?
Over the past several years, it has been getting more and more difficult to access customers in the
healthcare industry, and those that can be accessed are giving less and less time to sales representatives.
We will now have a look at some of the main reasons this is occurring:
1. Time Pressures – Today’s professionals try to squeeze more work into a day. Some physicians see
between 30 and 60 patients per day. In addition to seeing patients, physicians need to finish patient
charts, fill out insurance and lawyer’s reports, return phone calls and attend meetings. This is in addition
to trying to have a life outside the office and spending quality time with their families. Five minutes with
a representative is five minutes they could have spent completing other tasks.
2. Lack of Monetary Gain – Physicians do not get paid to see representatives but they do get paid to
see patients. If they could see a patient in the time it takes to talk to a representative then they are losing
money every time they talk to a representative. This reiterates the fact that you must provide value to
your target customers on each and every call if you want to continue to get face time with them.
3. Number of Representatives – In many offices that see representatives, it is not uncommon for six
or more representatives to visit on any given day. The sheer number representatives can be
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overwhelming, not only to the physician, but to the medical office assistants who have to deal with the
patients in the waiting room.
4. Lack of Value Seen – This is the most important factor to keep in mind as you work on your
territory. If a physician truly believes that seeing a particular sales representative will add value to his
practice, he will take the time away from his patients to hear what that representative has to say.
However, if he feels that a representative will bring no value, he will likely not spend any time with him
or her. There can be various reasons for this, but the number one reason is that only the best
representatives take the time to identify “true” needs of each customer and sell to that particular need.
There are a lot of representatives who do not take the time to identify needs, involve the customer in the
sales call, or prepare for each call to ensure value is seen every time. Without providing value to your
key customers you will not be able to get adequate selling time to be effective.
Key Terms
To be most successful as a healthcare sales representative, you must understand two key terms: targeting
and frequency.
Targeting: The Right Customer
When considering who your target customers are, there are two key questions to ask: how important is
this customer to your business and how accessible is the customer to you?
How important is this customer to your business?
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When considering this factor you need to look at not only how busy their practice is, but also what their
patient demographics are. Yes, you must call on customers who see many patients per day, but if they are
not the right types of patients for your products, then you are wasting your time. For example, if you are
selling a medication for high blood pressure and you are calling on a busy physician who sees mainly
younger women and children, this is not likely a good use of your time. It is crucial that you look at both
how busy your customer is and what types of patients they most commonly treat. Generally speaking,
the more patients a customer sees the better, as long as these are the types of patients your product will
help.
How does a representative find out what types of patients a customer may see?
There are many ways including viewing the waiting room to profile the patients waiting to see the
physician, looking to see what types of product samples are on the shelves, and asking the medical office
assistant or local pharmacist what types of patients the area services. If all else fails, ask your physician!
They will usually give you a straight up answer as to the types of patients they look after. Just remember,
it’s not just the busy physicians who are important to you – they may be busy, but may not be seeing your
targeted patient population. If this is the case, they may not be a true target physician for you.
How accessible is your customer?
If you have a customer who is extremely busy and services the types of patients that would be a great fit
for your product, it makes sense that they should be a target for you. However, what if this physician is
not willing to see you as a sales representative even though you have tried many ways to see him or her?
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In this situation, it may be wiser to take them off your target list and replace them with another customer
that you have access to. However, it is important to remember that just because you have tried a couple
of times to see this customer and have not had success, it does not mean they are not accessible. You
need to try every means possible (using all of the activities you read about in the Introduction to the
Pharmaceutical Sales Industry from PharmaCareer) to ensure that there is not some way that you can
access this customer. There are many times a customer seems inaccessible but somehow, someway, you
manage to make contact with them. These can end up being your best supporters as much of your
competition may have given up calling on them, giving you the opportunity to sell to them in a less
competitive environment. It is important to remember that on average you will need to make contact
with your targeted customers six to twelve times a year to make an impact. Seeing a customer once every
two years is not going to make much of an impact on your sales!
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Relationship between Sales and Marketing
Most people confuse between sales and marketing. It’s actually pretty straightforward: Marketers create
demand, and the sales team execute accordingly to fulfill that demand. Similar to design and marketing,
both teams share a symbiotic relationship – one cannot benefit without the other, yet they don’t speak the
same language. Each have their own jargons and lingoes they throw around one other, and it’s not
helping your company to grow. How can you put an end to the ceaseless sales and marketing dispute?
Let’s take a closer look at their dynamics.
We all know that poor communication discourages any form of relationship. A disconnect between your
teammates discourages your business efforts to maximize value for both your company and your
customers. Common conflicts include:
Losing focus
You may think that joint metrics in sales and marketing saves time, money, and energy. On the contrary,
this culture is exactly what’s causing that blurry distinction between sales and marketing – when they’ve
led a successful campaign, everyone shares the reward. When all else fails, team members blame one
another.
Separatistic culture
Each team is too focused on individual tasks. Marketers work out the grand plan, sales wants to close the
deal ASAP. Marketers work behind the desk, sales are out in the field. Marketers are strategic thinkers
who are highly analytical and data-oriented, and they’re motivated by providing creative solutions for the
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long haul. Sales wants to generate maximum revenue as they’re usually compensated by commissions,
quotas, bonuses, and so on.
What about the customers?
We’re living in the digital era, and as a business leader it’s your responsibility for everyone in your team
to understand that consumers’ buying behaviors are changing.
For your product or service to successfully penetrate the new demand, you need to redesign your strategy
through a coherent series of campaigns, promotions, advertising, and other efforts.
This is where your marketing and salesforce must learn to cooperate, because no matter how brilliant the
plan is, your company will never profit when people simply don’t buy.
There are 4 essential steps a customer goes through before they decide to buy from you:
1. Awareness They know your existence. They look forward to seeing you again.
2. Consideration They go home and think about you – a sign that you’ve addressed their needs and
you promise to deliver.
3. Preference They like you more than your competitors, thanks to your excellent presentations and
proposals.
