Enhancing the Efficiency of the Solid Phase Peptide Synthesis (SPPS) Process by High Shear Mixing
I. Alshanski, M. Bentolila, A. Gitlin-Domagalska, D. Zamir, S. Zorsky, S. Joubran, M. Hurevich, and C. Gilon. 2018. “Enhancing the Efficiency of the Solid Phase Peptide Synthesis (SPPS) Process by High Shear Mixing.” Organic Process Research & Development, 22, 9, Pp. 1318-1322. Publisher's Version Abstract

The brittle nature of the polymer beads used in SPPS dictates mild mixing techniques with low mass transfer. We demonstrate that vigorous overhead mechanical stirring with superior mass transfer properties kept the beads intact and significantly accelerates reaction kinetics and efficiency.


pH Controlled Impedimetric Sensing of Copper(II) Ion Using Oxytocin as Recognition Element
Kiran Kumar Tadi, Israel Alshanski, Mattan Hurevich, and Shlomo Yitzchaik. 2018. “pH Controlled Impedimetric Sensing of Copper(II) Ion Using Oxytocin as Recognition Element.” Surfaces, 1, 1, Pp. 8. Abstract

We report the modulation of the specific metal gation properties of a peptide and demonstrate a highly selective sensor for copper(II) ion. The neuropeptide oxytocin (OT) is reported for its high affinity towards Zn2+ and Cu2+ at physiological pH. The binding of the metal ions to OT is tuned by altering the pH of the medium. OT was self-assembled on glassy carbon electrode using surface chemistry, and electrochemical impedance spectroscopy (EIS) was used to probe the binding of Cu2+. Our results clearly indicate that at pH 10.0, the binding of Cu2+ to OT is increased compared to that at pH 7.0, while the binding to Zn2+ becomes almost negligible. This proves that the selectivity of OT towards each of the ions can be regulated simply by controlling the pH of the medium and hence allows the preparation of a sensing device with selectivity to Cu2+

surfaces 2018 TOC

Photodeprotection of up to Eight Photolabile Protecting Groups from a Single Glycan
Mamidi Samarasimhareddy, Israel Alshanski, Evgeniy Mervinetsky, and Mattan Hurevich. 2018. “Photodeprotection of up to Eight Photolabile Protecting Groups from a Single Glycan.” Synlett, 29, EFirst, Pp. A-E. Abstract

Permanent protecting groups are essential for oligosaccharide synthesis. However, the removal of the traditionally used protecting groups is not trivial and demands considerable expertise. Using photolabile protecting groups as permanent protection for glycan can
overcome many limitations associated with the traditional oligosaccharide synthesis approach. It is demonstrated here that up to eight photolabile protecting groups can be readily removed from a single glycan using a benchtop LED setup that is very easy to operate. This report suggests that further development of the strategy will offer an attractive
alternative for oligosaccharide synthesis.

Synlett 2019 TOC

Automated glycan assembly using the Glyconeer 2.1 synthesizer
H. S. Hahm, M. K. Schlegel, M. Hurevich, S. Eller, F. Schuhmacher, J. Hofmann, K. Pagel, and P. H. Seeberger. 2017. “Automated glycan assembly using the Glyconeer 2.1 synthesizer.” Proceedings of the National Academy of Sciences of the United States of America, 114, 17, Pp. E3385-E3389. Abstract

Reliable and rapid access to defined biopolymers by automated DNA and peptide synthesis has fundamentally altered biological research and medical practice. Similarly, the procurement of defined glycans is key to establishing structure–activity relationships and thereby progress in the glycosciences. Here, we describe the rapid assembly of oligosaccharides using the commercially available Glyconeer 2.1 automated glycan synthesizer, monosaccharide building blocks, and a linker-functionalized polystyrene solid support. Purification and quality-control protocols for the oligosaccharide products have been standardized. Synthetic glycans prepared in this way are useful reagents as the basis for glycan arrays, diagnostics, and carbohydrate-based vaccines.


Copper Induced Conformational Changes of Tripeptide Monolayer Based Impedimetric Biosensor
E. Mervinetsky, I. Alshanski, Y. Hamo, L. M. Sandonas, A. Dianat, J. Buchwald, R. Gutierrez, G. Cuniberti, M. Hurevich, and S. Yitzchaik. 2017. “Copper Induced Conformational Changes of Tripeptide Monolayer Based Impedimetric Biosensor.” Scientific Reports, 7. Abstract

Copper ions play a major role in biological processes. Abnormal Cu2+ ions concentrations are associated with various diseases, hence, can be used as diagnostic target. Monitoring copper ion is currently performed by non-portable, expensive and complicated to use equipment. We present a label free and a highly sensitive electrochemical ion-detecting biosensor based on a Gly-Gly-His tripeptide layer that chelate with Cu2+ ions. The proposed sensing mechanism is that the chelation results in conformational changes in the peptide that forms a denser insulating layer that prevents RedOx species transfer to the surface. This chelation event was monitored using various electrochemical methods and surface chemistry analysis and supported by theoretical calculations. We propose a highly sensitive ion-detection biosensor that can detect Cu2+ ions in the pM range with high SNR parameter.

