The Virtual Anemia Trial: An Assessment of Model‐Based <i>In Silico</i> Clinical Trials of Anemia Treatment Algorithms in Patients With Hemodialysis

Fuertinger, Doris; Topping, Alice; Kappel, Franz; Thijssen, Stephan; Kotanko, Peter

doi:10.1002/psp4.12276

Cited by 8 publications

(16 citation statements)

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“…A key idea is the shift from real-world clinical trial testing a single treatment option on many, mostly unselected, patients to first test in silico several treatment options, both approved or repurposed, for each individual patient. Importantly, mathematical models can also optimize the dosage and scheduling of the selected treatment [141, 162, 164–166].…”

Section: Discussionmentioning

confidence: 99%

System-based approaches as prognostic tools for glioblastoma

et al. 2019

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BackgroundThe evasion of apoptosis is a hallmark of cancer. Understanding this process holistically and overcoming apoptosis resistance is a goal of many research teams in order to develop better treatment options for cancer patients. Efforts are also ongoing to personalize the treatment of patients. Strategies to confirm the therapeutic efficacy of current treatments or indeed to identify potential novel additional options would be extremely beneficial to both clinicians and patients. In the past few years, system medicine approaches have been developed that model the biochemical pathways of apoptosis. These systems tools incorporate and analyse the complex biological networks involved. For their successful integration into clinical practice, it is mandatory to integrate systems approaches with routine clinical and histopathological practice to deliver personalized care for patients.ResultsWe review here the development of system medicine approaches that model apoptosis for the treatment of cancer with a specific emphasis on the aggressive brain cancer, glioblastoma.ConclusionsWe discuss the current understanding in the field and present new approaches that highlight the potential of system medicine approaches to influence how glioblastoma is diagnosed and treated in the future.

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Section: Discussionmentioning

confidence: 99%

System-based approaches as prognostic tools for glioblastoma

et al. 2019

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“…Individual patients were represented by a patientspecific parameter set (RBC life span, ESA half-life, endogenous Epo levels, and effective parameters accounting for the ESA's effect on erythroid progenitor apoptosis and maturation velocity) capturing their erythropoiesis-related physiology (Fuertinger FIGURE 5 | Estimation of physiological parameters in a HD patient population using a physiology-based model of erythropoiesis (Fuertinger et al, 2013). Shown are relative frequencies of estimated RBC life span (left) and endogenous Epo levels (right) obtained from patient-individual model adaptations to hemoglobin and ESA administration data of 6,659 HD patients, resulting in a virtual patient population (Fuertinger et al, 2018b) (see the main text for details).…”

Section: Relation Between Rbc Life Span and Epo Requirement: Insightsmentioning

confidence: 99%

“…10.2 U/L, 21.1 U/L). The relative frequencies of estimated RBC life spans and endogenous Epo levels among the population of virtual patients reported in Fuertinger et al (2018b) are shown in Figure 5.…”

Section: Relation Between Rbc Life Span and Epo Requirement: Insightsmentioning

confidence: 99%

“…This model explicitly represents the proliferative hierarchy of erythroid progenitor populations in the bone marrow including the dynamics of cell birth, maturation, differentiation, and apoptosis; in this modeling scheme, Epo acts as a regulator of apoptosis of the colony-forming unit-erythroid (CFU-E) and erythrocyte populations. Previously, this model has been adapted on a patient-individual level to a large population of HD patients treated with methoxy polyethylene glycol-epoetin beta (6,659 patients randomly sampled from a U.S. HD population comprising over 37,000 patients) ( Fuertinger et al, 2018b ). These model adaptations were carried out such that previously recorded hemoglobin responses to ESA therapy for the specific patient were described by the model within a predefined accuracy.…”

Section: Relation Between Rbc Life Span and Epo Requirement: Insightsmentioning

confidence: 99%

“…These model adaptations were carried out such that previously recorded hemoglobin responses to ESA therapy for the specific patient were described by the model within a predefined accuracy. Individual patients were represented by a patient-specific parameter set (RBC life span, ESA half-life, endogenous Epo levels, and effective parameters accounting for the ESA’s effect on erythroid progenitor apoptosis and maturation velocity) capturing their erythropoiesis-related physiology ( Fuertinger et al, 2018b ). Although iron availability is not an explicit part of the model, its effects are implicitly present in the effective bone marrow-related parameters.…”

Section: Relation Between Rbc Life Span and Epo Requirement: Insightsmentioning

confidence: 99%

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The Role of Eryptosis in the Pathogenesis of Renal Anemia: Insights From Basic Research and Mathematical Modeling

Dias

Grobe

Rogg

et al. 2020

Front. Cell Dev. Biol.

