Your search keyword '"Peter Bloomingdale"' showing total 12 results

1. Microglial roles in Alzheimer's disease: An agent‐based model to elucidate microglial spatiotemporal response to beta‐amyloid

Author

Catherine Weathered, Sophia Bardehle, Choya Yoon, Niyanta Kumar, Cheryl E. G. Leyns, Matthew E. Kennedy, Peter Bloomingdale, and Elsje Pienaar

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Alzheimer's disease (AD) is characterized by beta‐amyloid (Aβ) plaques in the brain and widespread neuronal damage. Because of the high drug attrition rates in AD, there is increased interest in characterizing neuroimmune responses to Aβ plaques. In response to AD pathology, microglia are innate phagocytotic immune cells that transition into a neuroprotective state and form barriers around plaques. We seek to understand the role of microglia in modifying Aβ dynamics and barrier formation. To quantify the influence of individual microglia behaviors (activation, chemotaxis, phagocytosis, and proliferation) on plaque size and barrier coverage, we developed an agent‐based model to characterize the spatiotemporal interactions between microglia and Aβ. Our model qualitatively reproduces mouse data trends where the fraction of microglia coverage decreases as plaques become larger. In our model, the time to microglial arrival at the plaque boundary is significantly negatively correlated (p

Published

2024

2. Hallmarks of neurodegenerative disease: A systems pharmacology perspective

Author

Peter Bloomingdale, Tatiana Karelina, Vidya Ramakrishnan, Suruchi Bakshi, Florence Véronneau‐Veilleux, Matthew Moye, Kazutaka Sekiguchi, Guy Meno‐Tetang, Aparna Mohan, R. Maithreye, Veena A. Thomas, Frank Gibbons, Antonio Cabal, Jean‐Marie Bouteiller, and Hugo Geerts

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Age‐related central neurodegenerative diseases, such as Alzheimer's and Parkinson's disease, are a rising public health concern and have been plagued by repeated drug development failures. The complex nature and poor mechanistic understanding of the etiology of neurodegenerative diseases has hindered the discovery and development of effective disease‐modifying therapeutics. Quantitative systems pharmacology models of neurodegeneration diseases may be useful tools to enhance the understanding of pharmacological intervention strategies and to reduce drug attrition rates. Due to the similarities in pathophysiological mechanisms across neurodegenerative diseases, especially at the cellular and molecular levels, we envision the possibility of structural components that are conserved across models of neurodegenerative diseases. Conserved structural submodels can be viewed as building blocks that are pieced together alongside unique disease components to construct quantitative systems pharmacology (QSP) models of neurodegenerative diseases. Model parameterization would likely be different between the different types of neurodegenerative diseases as well as individual patients. Formulating our mechanistic understanding of neurodegenerative pathophysiology as a mathematical model could aid in the identification and prioritization of drug targets and combinatorial treatment strategies, evaluate the role of patient characteristics on disease progression and therapeutic response, and serve as a central repository of knowledge. Here, we provide a background on neurodegenerative diseases, highlight hallmarks of neurodegeneration, and summarize previous QSP models of neurodegenerative diseases.

Published

2022

3. PBPK-PD modeling for the preclinical development and clinical translation of tau antibodies for Alzheimer’s disease

Author

Peter Bloomingdale, Daniela Bumbaca-Yadav, Jonathan Sugam, Steve Grauer, Brad Smith, Svetlana Antonenko, Michael Judo, Glareh Azadi, and Ka Lai Yee

Subjects

PBPK, QSP, antibody, tau, Alzheimer’s disease, Therapeutics. Pharmacology, RM1-950

Abstract

Disrupted tau proteostasis and transneuronal spread is a pathological hallmark of Alzheimer’s disease. Neurodegenerative diseases remain an unmet medical need and novel disease modifying therapeutics are paramount. Our objective was to develop a mechanistic mathematical model to enhance our understanding of tau antibody pharmacokinetics and pharmacodynamics in animals and humans. A physiologically-based pharmacokinetic-pharmacodynamic (PBPK-PD) modeling approach was employed to support the preclinical development and clinical translation of therapeutic antibodies targeting tau for the treatment of Alzheimer’s disease. The pharmacokinetics of a tau antibody was evaluated in rat and non-human primate microdialysis studies. Model validation for humans was performed using publicly available clinical data for gosuranemab. In-silico analyses were performed to predict tau engagement in human brain for a range of tau antibody affinities and various dosing regimens. PBPK-PD modeling enabled a quantitative understanding for the relationship between dose, affinity, and target engagement, which supported lead candidate optimization and predictions of clinically efficacious dosing regimens.

