An Extended Minimal Physiologically Based Pharmacokinetic Model: Evaluation of Type II Diabetes Mellitus and Diabetic Nephropathy on Human IgG Pharmacokinetics in Rats

Chadha, Gurkishan; Morris, Marilyn E.

doi:10.1208/s12248-015-9810-0

Cited by 5 publications

(5 citation statements)

References 54 publications

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“…The physiologically based pharmacokinetic (PBPK) approach provides novel opportunities to incorporate the relevant pathophysiological changes occurring in various diseases for the construction of disease models (Li et al, 2012;Park et al, 2017). There are some published examples of drug-disease PBPK models that incorporate pathophysiological modifications occurring in different chronic conditions (Edginton and Willmann, 2008;Johnson et al, 2010;Rowland Yeo et al, 2011;Li et al, 2012Li et al, , 2015Schaller et al, 2013;Sayama et al, 2014;Vogt, 2014;Chadha and Morris, 2015;Rasool et al, 2016;Shah et al, 2019). Although there are a few published reports of PBPK models for theophylline in adults and children (Ginsberg et al, 2004;Björkman, 2005), until now there has been no published report of a theophyllineasthma PBPK model that has been used to predict drug exposure in adult and pediatric patients with asthma after incorporation of changes in human serum albumin concentrations.…”

Section: Introductionmentioning

confidence: 99%

Investigating the Role of Altered Systemic Albumin Concentration on the Disposition of Theophylline in Adult and Pediatric Patients with Asthma by Using the Physiologically Based Pharmacokinetic Approach

et al. 2020

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Theophylline is commonly used for the treatment of asthma and has a low hepatic clearance. The changes in plasma albumin concentration occurring in asthma may affect the exposure of theophylline. The aim of the presented work was to predict theophylline pharmacokinetics (PK) after incorporating the changes in plasma albumin concentration occurring in patients with asthma into a physiologically based pharmacokinetic (PBPK) model to see whether these changes can affect the systemic theophylline concentrations in asthma. The PBPK model was developed following a systematic model building approach using Simcyp. The predictions were performed initially in healthy adults after intravenous and oral drug administration. Only when the developed adult PBPK model had adequately predicted theophylline PK in healthy adults, the changes in plasma albumin concentrations were incorporated into the model for predicting drug exposure in patients with asthma. After evaluation of the developed model in the adult population, it was scaled to children on physiologic basis. The model evaluation was performed by using visual predictive checks and comparison of ratio of observed and predicted (R obs/Pre ) PK parameters along with their 2-fold error range.The developed PBPK model has effectively described theophylline PK in both healthy and diseased populations, as R obs/Pre for all the PK parameters were within the 2-fold error limit. The predictions in patients with asthma showed that there were no significant changes in PK parameters after incorporating the changes in serum albumin concentration. The mechanistic nature of the developed asthma-PBPK model can facilitate its extension to other drugs. SIGNIFICANCE STATEMENTExposure of a low hepatic clearance drug like theophylline may be susceptible to plasma albumin concentration changes that occur in asthma. These changes in systemic albumin concentrations can be incorporated into a physiologically based pharmacokinetic model to predict theophylline pharmacokinetics in adult and pediatric asthma populations. The presented work is focused on predicting theophylline absorption, distribution, metabolism, and elimination in adult and pediatric asthma populations after incorporating reported changes in serum albumin concentrations to see their impact on the systemic theophylline concentrations.

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Section: Introductionmentioning

confidence: 99%

Investigating the Role of Altered Systemic Albumin Concentration on the Disposition of Theophylline in Adult and Pediatric Patients with Asthma by Using the Physiologically Based Pharmacokinetic Approach

et al. 2020

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“…The key determinants of antibody PK remained in the mPBPK models, such as convection as the major distribution pathway and the distribution space is limited in the interstitial fluid (ISF). The mPBPK models have been applied to characterize antibody PK profiles in various disease scenarios [ 25 , 26 , 27 , 28 , 29 , 30 , 31 ].…”

