Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease Platform

Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease Platform

Abstract For many years, clinical research in Alzheimer’s disease (AD) has focused on attempts to identify the most explicit biomarker, namely amyloid beta. Unfortunately, the numerous therapies that have been developed have failed in clinical practice. AD arises as a consequence of multiple factors...

Full description

Bibliographic Details
Main Authors: Tatiana Karelina, Stepan Lerner, Alexandr Stepanov, Mark Meerson, Oleg Demin
Format: Article
Language:English
Published: Wiley 2021-06-01
Series:CPT: Pharmacometrics & Systems Pharmacology
Online Access:https://doi.org/10.1002/psp4.12628
id doaj-1469ef7fa5664addaa330de58cbeb12d
record_format Article
spelling doaj-1469ef7fa5664addaa330de58cbeb12d2021-06-18T20:44:13ZengWileyCPT: Pharmacometrics & Systems Pharmacology2163-83062021-06-0110654355010.1002/psp4.12628Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease PlatformTatiana Karelina0Stepan Lerner1Alexandr Stepanov2Mark Meerson3Oleg Demin4InSysBio LLC Moscow RussiaInSysBio LLC Moscow RussiaInSysBio LLC Moscow RussiaInSysBio LLC Moscow RussiaInSysBio LLC Moscow RussiaAbstract For many years, clinical research in Alzheimer’s disease (AD) has focused on attempts to identify the most explicit biomarker, namely amyloid beta. Unfortunately, the numerous therapies that have been developed have failed in clinical practice. AD arises as a consequence of multiple factors, and as such it requires a more mechanistic analytical approach than statistical modeling. Quantitative systems pharmacology modeling is a valuable tool for drug development. It utilizes in vitro data for the calibration of parameters, embeds them into physiologically based structures, and explores translation between animals and humans. Such an approach allows for a quantitative study of the dynamics of the interactions between multiple factors or variables. Here, we present an overview of the quantitative translational model in AD, which embraces current preclinical and clinical data. The previously published description of amyloid physiology has been updated and joined with a model for tau pathology and multiple intraneuronal processes responsible for cellular transport, metabolism, or proteostasis. In addition, several hypotheses regarding the best correlates of cognitive deterioration have been validated using clinical data. Here, the amyloid hypothesis was unable to predict the aducanumab clinical trial data, whereas simulations of cognitive impairment coupled with tau seeding or neuronal breakdown (expressed as caspase activity) matched the data. A satisfactory validation of the data from multiple preclinical and clinical studies was followed by an attempt to predict the results of combinatorial treatment with targeted immunotherapy and activation of autophagy using rapamycin. The combination is predicted to yield better efficacy than immunotherapy alone.https://doi.org/10.1002/psp4.12628
collection DOAJ
language English
format Article
sources DOAJ
author Tatiana Karelina
Stepan Lerner
Alexandr Stepanov
Mark Meerson
Oleg Demin
spellingShingle Tatiana Karelina
Stepan Lerner
Alexandr Stepanov
Mark Meerson
Oleg Demin
Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease Platform
CPT: Pharmacometrics & Systems Pharmacology
author_facet Tatiana Karelina
Stepan Lerner
Alexandr Stepanov
Mark Meerson
Oleg Demin
author_sort Tatiana Karelina
title Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease Platform
title_short Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease Platform
title_full Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease Platform
title_fullStr Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease Platform
title_full_unstemmed Monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: Predictions using an integrated Alzheimer’s Disease Platform
title_sort monoclonal antibody therapy efficacy can be boosted by combinations with other treatments: predictions using an integrated alzheimer’s disease platform
publisher Wiley
series CPT: Pharmacometrics & Systems Pharmacology
issn 2163-8306
publishDate 2021-06-01
description Abstract For many years, clinical research in Alzheimer’s disease (AD) has focused on attempts to identify the most explicit biomarker, namely amyloid beta. Unfortunately, the numerous therapies that have been developed have failed in clinical practice. AD arises as a consequence of multiple factors, and as such it requires a more mechanistic analytical approach than statistical modeling. Quantitative systems pharmacology modeling is a valuable tool for drug development. It utilizes in vitro data for the calibration of parameters, embeds them into physiologically based structures, and explores translation between animals and humans. Such an approach allows for a quantitative study of the dynamics of the interactions between multiple factors or variables. Here, we present an overview of the quantitative translational model in AD, which embraces current preclinical and clinical data. The previously published description of amyloid physiology has been updated and joined with a model for tau pathology and multiple intraneuronal processes responsible for cellular transport, metabolism, or proteostasis. In addition, several hypotheses regarding the best correlates of cognitive deterioration have been validated using clinical data. Here, the amyloid hypothesis was unable to predict the aducanumab clinical trial data, whereas simulations of cognitive impairment coupled with tau seeding or neuronal breakdown (expressed as caspase activity) matched the data. A satisfactory validation of the data from multiple preclinical and clinical studies was followed by an attempt to predict the results of combinatorial treatment with targeted immunotherapy and activation of autophagy using rapamycin. The combination is predicted to yield better efficacy than immunotherapy alone.
url https://doi.org/10.1002/psp4.12628
work_keys_str_mv AT tatianakarelina monoclonalantibodytherapyefficacycanbeboostedbycombinationswithothertreatmentspredictionsusinganintegratedalzheimersdiseaseplatform
AT stepanlerner monoclonalantibodytherapyefficacycanbeboostedbycombinationswithothertreatmentspredictionsusinganintegratedalzheimersdiseaseplatform
AT alexandrstepanov monoclonalantibodytherapyefficacycanbeboostedbycombinationswithothertreatmentspredictionsusinganintegratedalzheimersdiseaseplatform
AT markmeerson monoclonalantibodytherapyefficacycanbeboostedbycombinationswithothertreatmentspredictionsusinganintegratedalzheimersdiseaseplatform
AT olegdemin monoclonalantibodytherapyefficacycanbeboostedbycombinationswithothertreatmentspredictionsusinganintegratedalzheimersdiseaseplatform
_version_ 1721372707973496832

Similar Items