Organ Transplantation and Organ Donation – A Social Responsibility? Experiences in Spain and Germany
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Organ Transplantation and Organ Donation – A Social Responsibility?
Experiences in Spain and Germany

Monday, September 15, 2025, 5:30 – 9:30 p.m.
Embajada de España | Embassy of Spain
Lichtensteinallee 1, 10787 Berlin

Organ transplantation is the therapy of choice for end-stage organ failure. Despite its life-saving potential, this therapy is not available to all patients in Germany, as a lack of willingness to donate has led to a shortage of organs. Together with the Embassy of Spain in Berlin, we would like to explore this topic further. By examining the different experiences of Spain and Germany—two European countries with very different approaches to organ donation—we aim to discuss opportunities, challenges, and possible ways to increase donation willingness. Experts in organ transplantation from both countries will highlight differences and engage in discussion with the audience.

We look forward to welcoming:
Dr. Beatriz Domínguez-Gil, Director of the Spanish Transplant Organization (ONT),
Dr. Luis Rodríguez-Bachiller Villaronga, Gregorio Marañón University Hospital,
Dr. Alberto Sandiumenge Camps, Vall d’Hebrón University Hospital
Franziska Bleis, Patient Ambassador,
Dr. Axel Rahmel, Medical Director of the German Foundation for Organ Transplantation,
Dr. Dr. Sandra Loder, Managing Physician, German Foundation for Organ Transplantation, and
Prof. Dr. Johann Pratschke, Director of the Department of Surgery, Charité.
The event will be moderated by Christian Maier.

The event takes place within the framework of the special exhibition “Vessels: Infrastructures of Life” of the Berliner Medizinhistorisches Museum and Experimental Surgery | Charité, in cooperation with the Cluster of Excellence “Matters of Activity” at Humboldt University of Berlin, as part of the __matter Festival 2025. We gratefully acknowledge the generous support of Stiftung Charité.

Please register for the event here.
ARTE documentary features Project Neo|Pancreas and Ersielda Keshi

The number of people needing donor organs continues to grow — but there simply aren't enough to meet demand. Could the future of transplant medicine lie in the laboratory? This arte documentary offers a fascinating look at the latest breakthroughs in artificial organs and artificial hearts, with insights from Germany, Japan, and Sweden.
The documentary “A Heart on Demand?” by Marcus Fitsch explores one of modern medicine’s most urgent challenges: How can we overcome the shortage of donor organs?

The film follows groundbreaking research projects in Germany, Japan, and Sweden — including work at Berlin’s Charité and Japan’s renowned Riken Institute. Scientists there aren’t just modifying existing organs — they’re creating them entirely in the lab, custom-built and in scalable quantities. From miniature kidneys grown from stem cells to liver cells tested in animal models, and even the vision of a fully functional artificial heart, the documentary dives deep into the innovations shaping the future. Ethical questions are also front and center: What does it mean to manufacture human organs? And just how close are we to a true revolution in transplant medicine?

This is a rich, informative, and visually striking documentary that reveals how science and technology are coming together to redefine the future of healthcare.
New Book: Virtual participation, real involvement – Transformative technologies for a more inclusive society
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Virtual reality (VR) and augmented reality (AR) are among the fastest-growing technologies of the 21st century. They also open up enormous opportunities for social integration: through cultural and educational offerings, through networked digital interaction spaces, or as a means of promoting citizen participation. The contributions in this volume present a wide range of application scenarios for VR and AR in the fields of education, health and public space. They demonstrate in a practical way how society, but also companies, can benefit from expanding their technological skills and taking diversity aspects into account. After all, genuine participation is only possible through a sustainable, transdisciplinary and citizen science approach.

Our book chapter ‘Human-Centred Design of Mixed Reality Applications in Medical Education – GreifbAR’ is now available in open access. Authors are Robert Luzsa, Moritz Queisner, Christopher Remde, Igor Sauer, Nadia Robertini and Susanne Mayr.

As part of the BMBF-funded project ‘Tangible Reality – Skilful Interaction of User Hands and Fingers with Real Tools in Mixed Reality Worlds’, we investigated how XR technology can be integrated into medical education. The chapter presents an interdisciplinary, XR-based training system for surgical knot tying. It describes key design principles and experiences from development and evaluation. In addition, it proposes a model for the human-centred design of comparable training applications that can also support other projects.

Opening Exhibition | »Vessels. Infrastructures of Life«
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We warmly invite you to the opening of »Vessels. Infrastructures of Life« at the Berlin Museum of Medical History at the Charité (bmm), a group exhibition curated by Igor M. Sauer and Navena Widulin with contributions by Assal Daneshgar, Emile de Visscher, Frédéric Eyl, Karl Hillebrandt, Eriselda Keshi, Dietrich Polenz, Moritz Queisner, Iva Rešetar and Igor M. Sauer.