Published

2022

4. Quantitative systems pharmacology in neuroscience: Novel methodologies and technologies

Author

Peter Bloomingdale, Tatiana Karelina, Murat Cirit, Sarah F. Muldoon, Justin Baker, William J. McCarty, Hugo Geerts, and Sreeraj Macha

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Abstract The development and application of quantitative systems pharmacology models in neuroscience have been modest relative to other fields, such as oncology and immunology, which may reflect the complexity of the brain. Technological and methodological advancements have enhanced the quantitative understanding of brain physiology and pathophysiology and the effects of pharmacological interventions. To maximize the knowledge gained from these novel data types, pharmacometrics modelers may need to expand their toolbox to include additional mathematical and statistical frameworks. A session was held at the 10th annual American Conference on Pharmacometrics (ACoP10) to highlight several recent advancements in quantitative and systems neuroscience. In this mini‐review, we provide a brief overview of technological and methodological advancements in the neuroscience therapeutic area that were discussed during the session and how these can be leveraged with quantitative systems pharmacology modeling to enhance our understanding of neurological diseases. Microphysiological systems using human induced pluripotent stem cells (IPSCs), digital biomarkers, and large‐scale imaging offer more clinically relevant experimental datasets, enhanced granularity, and a plethora of data to potentially improve the preclinical‐to‐clinical translation of therapeutics. Network neuroscience methodologies combined with quantitative systems models of neurodegenerative disease could help bridge the gap between cellular and molecular alterations and clinical end points through the integration of information on neural connectomics. Additional topics, such as the neuroimmune system, microbiome, single‐cell transcriptomic technologies, and digital device biomarkers, are discussed in brief.

Published

2021

5. Systems Pharmacology Modeling Identifies a Novel Treatment Strategy for Bortezomib-Induced Neuropathic Pain

Author

Peter Bloomingdale, Cristina Meregalli, Kevin Pollard, Annalisa Canta, Alessia Chiorazzi, Giulia Fumagalli, Laura Monza, Eleonora Pozzi, Paola Alberti, Elisa Ballarini, Norberto Oggioni, Louise Carlson, Wensheng Liu, Mehrnoosh Ghandili, Tracey A. Ignatowski, Kelvin P. Lee, Michael J. Moore, Guido Cavaletti, and Donald E. Mager

Subjects

bortezomib, dexanabinol, multiple myeloma, peripheral neuropathy, pharmacodynamics, systems pharmacology, Therapeutics. Pharmacology, RM1-950

Abstract

Chemotherapy-induced peripheral neurotoxicity is a common dose-limiting side effect of several cancer chemotherapeutic agents, and no effective therapies exist. Here we constructed a systems pharmacology model of intracellular signaling in peripheral neurons to identify novel drug targets for preventing peripheral neuropathy associated with proteasome inhibitors. Model predictions suggested the combinatorial inhibition of TNFα, NMDA receptors, and reactive oxygen species should prevent proteasome inhibitor-induced neuronal apoptosis. Dexanabinol, an inhibitor of all three targets, partially restored bortezomib-induced reduction of proximal action potential amplitude and distal nerve conduction velocity in vitro and prevented bortezomib-induced mechanical allodynia and thermal hyperalgesia in rats, including a partial recovery of intraepidermal nerve fiber density. Dexanabinol failed to restore bortezomib-induced decreases in electrophysiological endpoints in rats, and it did not compromise bortezomib anti-cancer effects in U266 multiple myeloma cells and a murine xenograft model. Owing to its favorable safety profile in humans and preclinical efficacy, dexanabinol might represent a treatment option for bortezomib-induced neuropathic pain.

