The proteins of the Bcl-2 family form a complex interaction network that determines the permeabilization of the mitochondrial outer membrane (MOM) in apoptosis. However, the molecular mechanism how the multiple interactions between Bcl-2 proteins are integrated to control MOM permeabilization remains one of the key questions in the field.The main objective of this project is to uncover the stoichiometry of homo- and hetero-complexes of Bcl-2 proteins in the membrane environment and to examine how protein concentration, phosphorylation, membrane curvature or other family members, regulate these complexes. We aim to achieve unprecedented detail thanks to the use of tailored single molecule techniques, which will provide quantitative information about binding affinity, structural organization, temporal and population heterogeneities, and direct visualization of individual complexes. Extending on our previous single molecule studies of Bax, we will address the following concrete questions:1) Role of protein concentration and membrane curvature in the distribution of Bax oligomeric species. 2) Stoichiometry and lifetime of cBid/Bax and Bcl-xL/Bax complexes in the membrane.3) Relative contribution of Bax auto-activation vs. activation by cBid in the final distribution of Bax oligomeric species. Effect of Bcl-xL on the process.4) Stoichiometry of Bok oligomers in the membrane and regulation by cBid and Bcl-xL, as well as the inhibitory mechanism of Bfl1.5) Affinity between Bcl-2 and PUMA, Bim or tBid, and role of phosphorylation on the interaction between these proteins and in apoptosis regulation. 6)Structural conformation of Bim alone and in complex with DLC1, Bax or Bcl-xL in the membrane environment.The outcome of this research will provide a detailed molecular description of the homo- and heterocomplexes of Bcl-2 proteins (including their regulation) that improves current mechanistic models and brings us closer to a functional understanding of how mitochondrial apoptosis is orchestrated. Given the implication of the Bcl-2 family in several diseases, the outcome of our research will also be important to design new ways of therapeutic intervention targeting the Bcl-2 family and improve the existing ones.

DFG Programme Research Units

Subproject of FOR 2036:  New Insights into Bcl-2 Family Interactions: From Biophysics to Function