Vernissage
Wed, 4 June 2025, 7:00 - 10:00 pm

Exhibition
5 June – 12 October 2025 Tue, Thu, Fri, Sun, 10:00 am - 5:00 pm Wed, Sat, 10:00 am - 7:00 pm Closed on Mondays

Venue
Berliner Medizinhistorisches Museum der Charité (bmm) Virchowweg 17 10117 Berlin

What do plants, animals, humans and cities have in common? They all have vascular systems and, therefore, an infrastructure without which they would not be able to survive.

In the human body, arteries and veins move the blood together with the heart. Plants have a finely branched vascular system for the transport of water and nutrients. And cities utilize an underground network of pipelines that supply clean water and remove wastewater. The temporary exhibition, co-curated by Igor Sauer and Navena Widulin, shows how these vessels function and how they can be visualized, used and reproduced.

What can medicine learn from these natural and technical supply systems? What role does the interdisciplinary view – between biology, design, materials research and medical technology – play for regenerative medicine? And what innovative approaches can be derived from this for the development of artificial and bioartificial donor organs?

»Vessels. Infrastructures of Life« provides insights into the work of designers, material scientists and surgical researchers who are working together on solutions for the future – inspired by nature, technology and the logic of living systems. From exhibits on transplantation and regenerative medicine to examples of architecture and design, the exhibition offers exciting insights into these often-hidden structures. The objects on display correspond with those in Rudolf Virchow’s historical collection of specimens. A particular focus lies on the connections between natural vessels and human-made networks, such as the regulation of temperature in buildings or the water and wastewater supply in cities.

The temporary exhibition »Vessels. Infrastructures of Life« is a collaboration between the Berlin Museum of Medical History and the Experimental Surgery at the Charité and the Cluster of Excellence »Matters of Activity« of Humboldt-Universität zu Berlin as part of the  _matter Festival 2025.
90-Day Mortality Prediction in Elective Visceral Surgery Using Machine Learning
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Our paper, "90-Day Mortality Prediction in Elective Visceral Surgery Using Machine Learning: A Retrospective Multicenter Development, Validation, and Comparison Study" has been published online ahead of print in the International Journal of Surgery.
Authors are C. Riepe, R. van de Water, A. Winter, B. Pfitzner, L. Faraj, R. Ahlborn, M. Schulze, D. Zuluaga, C. Schineis, K. Beyer, J. Pratschke, B. Arnrich, I.M. Sauer, and M.M. Maurer

Machine Learning (ML) is increasingly being adopted in biomedical research, however, its potential for outcome prediction in visceral surgery remains uncertain. This study compares the potential of ML methods for preoperative 90-day mortality (90DM) prediction of an aggregated multi-organ approach to conventional scoring systems and individual organ models.

This retrospective cohort study enrolled patients undergoing major elective visceral surgery between 2014 and 2022 across two tertiary centers. Multiple ML models for preoperative 90DM prediction were trained, externally validated and benchmarked against the American Society of Anesthesiologists (ASA) score and revised Charlson Comorbidity Index (rCCI). Areas under the receiver operating characteristic (AUROC) and precision recall curves (AUPRC) including standard deviations were calculated. Additionally, individual models for esophageal, gastric, intestinal, liver, and pancreatic surgery were developed and compared to an aggregated approach. A total of 7,711 cases encompassing 78 features were included. Overall 90DM was 4% (n = 309). An XBoost classifier demonstrated the best performance and high robustness following external validation (AUROC: 0.86 [0.01]; AUPRC: 0.2 [0.04]). All models outperformed the ASA score (AUROC: 0.72; AUPRC: 0.08) and rCCI (AUROC: 0.81; AUPRC: 0.11). rCCI, patient age and C-reactive protein emerged as most decisive model weights. Models for gastric (AUROC: 0.88 [0.13]; AUPRC: 0.24 [0.26]) and intestinal surgery (AUROC: 0.87 [0.05]; AUPRC: 0.17 [0.09]) revealed the highest organ-specific performances, while pancreatic surgery yielded the lowest results (AUROC: 0.66 [0.08]; AUPRC: 0.22 [0.12]). A combined multi-organ approach (AUROC: 0.84 [0.04]; AUPRC: 0.21 [0.06]) demonstrated superiority over the weighted average across all organ-specific models (AUROC: 0.82 [0.07]; AUPRC: 0.2 [0.13]).

ML offers robust preoperative risk stratification for 90DM in elective visceral surgery. Leveraging training across multi-organ cohorts may improve accuracy and robustness compared to organ-specific models. Prospective studies are needed to confirm the potential of ML in surgical outcome prediction.
Michael Tummings | Human Insights
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Michael TummingsArtist in Residence @ Experimental Surgery – has released his latest book, Human Insights.

