AI Article Synopsis

  • The skeletal system includes bones, ligaments, and cartilage, and is essential for body support; however, treating diseases affecting it is challenging due to regions like avascular cartilage.
  • Bone-targeting drugs aim to improve treatment effectiveness and reduce side effects by specifically targeting the skeletal system or certain cell types, often utilizing the affinity to hydroxyapatite, a key bone component.
  • Despite advancements in drug delivery methods for skeletal disorders such as osteoporosis and infections, challenges remain in maintaining drug activity and minimizing local adverse effects, prompting ongoing research into improved targeting strategies.

Article Abstract

The skeletal system, comprising bones, ligaments, cartilage and their connective tissues, is critical for the structure and support of the body. Diseases that affect the skeletal system can be difficult to treat, mainly because of the avascular cartilage region. Targeting drugs to the site of action can not only increase efficacy but also reduce toxicity. Bone-targeting drugs are designed with either of two general targeting moieties, aimed at the entire skeletal system or a specific cell type. Most bone-targeting drugs utilize an affinity to hydroxyapatite, a major component of the bone matrix that includes a high concentration of positively-charged Ca. The strategies for designing such targeting moieties can involve synthetic and/or biological components including negatively-charged amino acid peptides or bisphosphonates. Efficient delivery of bone-specific drugs provides significant impact in the treatment of skeletal related disorders including infectious diseases (osteoarthritis, osteomyelitis, etc.), osteoporosis, and metabolic skeletal dysplasia. Despite recent advances, however, both delivering the drug to its target without losing activity and avoiding adverse local effects remain a challenge. In this review, we investigate the current development of bone-targeting moieties, their efficacy and limitations, and discuss future directions for the development of these specific targeted treatments.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5535838PMC
http://dx.doi.org/10.3390/ijms18071345DOI Listing

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