Dynamic modeling of bone remodeling, osteolytic metastasis and PK/PD therapy: introducing variable order derivatives as a simplification technique.

J Math Biol

IDMEC, Instituto Superior Técnico, Universidade de Lisboa, Av. Rovisco Pais 1, 1049-001, Lisbon, Portugal.

Published: September 2021

AI Article Synopsis

  • Bone is continually renewed in adults through a balanced process of resorption and formation, but this environment also promotes tumor growth, particularly from breast and prostate cancers.
  • Mathematical models using differential equations can simulate both normal bone remodeling and the impact of metastases, highlighting how tumors disrupt this balance and contribute to their own growth.
  • The paper discusses new biochemical models, some featuring fewer parameters, that effectively represent interactions between tumors and bone, while also considering the effects of anti-cancer therapies on bone integrity.

Article Abstract

Bone is constantly being renewed: in the adult skeleton, bone resorption and formation are in a tightly coupled balance, allowing for a constant bone density to be maintained. Yet this micro-environment provides the necessary conditions for the growth and proliferation of tumor cells, and thus bone is a common site for the development of metastases, mainly from primary breast and prostate cancer. Mathematical and computational models with differential equations can replicate this bone remodeling process. These models have been extended to include the effects of disruptive tumor pathologies in the bone dynamics, as metastases contribute to the decoupling between bone resorption and formation and to the self-perpetuating tumor growth cycle. Such models may also contemplate the counteraction effects of currently used therapies, and, in the case of treatments with drugs, their pharmocokinetics and pharmacodynamics. We present a thorough overview of biochemical models for bone remodeling, in the presence of a tumour together with anti-cancer and anti-resorptive therapy, formulated as systems of first-order differential equations, or simplified using variable order derivatives. The latter models, of which some are new to this paper, result in equations with fewer parameters, and allow accounting for anomalous diffusion processes. In this way, more compact and parsimonious models, that promptly highlight tumorous bone interactions, are achieved, providing an effective framework to counteract the loss of bone integrity on the affected areas.

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Source
http://dx.doi.org/10.1007/s00285-021-01666-3DOI Listing

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