Introduction Medicine is directly related to human life and therefore, its manufacturers have massive social responsibility of providing

safe and effective medication. From its very initiation, Beximco Pharmaceuticals has always highlighted the need for rigid quality. Beximcos commitment to quality is clear from its progressive use of state of the skilled manufacturing technology. Beximco strictly follows WHO guidelines at every stage of manufacturing and procures its raw materials from the very best sources. But what makes Beximco a success story is its people. Beximcos team of highly skilled and motivated professionals work around the clock to guarantee the safety and efficacy of its products. Almost every professional subject demands proper practical knowledge in the own field. Thus industrial training program is one of the most important branch of a student studying in a professional subject like Pharmacy. Pharmacy is the art and science of preparing and dispensing medications and the provision of drug-related information to the community. It engross the explanation of prescription orders; the compounding, labeling, and dispensing of drugs and devices; drug product selection and drug utilization reviews; patient monitoring and interference; and the condition of cognitive services related to use of medications and devices. The American Pharmaceutical Association describes the mission of pharmacy as serving society as the profession responsible for the appropriate use of medical cons, devices, and services to achieve optimal therapeutic outcomes. As per the syllabus of Bachelor of Pharmacy (Hons.) degree of Pharmacy Department every graduation student must endure in-plant training in a pharmaceutical industry. We are very lucky to get the opportunity of undergoing a training session under the auspices of BEXIMCO PHARMACEUTICALS LTD, internationally renowned leading pharmaceutical company in Bangladesh. Our training period taught us that only theoretical knowledge is not enough for proper understanding. We got our training in the Tongi Plant of Beximco Pharma. This Plant is really well equipped with up-to-the-minute technologies, which not only ensure the highest quality and precision of medicine but also contribute to the future development of medicine in Bangladesh. We have gone through the books, read about the machinery, high tech process etc. of drug manufacturing We heard about the quality control, quality assurance etc. but when we were in Beximco Pharmaceutical Ltd. we found that only bookish knowledge is not enough to be a good pharmacist. Formerly we had only theoretical knowledge but now after the completion of four weeks in-plant training in BEXIMCO we have attained enough experience which would help us to make a career as a pharmacist with practical capability. In Beximco Pharmaceutical Ltd. we have seen more than what we had learnt. Company Profile History Beximco Pharmacuticals Limited (BPL) is a leading edge pharmaceutical company and is a member of the BEXIMCOGroup, the largest private sector industrial conglomerate in Bangladesh. BPLs strategic strengths include strong recognition of brands, highly skilled work force and diversified business mix. BPLs two brands Neoceptin R (Ranitidine) and Napa (Paracetamol) are the top two selling brands in the Bangladesh Pharmaceutical market. BPL started its operation in 1980, manufacturing products under the licenses of Bayer AG of Germany and Upjohn Inc. of USA and now have grown to become nations one of the leading pharmaceutical companies, supplying more than 10% of countrys total medicine need. Today Beximco Pharma

manufactures and markets its own `branded generics for almost all diseases from AIDS to cancer, from infection to asthma, from hypertension to diabetes for both national and international markets. BPL manufacture a range of dosage forms including tablets, capsules, dry syrup, powder, cream, ointment, suppositories, large volume intravenous fluids, metered dose inhalers etc. in several worldclass manufacturing plants, ensuring high quality standards complying with the World Health Organization (WHO) approved current Good Manufacturing Practices (cGMP). BPL also contract manufacture for major international brands of leading multinational companies. The recipient of three times `gold national export trophy, Beximco Pharma is the largest exporter of pharmaceuticals from Bangladesh. BPL is the only pharmaceutical company in Bangladesh received this highest national accolade for export, for record three times. BPL markets its brands through its own professional sales and marketing teams in African, South Asian and other markets. It also supply products to renowned hospitals and institutions in many countries, including Raffles Hospital and K K Women & Childrens Hospital in Singapore, MEDS and Kenyatta National Hospital (KNH) in Kenya, Jinnah Hospital, Agha Khan Hospital and Shaukat Khanum Memorial Hospital in Pakistan. BPL is also an enlisted supplier of World Health Organization (WHO) and UNICEF. BPL has a strong market focus and is anticipating continued future growth by leveraging business capabilities and developing superior product brands and markets. In particular BPL is very interested in developing a strong export market in USA and Europe. To meet the future demand BPL has invested over US 50 million dollar to build a new state-of-the-art manufacturing plant, confirming to USFDA and UK MHRA standards. This new plant will also offer contract-manufacturing facility to leading pharmaceutical companies, especially from Europe and US. BPL has employed over 2,300 staff and has an annual turnover of US 50 million dollar. Key Information
Year of Establishment Country of Incorporation Commercial Production Status Business Lines Public Limited Company Manufacturing and marketing of pharmaceutical Finished Formulation Products, Large Volume Parenterals and Active Pharmaceutical Ingredients (APIs) Main Country of operation Corporate Headquarter & Registered Address 17 Dhanmondi R/A, Road No. 2, Dhaka- 1205, Bangladesh Phone : +880-2-8611891 (5 lines) Fax : +880-2-8613470 Email : beximchq@bol-online.com Website : www.beximco.net Operational Headquarter 19 Dhanmondi R/A, Road No. 7, Dhaka- 1205, Bangladesh Phone : +880-2-8619151 (5 lines), +880-2-8619091 (5 lines) Fax : +880-2-8613888 Bangladesh 1980 1976 Bangladesh

Email : info@bpl.net Website : www.beximcopharma.com Overseas Offices & Associates Authorized Capital (Taka) Paid-up Capital (Taka) Number of Shareholders Stock Exchange Listings Number of Employees TIDM: (Tradable Instrument Display Mnemonic) Date shares were admitted to trading Dhaka Stock Exchange Chittagong Stock Exchange AIM ( Alternative Investment Market) : : : 3 July, 1985 11June, 1995 21 Octover,2005 Dhaka and Chittagong Stock Exchanges of Bangladesh and AIM of London Stock Exchange 2,043 BXP 1,040.97 million Around 49,000 UK, USA, Pakistan, Myanmar, Singapore, Kenya, Yemen, Nepal, Vietnam, Cambodia and Sri Lanka 2,000 million

ISIN

US0885792061

Milestones
1976 1980 Registration of the company Started manufacturing and marketing of licensee products of Bayer AG of Germany and Upjohn Inc. of USA 1983 1985 1990 1992 1993 1996 1997 Launching of Beximco Pharmas own brands Listing in the Dhaka Stock Exchange (DSE) as a Public Limited Company (PLC) Commissioning of Basic Chemical (APIs) unit Started export operation with Active Pharmaceutical Ingredients (APIs) First export market operation with finished formulations Introduction of Sustained Release Dosage form Introduction of Suppository Dosage form; Commissioning of Metered Dose Inhaler (MDI) plant; Introduction of Metered Dose Nasal Spray 1998 First pharmaceutical company of the country achieving National Export Trophy (Gold) for 1994 -

95 1999 2000 2001 UNICEF approval of Beximco Pharma as an enlisted supplier Agreement to manufacture Metered Dose Inhaler (MDI) for GlaxoSmithKline Introduction of Small Volume Parenteral (SVP) products; establishment of AnalgesicAntiinflammatory bulk drug plant 2002 Won the first prize of ICAB National Awards 2000 for Best Published Accounts and Reports in Non-Financial Sector Category The first Bangladeshi company to supply pharmaceuticals to Raffles Hospital- the most prestigious hospital in Singapore 2003 Received National Export Trophy (Gold) for consecutive 2 years (1998 -99, 1999-2000) Won the Silver prize of ICAB National Awards 2003 for Best Published Accounts and Reports in Non-Financial Sector Category Won a tender to supply Neoceptin R and Neofloxin to Raffles Hospital of Singapore for the whole years consumption Introduced Anti-HIV drugs for the first time in Bangladesh Diversification into Anti-Cancer therapeutic class 2004 Signed contract with Novartis to manufacture their liquid, cream, ointment and suppository products under Toll Manufacturing agreement 2005 Merger of Beximco Infusions Ltd. with Beximco Pharmaceuticals Ltd. Admission to Alternative Investment Market (AIM) of London Stock Exchange (LSE) 2008 Become the first Bangladeshi company to achieve GMP Clearance from TGA Australia. Also become the first Bangladeshi company to receive export approval to Gulf countries. Beximco Pharmaceuticals Ltd. Is the first Pharmceutical company from Bangladesh to enter into Latin America.

