Abstract
It is unclear whether the new anti-catabolic agent denosumab represents a viable alternative to the widely used anti-catabolic agent pamidronate in the treatment of Multiple Myeloma (MM)-induced bone disease. This lack of clarity primarily stems from the lack of sufficient clinical investigations, which are costly and time consuming. However, in silico investigations require less time and expense, suggesting that they may be a useful complement to traditional clinical investigations. In this paper, we aim to (i) develop integrated computational models that are suitable for investigating the effects of pamidronate and denosumab on MM-induced bone disease and (ii) evaluate the responses to pamidronate and denosumab treatments using these integrated models. To achieve these goals, pharmacokinetic models of pamidronate and denosumab are first developed and then calibrated and validated using different clinical datasets. Next, the integrated computational models are developed by incorporating the simulated transient concentrations of pamidronate and denosumab and simulations of their actions on the MM-bone compartment into the previously proposed MM-bone model. These integrated models are further calibrated and validated by different clinical datasets so that they are suitable to be applied to investigate the responses to the pamidronate and denosumab treatments. Finally, these responses are evaluated by quantifying the bone volume, bone turnover, and MM-cell density. This evaluation identifies four denosumab regimes that potentially produce an overall improved bone-related response compared with the recommended pamidronate regime. This in silico investigation supports the idea that denosumab represents an appropriate alternative to pamidronate in the treatment of MM-induced bone disease.
Highlights
Multiple Myeloma (MM) is a B cell malignancy that is associated with high morbidity and short survival duration after diagnosis
The optimized pharmacokinetic models of pamidronate and denosumab are suitable for simulating the transient concentrations of pamidronate and denosumab, which are incorporated into the MM-bone model to examine the responses to pamidronate and denosumab treatments in MMinduced bone disease
We illustrated how to investigate the anti-catabolic effects of pamidronate and denosumab treatments in MM-induced bone disease using integrated computational models that link a bone resorption marker with drug pharmacokinetics and drug actions on the MM-bone compartment
Summary
Multiple Myeloma (MM) is a B cell malignancy that is associated with high morbidity and short survival duration after diagnosis. Over 70% of patients with MM will develop bone lesions as the MM progress, resulting in osteolytic bone disease that includes severe bone pain, pathological fractures, osteoporosis and hypocalcaemia [1,2,3]. These osteolytic lesions may progress even if patients with MM respond to antiMM therapy [4,5]. MM-induced osteolytic bone disease is a major cause of morbidity and mortality in patients with MM [6], and the management of osteolysis in patients with MM is a key aspect in the treatment of this malignancy
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