Published

2022

6. An Artificial Intelligence Framework for Optimal Drug Design

Author

Grace Ramey, Santiago Vargas, Dinesh De Alwis, Anastassia N. Alexandrova, Joe Distefano, and Peter Bloomingdale

Subjects

Good Health and Well Being, 5.1 Pharmaceuticals, Neurosciences, Development of treatments and therapeutic interventions

Abstract

We introduce the concept of optimal drug design (ODD) as the use of an AI framework to optimize the exposure, safety, and efficacy of drugs. To exemplify the concept of ODD, we developed an artificial intelligence framework that integrates de novo molecular design, quantitative structure activity relationships, and pharmacokinetic-pharmacodynamic modeling. Specifically, our computational architecture has integrated a generative algorithm for small molecule design with a hybrid physiologically-based pharmacokinetic machine learning (PBPK-ML) model, which was applied to generate and optimize drug candidates for enhanced brain exposure. Publicly sourced data on the plasma and brain pharmacokinetics of 77 small molecule drugs in rats was used for model development. We have observed an approximate 30-fold and 120-fold increase on average in predicted brain exposure for AI generated molecules compared to known central nervous system drugs and randomly selected small organic molecules. We believe that with additional data and mechanistic modeling this in silico pipeline could facilitate the discovery of a new wave of optimally designed medicines for the treatment of CNS diseases.Graphical AbstractArtificial Intelligence Framework for the Optimization of Brain Pharmacokinetics.A genetic algorithm consisting of cross-breeding, mutating, scoring, and refining was used for de novo generation of a population of new molecular structures. SELFIE representations of molecules were used as input to a variational autoencoder for de novo generation/refinement of individual drug candidates. Molecular descriptors of individual drug candidates are generated and used as input into a trained neural network to generate drug-specific pharmacokinetic (PK) parameters. PK parameters are used as input into a physiologically-based pharmacokinetic (PBPK) model of the brain to predict brain PK of the drug candidate. Brain concentration-time profiles are integrated to obtain an area-under the curve (AUC), a metric of brain exposure, which is used to score and inform the design of new generations of molecules. Iterations of this framework generate novel drug candidates optimized for greater brain exposure. Created with BioRender.

Published

2022

7. Minimal brain PBPK model to support the preclinical and clinical development of antibody therapeutics for CNS diseases

Author

Christian Maass, Suruchi Bakshi, Cesar Pichardo-Almarza, Piet H. van der Graaf, Peter Bloomingdale, Eline van Maanen, Daniela Bumbaca Yadav, and Nitin Mehrotra

Subjects

Drug, Physiologically based pharmacokinetic modelling, PBPK, media_common.quotation_subject, Central nervous system, Context (language use), Drug development, Models, Biological, Antibodies, Pharmacokinetics, Central Nervous System Diseases, Medicine, Humans, Computer Simulation, Compartment (pharmacokinetics), Antibody, media_common, Pharmacology, Original Paper, business.industry, Area under the curve, Brain, medicine.anatomical_structure, business, Neuroscience

Abstract

There are several antibody therapeutics in preclinical and clinical development, industry-wide, for the treatment of central nervous system (CNS) disorders. Due to the limited permeability of antibodies across brain barriers, the quantitative understanding of antibody exposure in the CNS is important for the design of antibody drug characteristics and determining appropriate dosing regimens. We have developed a minimal physiologically-based pharmacokinetic (mPBPK) model of the brain for antibody therapeutics, which was reduced from an existing multi-species platform brain PBPK model. All non-brain compartments were combined into a single tissue compartment and cerebral spinal fluid (CSF) compartments were combined into a single CSF compartment. The mPBPK model contains 16 differential equations, compared to 100 in the original PBPK model, and improved simulation speed approximately 11-fold. Area under the curve ratios for minimal versus full PBPK models were close to 1 across species for both brain and plasma compartments, which indicates the reduced model simulations are similar to those of the original model. The minimal model retained detailed physiological processes of the brain while not significantly affecting model predictability, which supports the law of parsimony in the context of balancing model complexity with added predictive power. The minimal model has a variety of applications for supporting the preclinical development of antibody therapeutics and can be expanded to include target information for evaluating target engagement to inform clinical dose selection. Supplementary Information The online version contains supplementary material available at 10.1007/s10928-021-09776-7.