Vision Building a healthier tomorrow Products BPL manufacture a range of dosage forms including tablets, capsules, dry syrup, powder, cream, ointment, suppositories, large volume intravenous fluids, metered dose inhalers etc . Facilities BPLs manufacturing facilities are spread across a 20 acres site located in and around Dhaka, Bangladesh. They comprise of a number of purpose built plants, including the new Oral Solid Dosage (OSD) plant. The land and buildings are wholly owned by the company and approximately 13 of the 20 acres of land are currently in use. The site includes facilities for manufacturing intravenous fluids, liquids, creams, ointments, suppositories, metered dose inhalers, active pharmaceutical ingredients as well as the existing and new OSD plants for tablets and capsules, the research laboratory and a number of warehouses. The plant and machinery throughout the site has been designed, procured and installed by partners from Germany, Switzerland, Sweden, Italy and the United Kingdom, amongst others. The site has its own utility infrastructure to ensure the adequate generation and distribution of pure water at all times. The current installed electrical capacity is 4 MW and this will be increased to 8 MW soon.

There are also water purifying and liquid nitrogen generation facilities on site. The entire site is at least 10 meters above sea level and is approximately 250 kilometers from the nearest sea the Bay of Bengal. Products BPL manufacture a range of dosage forms including tablets, capsules, dry syrup, powder, cream, ointment, suppositories, large volume intravenous fluids, metered dose inhalers etc . New Oral Solid Dosage (OSD) Plant Beximco Pharma has invested over US $ 50 million on this new Oral Solid Dosage (OSD) plant complying with guidelines of highly regulated markets (for example, USFDA, UKMHRA, TGA Australia etc.). This state-of-the-art facility incorporates modern technological advancements. The building finishes have been made to comply with BPLs design standards which have been prepared with the global standards (e.g. non shedding materials, resistant to cleaning agents, flush fitting etc.). Same is the case for HVAC system which has been installed to meet the global standards for air classification, air changes etc. The manufacturing and packaging facilities have been designed to minimize generation and maximize containment of dust particles using closed transfer system and clean in place facility. All practicable measures have been taken to ensure that members of the staff are not exposed to unacceptable concentrations of dust particles. Process area, cubicles, storage area have been connected to vacuum dust cleaning. The design of the plant ensures automated materials handling systems and multilevel designs to enable gravity feed between processing stages. The building design has also allowed maximum engineering maintenance access without entering into the production areas. Precise selection of equipment is also critical to improve process capability and ensure process robustness. A wide range of equipment has been procured from world renowned companies like Glatt, Romaco, Noack, Korsch and Nicomac. A state-of-the-art chemical laboratory and dedicated microbiological laboratory equipped with a wide range of equipment have been set up to facilitate the quality control activities. The major equipment include HPLCs, UV spectrophotometer, FTIR spectrophotometer, AA Spectrophotometer, Karl Fischer titrator etc. This plant provides greater capacity and a strong platform to launch Beximco Pharmas pr oducts into highly regulated developed markets including Europe and the USA. State of the art MDI Plant The Metered Dose Inhaler (MDI) manufacturing plant of Beximco Pharma is one of the finest facilities in the world to produce Ozone benign HFA based MDI products. The plant was designed and installed under the technical collaboration of Pamasol, Switzerland. The facility has dedicated areas for dispensing, manufacturing, canister and valve cleaning, canister filling, quarantine storage area, spray testing, packaging, propellant storage and in process control. As the inhaler manufacturing operation requires stringent control of humidity and temperature, automatic monitoring equipment are in use to continuously record temperature and relative humidity in areas like dispensing room, suspension manufacturing room, filling room, quarantine room etc. The manufacturing equipment like manufacturing vessel, filling machine, weight checker, spray checking have been procured from Pamasol, Switzerland, a world renowned equipment supplier for Inhaler product manufacturing. The state-of-the-art Quality Control laboratory has been equipped with equipment like HPLC, Karl Fischer Titrator, Andersen Cascade Impactor etc. BPLs MDI facility is the only approved outsourced facility of GlaxoSmithKline for their Ventolin inhaler. They are happy to make their production and technical facilities open to inspection by existing and potential customers.

BPLs MDI plant has been audited by many local and overseas auditors and was acclaimed by them. Due to the potential risk to the environment posed by CFCs, the technology shift in MDI industry is currently towardsusing hydrofluoroalkane (HFA) as propellants. Considering this changing trend in pulmonary drug delivery technologies, the company has already developed the HFA based MDIs which inevitably requires very high level of expertise and sophisticated technology. We are among the very few companies in the world manufacturing CFC-free HFA MDIs. Now with this state-of-the-art MDI facility, the company aims at obtaining marketing approvals from stringent regulatory authorities of the developed markets. IV Fluid Manufacturing Plant Beximco Pharmas intravenous (IV) fluid manufacturing plant may be regarded as one of the most technologically advanced plants in the world. The plant was designed and installed in collaboration with Pharmaplan of Germany, a sister concern of Fresenius AG of Germany. In designing the whole process, special care has been taken by providing absolute sterile manufacturing conditions. The prime feature of the process is that there is no human physical contact with the product at any given time. This has been ensured by way of a series of fully automated manufacturing procedures including robotics. The bottle pack aseptic system (Form-Fill-Seal or FFS) is a unique and innovative manufacturing technology. Plastic bottles are blow moulded, filled with the solution and sealed under sterile conditions, in a single working cycle where there is no environmental exposure or human contact during manufacturing. The IV fluids are presented in a scientifically designed bottle where there is an extra protective eurohead cap and a resealable rubber disk. The whole process is performed in a class 100 clean room. The air inside this room is cleaned upto 100 particles per cubic feet passing it through HEPA (High Efficiency Particulate Air) filters. Thus, an advanced sterile environment is maintained in manufacturing the IV fluids in order to avoid the entry of bacteria, pyrogen and inert particles into products. This ensures the highest standards of quality and purity in order to ensure the highest level of safety. The plant is ISO 9001: 2000 certified. CHAPTER XII Engineering Department Major functions The main aim of this dept is to support the production department for smooth running. Machineries of this department are of 2 types1. Production machinery 2. Utilities A. Operation & maintenance of utility machineries are as follows: a) Power supply b) water system c) Steam d) Central compressor e) Central air conditioning system f) Dehumidification g) Fork lift h) Hand pallet truck i) Vacuum cleaner j) Gas B. Maintenance of production machinery.

a) Scheduled maintenance b) Troubleshooting or breakdown maintenance C. Maintenance of Q.C machinery. Utility Machineries Power station Machines Name Origin Capacity Generator-1 WAUKESHA U.S.A 920 KW Generator-2 CATERPILLAR U.S.A 1020 KW Generator-3 WAUKESHA U.S.A 900 KW Generator-4 WAUKESHA U.S.A 900 KW Diesel generator DETROIT DIESEL ALLISON Primary Requirements to run through Gas engine in the power station: Gas DM Water Soft Water Lube Oil Battery Compressed Air Air Boiler There are 2 boiler machines. Machines Name Origin Capacity Boiler-1 Cleeve Brooks U.S.A. 3 Ton steam/hr Boiler-2 Cleeve Brooks U.S.A. 2 Ton steam/hr Hapa Foil Printer Model: Hapa 226 Origin: Switzerlan Water Purifying System CHAPTER III Human Resources Department & Safety Major Functions This department is related to the management of affairs. It concerns with the following: HR recruitment planning, training & development, industrial relations, Performance appraisal, engineering, environmental safety & health etc. In a single word this department controls almost all the section in Beximco Pharmaceutical LTD. 1. Recruitment of personnel with appropriate qualification and experience to fill all position that has an effect upon quality. Different standard are considered for different position. 2. Assist new employees to complete joining activities and ensure placement of new comers. 3. To arrange, induction-training program (orientation program) for new employees. After joining each employee is introduced with all of the departments and their functions to know about company operation. 4. Prepare and Co-ordinate internship program for the students of different universities. 5. Prepare Human Resources Inventory Report of the plant monthly. It includes director to daily labor of the company.

