Topics
lipidBand
endothelialAnatomical structure
phosphatidylserineChemical substance
endotheliumAnatomical structure
hepatic sinusoidAnatomical structure
Liposomes of 400 nm in diameter can cross the 100-nm fenestrations in the endothelium of the hepatic sinusoid, provided they contain phosphatidylserine (PS) but not phosphatidylglycerol CPG) [Daemen et al. (1997) Hepatology 26, 416]. We present evidence indicating that (i) the PS effect does not involve a pharmacological action of this lipid on the size of the fenestrations, (ii) fluid-type but not solid-type PS liposomes have access to the hepatocytes and (iii) the lack of uptake of PG liposomes by hepatocytes is not due to a lack of affinity of the hepatocytes for PG surfaces. We conclude that the mechanism responsible for the uptake of large PS-containing liposomes by hepatocytes in vivo involves a mechanical deformation of these liposom...
Human serum albumin (HSA) derivatized with cis-aconitic anhydride was covalently coupled to liposome...
The authors's recent work on matters pertinent io the in vivo processing of systemically administere...
AbstractThe rate of liposome clearance from blood by the reticuloendothelial system (RES), primarily...
Liposomes of 400 nm in diameter can cross the 100-nm fenestrations in the endothelium of the hepatic...
AbstractLiposomes of 400 nm in diameter can cross the 100-nm fenestrations in the endothelium of the...
The architecture of the liver constitutes a favorable condition for cell-specific delivery of drugs ...
The interaction with liver cells of liposomes containing different mol fractions of phosphatidylseri...
The interaction with liver cells of liposomes containing different mol fractions of phosphatidylseri...
In this chapter we summarize literature and describe in more detail our own observations over a peri...
In this contribution we summarize our observations over a period of nearly two decennia on the role ...
Liposomes with diameters of 200 to 400 nm containing phosphatidylserine (PS) or phosphatidylglycerol...
We studied the kinetics of hepatic uptake of liposomes during serum-free recirculating perfusion of ...
AbstractWe studied the kinetics of hepatic uptake of liposomes during serum-free recirculating perfu...
Human serum albumin (HSA) derivatized with cis-aconitic anhydride was covalently coupled to liposome...
The authors's recent work on matters pertinent io the in vivo processing of systemically administere...
AbstractThe rate of liposome clearance from blood by the reticuloendothelial system (RES), primarily...
Liposomes of 400 nm in diameter can cross the 100-nm fenestrations in the endothelium of the hepatic...
AbstractLiposomes of 400 nm in diameter can cross the 100-nm fenestrations in the endothelium of the...
The architecture of the liver constitutes a favorable condition for cell-specific delivery of drugs ...
The interaction with liver cells of liposomes containing different mol fractions of phosphatidylseri...
The interaction with liver cells of liposomes containing different mol fractions of phosphatidylseri...
In this chapter we summarize literature and describe in more detail our own observations over a peri...
In this contribution we summarize our observations over a period of nearly two decennia on the role ...
Liposomes with diameters of 200 to 400 nm containing phosphatidylserine (PS) or phosphatidylglycerol...
We studied the kinetics of hepatic uptake of liposomes during serum-free recirculating perfusion of ...
AbstractWe studied the kinetics of hepatic uptake of liposomes during serum-free recirculating perfu...
Human serum albumin (HSA) derivatized with cis-aconitic anhydride was covalently coupled to liposome...
The authors's recent work on matters pertinent io the in vivo processing of systemically administere...
AbstractThe rate of liposome clearance from blood by the reticuloendothelial system (RES), primarily...
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