Nasal Spray Development And Manufacturing (1)
This white paper aims to provide a comprehensiveoverview of the CMC guidance by the U.S. Food and DrugAdministration and present a streamlined approach fordevelopment and manufacture of nasal spray products
Published on: Mar 3, 2016
Transcripts - Nasal Spray Development And Manufacturing (1)
SOLUTIONEnsuring a Streamlined In the pre‐formulation and formulation stages of Approach for Nasal Spray development, the physical characterization of nasal aerosol drug products must include a thorough examination of: Product Development & Solubility and particle characteristics Manufacturing API / excipient compatibility Plume characterization: Spray pattern, plume geometry and spray droplet size Spray content uniformity INTRODUCTION Container closure testing, under the standards found Nasal sprays are comprised of one or more therapeutically in USP <671> active ingredients that are either dissolved or suspended in solutions in non‐pressurized dispensers. The most common Challenges include: use is for allergy‐related symptoms, such as allergic rhinitis. Balancing droplet particle size so it stays in the nasal Nasal sprays can be unit dose, bi‐dose or multi‐dose cavity. Droplets must not be so small that they go devices. The 2002 U.S. Food and Drug Administration into the lungs, and not so large that they drip out guidance on “Nasal Spray and Inhalation Solution, quickly. Suspension, and Spray Drug Products ‐ Chemistry, The use of muco‐adhesives can help the drug adhere Manufacturing, and Controls Documentation” describes within the nasal cavity and reduce the effects several tests for characterizing nasal spray drug products. associated with nasal clearance. The regulatory guidance may have some differences in, or Formulas with large molecules, such as proteins and additions to, testing requirements in Europe, Canada or peptides. Larger molecules provide challenges other countries compared to that in the United States. relating to cellular penetration before getting into the bloodstream. Penetration enhancers can be used Because the efficacy of the drug product depends on the to reduce this effect. ability of the spray device to deliver reproducible plumes Spray characterization, an area in which clients often and uniform dose content, some aspects of nasal spray seek advice and help. A plume that coats the largest development are unique such as formulation, container possible area of the nasal cavity, for absorption into closure system, plume characterization, manufacturing and the blood stream, is ideal, and the CDMO should be stability testing. Therefore, these aspects need to be able to determine the best delivery device to achieve carefully considered during the development program. that goal with a given formulation. This white paper aims to provide a comprehensive overview of the CMC guidance by the U.S. Food and Drug Excipients Administration and present a streamlined approach for Typical excipients used in nasal sprays include: water, development and manufacture of nasal spray products. preservatives, buffer salts, viscosity modifying agents, suspending agents, pH adjusting agents and flavors. As the excipients may significantly influence the spray RATIONALE/NEED characteristics , an investigation of the effect of these The development of a successful nasal spray drug product materials within the formulation, as well as their is an intricate process that requires a good understanding compatibility with the active drug, are critical aspects of the of interactions between the formulation and the delivery product development. device. As the delivery device plays such a crucial role in the The following page contains a list of some typical excipients success of nasal sprays, it is beneficial to rely on a contract used in nasal spray aerosol products along with their development and manufacturing organization (CDMO) that functions and typical concentrations used in the formulation can provide expert advice on nasal spray drugs as well as (compiled from ): the type of packaging that should be used. The CDMO should also be able to identify potential problems and advantages of various packaging options.