6. Maintain & update personal files of all employees monthly. Such as Conformation of job, increment, promotion, transfer and other letters is adjusted in the employee file. 7. Supervise and monitor employee attendance, job cards, prepare monthly attendance summary and daily absent report etc. 8. Monitor and update leaves of plant employees. Each employee has a leave file which integrated the all kinds of leaves like i. AL (Annual Leave) ii. ML (Medical Leave) iii. CL (Casual Leave) iv. Special Leave v. Maternity Leave vi. Leave without pay etc Inform mangers and employees regarding, personnel polices and procedures of the company.

1.

2. Coordinate and monitor performance appraisal of plants employees annually. 3. Assess the training needs of personnel in light with cGMP and other work related issues. 4. Deal with industrial related issues like negotiation with employees union, ensure the labor rights etc. 5. Ensure proper implementation of labor laws applicable to factory employees. 6. Disciplinary action including suspension, punishment and termination. 7. Ensure healthy labor management relationship for smooth production. 8. Maintain liaison with Govt. regulatory Bodies. Human Resources department collaborate with following bodies for legal aid, help in any regulatory case. Ministry of industry Office of director of labor Explosive department Director of fire and Tongi fire station Tongi Thana, NSI, DB, SB. Custom & Vat, Tongi, circle DC office, Gazipur. SP office, Gazipur. Civil surgeon, Gazipur

1. Ensure safety of all employees and company assets. 2. Ensure proper security management of the plant. 3. Handle external visitor and arrange necessary uniforms and other accessories. 4. Supervise transport pool (Distribution, Repair, Maintance, etc). 5. Supervise over all House Keeping and Gardening of the plant. 6. Supervise washing facility to provide clean dress as per departmental daily requirement. Safety

The safety department of Beximco Pharmaceuticals Limited functions along with the Human Resources Department. It usually provides the basic safety measurements to the employee. 1. They provide first aid measures for chemicals in case of Eye contact Inhalation Skin contact Ingestion 2. They also give training to all employees about the activities in case of fire. Its the duty of all to make themselves familiar with Position of the fire alarm button Nearest escape from each room Location of fire fighting equipments and their operating instruction 3. They also train up the employees how to escape from fire If fire catches cloth If there is a lot of smoke
Classes of fires Class A Class B Class C Class D Definition Ordinary combustible materials such as wood ,paper Flammable liquid and gases such as kerosene and common organic solvents Electrical wires and equipments such as motor Combustible metals such Na, Mg etc Fire extinguisher Water, chemical foam Dry chemicals ,chemical foam Dry chemical Sand

CHAPTER XI Infusion Unit: Large Volume Parenteral Formulation Beximco Pharmas intravenous (IV) fluid manufacturing plant may be regarded as one of the most technologically advanced plants in the world. The plant was designed and installed in collaboration with Pharmaplan of Germany, a sister concern of Fresenius AG of Germany. In designing the whole process, special care has been taken by providing absolute sterile manufacturing conditions. The prime feature of the process is that there is no human physical contact with the product at any given time. This has been ensured by way of a series of fully automated manufacturing procedures including robotics. The bottle pack aseptic system (Form-Fill-Seal or FFS) is a unique and innovative manufacturing technology. Plastic bottles are blow moulded, filled with the solution and sealed under sterile conditions, in a single working cycle where there is no environmental exposure or human contact during manufacturing. The IV fluids are presented in a scientifically designed bottle where there is an extra protective eurohead cap and a resealable rubber disk. The whole process is performed in a class 100 clean room. The air inside this room is cleaned up to 100 particles per cubic feet passing it through HEPA (High Efficiency Particulate Air) filters. Thus, an advanced sterile environment is maintained in manufacturing the IV fluids in order to avoid the entry of bacteria, pyrogen and inert particles into products. This ensures the highest standards of quality and purity in order to ensure the highest level of safety. Water Treatment Process

Manufacturing and Packaging Steps

HVAC System The HVAC system means Heating ventilation and Air conditioning system. The main objective of HVAC system is to maintain a constant temperature and a constant RH in the infusion production area, microbiology laboratory and the office rooms. It is the most modern concept of air conditioning which is the most special features in the infusion unit. HVAC is needed in Pharmaceuticals: 1. To maintain specified temperature. 2. To maintain specific relative humidity. (Less than 40% for some hygroscopic material like ranitidine). 3. To remove dust particle from production area. 4. To maintain proper airflow to the rooms ensuring that cross contamination does not occur. 5. To prevent microbial contamination in some area by maintaining particle size within the tolerance range. (Using the HEPA Filters etc). The process is maintained in the different area by controlling the air pressure (positive and negative). Microbiology Laboratory According to the ICH guidelines the microbiological test of raw materials and finished product is an important parameter of the quality drug. Accordingly the Infusion unit has a special microbiology laboratory in order to carry out the microbiological tests of several sensitive products. The microbial test program includes the following: 1. Test of raw material and packaging material. 2. Test of finished product

3. Environmental control 4. Purified water test 5. Monitoring of surfaces 6. Personnel hygiene The microbiology laboratory of contains the following separate rooms: Testing room & Incubation room: Media preparation room: There is also a store room to store the reagents, cultures, standard microbes, chemicals and other testing instruments in a required condition The total testing procedure can be summarized as follows: Sample collection Media preparation Culture preparation Incubation Colony count Identification Final result 1. Test of Raw and Packaging Materials Microbial limit test is performed which include: 1)Total aerobic viable count 2)Total aerobic bacterial count 3)Total fungal count 4)Presence or absence of Pathogens (E.coli, Salmonella sp. , P. aeruginosa, S. aureus) Microbial Limit Test for Raw Materials and Finished Products (USP) 2. Test of Products Bioburden check of intermediate products. It is done with the help of membrane filtration method. First 4 and last 4 bottles are tested for microbes. Sterility test. 20 bottles of products are collected from critical points of the autoclave and are incubated for 14 days and observed. Bacterial endotoxin test/ LAL test. It is an in-vitro test method for pyrogen. It has been developed utilizing the gelling property of the lysate of amoebocytes of limulus polyphemus. The flow diagram of LAL test is given below: Sample Specified ml of LAL, dissolve 0 Incubation at 37 C for 1hr Gel formation Indicate presence of endotoxin from gram-negative bacteria. 3. For the Environmental inspections following tests are performed i) Settle Plate Method ii) Air Sampler 4. Purified Water Test It is done by membrane filtration method. Water is tested from 12 different points daily and 18 different points weekly. 5. Monitoring of surfaces

It is performed by: i) Contact Plate Method ii) Swap Test 6. Monitoring of personnel hygiene Hands, gloves, appearances/clothes are tested by contact plate method. List of Instrument of Infusion Unit
Sl. 1 Name of Instrument Deep Tube-well Aeration Chamber Sand Bed Filter 2 Raw water reservoir (Overhead tank 5000L) 3 Dosage station for chlorine with pump and container 4 5 6 7 Filter housing for raw water City water tank (2000L) Booster pumps (3000L/H) Activated carbon filter (1100L) Pall Beximco Infusions Ltd. Grundfos Hager + Elsasser, GmbH Germany Germany Replace organic substance from water and declorinate water for DM plant area 8 9 10 Filter house (2.5) Filter house (0.22) Demineralization plants (1 and 2) (Anion and cation exchanger) 11 12 13 14 Mixed bed filter (3.5m /h) Filter housing (0.22) Filter housing (0.22) Regeneration and neutralization system (9000L) 15 16 17 DM water tank (4870L) Distillation Plant 01 Distillation Plant 02 Pharma Plan EKSTROM & SONS KEMITERM ENGNEERING A/S 18 Distillate Storage Tank 01 (7000 L) Pharma Plan Germany Germany Sweden Sweden Production of WFI and pure steam
3

Manufacturer/ Supplier Sigma Eng.