Published

2021

8. High-Resolution Ex Vivo Tissue Clearing, Lightsheet Imaging, and Data Analysis to Support Macromolecular Drug and Biomarker Distribution in Whole Organs and Tumors

Author

Niyanta Kumar, Petr Hrobař, Martin Vagenknecht, Jindrich Soukup, Peter Bloomingdale, Tomoko Freshwater, Sophia Bardehle, Roman Peter, Nadia Patterson, Ruban Mangadu, Cinthia Pastuskovas, and Mark Cancilla

Subjects

Instrumentation

Published

2022

9. Quantitative systems pharmacology in neuroscience: Novel methodologies and technologies

Author

Sreeraj Macha, Murat Cirit, Justin T. Baker, William J. McCarty, Peter Bloomingdale, Sarah F. Muldoon, Hugo Geerts, and Tatiana Karelina

Subjects

Systems neuroscience, Connectomics, Digital device, Computer science, Mini‐reviews, Brain, Reviews, Neurodegenerative Diseases, RM1-950, Congresses as Topic, Network Pharmacology, Models, Biological, Pharmacometrics, Pharmacological interventions, Therapeutic Area, Modeling and Simulation, Mini‐review, Drug Discovery, Humans, Pharmacology (medical), Therapeutics. Pharmacology, Human Induced Pluripotent Stem Cells, Neuroscience, Systems pharmacology

Abstract

The development and application of quantitative systems pharmacology models in neuroscience have been modest relative to other fields, such as oncology and immunology, which may reflect the complexity of the brain. Technological and methodological advancements have enhanced the quantitative understanding of brain physiology and pathophysiology and the effects of pharmacological interventions. To maximize the knowledge gained from these novel data types, pharmacometrics modelers may need to expand their toolbox to include additional mathematical and statistical frameworks. A session was held at the 10th annual American Conference on Pharmacometrics (ACoP10) to highlight several recent advancements in quantitative and systems neuroscience. In this mini‐review, we provide a brief overview of technological and methodological advancements in the neuroscience therapeutic area that were discussed during the session and how these can be leveraged with quantitative systems pharmacology modeling to enhance our understanding of neurological diseases. Microphysiological systems using human induced pluripotent stem cells (IPSCs), digital biomarkers, and large‐scale imaging offer more clinically relevant experimental datasets, enhanced granularity, and a plethora of data to potentially improve the preclinical‐to‐clinical translation of therapeutics. Network neuroscience methodologies combined with quantitative systems models of neurodegenerative disease could help bridge the gap between cellular and molecular alterations and clinical end points through the integration of information on neural connectomics. Additional topics, such as the neuroimmune system, microbiome, single‐cell transcriptomic technologies, and digital device biomarkers, are discussed in brief.

Published

2020

10. Machine Learning in Drug Discovery and Development Part 1: A Primer

Author

Almut G. Winterstein, Gregory Hather, Juan Francisco Morales, Jagdeep T. Podichetty, Jackson Burton, Sarah Kim, Joshua D. Brown, Samuel Kim, Alan Talevi, Daniela J. Conrado, Jensen Kael White, Stephan Schmidt, and Peter Bloomingdale

Subjects

Computer science, Drug development, Machine learning, computer.software_genre, Machine Learning, Drug Development, Artificial Intelligence, Predictive Value of Tests, Drug Discovery, Tutorial, Humans, Pharmacology (medical), Model development, Drug Approval, business.industry, Drug discovery, lcsh:RM1-950, Pillar, Química, History, 20th Century, Models, Theoretical, Pharmacometrics, lcsh:Therapeutics. Pharmacology, Modeling and Simulation, Key (cryptography), Artificial intelligence, business, computer, Algorithms

