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Coupling of Metal Containing Homing Devices to Liposomes via a Maleimide Linker: Use of TCEP to Stabilize Thiol-groups without Scavenging Metals
Authors:Corine C. Visser  L. Heleen Voorwinden  Liesbeth R. Harders  Mohamed Eloualid  Louis van Bloois  Daan J.A. Crommelin
Affiliation:1. Leiden/Amsterdam Center for Drug Research (LACDR),Division of Pharmacology, Leiden University, P.O. Box, RA 2300, Leiden, The Netherlands;2. Department of Pharmaceutics, Utrecht Institute for Pharmaceutical Sciences (UIPS), P.O. Box, TB 3508, Utrecht, The Netherlands
Abstract:Liposomes for drug delivery are often prepared with maleimide groups on the distal end of PEG to enable coupling of homing devices, such as antibodies, or other proteins. EDTA is used to stabilize the thiol group in the homing device for attachment to the maleimide. However, when using a homing device that contains a metal, EDTA inactivates this by scavenging of the metal. Holo-transferrin (Tf) containing two iron atoms (Fe3+), has a much higher affinity for the Tf receptor than apo-Tf (which does not contain any Fe3+). To couple Tf to a liposome, the introduction of a thiol group is necessary. During this process, by using N-succinimidyl S-acetylthioacetate (SATA), followed by 2–3 h coupling to the liposomes, Fe3+ is scavenged by EDTA. This causes a decreased affinity of Tf for its receptor, resulting in a decreased targeting efficiency of the liposomes.

Tris(2-carboxyethyl)phosphine (TCEP) hydrochloride is a sulfhydryl reductant that is often used in protein biochemistry. We found that TCEP (0.01 mM) does not scavenge Fe3+ from Tf and is able to protect thiol groups for the coupling to maleimide. Furthermore, TCEP does not interfere with the maleimide coupling itself.

In this communication, we describe the preparation of liposomes, focussing on the coupling of Tf to the maleimide linker at the distal end of PEG, without loosing Fe3+ from Tf. This method can be applied to other metal-containing homing devices as well.
Keywords:Transferrin  Liposomes  Drug targeting  Drug delivery  DTT, dithiothreitol  EPC-35, egg phosphatidyl choline  HBS, Hepes buffered saline  PEG, Polyethylene glycol (MW 2000)  p.i., polydispersity index  SATA, N-succinimidyl S-acetylthioacetate  TCEP, Tris(2-carboxyethyl)phosphine hydrochloride  Tf, transferrin  TfR, transferrin receptor
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