Origin Bangladesh

Uses Raw water, supplied water for DM plant

Beximco Infusions Ltd.

LMI MILTON ROY

USA

Killing microorganisms

Pall Pall Hager + Elsasser, GmbH Germany Production of DM water for distillation plants, boiler etc. Hager + Elsasser, GmbH Pall Pall Pharma Plan Germany Germany Polishing DM waters

Sl. 19

Name of Instrument Distillate Storage Tank 02 (7500 L)

Manufacturer/ Supplier Getinge

Origin Sweden

Uses

20 21

Steam Boiler (2.6 T/H) Oil Free Air Compressor 01 & 02

StandardKessel Mehrer

Germany

Provide Technical steam Operating electronumeric valves & preparing sterile compressed air

22

Water Chiller 01

Finetee Century

Korea

Supply chilled water for HVAC & Production

23 24 25

Water Chiller 02 Water Chiller 03 Air Handling Unit 01 & 02

Linde Aktiengesellschaft Kyungwon-Century Co. Ltd. MEISSNER & WURST

Germany South Korea Germany

Do Do Supply & maintain clean class, positive air pressure

26 27 28

Cooling Tower 01 Cooling Tower 02 Injection Moulding Machine

Linde AG, Mainz BSC PO Yuen (Tos) Machine Factory

Germany Singapore Hong Kong

Provide cooling air Provide cooling air Produce Cap

29 30 31

Preparation Tank 01 & 02 Preparation Tank 01 & 02 Fully Automatic Bottlepack Machine for 1000ml & 100ml Bottles

Pharma Plan Getinge Rommelag

Germany Sweden Germany Bottlepacking

32

Cap Welding Machine for 1000ml & 100ml Bottles

Pharma Plan

Germany

Cap welding

33

Fully Automatic Bottlepack Machine for 500ml & 250ml Bottles

Rommelag

Germany

Bottlepacking

34

Cap Welding Machine for 500ml & 250ml Bottles

Pharma Plan

Germany

Cap Welding

35 36 37 38

Spray Type Autoclave Spray Type Autoclave Pressing Conveyor Belt Conveyor Belt

Sauter-Sulgen Getinge Pharma Plan Pharma Plan

Germany Sweden Germany Germany

Autoclaving Autoclaving Leak testing Conveying

Sl. 39 40 41

Name of Instrument Visual checking Devices Conveyor Belt Labeling Machine with Batch No. Printer

Manufacturer/ Supplier

Origin

Uses

Pharma Plan Pharma Plan

Germany Germany

Conveying Labeling

42

Ink Jet Printer

Image

France

Printing on Overpack

CHAPTER VIII Liquid Dosage Formulation LCO Department of Beximco Pharmaceuticals Limited produces about 84 products of various dosages form including (i) Syrup (example: Napa, Aristoplex) (ii) Suspension (example: Lactameal, Flatameal DS) (iii) Nasal spray (example: Decomit) (iv) Drops (Example: Deflux Ped. Drop) (v) Suppositories (example: Napa, Ultrafen) (vi) Cream, Ointment, Gel (example: Neostin cream, Anustat ointment, Ultrafen gel) LCO Department of BPL consist following 6 lines: i. Line-1: Syrup, Suspension. ii. Line-2: Antacid preparation iii. Line-3: Small volume oral liquid preparations iv. Line-4: Cream, Ointment v. Line-5: Oral liquid suppository facility (OLSF), Syrup vi. Line-6: Suppository Observed Manufactured Products
Product Category Syrup Syrup Suspension Cream Tofen Napa (60ml & paediatric drop) Flatameal DS Neostin Product Name Operations Observed Filling, sealing & packing Manufacturing Filling, sealing & packing Manufacturing

Machine list of Liquid, Cream, Ointment and Suppository Department, Line #01
SL No. 1. Manufacturing vessel Machine Name Model & Sr. No. MV- 5000 Tanners fabricated ltd, Australia. 5000L Manufacturing of liquid syrup & suspension. 2. Storage vessel & agitator SV 5000 Tanners fabricated ltd, Australia 3. Inline mixer & Transfer IM 600 Silverson, England 400L, Online mixing & 5000L Storage of liquid Manufacturer Capacity Use

pump

400psi

transfer of liquid syp & sus.

4. 5.

Filtering M/C millipore Vessel with Fluid agitator

FM-MP FA 942

Millipore, USA Lab. Equipment, India

5000L/hr 1000L

Filtering of fluid Stirring & mixing.

Line #02
SL No 1. Manufacturing vessel Machine Name Model & Sr. No. MV- 3000 Tanners fabricated ltd, Australia. 2. Storage vessel & agitator SV 3000 Tanners fabricated ltd, Australia. 3. Inline mixer IM 440 Silverson, England 600L , 440psi 3000L 3000L Manufacturing of liquid suspension Storage of liquid suspension Online mixing & transfer of liquid Manufacturer Capacity Use

Line #03
SL No 1. 2. Fluid agitator Liquid mixer Silverson Machine Name Model & Sr. No. FA 944 LM SIL Lab. Equipment, India Silverson, England 250 rpm 450L Stirring & mixing Liquid & cream homogenizer 3. 4. 5. Liquid transfer pump Filtering M/C Sartorious Seitz Kettle LTP- 40 FA- SA Frymamachinen, Switzerland Sartorious, Germany Germany 1000L/h 1000L/h 200 L/h Transfer of liquid Filter Manufacturing vessele 6. Vertical Ultrasonic cleaning machine 7. FAR Infrared sterilizing and drying tunnel 8. Filling and Plugging machine Changsha, China Changsha, China China 50-200 pcs/min 50-300 pcs/min 50-100 pcs/min Bottle filling and sealing Bottle drying Bottle washing Manufacturer Capacity Use

Line #04
SL No 1. 2. Planetary mixer Colloid mill Machine Name Model & Sr. No. PLM-100 COLL-M Gansons, India Probst & glass, Germany 50L 250 kg/hr Mixing Mixing and blending of Manufacturer Capacity Use

materials 3. General purpose mixing machine GP-MM Seitz, Germany 100L Mixing

Line #05
SL No 1. Manufacturing vessel Machine Name Model & Sr. No. Tanners fabricated ltd, Australia. 5000L Manufacturing of liquid syrup & suspension 2. Storage vessel & agitator Tanners fabricated ltd, Australia 3. Filtering Machine millipore 4. Auto Filling , Sealing, Bottle washing & Labeling machine Pharmalab, India 6000Bot./hr Washing, Filling, Sealing& Labeling of Bottles Millipore, USA 5000L/hr Filtering of fluid 5000L Storage of liquid Manufacturer Capacity Use

Line #06 (Suppository)

SL No 1. Sarong D-402 Italy 5000 suppo/hr 2. Manufacturing vessel Thailand 100L Filling & Sealing of Suppository Manufacturing Machine Name Model No. Manufacturer Capacity Use

Unit: Filling Line #01

SL No 1. Automatic liquid filling M/C(ATOMAT) S.S Industries,India 85-100b/m 1.Bottle washing & drying 2. Liquid filling & cap sealing 3.Labelling & printing Machine Name Model No. Manufacturer Capacity Use

Line #02
SL No 1. Automatic liquid filling M/C(ATOMAT) 2. Cap sealing machine CS-V46 Monobiock Filler S.S Industries, India Vaw, Germany 28-32b/m Cap sealing 3000b/h Liquid filling Machine Name Model & Sr. No. Manufacturer Capacity Use

3.

Self adhesive labeling machine

Clear pack, Singapore

110b/m

Bottle labeling

Line #03
SL No 1. Liquid filling machine 2. Cap sealing machine CS-V47 Vaw, Germany 28-32b/m Cap sealing LFM-L1 Local 30-35b/m Liquid filling Machine Name Model & Sr. No. Manufacturer Capacity Use

3.