4. Conversion They’re ready to negotiate contracts and proceed to sales.
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Converting leads to sales is tricky, and identifying qualified leads takes time. To foster strong customer
relationships, it takes a collaborative effort from every department of your company.
Teamwork: Two heads are better than one
True, your marketing plan should be solid, but it must also be flexible enough to integrate its
functions with the sales team. Similarly, salesforce must have a clear understanding of what is expected
out of each campaign.
When both teams start speaking the same language, they’re more engaged in executing every step of the
process from start to finish.
Align your sales and marketing operations to build on the following equities:
Loyalty This is the foundation for word-of-the-mouth marketing. At this point, your focus is to
educate and nurture first-time and regular customers. You’ve earned their trust, and you’ve got to
maintain that by giving quality service and continuous support.
Advocacy When customers are loyal to your brand, they help you build referrals for future
prospects. Consider it a success when your users, fans, and customers supports your brand more
than anything else.
In a nutshell, it’s your job as a leader to encourage effective communication among your teammates.
Instead of blaming one another, shift their focus on customers instead: What are their wants and needs?
Once demands are clearly outlined, it gets easier to guide your teams and define exactly you expect out of
each team.
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Ultimately, your goal as a leader is to manage a stable brand and reputation. Everyone in your company
must commit and connect to remain consistent with your vision and mission.
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Omeprazole
Drug Omeprazole
Omeprazole is a proton pump inhibitor used in the treatment of dyspepsia, peptic ulcer disease
(PUD), gastroesophageal reflux disease (GORD/GERD), laryngopharyngeal reflux (LPR), and
Zollinger-Ellison syndrome. It was first marketed in the US in 1989 by AstraZeneca under the brand
names Losec and Prilosec, and is now also available from generic manufacturers under various brand
names. AstraZeneca markets omeprazole as Losec, Antra, Gastroloc, Mopral, Omepral, and Prilosec.
Omeprazole is marketed as Zegerid by Santarus, Prilosec OTC by Procter & Gamble and Zegerid OTC
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by Schering-Plough. In India it is available as OMEZ (FGP). Omeprazole is one of the most widely
prescribed drugs internationally and is available over the counter in some countries.
Pharmacology
Omeprazole is a racemate. It contains a tricoordinated sulfur atom in a pyramidal structure and
therefore can exist in equal amounts of both the S and R enantiomers. In the acidic conditions of the
stomach, both are converted to achiral products, which react with a cysteine group in H + /K
+ ATPase ,
thereby inhibiting the ability of the parietal cells to produce gastric acid.
Name change
In 1990, at the request of the U.S. Food and Drug Administration (FDA), the brand name Losec
was changed to Prilosec to avoid confusion with the diuretic Lasix (furosemide). Unfortunately, the new
name has led to confusion between omeprazole (Prilosec) and fluoxetine (Prozac), an antidepressant.
Drug Profile
Generic Name: Omeprazole
Brand names: Losec & Prilosec
Category: proton pump inhibitor
Helicobacter pylori eradication
Molecular formula: C17 H19 N3 O3 S
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Chemical name: 6-methoxy-2-((4-methoxy-3,5-dimethylpyridin-2-yl)
(methylsulfinyl)-1H-benzo[d]imidazole
Chemical structure:
Molecular weight: 345.42
Colour: white to off-white
Solubility in water: 0.25 g/L
Solubility in methanol : 10 g/L.
Melting Point: 200°C
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Pka Values: benzimidazole (Omeprazole base)=8.8 and pyridinium ion=4.0
Physical appearance: crystalline powder having 2 to 4 waters of hydration
Dose:
Short-Term Treatment of Active Duodenal Ulcer :
The recommended adult oral dose of PRILOSEC is 20 mg once daily. Most patients heal within four
weeks. Some patients may require an additional four weeks of therapy.
Gastric Ulcer:
The recommended adult oral dose is 40 mg once daily for 4-8 weeks.
Gastro-esophageal Reflux Disease (GERD):
The recommended adult oral dose for the treatment of patients with symptomatic GERD and no
esophageal lesions is 20 mg daily for up to 4 weeks. The recommended adult oral dose for the treatment
of patients with erosive esophagitis and accompanying symptoms due to GERD is 20 mg daily for 4 to 8
weeks.
Maintenance of Healing of Erosive Esophagitis:
The recommended adult oral dose is 20 mg daily.
Pediatric Patients
For the treatment of GERD and maintenance of healing of erosive esophagitis, the recommended
daily dose for pediatric patients 1 to 16 years of age is as follows:
Patient Weight Omeprazole Daily Dose
5 < 10 kg 5 mg
10 < 20 kg 10 mg
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> 20 kg 20 mg
On a per kg basis, the doses of omeprazole required to heal erosive esophagitis in pediatric patients
are greater than those for adults.
Alternative administrative options can be used for pediatric patients unable to swallow an intact
capsule.
Dosage forms:
Omeprazole is available as tablets and capsules (containing omeprazole or omeprazole magnesium) in
strengths of 10 mg, 20 mg, 40 mg, and in some markets 80 mg; and as a powder (omeprazole sodium) for
intravenous injection. Most oral omeprazole preparations are enteric-coated, due to the rapid degradation
of the drug in the acidic conditions of the stomach. This is most commonly achieved by formulating
enteric-coated granules within capsules, enteric-coated tablets, and the multiple-unit pellet system
(MUPS).
It is also available for use in injectable form (I.V.) in Europe, but not in the U.S. The injection pack is a
combination pack consisting of a vial and a separate ampule of reconstituting solution. Each 10 ml clear
glass vial contains a white to off-white lyophilised powder consisting of omeprazole sodium 42.6 mg
equivalent to 40 mg of omeprazole.
.
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History
Omeprazole was first marketed in the U.S. in 1989 by Astra AB, now AstraZeneca under the brand
names Losec and Prilosec. An over the counter brand, Prilosec OTC, is available without prescription in
the US for treatment of heartburn. It is now also available from generic manufacturers under various
brand names.
