Contribution of the 37-kDa laminin receptor precursor in the anti-metastatic PSP94-derived peptide PCK3145 cell surface binding
详细信息 查看全文
- 作者:Borhane Annabi ; Jean-Christophe Currie ; Mounia Bouzeghrane ; Hé ; lè ; ne Dulude ; Luc Daigneault ; Seema Garde ; Shafaat A. Rabbani ; Chandra Panchal ; Jinzi J. Wu and Richard Bé ; liveau
- 刊名:Biochemical and Biophysical Research Communications
- 出版年:2006
- 出版时间:21 July 2006
- 年:2006
- 卷:346
- 期:1
- 页码:358-366
- 全文大小:444 K
文摘
PurposePCK3145 is an anti-metastatic synthetic peptide with promising therapeutic efficacy against hormone-refractory prostate cancer. The characterization of the PCK3145 peptide cell surface binding/internalization mechanisms and of the receptors involved remained to be explored.Results
[14C]PCK3145 cell surface binding assays showed rapid and transient kinetic profile, that was inhibited by RGD peptides, laminin, hyaluronan, and type-I collagen. RGD peptides were however unable to inhibit PCK3145 intracellular uptake. Far-Western ligand binding studies enabled the identification of the 37-kDa laminin receptor precursor (37LRP) as a potential ligand for PCK3145. Overexpression of the recombinant 37LRP indeed led to an increase in PCK3145 binding but unexpectedly not to its uptake.
Conclusions
Our data support the implication of laminin receptors in cell surface binding and in transducing PCK3145 anti-metastatic effects, and provide a rational for targeting cancers that express high levels of such laminin receptors.