Laminar Air Flow Cabinet

To control bacteria in the filling area

Line #04
SL No 1. Automatic tube filling & sealing machine 830920 Greatide, Taiwan 25-55 tube/min Cream & Ointment filling & sealing Machine Name Model & Sr. No. Manufacturer Capacity Use

Unit: Overprinting
SL No 1. Semi-automatic over printing Machine 2. Automatic over printing Machine 3. Semi-automatic printer SAP-L Local 1500p/h KK-610 Machine Name Model & Sr. No. HAPA-L Prontop hot hapa, Switzerland Jiangcozzer, Taiwan 4000p/h Printing label & carton Printing label & carton 4. Automatic over printing machine 5. Automatic over printing machine KK-550 Taiwan 4000p/h Printing carton KK-560 Taiwan 4000p/h Printing carton 4000p/h Printing label Manufacturer Capacity Use

Bottle washing area

SL No 1. Rotary bottle washer Machine Name Model & Sr. No. DR W3 Pharmalab, India 5000b/h Bottle washing Manufacturer Capacity Use

2. 3.

Rotary bottle dryer Hot air dryer

STD -

Gansons, India Heraeus

2500b/h 450b/load

Bottle drying Drying of (mainly pasteurization) bottle

4.

Hot air dryer

HAD78

Gansons, India

830b/load

Drying of (mainly pasteurization) bottle

5.

Sterilization oven Memmbrt

SO-MEM

MEMBRT, Germany

800-840 b/load

Sterilization &drying

6.

Rotary bottle washer

Pharmalab, India

5000b/h

Bottle washing

CHAPT-ER VI Product Development Departmen Product Development department deals with both new product formulation and reformulation of the existing products. BPL has the largest and well equipped Product Development Department ever in Bangladesh containing a group of competent and hard working personnel. The departments concerned is to develop a better formulation to meet the patients growing need and to make it cost effective as well. Functions of Product Development (i) Launching of new products (ii) Reformulation of existing products. (iii) Reprocessing. (iv) Market compliant handling. (v) Troubleshooting. (vi) Preparation of documents for export purpose. Recipe To develop a new drug the product development department has to collect DAR No. from Directorate of Drug Authority, Bangladesh after submission of recipe. A recipe contains: Technical data Batch formula Manufacturing instructions Control data for active materials Control data for finished product Pharmacological part Presentation Description Indications Contraindications Precautions Dosage and administration Adverse reactions

Drug interactions

Reformulation In case of existing products reformulation is performed when needed to improve the quality of the product or to minimize the cost of production to increase profit. Annexure Annexure is a document issued by the Drug Administration containing the DAR number Product name Pack size Composition Specification Overage There are two types of annexure. Annexure I: For drugs except vitamins and antibiotics. Annexure II: For vitamins and antibiotics.

Trial Batch Product Development Department manufactures trial batch for feasibility study. It also called Lab batch. It is the first batch of a product but it cant be dispensed for market. Pilot Batch After approval of product, Product Development Department manufactures 3 batches of product for stability study. These 3 batches called Pilot batches. Stability Study Stability test is done for the following purposes. To determine the expiry range To determine the packaging mode There are two methods of stability study Real time stability study Accelerated time stability study Products of pilot batches preserved in three separated stability chambers of three different specific conditions. These are 1.
Real time stability

2. 25 C , 60% Relative Humidity 3. 30 C , 65% Relative Humidity 4.

Accelerated time stability

5. 40 C , 75% Relative Humidity

Conditions 25 C , 60% RH 30 C , 65% RH 40 C , 75% RH Up to Shelf life Up to Shelf life First 6 month

Duration

If the degradation at accelerated stability study is less then 5% in 6 month, then the shelf life is 2 years. Analytical Method Development According to ICH guideline Analytical Method Development depends on the following parameters: Specificity Range Precision Linearity Accuracy Detection limit System stability testing Quantification limit BMR & BPR processing From the validation batches manufacturing, the validate procedures prepared as document record ship for each product. This is called Batch Manufacturing Record (BMR). Batch Packaging Record is prepared for each product according to the product safety & cost. List of Machines
Sl. 1 Name Compression machine (16 stations) 2 3 Coating machine Granulator N.R. Industries Ltd. Pharmaceutical and Medical Supply Ltd. 4 5 Fluid bed dryer Multi-mill machine Sapphire Machine Pvt. Ltd. Risesun Electrical & Industries Co. Ltd. 6 Moister analyzer (Sartorius MA 30) 7 8 9 10 Friability tester Stirrer Electronic balance Dissolution tester (DT 600) Erweka Silverson Shimadzu Erweka Germany England Japan Germany Imperial Corporation Ltd. Germany Determination of moisture content Determination of friability Mixing Weighing Determination of dissolution India Drying Milling Thailand Thailand Tablet coating Granulation Manufacturer/ Supplier Manesty Machines Ltd. Origin England Uses Tablet compression

Sl. 11 12 13 14

Name Disintegration tester Sonicator pH meter HPLC System 1

Manufacturer/ Supplier

Origin

Uses Disintegration testing

Ultrawave Ltd. Hanna Instrument Shimadzu

UK

Shaking pH determination

Japan

Identification, quantification, separation

15

HPLC System 2

Shimadzu

Japan

Identification, quantification, separation

CHAPTER IV Production Planning Department A well defined production plan is the pre-requisite for a well established & modern pharmaceutical industry, to achieve the following objectivesTo be a highly productive industry of good quality product. To exist as an expert pharmaceutical industry in the world market. A well-organized and modern pharmaceutical company like Beximco Pharmaceutical Ltd. always possesses a preplanned production schedule to ensure sound and uninterrupted production of medicine. BPL maintains a very well organized pragmatic production planning which is not only very easy to understand by the staffs but also very easy to apply to ensure the desired excellence of quality. Its main functions are Issue of B.P.R: According to the production plan B.P.R is issued by planning department. If any change required in B.P.R, planning will consult with product development for its correction. Preparation of monthly plan & Its analysis: According to the demand of the market, planning department prepare a monthly plan and according to that plan they suggest production department to manufacture the product. Ensure the availability of raw & Packing materials: Planning will arrange all types of raw & packing materials by consulting with head office for smooth production. To Arrange physician sample: Production department will separate physician sample from bulk production according to the order of the planning department. Arrange the products for international market: Planning will arrange & supply the products to the international market. After receiving information from E-mail, they take necessary action to meet that demand. Co ordinate all sections for smooth production: Planning co-ordinate all sections to give highest production will in minimum cost and time. Compare man hour & achievement: Planning compares man hour & achievement to know the actual efficiency of man and machine. Keep daily production report & all documentation: Planning department keeps all types of daily production reports & Maintain major documentation. Task of Production Planning Department at a glance

CHAPTER X Quality Assurance Department Quality assurance is a wide ranging concept covering all the matter which individually & collectively influences the quality of a product. It is the sum total of all organized arrangement made with the objective of ensuring that medicinal products are of the quality required for their intended use. Quality may be defined as level of excellence, which goes with the product. To assure this quality into the product is the main job of quality assurance department. QA department ensures that the quality is built in the product. Quality (Definition according to DIN ISO 8402) The totality of features and characteristics of a product or service that bear on its ability to satisfy stated or implied needs. Quality Assurance (Definition according to DIN ISO 8402) All planned and systematic actions necessary to provide adequate confidence that a product or service will satisfy given requirements for quality. The impact of total quality maintenance is Improved operating procedure. Greater customer satisfaction. Increased financial performance. The following equipments are observed in The Solid QA station
Machine Hardness, Thickness, Diameter tester Manufacturer Erweka, Germany Description/operation procedure It has 10 holes to hold 10 tablets to be tested. There are additional 2 holes,

one for measuring thickness, diameter and Other for excretion other tablet. Electronic balance Sartorius, Germany Disintegration tester Erweka, To perform weight variation of the Tablet Six tablet holders and six plastic disks

Germany Friabilator Erweka, Germany Heater

for performing DT test. Perform friability tests at 25 rpm for 4minutes. To maintain 37c of the water bath.

