Björn Friedrichs scite author profile

Maturation of cytochrome c peroxidase (Ccp1) in mitochondria occurs by the subsequent action of two conserved proteases in the inner membrane: the m-AAA protease, an ATP-dependent protease degrading misfolded proteins and mediating protein processing, and the rhomboid protease Pcp1, an intramembrane cleaving peptidase. Neither the determinants preventing complete proteolysis of certain substrates by the m-AAA protease, nor the obligatory requirement of the m-AAA protease for rhomboid cleavage is currently understood. Here, we describe an intimate and unexpected functional interplay of both proteases. The m-AAA protease mediates the ATPdependent membrane dislocation of Ccp1 independent of its proteolytic activity. It thereby ensures the correct positioning of Ccp1 within the membrane bilayer allowing intramembrane cleavage by rhomboid. Decreasing the hydrophobicity of the Ccp1 transmembrane segment facilitates its dislocation from the membrane and renders rhomboid cleavage m-AAA protease-independent. These findings reveal for the first time a non-proteolytic function of the m-AAA protease during mitochondrial biogenesis and rationalise the requirement of a preceding step for intramembrane cleavage by rhomboid.

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An Il12-Il2-Antibody Fusion Protein Targeting Hodgkin's Lymphoma Cells Potentiates Activation Of Nk And T Cells For An Anti-Tumor Attack

Jahn¹,

Zuther²,

Friedrichs³

et al. 2012

PLoS ONE

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Successful immunotherapy of Hodgkin's disease is so far hampered by the striking unresponsiveness of lymphoma infiltrating immune cells. To mobilize both adoptive and innate immune cells for an anti-tumor attack we fused the pro-inflammatory cytokines IL2 and IL12 to an anti-CD30 scFv antibody in a dual cytokine fusion protein to accumulate both cytokines at the malignant CD30+ Hodgkin/Reed-Sternberg cells in the lymphoma lesion. The tumor-targeted IL12-IL2 fusion protein was superior in activating resting T cells to amplify and secrete pro-inflammatory cytokines compared to targeted IL2 or IL12 alone. NK cells were also activated by the dual cytokine protein to secrete IFN-γ and to lyse target cells. The tumor-targeted IL12-IL2, when applied by i.v. injection to immune-competent mice with established antigen-positive tumors, accumulated at the tumor site and induced tumor regression. Data demonstrate that simultaneous targeting of two cytokines in a spatial and temporal simultaneous fashion to pre-defined tissues is feasible by a dual-cytokine antibody fusion protein. In the case of IL12 and IL2, this produced superior anti-tumor efficacy implying the strategy to muster a broader immune cell response in the combat against cancer.

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Discovering Types of Smartphone Usage Sessions from User-App Interactions

Friedrichs

Turner

Allen

2021

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Understanding how and why people use their smartphones has enabled use cases ranging from correlating behaviour with psychological states through to on-device tasks such as app recommendations. However, being able to effectively and pervasively capture usage behaviour is challenging due to the wide range of functions, apps and interactions that are possible. In this paper, we examine how embedding physical user-app activity (e.g., taps and scrolls) can provide a rich basis for summarising device usage. Using a large dataset of 82,758,449 interaction events from 86 users over an 8-week period we combine feature embedding and unsupervised learning to extract prominent interactions within clusters of smartphone usage sessions. We find that high-level features such as session length, unlock state, and app switches are not representative of these clusters and can give a false sense of similarity or dissimilarity between sessions. The results motivate further exploration of the utility of using user-app interaction behaviour as the basis for the aforementioned use cases.

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Utilising the co-occurrence of user interface interactions as a risk indicator for smartphone addiction

Friedrichs

Turner

Allen

2022

Pervasive and Mobile Computing

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