In 1990, at the request of the U.S. Food and Drug Administration (FDA), the brand name Losec was
changed to Prilosec to avoid confusion with the diuretic Lasix (furosemide).[29] The new name has led to
confusion between omeprazole (Prilosec) and fluoxetine (Prozac), an antidepressant.[29]
AstraZeneca markets omeprazole as Losec, Antra, Gastroloc, Mopral, Omepral, and Prilosec.
Omeprazole is marketed as Zegerid by Santarus, Prilosec OTC by Procter & Gamble and Zegerid OTC
by Schering-Plough and as Segazole by Star Laboratories in Pakistan.[30][31] In the Philippines, Ajanta
Pharma markets omeprazole under the brand name Zegacid. Dr. Reddy's Laboratories markets it as Omez
in India, Russia, Romania, and South Africa. In Bangladesh Healthcare Pharmaceuticals Ltd. marketed
omeprazole under the brand name Opal. In Bangladesh Apex Pharma also markets omeprazole under the
brand name Aspra. It is also available under the brand name Rome 20 marketed by Rephco
Pharmaceuticals Ltd. In Bangladesh the brand leader in this market is Seclo. In Argentina it is made by
Bago Laboratories S.A. and available there and in Ecuador as Ulcozol. In Indonesia Darya-Varia
Laboratories marketed omeprazole as Ozid. In Brazil, omeprazole is produced by Multilab under the
name Lozeprel. In Spain it is produced by Cantabria Pharma S.L. under the name emeprotón. In
Bangladesh, Eskayef Bangladesh Limited also marketed omeprazole under the brand name Losectil. The
Acme Laboratories Limited marketed it under the brand name PPI.
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In 1999, antiulcerants were the leading class of therapeutic drugs, with $15.6 billion in global sales. Of
that, Prilosec accounted for $5.91 billion, making it the best-selling drug on the market.[32]
Although Prilosec's U.S. patent expired in April 2001, AstraZeneca was able to delay the introduction of
generic versions through lawsuits and peripheral patent claims. It introduced Nexium as a patented
replacement drug.[33]
Dosage forms
This section does not cite any references or sources. Please help improve this section by adding citations to reliable
sources. Unsourced material may be challenged and removed. (April 2013)
Package of Losec (Omeprazole) 20 mg, purchased in Hong Kong
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Omeprazole 10 mg, From U.K.
Omeprazole is available as tablets and capsules (containing omeprazole or omeprazole magnesium) in
strengths of 10 mg, 20 mg, 40 mg, and in some markets 80 mg; and as a powder (omeprazole sodium) for
intravenous injection. Most oral omeprazole preparations are enteric-coated, due to the rapid degradation
of the drug in the acidic conditions of the stomach. This is most commonly achieved by formulating
enteric-coated granules within capsules, enteric-coated tablets, and the multiple-unit pellet system
(MUPS).
It is also available for use in injectable form (I.V.) in Europe, but not in the U.S. The injection pack is a
combination pack consisting of a vial and a separate ampule of reconstituting solution. Each 10 ml clear
glass vial contains a white to off-white lyophilised powder consisting of omeprazole sodium 42.6 mg
equivalent to 40 mg of omeprazole.
Multiple unit pellet system
Omeprazole tablets manufactured by AstraZeneca (notably Losec/Prilosec) are formulated as a "multiple
unit pellet system" (MUPS). Essentially, the tablet consists of extremely small enteric-coated granules
(pellets) of the omeprazole formulation inside an outer shell. When the tablet is immersed in an aqueous
solution, as happens when the tablet reaches the stomach, water enters the tablet by osmosis. The
contents swell from water absorption causing the shell to burst, releasing the enteric-coated granules. For
most patients, the multiple-unit pellet system is of no advantage over conventional enteric-coated
preparations. Patients for which the formulation is of benefit include those requiring nasogastric tube
feeding and those with difficulty swallowing (dysphagia) because the tablets can be mixed with water
ahead of time, releasing the granules into a slurry form, which is easier to pass down the feeding tube or
to swallow than the pill.[citation needed] The granules are manufactured in a fluid air bed system. Sugar spheres
27
in suspension are sequentially sprayed with aqueous suspensions of omeprazole, a protective layer, an
enteric coating and an outer layer to reduce granule aggregation. The granules are mixed with other
excipients and compressed into tablets. Finally, the tablets are film-coated to improve the stability and
appearance of the preparation. Also available in a liquid suspension form, from a compounding
pharmacy. Ideal for infants.
Immediate release formulation
In June 2004 the FDA approved an immediate release preparation of omeprazole and sodium bicarbonate
that does not require an enteric coating. This preparation employs sodium bicarbonate as a buffer to
protect omeprazole from gastric acid degradation. This allows for the production of chewable tablets.
This combination preparation is marketed in the United States by Santarus under the brand name Zegerid.
Zegerid is marketed as capsules, chewable tablets, and powder for oral suspension. Zegerid is most useful
for those patients who suffer from nocturnal acid breakthrough (NAB) or those patients who desire
immediate relief. In India it is marketed by Dr. Reddy's Laboratories as powder formulation with the
brand name OMEZ-INSTA. It is reported to have additional benefits with patients suffering from
alcoholic gastritis and life-style associated gastritis.
28
Mechanism of Action:
Omeprazole belongs to a class of antisecretory compounds, the substituted benzimidazoles, that suppress
gastric acid secretion by specific inhibition of the H+/K+ ATPase enzyme system at the secretory surface
of the gastric parietal cell. Because this enzyme system is regarded as the acid (proton) pump within the
gastric mucosa, omeprazole has been characterized as a gastric acid-pump inhibitor, in that it blocks the
final step of acid production. This effect is dose-related and leads to inhibition of both basal and
stimulated acid secretion irrespective of the stimulus. Animal studies indicate that after rapid
disappearance from plasma, omeprazole can be found within the gastric mucosa for a day or more.
