4.7 Article

Multiple Pathways for Pathological Calcification in the Human Body

期刊

ADVANCED HEALTHCARE MATERIALS
卷 10, 期 4, 页码 -

出版社

WILEY
DOI: 10.1002/adhm.202001271

关键词

apatite; biomineralization; breast cancer microcalcifications; cardiovascular calcifications; psammoma bodies

资金

  1. Human Frontier Science Program [RGP0016/2017]
  2. Center on the Physics of Cancer Metabolism from the National Cancer Institute [1U54CA210184-01]
  3. NSF MRSEC program [DMR-1719875]
  4. Ben-Gurion University of the Negev

向作者/读者索取更多资源

Biomineralization of skeletal components occurs under strict cellular regulation, producing mineral-organic composites optimized for their function. Pathological mineralization, driven by tissue abnormalities or disease, can have harmful health effects.
Biomineralization of skeletal components (e.g., bone and teeth) is generally accepted to occur under strict cellular regulation, leading to mineral-organic composites with hierarchical structures and properties optimized for their designated function. Such cellular regulation includes promoting mineralization at desired sites as well as inhibiting mineralization in soft tissues and other undesirable locations. In contrast, pathological mineralization, with potentially harmful health effects, can occur as a result of tissue or metabolic abnormalities, disease, or implantation of certain biomaterials. This progress report defines mineralization pathway components and identifies the commonalities (and differences) between physiological (e.g., bone remodeling) and pathological calcification formation pathways, based, in part, upon the extent of cellular control within the system. These concepts are discussed in representative examples of calcium phosphate-based pathological mineralization in cancer (breast, thyroid, ovarian, and meningioma) and in cardiovascular disease. In-depth mechanistic understanding of pathological mineralization requires utilizing state-of-the-art materials science imaging and characterization techniques, focusing not only on the final deposits, but also on the earlier stages of crystal nucleation, growth, and aggregation. Such mechanistic understanding will further enable the use of pathological calcifications in diagnosis and prognosis, as well as possibly provide insights into preventative treatments for detrimental mineralization in disease.

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