AI Article Synopsis
- Acute lung injury (ALI) is a serious condition in ICU patients with high mortality, and current treatments are not effective, creating a need for new therapies.
- The NLPR3 inflammasome plays a key role in ALI by releasing inflammatory factors and causing damaging cell death, but inhibiting its activation through the MM01 compound shows promise as a treatment.
- By utilizing drug delivery nanoparticles that target inflamed macrophages, MM01 can be effectively delivered to the lungs, demonstrating a potential new approach for treating ALI in animal models.
Article Abstract
Acute lung injury (ALI) is a severe pulmonary disorder responsible for high percentage of mortality and morbidity in intensive care unit patients. Current treatments are ineffective, so the development of efficient and specific therapies is an unmet medical need. The activation of NLPR3 inflammasome during ALI produces the release of proinflammatory factors and pyroptosis, a proinflammatory form of cell death that contributes to lung damage spreading. Herein, it is demonstrated that modulating inflammasome activation through inhibition of ASC oligomerization by the recently described MM01 compound can be an alternative pharmacotherapy against ALI. Besides, the added efficacy of using a drug delivery nanosystem designed to target the inflamed lungs is determined. The MM01 drug is incorporated into mesoporous silica nanoparticles capped with a peptide (TNFR-MM01-MSNs) to target tumor necrosis factor receptor-1 (TNFR-1) to proinflammatory macrophages. The prepared nanoparticles can deliver the cargo in a controlled manner after the preferential uptake by proinflammatory macrophages and exhibit anti-inflammatory activity. Finally, the therapeutic effect of MM01 free or nanoparticulated to inhibit inflammatory response and lung injury is successfully demonstrated in lipopolysaccharide-mouse model of ALI. The results suggest the potential of pan-inflammasome inhibitors as candidates for ALI therapy and the use of nanoparticles for targeted lung delivery.
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| http://dx.doi.org/10.1002/adhm.202301577 | DOI Listing |
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