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At EMBL, experts from institutes throughout the world speak on a wide range of scientific and technical topics

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11 December 2025, 14:30

The sex and geometry of organs

11 December 20252025External Faculty SpeakerEMBL Heidelberg, Virtual

Description Abstract I am interested in how information is encoded at the multi organ level Working at the interface between physiology and developmental biology we have explored the continued development of adult organs We have sought to understand how and why organs such as the intestine grow shrink and are metabolically remodelled even in adult fully developed animals and how this plasticity differs between the sexes We have tackled these questions across biological scales initially in Drosophila and more recently in mice and humans Our worked has uncovered new mechanisms of sex differentiation as well as previously unrecognised communication between gut and gonads that impacts food intake gamete production and tumour susceptibility Some of our work has also investigated how the intestine senses and responds to nutrients we discovered an intestinal zinc sensor that promotes Tor signalling to sustain food intake and developmental growth I have now become very interested in the idea that there is a logic to the shape and arrangement of organs within the body cavity We have developed new methods to visualise and quantify organs in 3D in their natural environment We can now interrogate these multi organ configurations to ask how organ shape impacts organ function and that of its neighbours and whether organ geometry enables or confines communication across organs Connection detailsZoom https embl org zoom us j 96374261689 pwd TnNxRWtQY2lyc2pSa2JpY3NGcDlhZz09 Meeting ID 963 7426 1689 Password DBU... Abstract:I am interested in how information is encoded at the multi-organ level. Working at the interface between physiology and developmental biology, we have explored the “continued development” of adult organs. We have sought to understand how and why organs such as the intestine grow, shrink and are metabolically remodelled even in adult, fully developed animals, and how this plasticity differs between the sexes. We have tackled these questions across biological scales, initially in Drosophila and more recently in mice and humans. Our worked has uncovered new mechanisms of sex differentiation as well as previously unrecognised communication between gut and gonads that impacts food intake, gamete production and tumour susceptibility. Some of our work has also investigated how the intestine senses and responds to nutrients: we discovered an intestinal zinc sensor that promotes Tor...

Speaker(s): Irene Miguel Aliaga, The Francis Crick Institute, United Kingdom
Host: Nicoletta Petridou

Place: Large Operon

EMBL Heidelberg, Virtual

Additional information

Abstract:

I am interested in how information is encoded at the multi-organ level. Working at the interface between physiology and developmental biology, we have explored the “continued development” of adult organs. We have sought to understand how and why organs such as the intestine grow, shrink and are metabolically remodelled even in adult, fully developed animals, and how this plasticity differs between the sexes. We have tackled these questions across biological scales, initially in Drosophila and more recently in mice and humans. Our worked has uncovered new mechanisms of sex differentiation as well as previously unrecognised communication between gut and gonads that impacts food intake, gamete production and tumour susceptibility. Some of our work has also investigated how the intestine senses and responds to nutrients: we discovered an intestinal zinc sensor that promotes Tor signalling to sustain food intake and developmental growth. I have now become very interested in the idea that there is a logic to the shape and arrangement of organs within the body cavity. We have developed new methods to visualise and quantify organs in 3D in their natural environment. We can now interrogate these multi-organ configurations to ask how organ shape impacts organ function and that of its neighbours, and whether organ geometry enables or confines communication across organs.

Connection details
Zoom*: [https://embl-org.zoom.us/j/96374261689?pwd=TnNxRWtQY2lyc2pSa2JpY3NGcDlhZz09] (Meeting ID: [963 7426 1689], Password: [DBU])

 


6 February 2026, 13:00

P05 Nanotomography at PETRA III: Structure - function studies in biology & materials science

6 February 20262026Hamburg SpeakerEMBL Hamburg

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Speaker(s): Imke Greving, Institute of Materials Physics Helmholtz-Zentrum Hereon, Germany
Host: Elisabeth Duke

Place: Seminar Room 48e

EMBL Hamburg


11 September 2026, 11:00

Polycomb proteins and 3D genome architecture in chromatin memory from flies to mouse

11 September 20262026External Faculty SpeakerEMBL Rome

Description AbstractEpigenetic components regulate many biological phenomena during development and normal physiology When dysregulated epigenetic components can also accompany or drive diseases One main class of epigenetic components are Polycomb group proteins Originally Polycomb proteins were shown to silence gene expression We found that this function involves the regulation of 3D chromosome folding and we found that Polycomb components can induce the formation of long distance interactions or chromatin loops that may play instructive roles in gene regulation as well as serve as scaffolding elements that contribute to enhancer promoter specificity Perturbation of Polycomb components is involved in human cancer and leads to tumorigenesis in flies Surprisingly even upon a transient depletion followed by restoration of the full Polycomb compendium epithelial cells lose their normal differentiated fate continue proliferating and establish aggressive tumors demonstrating that cancer can have a fully epigenetic origin Similarly transient perturbation of histone acetylation in mouse ES cells and gastruloids shows that they can record chromatin changes and that this results in cellular memory of the perturbation states The implication of these data will be discussed... AbstractEpigenetic components regulate many biological phenomena during development and normal physiology. When dysregulated, epigenetic components can also accompany or drive diseases. One main class of epigenetic components are Polycomb group proteins. Originally, Polycomb proteins were shown to silence gene expression. We found that this function involves the regulation of 3D chromosome folding and we found that Polycomb components can induce the formation of long-distance interactions or chromatin loops that may play instructive roles in gene regulation as well as serve as scaffolding elements that contribute to enhancer-promoter specificity. Perturbation of Polycomb components is involved in human cancer and leads to tumorigenesis in flies. Surprisingly, even upon a transient depletion followed by restoration of the full Polycomb compendium, epithelial cells lose their normal...

Speaker(s): Giacomo Cavalli, CNRS and University of Montpellier, France
Host: Jamie Hackett

Place: Conf Room/Building 14

EMBL Rome

Additional information

Abstract


Epigenetic components regulate many biological phenomena during development and normal physiology. When dysregulated, epigenetic components can also accompany or drive diseases. One main class of epigenetic components are Polycomb group proteins. Originally, Polycomb proteins were shown to silence gene expression. We found that this function involves the regulation of 3D chromosome folding and we found that Polycomb components can induce the formation of long-distance interactions or chromatin loops that may play instructive roles in gene regulation as well as serve as scaffolding elements that contribute to enhancer-promoter specificity. Perturbation of Polycomb components is involved in human cancer and leads to tumorigenesis in flies. Surprisingly, even upon a transient depletion followed by restoration of the full Polycomb compendium, epithelial cells lose their normal differentiated fate, continue proliferating and establish aggressive tumors, demonstrating that cancer can have a fully epigenetic origin. Similarly, transient perturbation of histone acetylation in mouse ES cells and gastruloids shows that they can record chromatin changes and that this results in cellular memory of the perturbation states. The implication of these data will be discussed.