Establishment of a functional cell line expressing both subunits of H1a and H2c of human hepatocyte surface molecule ASGPR

Bin Hu , Yan Yang , Jia Liu , Zhiyong Ma , Hongping Huang , Shenpei Liu , Yuan Yu , Youhua Hao , Baoju Wang , Mengji Lu , Dongliang YANG

Current Medical Science ›› 2010, Vol. 30 ›› Issue (5) : 556 -561.

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Current Medical Science ›› 2010, Vol. 30 ›› Issue (5) : 556 -561. DOI: 10.1007/s11596-010-0542-1
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Establishment of a functional cell line expressing both subunits of H1a and H2c of human hepatocyte surface molecule ASGPR

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Abstract

To better understand the effect of a new split variant of human asialoglycoprotein receptor (ASGPR H1b) on ASGPR ligands’ binding ability, we established a functional cell line which expresses ASGPR. The full lengths of ASGPRH1a and H2c fragments from human liver were amplified by reverse transcript PCR (RT-PCR) and inserted into eukaryotic expression vector pIRES2EGFP, pCDNA3.1 (Zeo+) respectively. The recombinants were co-transfected into HeLa cells. After selection by using Neocin and Zeocin, a stably transfected cell line was established, which was designated 4-1-6. The transcription and expression of ASGPRH1a and H2c in 4-1-6 were confirmed by RT-PCR, Western blotting and immunofluorescence. The endocytosis function of the artificial “ASGPR” on the surface of 4-1-6 was tested by FACS. It was found that the cell line 4-1-6 could bind ASGPR natural ligand molecular asialo-orosomucoid (ASOR). After the eukaryotic plasmid H1b/pCDNA3.1 (neo) was transfected into cell line 4-1-6, H1b did not down-regulate the ligand binding ability of ASGPR. The eukaryotic expression plasmid H1b/pcDNA3.1 (neo) and H2c/pcDNA3.1 (neo) were co-transfected transiently into Hela cell. Neither single H1b nor H1b and H2c could bind ASOR. In conclusion, a functional cell line of human asialoglycoprotein receptor (ASGPR) which expresses both H1a and H2c stably was established. The new split variant H1b has no effect on ASGPR binding to ASOR. ASGPRH1b alone can’t bind to ASOR, it yet can’t form functional complex with ASGPRH2c.

Keywords

ASGPR / eukaryotic expression vector / function cell line / split variant

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Bin Hu, Yan Yang, Jia Liu, Zhiyong Ma, Hongping Huang, Shenpei Liu, Yuan Yu, Youhua Hao, Baoju Wang, Mengji Lu, Dongliang YANG. Establishment of a functional cell line expressing both subunits of H1a and H2c of human hepatocyte surface molecule ASGPR. Current Medical Science, 2010, 30(5): 556-561 DOI:10.1007/s11596-010-0542-1

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References

Publishing order | Descend order by publishing year | Descend order by cited within
[1]

StockertR.J.. The asialoglycoprotein receptors: relationships between structure, function, and expression. Physiol Rev, 1995, 75(3): 591-609
[2]

SmithR.M., WuG.Y.. Hepatocyte-directed gene delivery by receptor-mediated endocytosis. Semin Liver Dis, 1999, 19(1): 83-92

[3]

WuG.Y., WuC.H.. Delivery systerms for gene therapy. Biotherapy, 1991, 3(1): 87-95

[4]

TrereD., FiumeL., DegorgiL.B., et al.. The asialoglycoprotein receptor in human hepatocellular carcinomas: Its expression on proliferating cells. Br J Cancer, 1999, 81(3): 404-408

[5]

SpiessM., LodishH. F.. Sequence of a second human asialoglycoprotein receptor: Conservation of two receptor genes during evolution. Proc Natl Acad Sci, 1985, 82(19): 6465-6469

[6]

PaiettaE., StockertR.J., RacevskisJ.. Differences in the abundance of variably spliced transcripts for the second asialoglycoprotein receptor polypeptide, H2, in normal and transformed human liver. Hepatology, 1992, 15(3): 395-402

[7]

LiuJ., DingH.H., YangY., et al.. Preparation and identification of polyclonal antibody against protein H1 b: The variant of major subunit of human ASGPR. Chin J Cell Mol Immunol (Chinese), 2009, 25(10): 917-919
[8]

TyckoB., KeithC.H., MaxfieldF.R., et al.. Rapid acidification of endocytic vesicles containing asialoglycoprotein in cells of a human hepatoma line. J Cell Biol, 1983, 97(6): 1762-1776

[9]

PengD.J., SunJ., WangY.Z., et al.. Inhibition of hepatocarcinoma by systemic delivery of Apoptin gene via the hepatic asialoglycoprotein receptor. Cancer Gene Ther, 2007, 14(1): 66-73

[10]

BiderM.D., CescatoR., JenöP., et al.. High-affinity ligand binding to subunit H1 of the asialoglycoprotein receptor in the absence of subunit H2. Eur J Biochem, 1995, 230(1): 207-212

[11]

ChiacchiakB., DrickamerK.. Direct evidence for the transmembrane orientation of the hepatic glycoprotein receptors. J Biol Chem, 1984, 259(24): 15440-15446
[12]

FuhrerC., GeffenI., HuggelK., et al.. The two subunits of the asialoglycoprotein receptor contain different sorting information. J Biol Chem, 1994, 269(5): 3277-3282
[13]

MeierM., BiderM.D., MalashkevichV.N., et al.. Crystal structure of the carbohydrate recognition domain of the H1 subunit of the asialoglycoprotein receptor. J Mol Biol, 2000, 300(4): 857-865

[14]

WeigelP.H.. Galactosyl and N-acetylgalactosaminyl homeostasis: a function for mammalian asialoglycoprotein receptors. BioEssays, 1994, 16(7): 519-524

[15]

WeigelP.H., YikJ.H.. Glycans as endocytosis signals: the cases of the asialoglycoprotein and hyaluronan/chondroitin sulfate receptors. Biochem Biophys Acta, 2002, 1572(2–3): 341-363
[16]

YikJ.H., SaxenaA., WeigelP.H.. The minor subunit splice variants, H2b and H2c, of the human asialoglycoprotein receptor are present with the major subunit H1 in different hetero-ligomeric receptor complexes. J Biol Chem, 2002, 277(25): 23076-23083

[17]

SaxenaA., YikJ.H.. Weigel PH. H2, the minor subunit of the human asialoglycoprotein receptor, trafficks intracellularly and forms homo-oligomers, but does not bind asialo-orosomucoid. J Biol Chem, 2002, 277(38): 35297-35304

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