Animal Pharmacology
Pharmacodynamics:
Antisecretory Activity:
After oral administration, the onset of the antisecretory effect of omeprazole occurs within one hour, with
the maximum effect occurring within two hours. Inhibition of secretion is about 50% of maximum at 24
hours and the duration of inhibition lasts up to 72 hours. The antisecretory effect thus lasts far longer than
would be expected from the very short (less than one hour) plasma half-life, apparently due to prolonged
binding to the parietal H+/K+ ATPase enzyme. When the drug is discontinued, secretory activity returns
gradually, over 3 to 5 days. The inhibitory effect of omeprazole on acid secretion increases with repeated
once-daily dosing, reaching a plateau after four days.
29
Results from numerous studies of the antisecretory effect of multiple doses of 20 mg and 40 mg of
omeprazole in normal volunteers and patients are shown below. The “max” value represents
determinations at a time of maximum effect (2-6 hours after dosing), while “min” values are those 24
hours after the last dose of omeprazole.
Serum Gastric Effects
In studies involving more than 200 patients, serum gastrin levels increased during the first 1 to 2 weeks
of once-daily administration of therapeutic doses of omeprazole in parallel with inhibition of acid
secretion. No further increase in serum gastrin occurred with continued treatment. In comparison with
histamine H2-receptor antagonists, the median increases produced by 20 mg doses of omeprazole were
higher (1.3 to 3.6 fold vs. 1.1 to 1.8 fold increase). Gastrin values returned to pretreatment levels, usually
within 1 to 2 weeks after discontinuation of therapy.
Enterochromaffin-like (ECL) Cell Effects
Human gastric biopsy specimens have been obtained from more than 3000 patients treated with
omeprazole in long-term clinical trials. The incidence of ECL cell hyperplasia in these studies increased
with time; however, no case of ECL cell carcinoids, dysplasia, or neoplasia has been found in these
patients. However, these studies are of insufficient duration and size to rule out the possible influence of
long-term administration of omeprazole on the development of any premalignant or malignant
conditions.
Other Effects
30
Systemic effects of omeprazole in the CNS, cardiovascular and respiratory systems have not been found
to date. Omeprazole, given in oral doses of 30 or 40 mg for 2 to 4 weeks, had no effect on thyroid
function, carbohydrate metabolism, or circulating levels of parathyroid hormone, cortisol, estradiol,
testosterone, prolactin, cholecystokinin or secretin.
No effect on gastric emptying of the solid and liquid components of a test meal was demonstrated after a
single dose of omeprazole 90 mg. In healthy subjects, a single I.V. dose of omeprazole (0.35 mg/kg) had
no effect on intrinsic factor secretion. No systematic dose-dependent effect has been observed on basal or
stimulated pepsin output in humans.
However, when intragastric pH is maintained at 4.0 or above, basal pepsin output is low, and pepsin
activity is decreased.
As do other agents that elevate intragastric pH, omeprazole administered for 14 days in healthy subjects
produced a significant increase in the intragastric concentrations of viable bacteria. The pattern of the
bacterial species was unchanged from that commonly found in saliva. All changes resolved within three
days of stopping treatment.
Pharmacokinetics
Absorption and Distribution:
OMEPRAZOLE Delayed-Release Capsules contain an enteric-coated granule formulation of omeprazole
(because omeprazole is acid-labile), so that absorption of omeprazole begins only after the granules leave
the stomach. Absorption is rapid, with peak plasma levels of omeprazole occurring within 0.5 to 3.5
hours. Peak plasma concentrations of omeprazole and AUC are approximately proportional to doses up to
31
40 mg, but because of a saturable first-pass effect, a greater than linear response in peak plasma
concentration and AUC occurs with doses greater than 40 mg. Absolute bioavailability (compared with
intravenous administration) is about 30-40% at doses of 20-40 mg, due in large part to presystemic
metabolism. In healthy subjects the plasma half-life is 0.5 to 1 hour, and the total body clearance is 500-
600 mL/min.
Based on a relative bioavailability study, the AUC and Cmax of OMEPRAZOLE (omeprazole
magnesium) for Delayed-Release Oral Suspension were 87% and 88% of those for OMEPRAZOLE
Delayed-Release Capsules, respectively.
The bioavailability of omeprazole increases slightly upon repeated administration of OMEPRAZOLE
Delayed-Release Capsules.
OMEPRAZOLE Delayed-Release Capsule 40 mg was bioequivalent when administered with and without
applesauce. However, OMEPRAZOLE Delayed-Release Capsule 20 mg was not bioequivalent when
administered with and without applesauce. When administered with applesauce, a mean 25% reduction in
Cmax was observed without a significant change in AUC for OMEPRAZOLE Delayed-Release Capsule
20 mg. The clinical relevance of this finding is unknown.
Distribution
Protein binding is approximately 95%.
Metabolism:
Omeprazole is extensively metabolized by the cytochrome P450 (CYP) enzyme system.
32
Excretion:
Following single dose oral administration of a buffered solution of omeprazole, little if any unchanged
drug was excreted in urine. The majority of the dose (about 77%) was eliminated in urine as at least six
metabolites. Two were identified as hydroxyomeprazole and the corresponding carboxylic acid. The
remainder of the dose was recoverable in feces. This implies a significant biliary excretion of the
metabolites of omeprazole. Three metabolites have been identified in plasma — the sulfide and sulfone
derivatives of omeprazole, and hydroxyomeprazole. These metabolites have very little or no antisecretory
activity.
Side Effects:
The safety data described below reflects exposure to OMEPRAZOLE Delayed-Release Capsules in 3096
patients from worldwide clinical trials (465 patients from US studies and 2,631 patients from
international studies). Indications clinically studied in US trials included duodenal ulcer, resistant ulcer,
and Zollinger-Ellison syndrome. The international clinical trials were double blind and open-label in
design. The most common adverse reactions reported (i.e., with an incidence rate ≥ 2%) from
OMEPRAZOLE-treated patients enrolled in these studies included headache (6.9%), abdominal pain
(5.2%), nausea (4.0%), diarrhea (3.7%), vomiting (3.2%), and flatulence (2.7%).