Flow chart for quality assurance activity

The functions of Q.A. in different section of the industry are given below

1. Handling of new source sample. 2. Artwork for packing material checking. 3. Dispensing A QA officer monitors dispensing process in the dispensing area and signs the dispensing card. 4. Production area In solid: 1. i. Before granulation, the granulation area and the machinery are checked which are ready for granulation. 1. ii. Before compression starts the machine and the rooms are checked to ensure proper cleaning. 1. iii. During compression of tablets the following parameters are checked at regular intervalHardness, thickness, friability, weight-variation, disintegration, organoleptic tests for chewable tablets and other relevant parameter. 1. iv. During capsule filling weight-variation & shell locking is tested. 1. v. After compression of tablets or filling of capsules, the finished products are sent to QC department for analysis. 1. vi. On the basis of the QC report &QA inspection of the tablets or capsules are approved for packing or rejected. 1. vii. Tablets that require coating are sent to QC department for various tests before coating & after coating, the finished products are monitored by QA officers. 1. viii. Before packaging starts the machine and the room conditions (temperature and humidity) are checked. During packing process the following parameters are checked: Product strength, batch number, manufacturing date, DAR no, exp date, MRP, license no. foil printing, pocket formation, sealing, cutting, slitting, carton (inner and shipping), leaflet etc & checking of visual appearance of finished products. 1. ix. Leak tests of plastic container, glass bottles, blisters and strips. are also performed. In liquid 1. i. The manufacturing vessels and area are checked before start manufacturing. 1. ii. During manufacturing weight of ingredients, mixing time, temperature and rpm etc are checked. 1. iii. Total volume is checked. 1. iv. During filling fill weight per bottle is checked. 1. v. Before packaging starts the machine and the room conditions (temperature and humidity) are checked. 1. vi. Labels on bottles and on shipping cartons are checked. In Suppository section 1. i. Before start up of manufacturing or filling machines/rooms are checked for proper cleaning and good house keeping. 1. ii. During manufacturing room temperature, vessel temperature, pump temperature, congealing temperature, room humidity, hardness, weight etc. are checked. In Inhalation section

1. manufacturing. 1. etc. are checked. 1.

i. ii.

The manufacturing vessel and area are checked properly before start up of During manufacturing weight of the ingredients, mixing time, temperature, rpm

iii. During packaging the containers are checked for leak, total actuation no., dose/actuation, batch printing etc. 1. iv. Sampling and approval/disapproval is done like other section. Documentation All kinds of documents related to production and control procedure are collected and preserved in QA department in an easily retrievable way. Some examples of the documents preserved in the QA department can be given below: Batch production record of a particular batch Raw material analytical sheet Packaging material analytical sheet Certificate of analysis of raw material Standard operating procedure (SOP) Material receiving report (MRR) sheet.

Retention control room To force or encounter product complain for any batch product retention sample for every batch is preserved by the QA department. Specific amount of samples are collected from the packing line and they are kept in the retention sample room as a representative of that particular batch for a year excess of their claimed shelf life. All samples are kept in the conditions indicated in their label. If any complaints come from the market, the retention samples from that particular batch are collected from the retention sample room to verify. CHAPTER IX Quality Control Department Keep the quality up with that slogan Quality Control Department of BEXIMCO PHAR MA performs its day-to-day duties. Quality control is responsible for the day-by-day control of quality within the company. This department is stuffed with scientist and technicians who asses and assure that entire production process has been completed satisfactorily and satisfied all the aspects of GMP through preserving the purity and quality of the product. Diagrammatic representation of present Q.C. activitiesActivities of Quality Control Department 1. Receiving of the samples to be tested from QA department. 2. Issuing release, reject or quarantine advice for each batch of raw material and final product. 3. Assessment of the intermediate products and bulk products for further processing. 4. Performing all test procedure for all incoming samples according to the schedule. 5. Maintaining batch wise full quality control tests record and signature of the persons who perform the test. 6. Performing environmental monitoring tests. 7. Calibrations and standardization of laboratory equipments. 8. Ensuring precision and accuracy of all testing methods. 8. Control of all laboratory reagents.

9. Research and development of any new method and its validation. 10. Testing of any return goods. 11. Stability tests for finished products. 12. Performing long time stability testing. Good Manufacturing Practice (GMP) GMP provides basic standards for the manufacturers of drugs and from the basis on which each company build its own systems procedures to assure the product quality. GMP ensures that products consistently produced and controlled to the quality standards appropriate to their intended use. There are number of national & international GMP regulatory boards: WHO PIC FDA MHRA TGA GLP norms and regulations To ensure a wide range of testing disciplines the laboratory has some facilities which are discussed in GLP. The major considerations that accounts for GLP functioning involves: 1. Organization & management: It is a basic requirement for establishing an effective QC system. QC department is a well organized department. It has the authority of approval or rejection of each batch of starting, packaging and final materials on the basis of testing. Personnel at all levels have accountability to carry out their responsibilities to meet the quality goal. 2. Personnel: Qualified personnel are a key factor in ensuring quality. Personnel have three important characteristics: Education. Experience. Training. 3. Premises: A well designed premise is an essential part of GLP. It has: Adequate space allocations Easy to clean Safety facilities Storage facilities Segregation of activities Proper environment for testing Every equipment has safety distance from others Microbiology lab is isolated from Analytical lab 4. Equipments: The laboratory is well equipped for performing all tests according to BP, USP. To maintain all equipments & machineries following measures are taken: Every equipment has a log book for records Regular maintenance is done.

All equipments are calibrated at specified intervals. Most of the equipments & machineries are connected with printers thus there remain no chance of manipulation. 5. Reference standards: Reference standards are substances with known purity or potency. Certified reference standards are available from many official sources. For routine laboratory tests it is worth considering working standards prepared by standardizing some good quality row materials against certified reference substance. A good stock of reference standards is maintained and used. 6. Reagents: To maintain reagents QC department has taken following initiatives: Laboratory has a complete list of all the reagents needed. Solid reagents are stored in alphabetic orders and separated from liquid reagents. The reagents need to be stored at low temperature is refrigerated. Flammable reagents have segregated area. Moisture sensitive reagents are stored in desiccants. 7. Procedure: For every operation in QC written instructions are available. It has master control procedure (MCP) for every material. It has SOP for every action. SOP is strictly followed by analysts. 8. Sampling: Appropriate sampling is a vital step in GLP. To facilitate correct and appropriate sampling procedures sampling must be done at conditions same as production environment e.g. sterile raw materials & products are sampled under laminar air flow. 9. Testing: The incoming goods and finished products are tested according to BP, USP, EP as per requirement laid down specifications. 10. Documentation: All test results are recorded on a test record sheet (TRS). All Q.C. records relating to a batch analysis are a part of the batch documentation. The purpose of documentation is to record important information with evidence. It is preserved at least one year after batch expired date. Control of Raw Materials Following characteristics are checked in raw materials. Description (Melting point, boiling point) IR Solubility LOD% Ash Impurities

Control of Packaging materials Following characteristics are checked in packaging materials: Text of the printed materials. Color of the materials. Locking of cartoons. Compatibility of closures with bottles.

