Diet-Induced Metabolic Alterations

Neurobiology and Metabolic Research

The consumption of palatable, energy-dense food is a major contributor to overeating and weight gain. This phenomenon is driven by mechanisms within the central nervous system (CNS) that respond to the sensory and nutritional properties of such foods. Circulating nutrients, metabolites, and hormones, released by peripheral organs such as adipose tissue, liver, pancreas, and the gastrointestinal tract, serve as critical feedback signals to the CNS. These signals are integrated by specific neuronal populations, which coordinate behavioral and metabolic responses aimed at maintaining energy and metabolic homeostasis. However, under conditions of sustained overconsumption, these finely tuned regulatory systems can become dysregulated, leading to the development of obesity and associated metabolic disorders.

Our laboratory is dedicated to advancing the understanding of CNS-driven mechanisms underlying the consumption of palatable, energy-dense foods. Specifically, we focus on identifying and characterizing the neurocircuitries activated by these foods. Using cutting-edge neuroscience techniques, we aim to map the anatomical distribution, molecular identity, and connectivity of neuronal populations involved in the processing of these sensory and nutritional stimuli. This includes employing approaches such as chemogenetics, optogenetics, and advanced imaging modalities to dissect the functional roles of these neurons in real-time.

Beyond characterizing the immediate effects of palatable food consumption on neural activity, our research seeks to uncover the long-term consequences of these neuronal activations. We investigate how chronic stimulation of specific neural pathways contributes to maladaptive changes in energy balance regulation, ultimately leading to obesity and metabolic dysfunction. By understanding these processes, we aim to identify critical points of intervention that could restore proper energy homeostasis.

Our ultimate goal is translational: to utilize the knowledge gained from these studies to develop novel, noninvasive therapeutic strategies for combating obesity and other widespread metabolic disorders.

The consumption of palatable, energy-dense food is a major contributor to overeating and weight gain. This phenomenon is driven by mechanisms within the central nervous system (CNS) that respond to the sensory and nutritional properties of such foods. Circulating nutrients, metabolites, and hormones, released by peripheral organs such as adipose tissue, liver, pancreas, and the gastrointestinal tract, serve as critical feedback signals to the CNS. These signals are integrated by specific neuronal populations, which coordinate behavioral and metabolic responses aimed at maintaining energy and metabolic homeostasis. However, under conditions of sustained overconsumption, these finely tuned regulatory systems can become dysregulated, leading to the development of obesity and associated metabolic disorders.

Our laboratory is dedicated to advancing the understanding of CNS-driven mechanisms underlying the consumption of palatable, energy-dense foods. Specifically, we focus on identifying and characterizing the neurocircuitries activated by these foods. Using cutting-edge neuroscience techniques, we aim to map the anatomical distribution, molecular identity, and connectivity of neuronal populations involved in the processing of these sensory and nutritional stimuli. This includes employing approaches such as chemogenetics, optogenetics, and advanced imaging modalities to dissect the functional roles of these neurons in real-time.

Beyond characterizing the immediate effects of palatable food consumption on neural activity, our research seeks to uncover the long-term consequences of these neuronal activations. We investigate how chronic stimulation of specific neural pathways contributes to maladaptive changes in energy balance regulation, ultimately leading to obesity and metabolic dysfunction. By understanding these processes, we aim to identify critical points of intervention that could restore proper energy homeostasis.

Our ultimate goal is translational: to utilize the knowledge gained from these studies to develop novel, noninvasive therapeutic strategies for combating obesity and other widespread metabolic disorders.

Neurocircuits Regulating (Diet-Induced) Adaptive Thermogenesis

This project investigates the role of prepronociceptin (PNOC) neurons in the hypothalamic preoptic area in regulating thermogenesis, energy expenditure, and inflammation in adipose tissue. By utilizing neuroscience tools, the research aims to unravel the mechanisms through which these neurons regulate metabolism.

