FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2022961136> ?p ?o ?g. }

• W2022961136 endingPage "2429" @default.
• W2022961136 startingPage "2419" @default.
• W2022961136 abstract "Efficient intracellular delivery of quantum dots (QDs) and unravelling the mechanism underlying the intracellular delivery are essential for advancing the applications of QDs toward in vivo imaging and therapeutic interventions. Here, we show that clathrin-mediated endocytosis is the most important pathway for the intracellular delivery of peptide-conjugated QDs. We selected an insect neuropeptide, namely, allatostatin (AST1, APSGAQRLYG FGL-NH(2)), conjugated it with CdSe-ZnS QDs, and investigated the intracellular delivery of the conjugate in living cells such as human epidermoid ovarian carcinoma cells (A431) and mouse embryonic fibroblast cells (3T3). We selected AST1 to investigate the intracellular delivery of QDs because we recently found it to be efficient for delivering QDs in living mammalian cells. Also, the receptors of AST1 in insects show functional and sequence similarity to G-protein-coupled galanin receptors in mammals. We employed flow cytometry and fluorescence microscopy and investigated the contributions of clathrin-mediated endocytosis, receptor-mediated endocytosis, and charge-based cell penetration or transduction to the intracellular delivery of QD-AST1 conjugates. Interestingly, the intracellular delivery was suppressed by approximately 57% when we inhibited the regulatory enzyme phosphoinositide 3-kinase (PI3K) with wortmannin and blocked the formation of clathrin-coated vesicles. In parallel, we investigated clathrin-mediated endocytosis by colocalizing QD560-labeled clathrin heavy-chain antibody and QD605-AST1. We also estimated galanin receptor-mediated endocytosis of QD-AST1 at <10% by blocking the cells with a galanin antagonist and transduction at <30% by both removing the charge of the peptide due to arginine and suppressing the cell-surface charge due to glycosaminoglycan. In short, the current work shows that multiple pathways are involved in the intracellular delivery of peptide-conjugated QDs, among which clathrin-mediated endocytosis is the most important." @default.
• W2022961136 created "2016-06-24" @default.
• W2022961136 creator A5007732916 @default.
• W2022961136 creator A5055785987 @default.
• W2022961136 creator A5071110371 @default.
• W2022961136 creator A5077052384 @default.
• W2022961136 creator A5078175172 @default.
• W2022961136 creator A5081903232 @default.
• W2022961136 creator A5090533318 @default.
• W2022961136 date "2009-08-04" @default.
• W2022961136 modified "2023-10-16" @default.
• W2022961136 title "Clathrin-Mediated Endocytosis of Quantum Dot−Peptide Conjugates in Living Cells" @default.
• W2022961136 cites W1972605174 @default.
• W2022961136 cites W1973590977 @default.
• W2022961136 cites W1974670254 @default.
• W2022961136 cites W1975638732 @default.
• W2022961136 cites W1978135232 @default.
• W2022961136 cites W1979260070 @default.
• W2022961136 cites W1979718354 @default.
• W2022961136 cites W1979919427 @default.
• W2022961136 cites W1984536659 @default.
• W2022961136 cites W1987787381 @default.
• W2022961136 cites W1987924718 @default.
• W2022961136 cites W1987975569 @default.
• W2022961136 cites W1991354544 @default.
• W2022961136 cites W1991837059 @default.
• W2022961136 cites W1994121958 @default.
• W2022961136 cites W1995555037 @default.
• W2022961136 cites W1998983638 @default.
• W2022961136 cites W2003258014 @default.
• W2022961136 cites W2006964253 @default.
• W2022961136 cites W2007024648 @default.
• W2022961136 cites W2010216487 @default.
• W2022961136 cites W2013557720 @default.
• W2022961136 cites W2015182838 @default.
• W2022961136 cites W2015622350 @default.
• W2022961136 cites W2015730635 @default.
• W2022961136 cites W2017069758 @default.
• W2022961136 cites W2021921508 @default.
• W2022961136 cites W2027175712 @default.
• W2022961136 cites W2028567429 @default.
• W2022961136 cites W2029130502 @default.
• W2022961136 cites W2037305018 @default.
• W2022961136 cites W2042143995 @default.
• W2022961136 cites W2043167746 @default.
• W2022961136 cites W2043453847 @default.
• W2022961136 cites W2046125114 @default.
• W2022961136 cites W2046968083 @default.
• W2022961136 cites W2047811610 @default.
• W2022961136 cites W2048053977 @default.
• W2022961136 cites W2049543990 @default.
• W2022961136 cites W2052762207 @default.
• W2022961136 cites W2054558294 @default.
• W2022961136 cites W2055048871 @default.
• W2022961136 cites W2055293617 @default.
• W2022961136 cites W2062485439 @default.
• W2022961136 cites W2062738447 @default.
• W2022961136 cites W2063575064 @default.
• W2022961136 cites W2063854773 @default.
• W2022961136 cites W2064548903 @default.
• W2022961136 cites W2064918500 @default.
• W2022961136 cites W2065858471 @default.
• W2022961136 cites W2067944387 @default.
• W2022961136 cites W2068608756 @default.
• W2022961136 cites W2069949257 @default.
• W2022961136 cites W2070554638 @default.
• W2022961136 cites W2073241541 @default.
• W2022961136 cites W2074571771 @default.
• W2022961136 cites W2078733693 @default.
• W2022961136 cites W2088713107 @default.
• W2022961136 cites W2094437628 @default.
• W2022961136 cites W2102884718 @default.
• W2022961136 cites W2108524724 @default.
• W2022961136 cites W2118685639 @default.
• W2022961136 cites W2123650819 @default.
• W2022961136 cites W2127457668 @default.
• W2022961136 cites W2139980848 @default.
• W2022961136 cites W2144175668 @default.
• W2022961136 cites W2144196643 @default.
• W2022961136 cites W2148357165 @default.
• W2022961136 cites W2148924929 @default.
• W2022961136 cites W2153878662 @default.
• W2022961136 cites W2154321074 @default.
• W2022961136 cites W2160401113 @default.
• W2022961136 cites W2170932434 @default.
• W2022961136 cites W4254040305 @default.
• W2022961136 doi "https://doi.org/10.1021/nn900663r" @default.
• W2022961136 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/19653641" @default.
• W2022961136 hasPublicationYear "2009" @default.
• W2022961136 type Work @default.
• W2022961136 sameAs 2022961136 @default.
• W2022961136 citedByCount "92" @default.
• W2022961136 countsByYear W20229611362012 @default.
• W2022961136 countsByYear W20229611362013 @default.
• W2022961136 countsByYear W20229611362014 @default.
• W2022961136 countsByYear W20229611362015 @default.
• W2022961136 countsByYear W20229611362016 @default.
• W2022961136 countsByYear W20229611362017 @default.

• next