Abstract

Artificial intelligence, in particular machine learning (ML), has emerged as a key promising pillar to overcome the high failure rate in drug development. Here, we present a primer on the ML algorithms most commonly used in drug discovery and development. We also list possible data sources, describe good practices for ML model development and validation, and share a reproducible example. A companion article will summarize applications of ML in drug discovery, drug development, and postapproval phase., Laboratorio de Investigación y Desarrollo de Bioactivos

Published

2020

11. Boolean network modeling in systems pharmacology

Author

Jin Niu, Peter Bloomingdale, Van Anh Nguyen, and Donald E. Mager

Subjects

0301 basic medicine, Pharmacology, Theoretical computer science, Process (engineering), Drug discovery, Computer science, Systems Biology, Systems biology, Ode, Antineoplastic Agents, Models, Biological, Article, Modeling and simulation, 03 medical and health sciences, 030104 developmental biology, Boolean network, Drug Discovery, Cellular network, Humans, Multiple Myeloma, Signal Transduction, Systems pharmacology

Abstract

Quantitative systems pharmacology (QSP) is an emerging discipline that aims to discover how drugs modulate the dynamics of biological components in molecular and cellular networks and the impact of those perturbations on human pathophysiology. The integration of systems-based experimental and computational approaches is required to facilitate the advancement of this field. QSP models typically consist of a series of ordinary differential equations (ODE). However, this mathematical framework requires extensive knowledge of parameters pertaining to biological processes, which is often unavailable. An alternative framework that does not require knowledge of system-specific parameters, such as Boolean network modeling, could serve as an initial foundation prior to the development of an ODE-based model. Boolean network models have been shown to efficiently describe, in a qualitative manner, the complex behavior of signal transduction and gene/protein regulatory processes. In addition to providing a starting point prior to quantitative modeling, Boolean network models can also be utilized to discover novel therapeutic targets and combinatorial treatment strategies. Identifying drug targets using a network-based approach could supplement current drug discovery methodologies and help to fill the innovation gap across the pharmaceutical industry. In this review, we discuss the process of developing Boolean network models and the various analyses that can be performed to identify novel drug targets and combinatorial approaches. An example for each of these analyses is provided using a previously developed Boolean network of signaling pathways in multiple myeloma. Selected examples of Boolean network models of human (patho-)physiological systems are also reviewed in brief.

Published

2018

12. Quantitative systems toxicology

Author

Conrad Housand, John M. Burke, Joshua F. Apgar, Peter Bloomingdale, Dhaval K. Shah, Bjorn L. Millard, and Donald E. Mager

Subjects

0301 basic medicine, Drug, Systems toxicology, business.industry, media_common.quotation_subject, Pharmacology, Toxicology, 030226 pharmacology & pharmacy, Article, 3. Good health, 03 medical and health sciences, Patient safety, 030104 developmental biology, 0302 clinical medicine, Drug development, Risk analysis (engineering), Organ specific, Medicine, Experimental methods, business, Adverse effect, media_common, Systems pharmacology

Abstract

The overarching goal of modern drug development is to optimize therapeutic benefits while minimizing adverse effects. However, inadequate efficacy and safety concerns remain to be the major causes of drug attrition in clinical development. For the past 80 years, toxicity testing has consisted of evaluating the adverse effects of drugs in animals to predict human health risks. The U.S. Environmental Protection Agency recognized the need to develop innovative toxicity testing strategies and asked the National Research Council to develop a long-range vision and strategy for toxicity testing in the 21st century. The vision aims to reduce the use of animals and drug development costs through the integration of computational modeling and in vitro experimental methods that evaluates the perturbation of toxicity-related pathways. Towards this vision, collaborative quantitative systems pharmacology and toxicology modeling endeavors (QSP/QST) have been initiated amongst numerous organizations worldwide. In this article, we discuss how quantitative structure-activity relationship (QSAR), network-based, and pharmacokinetic/pharmacodynamic modeling approaches can be integrated into the framework of QST models. Additionally, we review the application of QST models to predict cardiotoxicity and hepatotoxicity of drugs throughout their development. Cell and organ specific QST models are likely to become an essential component of modern toxicity testing, and provides a solid foundation towards determining individualized therapeutic windows to improve patient safety.

Published

2017