Model‐informed drug repurposing: A pharmacometric approach to novel pathogen preparedness, response and retrospection

Dodds, Michael; Xiong, Yuning; Mouksassi, Samer; Kirkpatrick, Carl M.; Hui, Katrina; Doyle, Eileen; Patel, Kashyap; Cox, Eugène; Wesche, David; Brown, Frances C.; Rayner, Craig R.

doi:10.1111/bcp.14760

Cited by 14 publications

(13 citation statements)

References 36 publications

(74 reference statements)

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“…Additional collaborations are also possible with the health economics and outcomes research (HEOR) function, with which outputs from the MBMA could be integrated into other, non-clinically focused models, such as cost-effectiveness models or financial forecasting models, potentially leading to improved commercial and financial strategies [45]. Therefore, continued education and communication among project stakeholders, team collaborators, and [19,[107][108][109][110] Correlation between early and late endpoints Allow the use of a biomarker or an early clinical efficacy time point to detect a signal of the treatment effect [38,42,63,111] Pharmacokinetic and pharmacodynamic relationship Establishing the relationship between exposure and an efficacy or safety biomarker, possibly a less frequently reported one and would need data from a large population to be detected [41,[112][113][114][115][116][117] Simulation of established MBMA models Simulate various scenarios using established MBMA models to optimize clinical trial design [62,118] Pharmacoeconomics Incorporate cost-effectiveness into a MBMA model [119] other pharmacometric specialty experts regarding MBMA and MIDD approaches in general are warranted [1]. Another important ally of MIDD approaches is from statistics.…”

Section: Collaboration Between Pharmacometrics and Other Drug Develop...mentioning

confidence: 99%

Applications of Model-Based Meta-Analysis in Drug Development

Chan¹,

Peskov

Song

2022

Pharm Res

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Model-based meta-analysis (MBMA) is a quantitative approach that leverages published summary data along with internal data and can be applied to inform key drug development decisions, including the benefit-risk assessment of a treatment under investigation. These risk–benefit assessments may involve determining an optimal dose compared against historic external comparators of a particular disease indication. MBMA can provide a flexible framework for interpreting aggregated data from historic reference studies and therefore should be a standard tool for the model-informed drug development (MIDD) framework.In addition to pairwise and network meta-analyses, MBMA provides further contributions in the quantitative approaches with its ability to incorporate longitudinal data and the pharmacologic concept of dose–response relationship, as well as to combine individual- and summary-level data and routinely incorporate covariates in the analysis.A common application of MBMA is the selection of optimal dose and dosing regimen of the internal investigational molecule to evaluate external benchmarking and to support comparator selection. Two case studies provided examples in applications of MBMA in biologics (durvalumab + tremelimumab for safety) and small molecule (fenebrutinib for efficacy) to support drug development decision-making in two different but well-studied disease areas, i.e., oncology and rheumatoid arthritis, respectively.Important to the future directions of MBMA include additional recognition and engagement from drug development stakeholders for the MBMA approach, stronger collaboration between pharmacometrics and statistics, expanded data access, and the use of machine learning for database building. Timely, cost-effective, and successful application of MBMA should be part of providing an integrated view of MIDD.

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Section: Collaboration Between Pharmacometrics and Other Drug Develop...mentioning

confidence: 99%

Applications of Model-Based Meta-Analysis in Drug Development

Chan¹,

Peskov

Song

2022

Pharm Res

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“…28 A more rational stepwise model-informed drug repurposing approach has been proposed, integrating preparatory, reactive, and retrospective action in response to new pathogens. 29,30 In essence, situations of desperation call for more highquality rational science, and not less.…”

Section: Why Do Neglected Populations Present a Particular Challenge?mentioning

confidence: 99%

Twice neglected? Neglected diseases in neglected populations

Weld

Waitt

Barnes

et al. 2021

Brit J Clinical Pharma

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It is unfortunately true that clinicians lack the necessary evidence to know how to use medications properly in large sections of the population and do not have optimal treatments to use for many neglected tropical diseases (NTDs). NTDs often disproportionately affect neglected populations that are left out of research efforts, such as children and pregnant women. As reliable access to safe, effective preventives and treatments can break the cycle of poverty, illness, and ensuing debility that further perpetuates poverty, it is of paramount importance to investigate and develop new medicines for neglected populations suffering from NTDs. Furthermore, there is not only a need to develop and evaluate novel therapies, but also to ensure that these are affordable, available, and adapted to the communities who need them. The NIH has proposed a "4 C's" framework which is relevant for neglected diseases and populations and should be leveraged for the study of the Twice Neglected: Consider inclusion; Collect data from neglected populations with neglected conditions; Characterize differences through meaningful analysis; Communicate findings pertaining to neglected diseases and populations. With this editorial, the British Journal of Clinical Pharmacology hereby launches a call for high-quality articles focusing on NTDs in special populations, to facilitate and encourage the reversal of this dual neglect.

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“…Preparedness for future pandemics therefore requires the development of policies and processes to identify, react to, and control future pandemics in a timely and efficient manner. This is introduced by Dodds et al [5] and further developed by Davda et al [6] who present a five-stage blueprint that will allow us to be prepared for, and react to, future viral outbreaks. Importantly, the blueprint is centred on pre-pandemic preparedness, including surveillance for new pathogens, high through-put screening for potential therapeutic options using human derived pulmonary cells and the identification of key pharmacological indices such as IC50 values (or better EC90 values) using prior work on reference viruses [6].…”

Section: Tables: Nilmentioning

confidence: 99%

“…This concept was extended by Dodds et al [10], who used a similar platform to show how targeting different aspects of the viral lifecycle with combinations of repurposed (or novel) agents will optimise treatment success. The use of in silico tools was also emphasised by Dodds et al [5] and Davda et al [6] as important platforms to allow for expedited drug repurposing efforts and drug development in future pandemics. In addition, in silico tools can be used to ensure that the basic principles of clinical pharmacology are not ignored in the haste to propose possible treatments, an important lesson from early in the COVID-19 crisis echoed in the contribution from Smith et al [11] and the ASCEPT-BPS statement on drug repurposing [12].…”

Section: Tables: Nilmentioning

confidence: 99%