| Literature DB >> 33603238 |
Mingjing Cao1,2,3, Rong Cai1, Lina Zhao4, Mengyu Guo1,3, Liming Wang4, Yucai Wang5, Lili Zhang6, Xiaofeng Wang4, Haodong Yao4, Chunyu Xie1, Yalin Cong1, Yong Guan7, Xiayu Tao7, Yaling Wang1, Shaoxin Xu1, Ying Liu1,8, Yuliang Zhao1,3,8, Chunying Chen9,10,11,12.
Abstract
Many nanoscale biomaterials fail to reach the clinical trial stage due to a poor understanding of the fundamental principles of their in vivo behaviour. Here we describe the transport, transformation and bioavailability of MoS2 nanomaterials through a combination of in vivo experiments and molecular dynamics simulations. We show that after intravenous injection molybdenum is significantly enriched in liver sinusoid and splenic red pulp. This biodistribution is mediated by protein coronas that spontaneously form in the blood, principally with apolipoprotein E. The biotransformation of MoS2 leads to incorporation of molybdenum into molybdenum enzymes, which increases their specific activities in the liver, affecting its metabolism. Our findings reveal that nanomaterials undergo a protein corona-bridged transport-transformation-bioavailability chain in vivo, and suggest that nanomaterials consisting of essential trace elements may be converted into active biological molecules that organisms can exploit. Our results also indicate that the long-term biotransformation of nanomaterials may have an impact on liver metabolism.Entities:
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Year: 2021 PMID: 33603238 DOI: 10.1038/s41565-021-00856-w
Source DB: PubMed Journal: Nat Nanotechnol ISSN: 1748-3387 Impact factor: 39.213