Delivering aminopyridine ligands into cancer cells through conjugation to the cell-penetrating peptide BP16. Issue 17 (8th April 2016)
- Record Type:
- Journal Article
- Title:
- Delivering aminopyridine ligands into cancer cells through conjugation to the cell-penetrating peptide BP16. Issue 17 (8th April 2016)
- Main Title:
- Delivering aminopyridine ligands into cancer cells through conjugation to the cell-penetrating peptide BP16
- Authors:
- Soler, M.
González-Bártulos, M.
Figueras, E.
Massaguer, A.
Feliu, L.
Planas, M.
Ribas, X.
Costas, M. - Abstract:
- Abstract : Peptide conjugates incorporating a red-ox active aminopyridine ligand bound to the cell-penetrating peptideBP16 display high cytotoxicity. Abstract : Peptide conjugates incorporating the N-based ligands Me2 PyTACN or ( S, S ′)-BPBP at the N- or the C-terminus of the cell-penetrating peptideBP16 were synthesized (PyTACN–BP16 (BP341 ), BP16-PyTACN (BP342 ), BPBP–BP16 (BP343 ), and BP16-BPBP (BP344 )). Metal binding peptides bearing at the N-terminus the ligand, an additional Lys and a β-Ala were also prepared (PyTACN-βAK–BP16 (BP345 ) and BPBP-βAK–BP16 (BP346 )). Moreover, taking into account the clathrin-dependent endocytic mechanism ofBP16, the enzymatic cleavable tetrapeptide Gly-Phe-Leu-Gly was incorporated between the ligand and the N- or C-terminus ofBP16 (BPBP-GFLG-BP16 (BP347 ) and BP16-GLFG-BPBP (BP348 )). Analysis of the cytotoxicity of all the peptide conjugates showed that: (i) the position of the ligand influenced the IC50 values, (ii) the incorporation of the βAla-Lys dipeptide rendered non active sequences, (iii) peptide conjugates derived from the ( S, S ′)-BPBP ligand were more active than those bearing Me2 PyTACN, and (iv) the introduction of the cleavable tetrapeptide significantly enhanced the activity of the BPBP conjugates (IC50 of 4.3 to 11.7 μM (BP347 andBP348 ) compared to 26.0 to >50 μM (BP343, BP344 andBP346 )). The most active peptide was BPBP-GFLG-BP16 (BP347 ) (IC50 of 4.3 to 5.0 μM). This high activity was attributed to its highAbstract : Peptide conjugates incorporating a red-ox active aminopyridine ligand bound to the cell-penetrating peptideBP16 display high cytotoxicity. Abstract : Peptide conjugates incorporating the N-based ligands Me2 PyTACN or ( S, S ′)-BPBP at the N- or the C-terminus of the cell-penetrating peptideBP16 were synthesized (PyTACN–BP16 (BP341 ), BP16-PyTACN (BP342 ), BPBP–BP16 (BP343 ), and BP16-BPBP (BP344 )). Metal binding peptides bearing at the N-terminus the ligand, an additional Lys and a β-Ala were also prepared (PyTACN-βAK–BP16 (BP345 ) and BPBP-βAK–BP16 (BP346 )). Moreover, taking into account the clathrin-dependent endocytic mechanism ofBP16, the enzymatic cleavable tetrapeptide Gly-Phe-Leu-Gly was incorporated between the ligand and the N- or C-terminus ofBP16 (BPBP-GFLG-BP16 (BP347 ) and BP16-GLFG-BPBP (BP348 )). Analysis of the cytotoxicity of all the peptide conjugates showed that: (i) the position of the ligand influenced the IC50 values, (ii) the incorporation of the βAla-Lys dipeptide rendered non active sequences, (iii) peptide conjugates derived from the ( S, S ′)-BPBP ligand were more active than those bearing Me2 PyTACN, and (iv) the introduction of the cleavable tetrapeptide significantly enhanced the activity of the BPBP conjugates (IC50 of 4.3 to 11.7 μM (BP347 andBP348 ) compared to 26.0 to >50 μM (BP343, BP344 andBP346 )). The most active peptide was BPBP-GFLG-BP16 (BP347 ) (IC50 of 4.3 to 5.0 μM). This high activity was attributed to its high internalization in MCF-7 cells, as shown by flow cytometry, and to the subsequent release of the ligand by the intracellular cleavage of the enzyme-labile spacer, as observed in cathepsin B enzymatic assays. Therefore, these results pave the way for the design of novel peptide conjugates to be used in pro-oxidant anticancer therapies. … (more)
- Is Part Of:
- Organic & biomolecular chemistry. Volume 14:Issue 17(2016)
- Journal:
- Organic & biomolecular chemistry
- Issue:
- Volume 14:Issue 17(2016)
- Issue Display:
- Volume 14, Issue 17 (2016)
- Year:
- 2016
- Volume:
- 14
- Issue:
- 17
- Issue Sort Value:
- 2016-0014-0017-0000
- Page Start:
- 4061
- Page End:
- 4070
- Publication Date:
- 2016-04-08
- Subjects:
- Chemistry, Organic -- Periodicals
Bioorganic chemistry -- Periodicals
Chemistry, Physical organic -- Periodicals
547 - Journal URLs:
- http://pubs.rsc.org/en/journals/journalissues/ob#!recentarticles&all ↗
http://www.rsc.org/ ↗ - DOI:
- 10.1039/c6ob00470a ↗
- Languages:
- English
- ISSNs:
- 1477-0520
- Deposit Type:
- Legaldeposit
- View Content:
- Available online (eLD content is only available in our Reading Rooms) ↗
- Physical Locations:
- British Library DSC - 6286.350000
British Library DSC - BLDSS-3PM
British Library STI - ELD Digital store - Ingest File:
- 36.xml