Additional adverse reactions that were reported with an incidence ≥ 1% included acid regurgitation
(1.9%), upper respiratory infection (1.9%), constipation (1.5%), dizziness (1.5%), rash (1.5%), asthenia
(1.3%), back pain (1.1%), and cough (1.1%).
33
The clinical trial safety profile in patients greater than 65 years of age was similar to that in patients 65
years of age or less.
The clinical trial safety profile in pediatric patients who received OMEPRAZOLE Delayed-Release
Capsules was similar to that in adult patients. Unique to the pediatric population, however, adverse
reactions of the respiratory system were most frequently reported in both the 1 to < 2 and 2 to 16 year age
groups (75.0% and 18.5%, respectively). Similarly, fever was frequently reported in the 1 to 2 year age
group (33.0%), and accidental injuries were reported frequently in the 2 to 16 year age group (3.8%).[See
Use in Specific Populations]
Clinical Trials Experience with OMEPRAZOLE in Combination Therapy for H. pylori Eradication
In clinical trials using either dual therapy with OMEPRAZOLE and clarithromycin, or triple therapy with
OMEPRAZOLE, clarithromycin, and amoxicillin, no adverse reactions unique to these drug
combinations were observed. Adverse reactions observed were limited to those previously reported with
omeprazole, clarithromycin, or amoxicillin alone.
Dual Therapy (OMEPRAZOLE/clarithromycin)
Adverse reactions observed in controlled clinical trials using combination therapy with OMEPRAZOLE
and clarithromycin (n = 346) that differed from those previously described for OMEPRAZOLE alone
were taste perversion (15%), tongue discoloration (2%), rhinitis (2%), pharyngitis (1%) and flu-syndrome
(1%). (For more information on clarithromycin, refer to the clarithromycin prescribing information,
Adverse Reactions section).
Triple Therapy (OMEPRAZOLE/clarithromycin/amoxicillin)
34
The most frequent adverse reactions observed in clinical trials using combination therapy with
OMEPRAZOLE, clarithromycin, and amoxicillin (n = 274) were diarrhea (14%), taste perversion (10%),
and headache (7%). None of these occurred at a higher frequency than that reported by patients taking
antimicrobial agents alone. (For more information on clarithromycin or amoxicillin, refer to the
respective prescribing information, Adverse Reactions sections).
The following adverse reactions have been identified during post-approval use of OMEPRAZOLE
Delayed-Release Capsules. Because these reactions are voluntarily reported from a population of
uncertain size, it is not always possible to reliably estimate their actual frequency or establish a causal
relationship to drug exposure.
Body As a Whole: Hypersensitivity reactions including anaphylaxis, anaphylactic shock, angioedema,
bronchospasm, interstitial nephritis, urticaria, (see also Skin below); fever; pain; fatigue; malaise;
Cardiovascular: Chest pain or angina, tachycardia, bradycardia, palpitations, elevated blood pressure,
peripheral edema
Endocrine: Gynecomastia
Gastrointestinal: Pancreatitis (some fatal), anorexia, irritable colon, fecal discoloration, esophageal
candidiasis, mucosal atrophy of the tongue, stomatitis, abdominal swelling, dry mouth. During treatment
35
with omeprazole, gastric fundic gland polyps have been noted rarely. These polyps are benign and appear
to be reversible when treatment is discontinued.
Gastroduodenal carcinoids have been reported in patients with ZE syndrome on long-term treatment with
OMEPRAZOLE. This finding is believed to be a manifestation of the underlying condition, which is
known to be associated with such tumors.
Hepatic: Liver disease including hepatic failure (some fatal), liver necrosis (some fatal), hepatic
encephalopathy hepatocellular disease, cholestatic disease, mixed hepatitis, jaundice, and elevations of
liver function tests [ALT, AST, GGT, alkaline phosphatase, and bilirubin]
Metabolic/Nutritional: Hypoglycemia, hyponatremia, weight gain
Musculoskeletal: Muscle weakness, myalgia, muscle cramps, joint pain, leg pain
Nervous System/Psychiatric: Psychiatric and sleep disturbances including depression, agitation,
aggression, hallucinations, confusion, insomnia, nervousness, apathy, somnolence, anxiety, and dream
abnormalities; tremors, paresthesia; vertigo
Respiratory: Epistaxis, pharyngeal pain
36
Skin: Severe generalized skin reactions including toxic epidermal necrolysis (some fatal), Stevens-
Johnson syndrome, and erythema multiforme; photosensitivity; urticaria; rash; skin inflammation;
pruritus; petechiae; purpura; alopecia; dry skin; hyperhidrosis
Special Senses: Tinnitus, taste perversion
Ocular: Optic atrophy, anterior ischemic optic neuropathy, optic neuritis, dry eye syndrome, ocular
irritation, blurred vision, doublevision
Urogenital: Interstitial nephritis, hematuria, proteinuria, elevated serum creatinine, microscopic pyuria,
urinary tract infection, glycosuria, urinary frequency, testicular pain
Hematologic: Agranulocytosis (some fatal), hemolytic anemia, pancytopenia, neutropenia, anemia,
thrombocytopenia, leukopenia, leucocytosis
DRUG INTERACTIONS:
Interference with Antiretroviral Therapy:
Concomitant use of atazanavir and nelfinavir with proton pump inhibitors is not recommended. Co-
administration of atazanavir with proton pump inhibitors is expected to substantially decrease atazanavir
plasma concentrations and may result in a loss of therapeutic effect and the development of drug
37
resistance. Co-administration of saquinavir with proton pump inhibitors is expected to increase
saquinavir concentrations, which may increase toxicity and require dose reduction.
Omeprazole has been reported to interact with some antiretroviral drugs. The clinical importance and the
mechanisms behind these interactions are not always known. Increased gastric pH during omeprazole
treatment may change the absorption of the antiretroviral drug. Other possible interaction mechanisms are
via CYP 2C19.