Section: Modeling Pharmacokinetics Of Therapeutic Antibodiesmentioning

confidence: 99%

“…PBPK models are usually applied for more mechanistic exploration and species translation, while the mPBPK models could provide a simpler alternative at the systemic level but potential elaborations of tissue-of-interest. The mPBPK model has been adopted to assess the target binding dynamics in the target tissues and the effect of endosome trafficking on FcRn-mediated antibody recycling [ 23 , 25 , 26 , 27 , 28 , 30 , 115 ]. For example, Zheng et al investigated the distribution of an anti-TNF antibody candidate CNTO5048 and its TNF-suppression effect by developing an mPBPK model with an extended compartment representing mice colon [ 26 ].…”

Section: Assessing Antibody Low Tissue Distributionmentioning

confidence: 99%

Modeling Pharmacokinetics and Pharmacodynamics of Therapeutic Antibodies: Progress, Challenges, and Future Directions

Tang

Cao

2021

Pharmaceutics

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With more than 90 approved drugs by 2020, therapeutic antibodies have played a central role in shifting the treatment landscape of many diseases, including autoimmune disorders and cancers. While showing many therapeutic advantages such as long half-life and highly selective actions, therapeutic antibodies still face many outstanding issues associated with their pharmacokinetics (PK) and pharmacodynamics (PD), including high variabilities, low tissue distributions, poorly-defined PK/PD characteristics for novel antibody formats, and high rates of treatment resistance. We have witnessed many successful cases applying PK/PD modeling to answer critical questions in therapeutic antibodies’ development and regulations. These models have yielded substantial insights into antibody PK/PD properties. This review summarized the progress, challenges, and future directions in modeling antibody PK/PD and highlighted the potential of applying mechanistic models addressing the development questions.

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“…In addit ion to these general examples demonstrating the utility of this model structure, Chen and colleagues have extended the mPBPK model to include a diseased tissue (synovial fluid) and have used this structure to characterize the time course of plasma and joint concentrations of CNTO 345 (anti-interleukin 6 (IL-6)) and IL-6 in a collagen-induced arthritis mouse model [79], as well as for the PK/PD of an anti-IL-23 mAb in a psoriasis model [27]. Another extension of the mPBPK model was proposed by Chadha and Morris, who linked a mechanistic kidney model to a mPBPK model to describe the influence of diabetic nephropathy on IgG PK in a rat model [80]. While these models do not have the capacity to predict drug concentrations in all tissues simultaneously, they do represent a potential platform for groups whose interest lies in characterization of mAb PK in plasma and a tissue of interest.…”

Section: Minimal Pbpk Modelsmentioning

confidence: 99%

Physiologically-based modeling of monoclonal antibody pharmacokinetics in drug discovery and development

Glassman

Balthasar

2019

Drug Metabolism and Pharmacokinetics

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Over the past few decades, monoclonal antibodies (mAbs) have become one of the most important and fastest growing classes of therapeutic molecules, with applications in a wide variety of disease areas. As such, understanding of the determinants of mAb pharmacokinetic (PK) processes (absorption, distribution, metabolism, and elimination) is crucial in developing safe and efficacious therapeutics. In the present review, we discuss the use of physiologically-based pharmacokinetic (PBPK) models as an approach to characterize the in vivo behavior of mAbs, in the context of the key PK processes that should be considered in these models. Additionally, we discuss current and potential future applications of PBPK in the drug discovery and development timeline for mAbs, spanning from identification of potential target molecules to prediction of potential drug-drug interactions. Finally, we conclude with a discussion of currently available PBPK models for mAbs that could be implemented in the drug development process.

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An Extended Minimal Physiologically Based Pharmacokinetic Model: Evaluation of Type II Diabetes Mellitus and Diabetic Nephropathy on Human IgG Pharmacokinetics in Rats

Cited by 5 publications

References 54 publications

Investigating the Role of Altered Systemic Albumin Concentration on the Disposition of Theophylline in Adult and Pediatric Patients with Asthma by Using the Physiologically Based Pharmacokinetic Approach

Investigating the Role of Altered Systemic Albumin Concentration on the Disposition of Theophylline in Adult and Pediatric Patients with Asthma by Using the Physiologically Based Pharmacokinetic Approach

Modeling Pharmacokinetics and Pharmacodynamics of Therapeutic Antibodies: Progress, Challenges, and Future Directions

Physiologically-based modeling of monoclonal antibody pharmacokinetics in drug discovery and development

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