GGH Sci Rep 2018 TOC

DMAP-assisted sulfonylation as an efficient step for the methylation of primary amine motifs on solid support
J. N. Naoum, K. Chandra, D. Shemesh, R. B. Gerber, C. Gilon, and M. Hurevich. 2017. “DMAP-assisted sulfonylation as an efficient step for the methylation of primary amine motifs on solid support.” Beilstein Journal of Organic Chemistry, 13, Pp. 806-816. Abstract

Several multistep strategies were developed to ensure single methylation of amines on solid support. These strategies rely on the introduction of the o-NBS protecting/activating group as a key step. We found that the state-of-the-art strategies fail for the methylation of several primary amine motifs, largely due to inefficient sulfonylation. Here we show that using the superior nucleophilic base DMAP instead of the commonly used base collidine as a sulfonylation additive is essential for the introduction of the o-NBS group to these amine motifs. DFT calculations provide an explanation by showing that the energy barrier of the DMAP intermediate is significantly lower than the one of the collidine. We demonstrate that using DMAP as a sole additive in the sulfonylation step results in an overall effective and regioselective N-methylation. The method presented herein proved highly efficient in solid-phase synthesis of a somatostatin analogue bearing three N α-methylation sites that could not be synthesized using the previously described state-of-the-art methods.



Oxytocin-Monolayer-Based Impedimetric Biosensor for Zinc and Copper Ions
Kiran Kumar Tadi, Israel Alshanski, Evgeniy Mervinetsky, Gerard Marx, Panayiota Petrou, Karussis M. Dimitrios, Chaim Gilon, Mattan Hurevich, and Shlomo Yitzchaik. 2017. “Oxytocin-Monolayer-Based Impedimetric Biosensor for Zinc and Copper Ions.” ACS Omega, 2, 12, Pp. 8770-8778. Abstract

Zinc and copper are essential metal ions for numerous biological processes. Their levels are tightly maintained in all body organs. Impairment of the Zn2+ to Cu2+ ratio in serum was found to correlate with many disease states, including immunological and inflammatory disorders. Oxytocin (OT) is a neuropeptide, and its activity is modulated by zinc and copper ion binding. Harnessing the intrinsic properties of OT is one of the attractive ways to develop valuable metal ion sensors. Here, we report for the first time an OT-based metal ion sensor prepared by immobilizing the neuropeptide onto a glassy carbon electrode. The developed impedimetric biosensor was ultrasensitive to Zn2+ and Cu2+ ions at physiological pH and not to other biologically relevant ions. Interestingly, the electrochemical impedance signal of two hemicircle systems was recorded after the attachment of OT to the surface. These two semicircles suggest two capacitive regions that result from two different domains in the OT monolayer. Moreover, the change in the charge-transfer resistance of either Zn2+ or Cu2+ was not similar in response to binding. This suggests that the metal-dependent conformational changes of OT can be translated to distinct impedimetric data. Selective masking of Zn2+ and Cu2+ was used to allow for the simultaneous determination of zinc to copper ions ratio by the OT sensor. The OT sensor was able to distinguish between healthy control and multiple sclerosis patients diluted sera samples by determining the Zn/Cu ratio similar to the state-of-the-art techniques. The OT sensor presented herein is likely to have numerous applications in biomedical research and pave the way to other types of neuropeptide-derived sensors.

OT Omega 2017 TOC

M. W. Weishaupt, S. Matthies, M. Hurevich, C. L. Pereira, H. S. Hahm, and P. H. Seeberger. 2016. “Automated glycan assembly of a S-pneumoniae serotype 3 CPS antigen.” Beilstein Journal of Organic Chemistry, 12, Pp. 1440-1446. Publisher's Version
K. Chandra, P. Das, S. Mamidi, M. Hurevich, A. Iosub-Amir, N. Metanis, M. Reches, and A. Friedler. 2016. “Covalent Inhibition of HIV-1 Integrase by N-Succinimidyl Peptides.” Chemmedchem, 11, 18, Pp. 1987-1994. Publisher's Version
Automated assembly of oligosaccharides containing multiple cis-glycosidic linkages
H. S. Hahm, M. Hurevich, and P. H. Seeberger. 2016. “Automated assembly of oligosaccharides containing multiple cis-glycosidic linkages.” Nature Communications, 7. Abstract