Reduced concentrations of atazanavir and nelfinavir
For some antiretroviral drugs, such as atazanavir and nelfinavir, decreased serum levels have been
reported when given together with omeprazole. Following multiple doses of nelfinavir (1250 mg, twice
daily) and omeprazole (40 mg daily), AUC was decreased by 36% and 92%, Cmax by 37% and 89% and
Cmin by 39% and 75% respectively for nelfinavir and M8. Following multiple doses of atazanavir (400
mg, daily) and omeprazole (40 mg, daily, 2 hr before atazanavir), AUC was decreased by 94%, Cmax by
96%, and Cmin by 95%. Concomitant administration with omeprazole and drugs such as atazanavir and
nelfinavir is therefore not recommended.
Increased concentrations of saquinavir
For other antiretroviral drugs, such as saquinavir, elevated serum levels have been reported, with an
increase in AUC by 82%, in Cmax by 75%, and in Cmin by 106%, following multiple dosing of
saquinavir/ritonavir (1000/100 mg) twice daily for 15 days with omeprazole 40 mg daily co-administered
days 11 to 15. Therefore, clinical and laboratory monitoring for saquinavir toxicity is recommended
38
during concurrent use with PRILOSEC. Dose reduction of saquinavir should be considered from the
safety perspective for individual patients.
There are also some antiretroviral drugs of which unchanged serum levels have been reported when given
with omeprazole.
Drugs for Which Gastric pH Can Affect Bioavailability
Because of its profound and long lasting inhibition of gastric acid secretion, it is theoretically possible
that omeprazole may interfere with absorption of drugs where gastric pH is an important determinant of
their bioavailability (e.g., ketoconazole, ampicillin esters, and iron salts). In the clinical trials, antacids
were used concomitantly with the administration of PRILOSEC.
Effects on Hepatic Metabolism/Cytochrome P-450 Pathways
Omeprazole can prolong the elimination of diazepam, warfarin and phenytoin, drugs that are metabolized
by ^oxidation in the liver. There have been reports of increased INR and prothrombin time in patients
receiving proton pump inhibitors, including omeprazole, and warfarin concomitantly. Increases in INR
and prothrombin time may lead to abnormal bleeding and even death. Patients treated with proton pump
inhibitors and warfarin may need to be monitored for increases in INR and prothrombin time.
Although in normal subjects no interaction with theophylline or propranolol was found, there have been
clinical reports of interaction with other drugs metabolized via the cytochrome P450 system (e.g.,
cyclosporine, disulfiram, benzodiazepines). Patients should be monitored to determine if it is necessary to
adjust the dosage of these drugs when taken concomitantly with PRILOSEC.
39
Concomitant administration of omeprazole and voriconazole (a combined inhibitor of CYP2C19 and
CYP3A4) resulted in more than doubling of the omeprazole exposure. Dose adjustment of omeprazole is
not normally required. However, in patients with Zollinger-Ellison syndrome, who may require higher
doses up to 240 mg/day, dose adjustment may be considered. When voriconazole (400 mg Q12h x 1 day,
then 200 mg x 6 days) was given with omeprazole (40 mg once daily x 7 days) to healthy subjects, it
significantly increased the steady-state Cmax and AUC0-24 of omeprazole, an average of 2 times (90%
CI: 1.8, 2.6) and 4 times (90% CI: 3.3, 4.4) respectively as compared to when omeprazole was given
without voriconazole.
Omeprazole acts as an inhibitor of CYP 2C19. Omeprazole, given in doses of 40 mg daily for one week
to 20 healthy subjects in cross over study, increased Cmax and AUC of cilostazol by 18% and 26%
respectively. Cmax and AUC of one of its active metabolites, 3,4-dihydro-cilostazol, which has 4-7 times
the activity of cilostazol, were increased by 29% and 69% respectively. Co-administration of cilostazol
with omeprazole is expected to increase concentrations of cilostazol and its above mentioned active
metabolite. Therefore a dose reduction of cilostazol from 100 mg b.i.d. to 50 mg b.i.d. should be
considered.
40
Drugs affecting Omeprazole:
Before taking omeprazole, tell your doctor if you are taking any of the following drugs:
* a blood thinner such as warfarin (Coumadin);
* clopidogrel (Plavix);
* atazanavir (Reyataz);
* disulfiram (Antabuse);
* cyclosporine (Gengraf, Neoral, Sandimmune);
* tacrolimus (Prograf);
* phenytoin (Dilantin);
* theophylline (TheoBid, Theo-Dur, Theochron, Theolair, Elixophyllin, Slo-Phyllin);
* ketoconazole (Nizoral), voriconazole (Vfend);
* ampicillin (Omnipen, Principen);
* iron (Feosol, Mol-Iron, Fergon, Femiron, others); or
* a medicine for insomnia or anxiety such as diazepam (Valium), alprazolam (Xanax), lorazepam
(Ativan), temazepam (Restoril), clorazepate (Tranxene), chlordiazepoxide (Librium), and others.
Nonclinical Toxicology:
Carcinogenesis, Mutagenesis, Impairment of Fertility:
In two 24-month carcinogenicity studies in rats, omeprazole at daily doses of 1.7, 3.4, 13.8, 44.0 and
140.8 mg/kg/day (about 0.7 to 57 times a human dose of 20 mg/day, as expressed on a body surface area
41
basis) produced gastric ECL cell carcinoids in a dose-related manner in both male and female rats; the
incidence of this effect was markedly higher in female rats, which had higher blood levels of omeprazole.
