Efficient Liver Targeting by Polyvalent Display of a Compact Ligand for the Asialoglycoprotein Receptor

被引:79
|
作者
Sanhueza, Carlos A. [1 ,2 ,3 ]
Baksh, Michael M. [1 ,2 ,3 ]
Thuma, Benjamin [4 ]
Roy, Marc D. [5 ]
Dutta, Sanjay [2 ,3 ]
Preville, Cathy [4 ]
Chrunyk, Boris A. [4 ]
Beaumont, Kevin [6 ]
Dullea, Robert [7 ]
Ammirati, Mark [4 ]
Liu, Shenping [4 ]
Gebhard, David [4 ]
Finley, James E. [5 ]
Salatto, Christopher T. [7 ]
King-Ahmad, Amanda [4 ]
Stock, Ingrid [4 ]
Atkinson, Karen [4 ]
Reidich, Benjamin [7 ]
Lin, Wen [4 ]
Kumar, Rajesh [8 ]
Tu, Meihua [6 ]
Menhaji-Klotz, Elnaz [6 ]
Price, David A. [6 ]
Liras, Spiros [6 ]
Finn, M. G. [1 ,2 ,3 ]
Mascitti, Vincent [4 ]
机构
[1] Georgia Inst Technol, Sch Chem & Biochem, 901 Atlantic Ave, Atlanta, GA 30332 USA
[2] Scripps Res Inst, Dept Chem, 10550 N Torrey Pines Rd, La Jolla, CA 92037 USA
[3] Scripps Res Inst, Skaggs Inst Chem Biol, 10550 N Torrey Pines Rd, La Jolla, CA 92037 USA
[4] Pfizer Med Design, Eastern Point Rd, Groton, CT 06340 USA
[5] Pfizer Drug Safety R&D, Eastern Point Rd, Groton, CT 06340 USA
[6] Pfizer Med Design, Main St, Cambridge, MA 02139 USA
[7] Pfizer CVMET Biol, Main St, Cambridge, MA 02139 USA
[8] Pfizer Med Sci, Eastern Point Rd, Groton, CT 06340 USA
关键词
CARBOHYDRATE-RECOGNITION DOMAIN; N-ACETYLGALACTOSAMINE BINDING; SILENCING IN-VIVO; CELL INTERNALIZATION; MAXIMAL AFFINITY; GALACTOSE; HEPATOCYTES; DELIVERY; GLYCOPROTEINS; DISCOVERY;
D O I
10.1021/jacs.6b12964
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
A compact and stable bicyclic bridged ketal was developed as a ligand for the asialoglycoprotein receptor (ASGPR). This compound showed excellent ligand efficiency, and the molecular details of binding were revealed by the first Xray crystal structures of ligand-bound ASGPR This analogue was used to make potent di- and trivalent binders of ASGPR. Extensive characterization of the function of these compounds showed rapid ASGPR-dependent cellular uptake in vitro and high levels of liver/plasma selectivity in vivo. Assessment of the biodistribution in rodents of a prototypical Alexa647-labeled trivalent conjugate showed selective hepatocyte targeting with no detectable distribution in nonparenchymal cells. This molecule also exhibited increased ASGPR-directed hepatocellular uptake and prolonged retention compared to a similar Ga1NAc derived trimer conjugate. Selective release in the liver of a passively permeable small-molecule cargo was achieved by retro-Diels Alder cleavage of an oxanorbornadiene linkage, presumably upon encountering intracellular thiol. Therefore, the multicomponent construct described here represents a highly efficient delivery vehicle to hepatocytes.
引用
收藏
页码:3528 / 3536
页数:9
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