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Home SCIENCE NEWS Technology and Engineering

Investigating the effects on amide-to-ester substitutions on membrane permeability of cyclic peptides

March 17, 2023
in Technology and Engineering
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Cyclic peptides often exhibit low membrane permeability which can be significantly improved via amide-to-ester substitutions—as demonstrated by researchers from Tokyo Institute of Technology (Tokyo Tech). The utilization of substitutions shown in this study can be used to develop cyclic peptides with high membrane permeability and oral bioavailability for clinical and therapeutic applications.

Figure 1. Analyzing the effect of amide-to-ester substitution on the permeability of cyclic peptides.

Credit: Nature Communications

Cyclic peptides often exhibit low membrane permeability which can be significantly improved via amide-to-ester substitutions—as demonstrated by researchers from Tokyo Institute of Technology (Tokyo Tech). The utilization of substitutions shown in this study can be used to develop cyclic peptides with high membrane permeability and oral bioavailability for clinical and therapeutic applications.

Interest in cyclic peptides, a class of organic molecules, has reached a new high recently. Their ability as inhibitors has made them potential candidates for clinical and therapeutic applications. Unlike their linear counterparts, peptides with macrocyclization have better resistance to proteolysis—the disintegration of peptides into amino acids in the presence of enzymes—which makes them stable in the bloodstream—desired property for any material being used for therapeutic purposes.

However, the membrane permeability—the ability of a molecule to pass through cell membranes in our body—of cyclic peptides is quite low in general. This downside not only makes formulation of orally bioavailable peptides difficult, but also severely affects their ability to target intracellular protein interactions. On the other hand, some natural cyclic peptides show great membrane permeability and oral bioavailability. These naturally occurring membrane-permeable cyclic peptides often have N-methylamide bonds, ester bonds, or both on their backbone, instead of amide bonds those are the most common for amino acids in proteins and peptides. While studies have explored the effects of N-methylation on cyclic peptides, the impact of amide-to-ester substitution remains unexplored. 

That was until a multinational and interdisciplinary group of researchers from Tokyo Tech, The University of Tokyo, and University of California, Santa Cruz, came together to discover the unknown. In their recent breakthrough published in Nature Communications, the team reported a direct evaluation of amide-to-ester substitutions and their effect on the membrane permeability of cyclic peptides. Prof. Yutaka Akiyama from Tokyo Tech, a corresponding author of this paper explains, “We know that naturally occurring depsipeptides, which are peptides where one or more of the amide bonds are replaced with an ester bond, show high membrane permeability. This is why our team decided to see if amide-to-ester substitutions can improve membrane permeability.  In the team, Tokyo Tech scientists employed a newly developed method on enhanced sampling molecular dynamics (MD) simulations to unravel the mechanism behind this.”

The team first synthesized a series of model dipeptides and their derivatives containing amide-to-ester substitutions. They then compared the membrane permeability of these peptides using wet lab techniques and found that the substituted dipeptides had significantly higher membrane permeability (Figure 1, Left).

To better understand the scope of these substitutions, the team tried amide-to-ester replacements on larger cyclic hexapeptides. The findings indicated that amide-to-ester substitution enhanced the membrane permeability of cyclic hexapeptides much more than the conventional N-methylation process (Figure 1, Right).

The team also carried out enhanced sampling MD simulations on three cyclic hexapeptides (CP1, DP1, and MP1) using the TSUBAME3.0 supercomputer at Tokyo Tech. The large-scale simulations revealed that the substituted peptides dynamically transition between their open and closed conformations in aqueous solution and at the membrane interface (Figure 2). They also revealed that the amine-to-ester substitution led to a corresponding reduction in the free energy barrier for the substituted peptides, thereby leading to their enhanced membrane permeability.

The insights provided by this study could help expand the utility of cyclic peptides by providing a simple solution to the low permeability problem. “We envision that this amide-to-ester substitution strategy will be utilized for the development of peptides with better oral bioavailability, ability to target intracellular biomolecules, or both,” concludes Prof. Akiyama.

###

Related Links

TSUBAME supercomputer predicts cell-membrane permeability of cyclic peptides | Tokyo Tech News, July 13, 2021

https://www.titech.ac.jp/english/news/2021/061264

Tokyo Tech and Kawasaki City, combining forces in R&D on Computational Drug Discovery for Middle Molecules at KING SKYFRONT | Toyo Tech News, August 9, 2017

https://www.titech.ac.jp/english/news/2017/038972

Akiyama Laboratory

http://www.bi.cs.titech.ac.jp/web/top_en.html

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About Tokyo Institute of Technology

Tokyo Tech stands at the forefront of research and higher education as the leading university for science and technology in Japan. Tokyo Tech researchers excel in fields ranging from materials science to biology, computer science, and physics. Founded in 1881, Tokyo Tech hosts over 10,000 undergraduate and graduate students per year, who develop into scientific leaders and some of the most sought-after engineers in the industry. Embodying the Japanese philosophy of “monotsukuri,” meaning “technical ingenuity and innovation,” the Tokyo Tech community strives to contribute to society through high-impact research.

https://www.titech.ac.jp/english/



Journal

Nature Communications

DOI

10.1038/s41467-023-36978-z

Method of Research

Experimental study

Subject of Research

Animal tissue samples

Article Title

Nature Communications

Article Publication Date

17-Mar-2023

COI Statement

The authors declare no competing interests.

Tags: amidetoestercycliceffectsInvestigatingMembranepeptidespermeabilitysubstitutions
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