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Red blood cells (RBC) are the most abundant cells in the blood. Despite powerful defense systems against chemical and mechanical stressors, their life span is limited to about 120 days in healthy humans and further shortened in patients with kidney failure. Changes in the cell membrane potential and cation permeability trigger a cascade of events that lead to exposure of phosphatidylserine on the outer leaflet of the RBC membrane. The translocation of phosphatidylserine is an important step in a process that eventually results in eryptosis, the programmed death of an RBC. The regulation of eryptosis is complex and involves several cellular pathways, such as the regulation of non-selective cation channels. Increased cytosolic calcium concentration results in scramblase and floppase activation, exposing phosphatidylserine on the cell surface, leading to early clearance of RBCs from the circulation by phagocytic cells. While eryptosis is physiologically meaningful to recycle iron and other RBC constituents in healthy subjects, it is augmented under pathological conditions, such as kidney failure. In chronic kidney disease (CKD) patients, the number of eryptotic RBC is significantly increased, resulting in a shortened RBC life span that further compounds renal anemia. In CKD patients, uremic toxins, oxidative stress, hypoxemia, and inflammation contribute to the increased eryptosis rate. Eryptosis may have an impact on renal anemia, and depending on the degree of shortened RBC life span, the administration of erythropoiesis-stimulating agents is often insufficient to attain desired hemoglobin target levels. The goal of this review is to indicate the importance of eryptosis as a process closely related to life span reduction, aggravating renal anemia.

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In silico trial for the assessment of givinostat dose adjustment rules based on the management of key hematological parameters in polycythemia vera patients

Tosca,

De Carlo,

Bartolucci

et al. 2024

CPT Pharmacom & Syst Pharma

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Polycythemia vera (PV) is a chronic myeloproliferative neoplasm characterized by excessive levels of platelets (PLT), white blood cells (WBC), and hematocrit (HCT). Givinostat (ITF2357) is a potent histone‐deacetylase inhibitor that showed a good safety/efficacy profile in PV patients during phase I/II studies. A phase III clinical trial had been planned and an adaptive dosing protocol had been proposed where givinostat dose is iteratively adjusted every 28 days (one cycle) based on PLT, WBC, and HCT. As support, a simulation platform to evaluate and refine the proposed givinostat dose adjustment rules was developed. A population pharmacokinetic/pharmacodynamic model predicting the givinostat effects on PLT, WBC, and HCT in PV patients was developed and integrated with a control algorithm implementing the adaptive dosing protocol. Ten in silico trials in ten virtual PV patient populations were simulated 500 times. Considering an eight‐treatment cycle horizon, reducing/increasing the givinostat daily dose by 25 mg/day step resulted in a higher percentage of patients with a complete hematological response (CHR), that is, PLT ≤400 × 109/L, WBC ≤10 × 109/L, and HCT < 45% without phlebotomies in the last three cycles, and a lower percentage of patients with grade II toxicity events compared with 50 mg/day adjustment steps. After the eighth cycle, 85% of patients were predicted to receive a dose ≥100 mg/day and 40.90% (95% prediction interval = [34, 48.05]) to show a CHR. These results were confirmed at the end of 12th, 18th, and 24th cycles, showing a stability of the response between the eighth and 24th cycles.

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The Virtual Anemia Trial: An Assessment of Model‐Based In Silico Clinical Trials of Anemia Treatment Algorithms in Patients With Hemodialysis

Cited by 8 publications

References 30 publications

System-based approaches as prognostic tools for glioblastoma

System-based approaches as prognostic tools for glioblastoma

The Role of Eryptosis in the Pathogenesis of Renal Anemia: Insights From Basic Research and Mathematical Modeling

In silico trial for the assessment of givinostat dose adjustment rules based on the management of key hematological parameters in polycythemia vera patients

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