Dr Thimmalapura Marulappa Vishwanatha

Nationality: 
India
Programme: 
SMART LOIRE VALLEY GENERAL PROGRAMME
Scientific Field: 
Period: 
July, 2018 to January, 2019
February, 2019 to January, 2020

LE STUDIUM Guest Research Fellow (1st period)

LE STUDIUM / Marie Skłodowska-Curie Research Fellow (2nd period)

From

University Medical College Groningen - NL

In residence at

Molecular Biophysics Center (CBM), CNRS - FR

Host scientist

Dr Vincent Aucagne

PROJECT

Development of novel chemoselective ligation techniques for protein synthesis

An ingenious stratagem useful to understand and modulate the structural and functional features of the proteins refers to the modification of their chemical structure. In this regard, the chemical synthesis of proteins appears a key tool, as it allows the unlimited modification of a polypeptide chain with any kind and number of labels. The last decade has seen the introduction of several techniques of chemical protein synthesis that allow the manipulation of proteins structure. Among these approaches, the Native Chemical Ligation (NCL) reaction appears as the most useful and advantageous strategy and numerous researches are currently ongoing on in this area. Many of the developed ligation methods have their own drawbacks. In particularly, NCL requires a cysteine residue as ligation site which is a rare amino acid. Many other synthetic strategies rely on the same reaction with the use of amino acid-derived β-amino thiols. However, their preparations require long multistep synthesis and an additional desulfurization step is necessary after NCL. Thus, the development of original chemical methods based on easily preparable starting materials could not only unlock major technological limitations of protein chemical synthesis but also provide alternative synthetic pathway to provide simple amides.
The project I propose to develop utilizes peptide thioacids as important coupling partner. Peptide thioacids will be coupled with peptide isocyanides using a known methodology, but to date only applied to small protected peptide segments: chemoselectivity and large protein synthesis will be studied in detail, requiring in particular the development of a synthetic route to unprotected peptide isocyanides. Secondly, following a similar strategy, peptide thioacids will be coupled to N-activated peptides (imidazolyl ureas) and the chemoselectivity of the reaction will be scrutinized.