Gastric carcinoids seldom occur in the untreated rat. In addition, ECL cell hyperplasia was present in all
treated groups of both sexes. In one of these studies, female rats were treated with 13.8 mg
omeprazole/kg/day (about 6 times a human dose of 20 mg/day, based on body surface area) for one year,
and then followed for an additional year without the drug. No carcinoids were seen in these rats. An
increased incidence of treatment-related ECL cell hyperplasia was observed at the end of one year (94%
treated vs 10% controls). By the second year the difference between treated and control rats was much
smaller (46% vs 26%) but still showed more hyperplasia in the treated group. Gastric adenocarcinoma
was seen in one rat (2%). No similar tumor was seen in male or female rats treated for two years. For this
strain of rat no similar tumor has been noted historically, but a finding involving only one tumor is
difficult to interpret. In a 52-week toxicity study in Sprague-Dawley rats, brain astrocytomas were found
in a small number of males that received omeprazole at dose levels of 0.4, 2, and 16 mg/kg/day (about
0.2 to 6.5 times the human dose on a body surface area basis). No astrocytomas were observed in female
rats in this study. In a 2-year carcinogenicity study in Sprague-Dawley rats, no astrocytomas were found
in males or females at the high dose of 140.8 mg/kg/day (about 57 times the human dose on a body
surface area basis). A 78-week mouse carcinogenicity study of omeprazole did not show increased tumor
occurrence, but the study was not conclusive. A 26-week p53 (+/-) transgenic mouse carcinogenicity
study was not positive.
Omeprazole was positive for clastogenic effects in an in vitro human lymphocyte chromosomal
aberration assay, in one of two in vivo mouse micronucleus tests, and in an in vivo bone marrow cell
42
chromosomal aberration assay. Omeprazole was negative in the in vitro Ames test, an in vitro mouse
lymphoma cell forward mutation assay, and an in vivo rat liver DNA damage assay.
Omeprazole at oral doses up to 138 mg/kg/day in rats (about 56 times the human dose on a body surface
area basis) was found to have no effect on fertility and reproductive performance.
OVERDOSE:
Reports have been received of overdosage with omeprazole in humans. Doses ranged up to 2400 mg (120
times the usual recommended clinical dose). Manifestations were variable, but included confusion,
drowsiness, blurred vision, tachycardia, nausea, vomiting, diaphoresis, flushing, headache, dry mouth,
and other adverse reactions similar to those seen in normal clinical experience.
Symptoms were transient, and no serious clinical outcome has been reported when PRILOSEC was taken
alone. No specific antidote for omeprazole overdosage is known. Omeprazole is extensively protein
bound and is, therefore, not readily dialyzable. In the event of overdosage, treatment should be
symptomatic and supportive.
Single oral doses of omeprazole at 1350, 1339, and 1200 mg/kg were lethal to mice, rats, and dogs,
respectively. Animals given these doses showed sedation, ptosis, tremors, convulsions, and decreased
activity, body temperature, and respiratory rate and increased depth of respiration.
MISSED DOSE:
43
If you miss a dose, use it as soon as you remember. If it is near the time of the next dose, skip the missed
dose and resume your usual dosing schedule. Do not double the dose to catch up.
CONTRAINDICATIONS:
OMEPRAZOLE Delayed-Release Capsules are contraindicated in patients with known hypersensitivity
to substituted benzimidazoles or to any component of the formulation. Hypersensitivity reactions may
include anaphylaxis, anaphylactic shock, angioedema, bronchospasm, interstitial nephritis, and urticaria
STORAGE:
Store at room temperature between 59-86 degrees F (15-30 degrees C) away from light and moisture. Do
not store in the bathroom. Keep all medicines away from children and pets.
Do not flush medications down the toilet or pour them into a drain unless instructed to do so. Properly
discard this product when it is expired or no longer needed.
44
Omeprazole
BRAND
NAME COMPOSITION COMPANY
PACKIN
G MRP
ABCID cap Omeprazole 20mg ARBRO PHARMA 10 36.25
ACICHEK
cap Omeprazole 20mg SANOFI AVENTIS 10 36.00
ACIDOF
cap Omeprazole 20mg CHEMO DRUGS 10x20 780.00
ADOLOC
cap Omeprazole 20mg ADOC PHARMA 10 35.00
ADZOLE
cap Omeprazole 20mg ADLEY FORM. 10 N.A.
ALPHACI
D-20 cap Omeprazole 20mg
ALPHA
HEALTHCARE 10 32.00
45
ATOZOL
cap Omeprazole 20mg ATOZ PHARMA 10 34.90
AZOL cap Omeprazole 20mg D.R. JOHN’S LAB 10 38.50
BINACID
cap Omeprazole 20mg
BIOCIN
HEALTHCARE 10 34.50
BIOCID
cap Omeprazole 10mg BIOCHEM 10 19.96
BIOCID
cap Omeprazole 20mg BIOCHEM 10 28.80
BIOCID
cap Omeprazole 40mg BIOCHEM 10 39.96
BIOMEZO
LE cap Omeprazole 20mg BIOCHEM 10 N.A.
BLANCID
cap Omeprazole 20mg PRG PHARMA 10 35.00
46
COSZOL
cap Omeprazole 20mg CFL 10 39.00
COZEP
cap Omeprazole 20mg
NICHOLAS
PIRAMAL 10 37.27
DIOCID
cap Omeprazole 20mg INTRA LABS 10 39.00
DIOMED
cap Omeprazole 20mg DYNAMIC 10 N.A.
KLOCID-
20 cap Omeprazole 20mg KLOKTER 10 40.00
KULGUT
cap Omeprazole 20mg SANDOZ 20x10 700.00
LOKIT cap Omeprazole 10mg KOPRAN 10 23.05
LOKIT cap Omeprazole 20mg KOPRAN 10 39.88
LOMAC Omeprazole 10mg CIPLA 10 22.75
47
cap
LOMAC
cap Omeprazole 20mg CIPLA 10 42.25
LORESS
cap Omeprazole 20mg BIOLOGICAL E. 10 39.00
MAGO cap Omeprazole 20mg RAPROSS 10 32.50
MOZAC
cap Omeprazole 20mg MARC LAB 10 39.50
OCID cap Omeprazole 10mg ZYDUS CADILA 20 54.68
OCID cap Omeprazole 20mg ZYDUS CADILA 20 86.28
OLIT cap Omeprazole 10mg CADILA PHARMA 10 24.20
OLIT cap Omeprazole 20mg CADILA PHARMA 10 42.00
OMAG 20
cap Omeprazole 20mg
ORDAIN
HEALTHCARE 10 42.40
48
OMALCE
R cap Omeprazole 20mg WOCKHARDT 7 73.39
OMAPIN cap Omeprazole 20mg BRAWN LAB 10 20.00
OMECER cap Omeprazole 20mg ALPHA LAB 10 32.00
OMELAX cap Omeprazole 20mg ZYTRAS LIFE 10 35.50
OMENAT cap Omeprazole 20mg NATCO 10 39.87
OMENAT inj Omeprazole 40mg NATCO 10ml 43.00
OMEPRALE cap Omeprazole 10mg FDC 10 21.15
OMEPRALE cap Omeprazole 20mg FDC 10 35.25
OMEPRAZ cap Omeprazole 20mg ALKEM 10 46.00
OMEPREN cap Omeprazole 20mg BLUE CROSS 10 25.00
OMEPRON-20
cap Omeprazole 20mg MESCKON 10 N.A.
