Targeting small GTPases and their downstream pathways with intracellular macromolecule binders to define alternative therapeutic strategies in cancer

Author:

Sorbara Marie1,Bery Nicolas1ORCID

Affiliation:

1. Centre de Recherches en Cancérologie de Toulouse (CRCT), U1037 INSERM, Université Toulouse III - U5071 CNRS, ImPact, Therapeutic Innovation in Pancreatic Cancer, Toulouse 31100, France

Abstract

The RAS superfamily of small GTPases regulates major physiological cellular processes. Mutation or deregulation of these small GTPases, their regulators and/or their effectors are associated with many diseases including cancer. Hence, targeting these classes of proteins is an important therapeutic strategy in cancer. This has been recently achieved with the approval of the first KRASG12C covalent inhibitors for the clinic. However, many other mutants and small GTPases are still considered as ‘undruggable' with small molecule inhibitors because of a lack of well-defined pocket(s) at their surface. Therefore, alternative therapeutic strategies have been developed to target these proteins. In this review, we discuss the use of intracellular antibodies and derivatives — reagents that bind their antigen inside the cells — for the discovery of novel inhibitory mechanisms, targetable features and therapeutic strategies to inhibit small GTPases and their downstream pathways. These reagents are also versatile tools used to better understand the biological mechanisms regulated by small GTPases and to accelerate the drug discovery process.

Publisher

Portland Press Ltd.

Subject

Biochemistry

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