A flowsheet model for the development of a continuous process for pharmaceutical tablets: An industrial perspective

García‐Muñoz, Salvador; Butterbaugh, Adam S.; Leavesley, Ian M.; Manley, Leo Francis; Slade, David; Bermingham, Sean K.

doi:10.1002/aic.15967

Cited by 75 publications

(37 citation statements)

References 32 publications

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“…First, we defined six independent and mostly nonoverlapping peaks; intended to represent the pure spectra of six species (A to F), spectra for species D and E have a strong overlap (Figure a). Using a flowsheet model of a continuous direct compression system, a simulation was performed to generate the concentration curves (Figure b) obtained, when the material feeders are switched off one by one, compensating the mass flow into the system with the feed rate of the major filler excipient. Excipient B has the lowest nominal mass fraction in the blend, while excipient C has the largest.…”

Section: A Simulated Examplementioning

confidence: 99%

“…As can be seen in the magnified insert in the figure, both PLS models had difficulty accurately predicting the API concentration from the placebo spectra. In comparison, EIOT was able to accurately predict the API concentration in placebo spectra This accuracy is attributed to the effect of the constraint in Eq.. Having a predicted concentration that follows the expected behavior of a mass fraction (nonnegative between 0 and 1) allows the straightforward use of such predictions to estimate the parameters from a deterministic model of the system …”

Section: Case Studiesmentioning

confidence: 99%

“…The various materials are continuously fed at the top of the unit and moved downward by gravity through a mixing unit and into the tablet press. Mixing in the system occurs by forced convection as well as by dispersion as the material moves from top to bottom and is not limited to occur exclusively in the mixing unit but throughout the length of transit . The last free volume where mixing occurs is the feed‐frame of the tablet press; the mixing of the powders is incomplete before this point.…”

Section: Introductionmentioning

confidence: 99%

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Estimation of mass‐based composition in powder mixtures using Extended Iterative Optimization Technology (EIOT)

2018

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The Extended Iterative Optimization Technology (EIOT) method is proposed as an extension to Muteki's [I&ECR 2013;52 (35):12258-12268] Iterative Optimization Technology to address deviations from Beer-Lambert's law in powders. The new method estimates the apparent spectrum for the pure species, rather than using the measured spectrum and augments Beer-Lambert's law with a bilinear term to capture the signature and strength of the nonchemical interferences. The proposed method has exhibited acceptable performance in spite of using a lean data set to estimate its parameters. The method provides robust and coherent estimates within the physical boundaries of the system and exhibits robustness to instrument transfer. The lean effort needed to build the EIOT method positions it as an attractive option in early stages of pharmaceutical drug product development. Its robustness to distinguish chemical from nonchemical signals implies a potential to lower the total cost of ownership for an EIOT-based solution in manufacturing.

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Section: A Simulated Examplementioning

confidence: 99%

Section: Case Studiesmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Estimation of mass‐based composition in powder mixtures using Extended Iterative Optimization Technology (EIOT)

2018

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“…Several authors have covered the entire manufacturing process. Flowsheet models have been developed to predict dynamics for processes based on direct compression [16], dry granulation [17], and wet granulation [18]. Singh et al developed a control strategy for dry granulation and implemented it into a process-wide flowsheet based on firstprinciples models [19].…”

Section: Introductionmentioning

confidence: 99%

Superstructure-based process synthesis and economic assessment under uncertainty for solid drug product manufacturing

et al. 2020

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This paper presents a new method for process synthesis and economic assessment for solid drug product manufacturing, considering continuous manufacturing as a prominent process alternative. Of the three phases of drug development, phase II was targeted where the dosage form, formulation, and processing technology are determined. For a comprehensive alternative generation, a superstructure was developed that covered 9452 options for the unit level, which was combined with two options on the formulation strategy. The generated alternative was assessed by a net present value calculation model, which was adapted for dynamic cash flow consideration in the drug lifecycle. The model can incorporate uncertainty in the drug development and manufacturing in the result, and can perform global sensitivity analysis by Monte Carlo simulation. The method was demonstrated in a case study where two different scenarios regarding the price of the active pharmaceutical ingredient and the demand for the product were assumed. The results showed that when the demand and price are both low, the labor-related costs are dominant, and in the opposite case, the material-related costs become relevant. We also introduce the prototype version of the software "SoliDecision," by which the presented method was implemented for industrial application.

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“…Previous work on the development of flowsheet models are restricted to direct compaction [3][4][5][6] and dry granulation routes [7,8] for continuous solid oral dosage manufacturing. Park et al [7] created a flowsheet model of continuous dry granulation and applied it for optimization.…”

Section: Introductionmentioning

confidence: 99%

Dynamic Flowsheet Model Development and Sensitivity Analysis of a Continuous Pharmaceutical Tablet Manufacturing Process Using the Wet Granulation Route

et al. 2019

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In view of growing interest and investment in continuous manufacturing, the development and utilization of mathematical model(s) of the manufacturing line is of prime importance. These models are essential for understanding the complex interplay between process-wide critical process parameters (CPPs) and critical quality attributes (CQAs) beyond the individual process operations. In this work, a flowsheet model that is an approximate representation of the ConsiGma TM -25 line for continuous tablet manufacturing, including wet granulation, is developed. The manufacturing line involves various unit operations, i.e., feeders, blenders, a twin-screw wet granulator, a fluidized bed dryer, a mill, and a tablet press. The unit operations are simulated using various modeling approaches such as data-driven models, semi-empirical models, population balance models, and mechanistic models. Intermediate feeders, blenders, and transfer lines between the units are also simulated. The continuous process is simulated using the flowsheet model thus developed and case studies are provided to demonstrate its application for dynamic simulation. Finally, the flowsheet model is used to systematically identify critical process parameters (CPPs) that affect process responses of interest using global sensitivity analysis methods. Liquid feed rate to the granulator, and air temperature and drying time in the dryer are identified as CPPs affecting the tablet properties.

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A flowsheet model for the development of a continuous process for pharmaceutical tablets: An industrial perspective

Cited by 75 publications

References 32 publications

Estimation of mass‐based composition in powder mixtures using Extended Iterative Optimization Technology (EIOT)

Estimation of mass‐based composition in powder mixtures using Extended Iterative Optimization Technology (EIOT)

Superstructure-based process synthesis and economic assessment under uncertainty for solid drug product manufacturing

Dynamic Flowsheet Model Development and Sensitivity Analysis of a Continuous Pharmaceutical Tablet Manufacturing Process Using the Wet Granulation Route

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