Self-organized criticality as a fundamental property of neural systems

The neural criticality hypothesis states that the brain may be poised in a critical state at a boundary between different types of dynamics. Theoretical and experimental studies show that critical systems often exhibit optimal computational properties, suggesting the possibility that criticality has been evolutionarily selected as a useful trait for our nervous system. Evidence for criticality has been found in cell cultures, brain slices, and anesthetized animals. Yet, inconsistent results were reported for recordings in awake animals and humans, and current results point to open questions about the exact nature and mechanism of criticality, as well as its functional role. Therefore, the criticality hypothesis has remained a controversial proposition. Here, we provide an account of the mathematical and physical foundations of criticality. In the light of this conceptual framework, we then review and discuss recent experimental studies with the aim of identifying important next steps to be taken and connections to other fields that should be explored.Peer Reviewe

An Optimal Time for Treatment-Predicting Circadian Time by Machine Learning and Mathematical Modelling

Tailoring medical interventions to a particular patient and pathology has been termed personalized medicine. The outcome of cancer treatments is improved when the intervention is timed in accordance with the patient's internal time. Yet, one challenge of personalized medicine is how to consider the biological time of the patient. Prerequisite for this so-called chronotherapy is an accurate characterization of the internal circadian time of the patient. As an alternative to time-consuming measurements in a sleep-laboratory, recent studies in chronobiology predict circadian time by applying machine learning approaches and mathematical modelling to easier accessible observables such as gene expression. Embedding these results into the mathematical dynamics between clock and cancer in mammals, we review the precision of predictions and the potential usage with respect to cancer treatment and discuss whether the patient's internal time and circadian observables, may provide an additional indication for individualized treatment timing. Besides the health improvement, timing treatment may imply financial advantages, by ameliorating side effects of treatments, thus reducing costs. Summarizing the advances of recent years, this review brings together the current clinical standard for measuring biological time, the general assessment of circadian rhythmicity, the usage of rhythmic variables to predict biological time and models of circadian rhythmicity

A statement by Scientists for Future concerning the protests for more climate protection

In March 2019, German-speaking scientists and scholars calling themselves Scientists for Future, published a statement in support of the youth protesters in Germany, Austria, and Switzerland (Fridays for Future, Klimastreik/Climate Strike), verifying the scientific evidence that the youth protestors refer to. In this article, they provide the full text of the statement, including the list of supporting facts (in both English and German) as well as an analysis of the results and impacts of the statement. Furthermore, they reflect on the challenges for scientists and scholars who feel a dual responsibility: on the one hand, to remain independent and politically neutral, and, on the other hand, to inform and warn societies of the dangers that lie ahead

A keratin scaffold regulates epidermal barrier formation, mitochondrial lipid composition, and activity.

Keratin intermediate filaments (KIFs) protect the epidermis against mechanical force, support strong adhesion, help barrier formation, and regulate growth. The mechanisms by which type I and II keratins contribute to these functions remain incompletely understood. Here, we report that mice lacking all type I or type II keratins display severe barrier defects and fragile skin, leading to perinatal mortality with full penetrance. Comparative proteomics of cornified envelopes (CEs) from prenatal KtyI(-/-) and KtyII(-/-)(K8) mice demonstrates that absence of KIF causes dysregulation of many CE constituents, including downregulation of desmoglein 1. Despite persistence of loricrin expression and upregulation of many Nrf2 targets, including CE components Sprr2d and Sprr2h, extensive barrier defects persist, identifying keratins as essential CE scaffolds. Furthermore, we show that KIFs control mitochondrial lipid composition and activity in a cell-intrinsic manner. Therefore, our study explains the complexity of keratinopathies accompanied by barrier disorders by linking keratin scaffolds to mitochondria, adhesion, and CE formation

Implications of neuronal excitability and morphology for spike-based information transmission

Signalverarbeitung im Nervensystem hängt sowohl von der Netzwerkstruktur, als auch den zellulären Eigenschaften der Nervenzellen ab. In dieser Abhandlung werden zwei zelluläre Eigenschaften im Hinblick auf ihre funktionellen Anpassungsmöglichkeiten untersucht: Es wird gezeigt, dass neuronale Morphologie die Signalweiterleitung unter Berücksichtigung energetischer Beschränkungen verstärken kann, und dass selbst kleine Änderungen in biophysikalischen Parametern die Aktivierungsbifurkation in Nervenzellen, und damit deren Informationskodierung, wechseln können. Im ersten Teil dieser Abhandlung wird, unter Verwendung von mathematischen Modellen und Daten, die Hypothese aufgestellt, dass Energie-effiziente Signalweiterleitung als starker Evolutionsdruck für unterschiedliche Zellkörperlagen bei Nervenzellen wirkt. Um Energie zu sparen, kann die Signalweiterleitung vom Dendrit zum Axon verstärkt werden, indem relativ kleine Zellkörper zwischen Dendrit und Axon eingebaut werden, während relativ große Zellkörper besser ausgelagert werden. Im zweiten Teil wird gezeigt, dass biophysikalische Parameter, wie Temperatur, Membranwiderstand oder Kapazität, den Feuermechanismus des Neurons ändern, und damit gleichfalls Aktionspotential-basierte Informationsverarbeitung. Diese Arbeit identifiziert die sogenannte "saddle-node-loop" (Sattel-Knoten-Schlaufe) Bifurkation als den Übergang, der besonders drastische funktionale Auswirkungen hat. Neben der Änderung neuronaler Filtereigenschaften sowie der Ankopplung an Stimuli, führt die "saddle-node-loop" Bifurkation zu einer Erhöhung der Netzwerk-Synchronisation, was möglicherweise für das Auslösen von Anfällen durch Temperatur, wie bei Fieberkrämpfen, interessant sein könnte.Signal processing in nervous systems is shaped by the connectome as well as the cellular properties of nerve cells. In this thesis, two cellular properties are investigated with respect to the functional adaptations they provide: It is shown that neuronal morphology can improve signal transmission under energetic constraints, and that even small changes in biophysical parameters can switch spike generation, and thus information encoding. In the first project of the thesis, mathematical modeling and data are deployed to suggest energy-efficient signaling as a major evolutionary pressure behind morphological adaptations of cell body location: In order to save energy, the electrical signal transmission from dendrite to axon can be enhanced if a relatively small cell body is located between dendrite and axon, while a relatively large cell body should be externalized. In the second project, it is shown that biophysical parameters, such as temperature, membrane leak or capacitance, can transform neuronal excitability (i.e., the spike onset bifurcation) and, with that, spike-based information processing. This thesis identifies the so-called saddle-node-loop bifurcation as the transition with particularly drastic functional implications. Besides altering neuronal filters and stimulus locking, the saddle-node-loop bifurcation leads to an increase in network synchronization, which may potentially be relevant for the initiation of seizures in response to increased temperature, such as during fever cramps

An integrative mathematical model for timing treatment toxicity and Zeitgeber impact in colorectal cancer cells

Abstract Increasing evidence points to a role of the circadian clock in the regulation of cancer hallmarks with a strong impact on the understanding and treatment of this disease. Anti-cancer treatment can be personalized considering treatment timing. Here we present a new mathematical model based on data from three colorectal cancer cell lines and core-clock knock-outs, which couples the circadian and drug metabolism network, and that allows to determine toxicity profiles for a given drug and cell type. Moreover, this model integrates external Zeitgebers and thus may be used to fine-tune toxicity by using external factors, such as light, and therefore, to a certain extent, help fitting the endogenous rhythms of the patients to a defined clinic routine facilitating the implementation of time-dependent treatment in clinical practice