Thickness of foils. Pasting of cartoons. Weight (gram per m ) of cartoons for checking materials. Transmittance test for glass bottle PVC-PVDC differentiation test
2

Control of finished products: Final testing of finished product is made in the quality control laboratories. The testing of finished product for compliance with predetermined standards is a critical factor for product release. Following characteristics are checked in finished products. Description Identification DT and Dissolution Uniformity of weight Uniformity of content

Criteria of Validation (i) System suitability (ii) Accuracy (iii) Precision (iv) Linearity (v) Specificity (vi) Robustness & rigidness (vii) Limit of detection (viii) Limit of quantification (ix) Range Process validation: Establishing documented evidence that provides a high degree of assurance that a specific process will consistently produce a product meeting its predefined specification & quality attributes. Good validation practice requires the close collaboration of departments such as those concerned with development, production, engineering quality assurance & control. An adequate validation may be beneficial for the manufacturing in many ways It deepens the understanding of process, decrease the risk of processing problem & thus assure the smooth running of the process. It decreases the risk of defect cost. It decreases the risk of regulatory non-compliance. A fully validated process may require less in process control & end product testing. Sampling Sampling may be defined as the process of removing an appropriate numbers of items from a population in order to make inferences to the entire population. The object of sampling and subsequent testing is to provide an effective check on the quality of the product or substances being processed. In Beximco Pharmaceuticals Ltd, sampling is performed by the quality control department. For the active ingredients, the sample is withdrawn from each container. For the excipients, sampling is performed by the following formula- n+1

Stability Study Stability test is done for the following purposes. For registration Formulation changes New drug development Changes in primary package To determine the expiry range To determine the packaging mode According to ICH Guidelines our country fall in zone III and IV. As a consequence the following conditions apply for the stability study.
Condition Storage condition Temperature 1) Real Time 25C 2C Or,30C2C 2) Accelerated 40C2C Relative Humidity 60% 5% 65% 5% 75% 5% Initial-0,3,6,9,12 months 2 -18,24 month 3 -Annually 0,3,6 months
rd nd

Testing frequency

In Beximco Pharmaceuticals Ltd. Real time & Accelerated condition is maintained. If significant changes occur in accelerated conditions then the product is observed for any significant changes in real time stability study for 1 year. The significant changes in accelerated condition include Appearance of the product Dissolution for 12 minutes if not passed pH Impurities level Potency variation QC Instrument List
Sl. 1 Name of Instrument Electronic analytical precision balances 2 3 4 Electronic balance Electronic balance Electronic balance (Top loading) 5 IR Moisture Analyser MA 30 Sartorius AG Germany Moisture determination 6 Disintegration Test Apparatus ZT 3/6 Erweka, GmbH Germany Disintegration testing PT 310 EL 300 BD 1201 Sartorius AG Shimadzu Mettler Tledo AG Germany Japan USA Weighing Do Do Model BP 210s Manufacturer Sartorius AG Origin Germany Uses Analytical weighing

Sl. 7

Name of Instrument Dissolution Tester

Model DT 6L

Manufacturer Erweka, GmbH

Origin Germany

Uses Determination of dissolution

8 9 10

Dissolution Tester Dissolution Tester Rotating bottle disintegration tester

DT 700LH DT 608HH None

Erweka, GmbH Erweka, GmbH Fabricated in BPL

Germany Germany

Do Do Do

11

Suppository disintegration tester

ST 30

Erweka, GmbH

Germany

Disintegration testing of suppository

12

Suppository melting point apparatus

SSP

Erweka, GmbH

Germany

Determination of melting point of suppository

13

Suppository softening time tester

PM3

Erweka, GmbH

Germany

Determination of softening time of suppository

14

pH meter

PHI 32

Bechman Instrument Inc.

USA

Determination of pH

15 16 17 18

Oven Oven (Dry heat sterilizer) Vacuum oven Humidity control oven

UM600 TV 30U

Memmert Memmert Gallenkamp

Germany Germany UK India

Drying Drying Drying Drying

NEC-234R

Newtronic Equipment 10

19 20

Incubator Jolting StanPF volumeter STAV2003

Kottermann Karl-Kolb Scientific Supplies

Germany Germany

Incubation Tapping

21 22

Electromantle water Melting point apparatus

EM0500/C 7B1667C

Electromantle Gallencamp

UK England Identification by measuring melting point

23 24

Waterbath Aerosizer LD

Gallencamp Amherst Process Instrument

UK USA

Controlled heating Size determination

25

Gas chromatography system

Shimadzu Corp.

Japan

Identification

Sl. 26

Name of Instrument UV-Visible Spectrophotometer

Model UV-160A

Manufacturer Shimadzu Corp.

Origin Japan

Uses Identification

27

HPLC System No.1

Waters

USA

Identification, quantification, separation

28 29 30 31 32

HPLC System No. 2 HPLC System No. 3 HPLC System No.4 Waters Breeze HPLC system Potentiometer autotitrator 702 SM

Waters Waters Shimadzu Waters Metrohm Ltd.

USA USA Japan USA

Do Do Do Do Potentiometric titration for ions

33

Karl-Fisher titrator

DL 18

Mettler

Switzerland

Moisture determination

34 35 36 37

Steam sterilizer (Autoclave) Fume chamber Digital hygrometer Hotspot furnace (Muffle furnace)

NI-109-3S 7591/F Testo-625 Tactical 308

Naniwa Ikakgyo Co. Kottermann Testo Gallenkamp

Japan Germany Germany UK Determination of ash content

38

Leica AR-600 automatic refractometer

AR-600

Leica

USA

To determine refractive index

39 40 41

Centrifuge Centrifuge Polarizing Microscope

BB3V 1000S3A BHSP

Jouan Gallenkamp Olympus Optical Company Ltd.

France England Japan

Separation Separation Identification

42 43

Brookfield viscometer Fourier trasformation Infrared spectrophotometer

LVDVII+RT IRPrestige-21

Brookfield Shimadzu Corp.

USA Japan

Determine viscosity Identification

44

UV-Vis Spectrophotometer UV-1700 Pharmasec

UV-1700

Shimadzu Corp.

Japan

Wide range analytical test

45

Atomic absorption spectrophotometer

AI 1200-FlameVG pH 302

Aurora Instrument Ltd.

Canada

To identify and measure minerals

46

pH meter (Desktop)

Hanna Instrument

Singapore

pH determination

Sl.

Name of Instrument

Model

Manufacturer Private Ltd.

Origin

Uses

47

ARIUM 611D1 Water purifying equipment

Sartorius AG

Germany

Water purification

48

Automatic polarimeter

AA10

England

To determine optical rotation

49

Melting point apparatus

B530

Buchi Laboratoriums Technic AG

Switzerland

Identification

50

Horizontal shaker

Shaking

CHAPTER VII Solid Dosage Formulation Solid Department of BPL comprises the maximum number of products and also covers the major portion of its sales. Its current number of products is 261 consisting 83 plain tablets, 131 coated tablets, 37 capsules and 8 powders for suspensions. Lay out of the general production (GP) area: Raw material ware house Dispensing Dispensed material store Sieving (If applicable) Manufacturing Area Granulation Unit Granulation is the most preliminary process in the solid manufacturing area. Granulation is the process in which powder particles of raw materials are made to adhere to form larger particles called granules 1. To improve the flow of powdered materials by forming sphere like or regularly shaped aggregates 2. To improve the compression characteristics of the mix (blend.) 3. To prevent segregation of the constituents in the powder mix. Two types of granulation processes are performed in this unit: -Dry granulation -Wet granulation Granulation units perform the following steps of tablet formulation to form larger particles in order to facilitate compression. Packaging Unit Packing can be defined as an economical means of providing, presentation, protection, identification/information, containment, convenience, and compliance for a product during storage, carriage, display and use until such time as the product is used or administered. After compression of tablets and coating [if required] the tablets are packed either in blister pack or in the strip. There are two packaging areas: a) Primary packaging area In the primary packaging area, 10 machines are involved for packing. Among them, 8 for blister pack & 2 for strip pack.

b)

Secondary packaging area

Types of packaging: Packaging of Solid dosage form is of two types: 1) Strip packaging: Striping materials is: a) ALU-ALU type b) PVC-ALU-PVC type 2) Blister Packaging: Blistering materials are of three typesa) ALU-ALU type b) ALU-PVC type c) ALU-PVDC type Different parts of a blister pack machine Different parts of a blister pack machine and their functions are giver in the following table:
Parts of blister machine 1. Base grid 2. Forming Station Function Draws the base material, which may be PVC, PVDC, Aluminum foil. Forms blister in the base material either by hydraulic pressure or by air pressure and temperature 3. Hopper 4. Chute and Spiral Feeder Tablets are kept in the hopper Regulate the vibration so that table can move and fall in the feeding channel 5. Feeding Channel 6. Deduster 7. Scanner 8. Sealing station 9. Cooling station 10. Marking station 11. Code embosser 12. Slitting station 13. Web clump 14. Punching Station 15. Timer 16. Detector Feed the blister with tablet Collects dust by creating vacuum Scan the empty blister Seal the blister pack Cool the blister pack Marks the empty blister Emboss code number Slit the blister pack Draws the blister Cut the blister and slit down Regulate the passage of blisters Detect the empty packet

Parts of blister machine 17. Rejecter 18. Conveyer belt

Function Rejects the empty blister packet Convey the pack for further processing.

