APPLICATIONS

Process development at ______ covers a significant broad ________ of R&D activities coupled ____ various input parameters based __ in silico analysis, real-world evidence ___ analytical data. Process development _________ with significant clone development __________; which then is concomitantly ______ up from shake flasks, __ small scale bioreactors (0.5-2.0L) ___ subsequently into 5L-50L-500L-1100L capacities.

Our upstream process ___________ group develops high cell _______ E. coli batch, fed-batch ___ semi-continuous processes for therapeutic ___________ proteins. This group interacts ____ the strategy and clone ___________ groups from the initiation __ the project. This allows ___ the final objective to _______ evident and visible to ___ PD group and subsequent __________ and manufacturing groups. COGS, ___ process simplicity is one __ our target hallmarks of _______ with Premas.

Monoclonal antibodies and _________ derived proteins, produced from _________ cell cultures are process _________ with similar thoughts. Our ________ is flexible, partnership based _______ our clients’ needs. ____ bioreactors (5-25L) and Single ___ (1-10L) constitute the first ____ of process development and _______ up. Gram level yields __ the clone /shake flask ______ are enhanced with media ___________, optimizing feed strategies, upstream _______ development and multi-parametric inputs ___ controls.

Our downstream process ___________ team has delivered over >650 proteins, of which about 100’_ of them have ____ scale up to > 100_ culture volumes. With unit __________ scalable to 1000’s of _____ of product, harvesting and _____________ steps have significant capacities, __________, and access to multiple _______, e.g. high speed continuous ___________, concentrations and diafiltrations systems (1000’_ of Liters), both cassette ___ hollow fiber based systems.

Chromatography systems and ______ defined process protocols exist __ Premas. With the vast __________ of over 14 years, ______ has developed unique scale ____ models (ml to 100’sof _) and processes to rapidly ________ on possible steps, yields ___ outcomes. (Reference: Application Note: ____ to Phase 1 material __ 10 months). Use of _____-_____ components and analysis, Premas ___ been able to deliver ____ of the significantly challenging ________ and processes at low ____.

Further downstream process ___________ is possible at Premas _____ we develop high protein _____________ formulations and lyophilization cycles. ______ has both small and _____ scale development lyophilizers.

Premas has multiple _____ and suites dedicated to ________ and downstream processing technologies, _________ fully disposable single-use bioreactor _______. We are capable of _______ our customers’ demands on ____, flexibility and productivity. Processes ___________ from our PD labs __________ scale up in our _____-_____ GMP compliant facility. We ____ also successfully performed the __________ and registration of several 2__ and 3rd generation processes.

Our 24/7 running ____ of our processes enable __ to design semi-continuous processes, __________ operations and significantly lower ____ processes. We developed different ____________ and processes to offer ___________ advantages to a number __ new molecule formats and _____________ processes. Some of the ________ include a concomitant increase __ productivity as well as __________ purification, along with low ____.

Premas has the ________ to deliver grams to ___ product and drug substance. __ have now for a __________ product line expanded our ________ to 5kg/week delivery schedules.

This allows Premas __ accelerate development of our ________’ product pipeline and enable ________ deliveries for their clinical ______ in various geographies. We ____ been audited by various __________ and regulatory consultants and _______ assurance groups of our _________.