OMERON cap Omeprazole 20mg AGRON REMEDIES 10 N.A.
49
OMEROX cap Omeprazole 20mg SHINTO BIOTEC 10 N.A.
OMETAB tab Omeprazole 10mg INTAS 10 N.A.
OMETAB tab Omeprazole 20mg INTAS 10 32.40
OMEZ cap Omeprazole 10mg DR. REDDY’S 10 23.67
OMEZ cap Omeprazole 20mg DR. REDDY’S 15 64.80
OMIND-20 cap Omeprazole 20mg INDOCO 10 34.50
OMIZAC cap Omeprazole 10mg TORRENT 10 23.45
OMIZAC cap Omeprazole 20mg TORRENT 10 43.10
OMPEP cap Omeprazole 20mg
CHEMO
BIOLOGICAL 10 37.00
OPAZ cap Omeprazole 10mg AGLOWMED 10 N.A.
OPAZ cap Omeprazole 20mg AGLOWMED 10 N.A.
OSKAR-20 cap Omeprazole 20mg
DISCOVERY
MANKIND 10 12.50
OVEVAR cap Omeprazole 20mg ZOTA HEALTHCARE 10 38.00
PIRAZOLE cap Omeprazole 20mg NICHOLAS 10 N.A.
50
PROMISEC cap Omeprazole 20mg ARISTO 10 27.26
PROTOLOC cap Omeprazole 20mg USV 10 39.00
PROTOLOC cap Omeprazole 40mg USV 10 73.00
PROZEX-20 cap Omeprazole 20mg SYNOKEM 10 36.95
RELOC-20 cap Omeprazole 20mg RHYDBURG 10 30.00
SANPOL-20 cap Omeprazole 20mg SHILAR PHARMA 10 19.50
SIOZOLE cap Omeprazole 20mg ALBERT DAVID 10 41.89
TACKO-M tab
Omeprazole magnesium
inSYSTOPIC 10 24.50
betacyclodextrin 20mg
TRAZ-20 cap Omeprazole 20mg EAST AFRICAN (R) 10 37.50
ZECID cap Omeprazole 20mg ZEE LAB 10x30 1200.00
ZOLCER cap Omeprazole 20mg
AUROBINDO
PHARMA 10 31.89
ZOMEP-20 cap Omeprazole 20mg ZOTA PHARMA 10 19.90
51
Omeprazole
Systematic (IUPAC) name
(RS)-5-methoxy-2-((4-methoxy-3,5-dimethylpyridin-2-yl)
methylsulfinyl)-1H-benzo[d]imidazole
Clinical data
Licence data US FDA :link
Pregnancy cat. B3 (AU) C (US)
Legal statusPrescription Only (S4) (AU) POM (UK) OTC
(US)
Routes Oral, IV
Pharmacokinetic data
Bioavailability 35–76%[1][2]
Protein binding 95%
Metabolism Hepatic (CYP2C19, CYP3A4)
Half-life 1–1.2 hours
52
Excretion
80%
Renal
20% Faecal
Identifiers
CAS number 73590-58-6
ATC code A02 BC01
PubChem CID 4594
DrugBank DB00338
ChemSpider 4433
UNII KG60484QX9
KEGG D00455
ChEBI CHEBI:7772
ChEMBL CHEMBL1503
Chemical data
Formula C17H19N3O3S
Mol. mass 345.4 g/mol
SMILES [show]
InChI [show]
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BRANDS SHORTLISTED
BRAND NAME COMPANY COMPOSITIONPACKING /
PRESENTATION
Ocid – 10 Zydus cadila Omeprazole -10 mg 10 x 6×10
Omez– 20 Dr. Reddy’s Omeprazole– 20 mg 5×5×20
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References
1. AB Astra.
Omeprazole Monograph. Oxford Clinical Communications, 1988.
2. Alumets J, El Munshid HA, et al.
Effect of antrum exclusion on endocrine cells of rat stomach.
J Physiol 1979;286:145-155.
3 Pharmacokinetics, metabolism and interactions of acid pump inhibitors.
Clin Pharmacokinet 1996;31:9-28.
4. Bardhan KD, Bianchi Porro G, Bose K, et al.
A comparison of two different doses of omeprazole versus ranitidine in treatment of
duodenal ulcers. J Clin Gastroenterol 1986;8(4):408-413.
5. Brunner G, Creutzfeldt W.
Omeprazole in the long-term management of patients with acid-related diseases resistant
to ranitidine. Scand J Gastroenterol 1989;24(Suppl 166):101-105.
6. Cederberg C, Ekenved G, et al.
Acid inhibitory characteristics of omeprazole in man. Scand J Gastroenterol
1985;20(108):105-112.
7. Clissold SP, Campoli-Richards DM.
Omeprazole - a preliminary review of its pharmacodynamic and pharmacokinetic
properties, and therapeutic potential in peptic ulcer disease and Zollinger-Ellison
syndrome. Drugs 1986;32:15-47.
8. Ekman L, Hansson E, et al.
Toxicological studies on omeprazole. Scand J Gastroenterol 1985;20(108):53-69.
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