Steps of Blister packing

Formation of pocket (By pneumatic pressure)

Filling (Through Channel / Feeder)

Dedusting

Scanning

Sealing

Code embossing

Cooling

Punching

Collection or rejection of blister

Steps of Strip Packing

Formation of pocket of Aluminum foil from 2 sides

Filling

Sealing

Cooling

Batch No. and Exp. No. Printing

Slitting of Strip

List of Machines in Solid Department

Sl.

Name of Instrument

Manufacturer/ Supplier

Origin

Capacity

Granulation Unit #1 1 2 3 4 Planetary Mixer Fluid Bed Dryer Multi Mill Vac-U-Max Gansons Saphire Gansons Belleville India India India USA 60 Kg 60 Kg 100 Kg/h 2000 Kg/h

Granulation Unit #2 5 6 7 8 Planetary Mixer Fluid Bed Dryer Multi Mill Vac-U-Max Gansons Saphire Gansons Belleville India India India USA 120 Kg 120 Kg 100 Kg/h 2000 Kg/h

Granulation Unit #3 9 High Speed Mixer Granulator (HSMG) 10 11 12 13 14 Fluid Bed Dryer Fluid Bed Dryer Multi Mill Vac-U-Max Lift Lever (Stacker) Saphire Saphire Mark Belleville Toyota Tuscho Corp. India India Bangladesh USA Japan 2000 Kg/h 650 Kg 150 Kg 150 Kg Thailand 250 Kg

Granulation Unit #4 15 16 Solace Aero Dryer High Speed Mixer Granulator (HSMG) 17 18 Multi Mill Vac-U-Max Gansons Belleville India USA 100 Kg/h 2000 Kg/h Solace India Thailand 120 Kg 250 Kg

Sl.

Name of Instrument

Manufacturer/ Supplier

Origin

Capacity

Compression Units 19 20 16 Station Rotary Press 35 Station Rotary Press (Double Channel) (BB4) 21 35 Station Rotary Press (Double Channel) (BB4) 22 35 Station Rotary Press (Double Channel) (BB4) 23 24 25 26 Fette P3100 (55 Station) Fette P1200 (30 Station) SEJONG (45 Station) Weighing Balances Fette Fette Sejong Sartorius Germany Germany South Korea Germany Max. 594000 TPH Max. 216000 TPH Max. 380000 TPH Manesty England 70000-210000 TPH Manesty England 70000-210000 TPH Manesty Manesty England England 10560-29760 TPH 70000-210000 TPH

Coating Units 27 28 29 30 Accela Cota 150 Accela Cota 350 A Accela Cota 350 B Sejong Cota Manesty Manesty Manesty Sejong Pharmatek Ltd. England England England South Korea 150 Kg 350 Kg 350 Kg 450 kg

Packaging Area 31 32 33 34 35 36 37 38 39 Blister Machine (PG) Blister Machine (085) Blister Machine (042) Blister Machine (043) Blister Machine (074) ELMAC PACK Blister Machine PAM-PAC Blister Machine HOONG-A Blister Machine Strip Machine Gansons Klockner Hansel ELMAC Germany India India Korea India Max. 80/min 48000 TPH (2 Track) 36000 TPH (usually) 120000 TPH Precision Gear Klockner Hansel Otto Hansel India Germany Germany 66000 TPH (4 Track) 50000 TPH (2 Track)

Sl.

Name of Instrument

Manufacturer/ Supplier

Origin

Capacity

40

Strip Machine

Hemson

CHAPTER XIII Training Department Training plays a vital role in translating organization objectives and plans into desired results. Objectives: 1. I. To expose the participants to the new concepts pharmaceutical manufacturing. 2. 3. 4. 5. II. III. IV. V. To expose participants knowledge. To improve job skill. To change attitude. To make GMP as a culture.

Training procedure: Training need analysis Select Resource Person Preparing Training Calendar Conducting Training Session Evaluation of Training ,Trainee Documentation Retraining Training type Classroom Training Audio-visual Training Interactive learning On the job Training Group Exercise Training Applies to All persons engaged in manufacturing directly and indirectly. Manager Officer Workman Training Topics: For New Employees Induction training is conducted for New Employees on Basic GMP Safety overview On the job SOPs For Existing Employees Train the trainers GMP Safety

Utility System General Self Development On the job training v SOPs CHAPTER V WAREHOUSE Warehouse is a part of pharmaceutical industry where raw materials, packaging materials are stored before production and finished products are stored after production maintaining the specifications properly. BPL has a large and organized warehouse maintained by a group of sincere and hard working personnels. Different units of warehouse 1. BPL Warehouse 2. BIL Ware-house 3. Pharmatek Ware-house Areas of Ware-house 1. Quarantine area: After receiving raw and packaging materials are kept here for QA approval. 1. Released area: After getting approval raw and packaging materials are kept here with great safety. Released area is generally the central area of ware-house. 2. In process area: According to store requisition(SR)dispensed materials for manufacturing are kept here. 1. Rejected area: Raw material, packaging material and finished products which are unable to get approval from QA are retained here with great safety .Usually this area is located at the corner of the warehouse. 1. Finished product area:-Generally finished products are started here for delivery to I & I service. 2. Special area:-It includes cool room, for heat sensitive and flammable materials. Identification of products and raw or packaging material in Ware-house Raw materials and finished products are easily identified here with the help of an index which includes different code for different area also. Packaging materials in warehouse are kept or placed following Alphabetical order.

Activities of ware-house Activities of ware-house can be divided into 2 parts. 1. Routine Activities 2. Periodic Activities. Product release Dispensing areas of Warehouse One dispensing officer always responsible for dispensing the raw materials to the production and packing materials to the packing areas. Following things must be checked by the dispensing officer. 1) Check that only approved (green tag) materials are brought to the dispensing area. 2) Check that dispensing area is completely free from others materials.

3) Check that cleaning is done with IPA and savlon solution. 4) Check that correct quantity and approved quality of materials are being dispensed as per requisition. 5) Check that materials come first are being dispensed first, to follow FIFO (First In First Out). Documentation in Dispensing Documentation includes, a) Serial number b) Product name and code c) Product batch number d) Requisition entry e) Cleaning f) Material exit g) Remarks h) Tags i) Signature of authorized person etc. Inventory Functions of Warehouse Inventory After reading MRR to QA department materials will be kept pending list in computer After getting released from QA department product will be at Norma inventory Stock will be deducted from stock against S.R.(Store requisition) after dispensing. Conclusion We are fortunate enough to get in-plant training opportunity in BPL covering a large number of dosage forms. Our four weeks observation in various departments helped us to make our theoretical knowledge clear. We have observed manufacturing procedures, quality control, packaging and other related activities of pharmaceutical products and fulfilled our thirst. We have found a very friendly and cordial environment during our training periods. The personnel were cordial to make us known to various departmental activities and machines as well. We have observed various latest technology applied valuable machines and large industrial area in BPL containing own power stations and liquid nitrogen plant. We have also observed strict quality assurance in every step before supplying the product to the national and international market. In this sense we are lucky and happy to see such practice of GMP. At last we would like to give hearty thanks to BPL and our gratitude goes to its all personnel. We wish better cooperation between our Department and BPL day by day. We wish BPLs good luck to attain the desired goals in national and international market