Atavistic strategy for the treatment of hyperuricemia via ionizable liposomal mRNA.
Mengjie ZhangAbid HussainBo HuHaiyin YangChunhui LiShuai GuoXiaofeng HanBei LiYulun DaiYuhong CaoHang ChiYuhua WengCheng-Feng QinYuanyu HuangPublished in: Nature communications (2024)
Hyperuricemia is associated with an increased risk of gout, hypertension, diabetes, and cardiovascular diseases. Most mammals maintain normal serum uric acid (SUA) via urate oxidase (Uox), an enzyme that metabolizes poorly-soluble UA to highly-soluble allantoin. In contrast, Uox became a pseudogene in humans and apes over the long course of evolution. Here we demonstrate an atavistic strategy for treating hyperuricemia based on endogenous expression of Uox in hepatocytes mediated by mRNA (mUox) loaded with an ionizable lipid nanoparticle termed iLAND. mUox@iLAND allows effective transfection and protein expression in vitro. A single dose of mUox@iLAND lowers SUA levels for several weeks in two female murine models, including a novel long-lasting model, which is also confirmed by metabolomics analysis. Together with the excellent safety profiles observed in vivo, the proposed mRNA agent demonstrates substantial potential for hyperuricemia therapy and the prevention of associated conditions.
Keyphrases
- uric acid
- metabolic syndrome
- cardiovascular disease
- binding protein
- blood pressure
- poor prognosis
- type diabetes
- drug delivery
- mass spectrometry
- magnetic resonance
- magnetic resonance imaging
- cardiovascular risk factors
- coronary artery disease
- skeletal muscle
- glycemic control
- fatty acid
- long non coding rna
- adipose tissue
- bone marrow
- cardiovascular events
- smoking cessation
- gestational age
- replacement therapy