Physical, Chemical & Ensuring a Streamlined Microbiological Tests Approach for Nasal Spray Description of drug product: appearance and color Product Development & Identification of drug substance in drug product Manufacturing (cont’d.) Assays: API, and drug product Impurities and degradation products Extractables and Leachables An important part of the stability testing of a drug product is Particulate matter an examination of extractables and leachables in a packaging component. An extractable is any chemical species that can Preservatives and stabilizing excipients assays be extracted from a packaging component under “harsh” conditions in laboratory studies. A leachable is an extractable Microbial limits, Preservative efficacy, Sterility that actually migrates (partitions) into a drug product under maintenance storage conditions. pH, Osmolality, Viscosity Extractable data typically is supplied by the device supplier. Particle size distribution (for suspended Leachables are tested as part of stability protocol. Testing formulations) methods include liquid chromatography‐mass spectrometry Net content, weight loss on stability and effect of and gas chromatography‐mass spectrometry. device orientation A typical approach includes these steps: Leachables 1. Review supplier’s (supplier of device and pumps) Priming and re‐priming in various orientations, specifications for extractables effect of resting time 2. If necessary do additional extractable studies (identify, assess risk, and validate the method) Effect of temperature cycling 3. Perform leachables study [3,4] as part of stability protocol – USP <381> (for elastomers) and <661> (for plastics and other polymers) Spray & Device Characterization Manufacturing Pump‐to‐pump reproducibility Selection of quality valves and devices appropriate for a given drug product is an important part of the Spray content uniformity manufacturing process. It is essential to review the manufacturers’ specifications and to check their dimensions Droplet size distribution for the assembly line. Spray pattern and plume geometry Quality performs physical and chemical characterization analytical methods using a scaled‐up drug product batch. Device robustness Here are some of the test requirements according to the Effect of dosing orientation 2002 FDA Nasal Spray and Inhalation Solution, Suspension Tail‐off characteristics: profiling of and Spray Drug Products—CMC guidance document: spray near container exhaustion Pump delivery Aerodynamic particle size (for inhalation sprays)
AUTHOREnsuring a Streamlined Charles Shaw, Senior Manager of Research and Approach for Nasal Spray Development at DPT Laboratories, Ltd., BSc, PhD, EurChem, CSci, CChem, FRSC. Dr. Shaw is an expert in Product Development & formulation and packaging development. His Manufacturing (cont’d.) professional qualifications include: European Chemist, Chartered Chemist, Fellow of the Royal Society of Chemistry (London), and Chartered Scientist. He is also a member of AAPS. CONCLUSION With many products, packaging often is a secondary consideration. But with nasal products, the packaging or CONTACT INFORMATION delivery device is a more important consideration. The 318 McCullough packaging used with nasal sprays plays a crucial role in: San Antonio, TX 78215 Uniformity of the size of the dose delivered with 1‐866‐CALL‐DPT each use (210) 476‐8100 Spray droplet size – to make sure the droplets are neither so large that the product simply drips out of the nose, nor so small that they are inhaled into the About DPT Laboratories lungs DPT, a DFB company, is a contract development and Size of plume to properly coat the inside of the nose, manufacturing organization (CDMO) providing as it is no good to have an elegant product that goes companies the best solutions to their sterile and non‐ to waste by squirting out in a solid stream sterile drug development and manufacturing needs through innovation, technology and service. A CDMO that understands the importance of Specializing in semi‐solid and liquid dosage forms, DPT matching the formulation with the proper delivery device has a reputation for quality, unmatched technical will offer the best means of bringing to market a expertise, extensive manufacturing capabilities and an pharmaceutical product that performs as intended. exemplary regulatory compliance record. With five cGMP facilities, including R&D, manufacturing and packaging operations in San Antonio and Lakewood, REFERENCES N.J., DPT offers full service outsourcing solutions. For 1. “Investigating the influences of various excipients of more information, call 210‐476‐8100 or visit the nasal spray formulations on droplet size www.DPTLabs.com. and spray pattern” V. S. Kulkarni, J. Brunotte, M. Smith, F. Sorgi AAPS Annual Meeting 2008; (www.aapsj.org/abstracts/AM_2008/AAPS200 8‐001104.PDF) 2. “Aqueous nasal dosage forms” N. Day; “Pharmaceutical Preformulation and Formulation” Ed. M. Gibson, HIS Health Group, Englewood, CO, USA, 2001, pp.491‐513. 3. Safety Thresholds and Best Practices for Extractables and Leachables in Orally Inhaled and Nasal Drug Products (2006) www.pqri.org/pdfs/LE_Recommendations_to_F DA_09‐29‐06.pdf 4. FDA Guidance for Industry: Container Closure Systems for Packaging Human Drugs and Biologics, (1999) www.fda.gov/downloads/Drugs/GuidanceCom plianceRegulatoryInformation/Guidances/UCM 070551.pdf )