Automated glycan assembly (AGA) has advanced from a concept to a commercial technology that rapidly provides access to diverse oligosaccharide chains as long as 30-mers. To date, AGA was mainly employed to incorporate trans-glycosidic linkages, where C2 participating protecting groups ensure stereoselective couplings. Stereocontrol during the installation of cis-glycosidic linkages cannot rely on C2-participation and anomeric mixtures are typically formed. Here, we demonstrate that oligosaccharides containing multiple cis-glycosidic linkages can be prepared efficiently by AGA using monosaccharide building blocks equipped with remote participating protecting groups. The concept is illustrated by the automated syntheses of biologically relevant oligosaccharides bearing various cis-galactosidic and cis-glucosidic linkages. This work provides further proof that AGA facilitates the synthesis of complex oligosaccharides with multiple cis-linkages and other biologically important oligosaccharides.

Nat Comm 2016 TOC

J. Fanous, A. Swed, S. Joubran, M. Hurevich, E. Britan-Rosich, M. Kotler, C. Gilon, and A. Hoffman. 2015. “Superiority of the S,S conformation in diverse pharmacological processes: Intestinal transport and entry inhibition activity of novel anti-HIV drug lead.” International Journal of Pharmaceutics, 495, 2, Pp. 660-663. Publisher's Version
M. Hurevich, A. Talhami, D. E. Shalev, and C. Gilon. 2014. “Allosteric Inhibition of G-Protein Coupled Receptor Oligomerization: Strategies and Challenges for Drug Development.” Current Topics in Medicinal Chemistry, 14, 15, Pp. 1842-1863. Publisher's Version
M. Hurevich and P. H. Seeberger. 2014. “Automated glycopeptide assembly by combined solid-phase peptide and oligosaccharide synthesis.” Chemical Communications, 50, 15, Pp. 1851-1853. Publisher's Version
M. Hurevich, J. Kandasamy, B. M. Ponnappa, M. Collot, D. Kopetzki, D. T. McQuade, and P. H. Seeberger. 2014. “Continuous Photochemical Cleavage of Linkers for Solid-Phase Synthesis.” Organic Letters, 16, 6, Pp. 1794-1797. Publisher's Version
J. Kandasamy, M. Hurevich, and P. H. Seeberger. 2013. “Automated solid phase synthesis of oligoarabinofuranosides.” Chemical Communications, 49, 40, Pp. 4453-4455. Publisher's Version
M. Hurevich, M. Ratner-Hurevich, Y. Tal-Gan, D. E. Shalev, S. Z. Ben-Sasson, and C. Gilon. 2013. “Backbone cyclic helix mimetic of chemokine (C-C motif) receptor 2: A rational approach for inhibiting dimerization of G protein-coupled receptors.” Bioorganic & Medicinal Chemistry, 21, 13, Pp. 3958-3966. Publisher's Version
D. Esposito, M. Hurevich, B. Castagner, C. C. Wang, and P. H. Seeberger. 2012. “Automated synthesis of sialylated oligosaccharides.” Beilstein Journal of Organic Chemistry, 8, Pp. 1601-1609. Publisher's Version
C. Gilon, M. Ratner-Hurevich, Y. Tal-Gan, D. E. Shalev, S. Z. Ben-Sasson, and M. Hurevich. 2012. “Backbone Cyclic Helix Mimetic of Chemokine (C-C Motif) Receptor 2: A Novel Rational Approach for Inhibiting Dimerization of G Protein-Coupled Receptors.” Journal of Peptide Science, 18, Pp. S48-S48. Publisher's Version
Z. Hayouka, A. Levin, M. Hurevich, D. E. Shalev, A. Loyter, C. Gilon, and A. Friedler. 2012. “A comparative study of backbone versus side chain peptide cyclization: Application for HIV-1 integrase inhibitors.” Bioorganic & Medicinal Chemistry, 20, 10, Pp. 3317-3322. Publisher's Version
Y. Tal-Gan, M. Hurevich, S. Klein, A. Ben-Shimon, D. Rosenthal, C. Hazan, D. E. Shalev, M. Y. Niv, A. Levitzki, and C. Gilon. 2011. “Backbone Cyclic Peptide Inhibitors of Protein Kinase B (PKB/Akt).” Journal of Medicinal Chemistry, 54, 14, Pp. 5154-5164. Publisher's Version