PNOC neurons, hypothalamus, adaptive thermogenesis, neurocircuits, energy balance, adipose tissue, brown adipose tissue, inflammation, Jais-Lab, HI-MAG, Helmholtz Institute, obesity research, CNS signaling, metabolic health, energy expenditure, metabolic disorders, thermoregulation

Unbiased identification of sucrose-responsive neuronal circuits in control of glucose metabolism

To gain new knowledge on the CNS-dependent regulation of glucose homeostasis, we employed an unbiased experimental approach to profile molecular signatures that define the neuronal populations activated after the ingestion of a hypercaloric high-sucrose diet (HSD). The overarching goal is to gain deeper insights into the neuronal regulation of systemic glucose homeostasis and insulin sensitivity during caloric overload, as a first step toward developing new therapies to treat diabetes—a disease that is rapidly becoming a major health problem in Europe and beyond, with concurrent negative impacts on quality of life as well as public health costs.

Peripheral Neuropeptide Signaling

Our research focuses on understanding how immune-derived opioid peptides, particularly nociceptin/orphanin FQ (N/OFQ), influence glucose metabolism and insulin sensitivity during obesity. By studying the interactions between immune cells and the central nervous system (CNS), we aim to uncover novel mechanisms that drive metabolic inflammation and contribute to insulin resistance.

MA-Foto Julia Schuller EH6A2724_freigestellt

Dr. Julia Schuller

PostDoc

Dr. Adel Ben-Kraiem

PostDoc

Stephanie Puente Ruiz

PhD Candidate

Lea Dropmann

PhD Candidate

Asma Saidi

PhD Candidate

Anja Moll

Technician

Dr. Alexander Jais

Group Leader Profil anzeigen

S. C. Puente-Ruiz, A. Jais

Reciprocal Signaling between Adipose Tissue Depots and the Central Nervous System

A. Jais, L. Paeger, T. Sotelo-Hitschfeld, S. Bremser, M. Prinzensteiner, P. Klemm, V. Mykytiuk, P. J. M. Widdershooven, A. J. Vesting, K. Grzelka, M. Minere, A. L. Cremer, J. Xu, T. Korotkova, B. B. Lowell, H. U. Zeilhofer, H. Backes, H. Fenselau, F. T. Wunderlich, P. Kloppenburg and J. C. Bruning

PNOC(ARC) Neurons Promote Hyperphagia and Obesity upon High-Fat-Diet Feeding

A. Jais, M. Solas, H. Backes, B. Chaurasia, A. Kleinridders, S. Theurich, J. Mauer, S. M. Steculorum, B. Hampel, J. Goldau, J. Alber, C. Y. Forster, S. A. Eming, M. Schwaninger, N. Ferrara, G. Karsenty and J. C. Bruning

Myeloid-Cell-Derived VEGF Maintains Brain Glucose Uptake and Limits Cognitive Impairment in Obesity

A. Jais, E. Einwallner, O. Sharif, K. Gossens, T. T. Lu, S. M. Soyal, D. Medgyesi, D. Neureiter, J. Paier-Pourani, K. Dalgaard, J. C. Duvigneau, J. Lindroos-Christensen, T. C. Zapf, S. Amann, S. Saluzzo, F. Jantscher, P. Stiedl, J. Todoric, R. Martins, H. Oberkofler, S. Muller, C. Hauser-Kronberger, L. Kenner, E. Casanova, H. Sutterluty-Fall, M. Bilban, K. Miller, A. V. Kozlov, F. Krempler, S. Knapp, C. N. Lumeng, W. Patsch, O. Wagner, J. A. Pospisilik and H. Esterbauer

Heme oxygenase-1 drives metaflammation and insulin resistance in mouse and man

A. Jais, J. C. Brüning

Arcuate nucleus-dependent regulation of metabolism - pathways to obesity and diabetes mellitus

A. Jais, J. C. Brüning

Hypthalamic inflammation on obesity and metabolic disease