In this powerful work, Tummings turns his lens toward the operating theatre, capturing intimate moments of surgical intervention. His photographs explore the human body not as an object of clinical analysis, but as a site of vulnerability, resilience, and transformation. As noted by Jörg Christian Tonn, Tummings' work "reveals the mysteries of the body," offering entirely new perspectives on physical existence and the role of modern medicine.

With the consent of both patients and surgical teams of several university hospitals, Tummings was granted rare access to document procedures involving organ implants and artificial prostheses. The resulting imagery bridges the worlds of art and science, bringing us face-to-face with the beauty of the human body—beyond the rational and dissecting eye.

Human Insights invites viewers to reconsider how we see ourselves and our bodies, especially in moments of repair and healing.
Dr. Agnes Böhm
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Today Agnes Klara Böhm successfully defended her doctoral thesis entitled "Multidimensional analysis of different decellularization methods for diaphragmatic extracellular matrices in a murine model" summa cum laude!

Congratulations !
_matter Festival 2025


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Matter shapes our existence, although we tend to forget about its activity in everyday life. The _matter Festival 2025 shines a new light on material agencies.
We invite you to explore exhibitions, workshops and debates at 12 venues across Berlin.
Discover the program spanning from April to October here!

The special exhibition »Gefäße – Infrastrukturen des Lebens« (Vessels – Infrastructures of Life) at the Berliner Medizinhistorisches Museum shows how these vessels function and how they can be visualized, used and reproduced. From exhibits on transplantation and regenerative medicine to examples of architecture and design, the exhibition offers exciting insights into these often hidden structures. Surgical procedures in general and transplant surgery, in particular, are inconceivable without the consideration of macro- and microscopic vessels. Vascular structures also play a central role in the field of regenerative medicine and tissue engineering. The exhibits correspond with those in Virchow’s collection of specimens. A particular focus lies on the connections between natural vessels and human-made networks, such as the regulation of temperature in buildings or the water and wastewater supply in cities.

Team Credits
Curation: Igor Sauer & Navena Widulin
Coordination: Sophia Gräfe
Production and Design: Julia Blumenthal
Contributors: Assal Daneshgar, Emile De Visscher, Frédéric Eyl, Eriselda Keshi, Moritz Queisner, Iva Rešetar and Igor Sauer

Dates
Vernissage: Wed, 4 June 2025, 7:00–10:00 pm
Exhibition: 5 June–12 October 2025
Opening Hours:
Tue, Thu, Fri, Sun: 10:00 am–5:00 pm
Wed, Sat: 10:00 am–7:00 pm

Public Program
28 June 2025, 7:00–8:00 pm
Lecture Hall Ruin
Vessels. Infrastructures of Life – Presentation as Part of the Lange Nacht der Wissenschaften 2025 (language: German)
Lecture Program and Guided Tours: Details tbc
Sparse camera volumetric video applications
The paper "Sparse camera volumetric video applications. A comparison of visual fidelity, user experience, and adaptability" is available open access in Frontiers in Signal Processing.
Authors are Christopher Remde, Igor M. Sauer, and Moritz Queisner.

Volumetric video production in commercial studios is predominantly produced using a multi-view stereo process that relies on a high two-digit number of cameras to capture a scene. Due to the hardware requirements and associated processing costs, this workflow is resource-intensive and expensive, making it unattainable for creators and researchers with smaller budgets. Low-cost volumetric video systems using RGBD cameras offer an affordable alternative. As these small, mobile systems are a relatively new technology, the available software applications vary in terms of workflow and image quality. In this paper we provide an overview of the technical capabilities of sparse camera volumetric video capture applications and assess their visual fidelity and workflow.

We selected volumetric video applications that are publicly available, support capture with multiple Microsoft Azure Kinect cameras and run on consumer-grade computer hardware. We compared the features, usability, and workflow of each application and benchmarked them in five different scenarios. Based on the benchmark footage, we analyzed spatial calibration accuracy, artifact occurrence and conducted a subjective perception study with 19 participants from a game design study program to assess the visual fidelity of the captures.

We evaluated three applications, Depthkit Studio, LiveScan3D and VolumetricCapture. We found Depthkit Studio to provide the best experience for novel users, while LiveScan3D and VolumetricCapture require advanced technical knowledge to be operated. The footage captured by Depthkit Studio showed the least amount of artifacts by a larger margin, followed by LiveScan3D and VolumetricCapture. These findings were confirmed by the participants who preferred Depthkit Studio over LiveScan3D and VolumetricCapture. Based on the results, we recommend Depthkit Studio for the highest fidelity captures. LiveScan3D produces footage of only acceptable fidelity but is the only candidate that is available as open-source software. We therefore recommend it as a platform for research and experimentation. Due to the lower fidelity and high setup complexity, we recommend VolumetricCapture only for specific use-cases where its ability to handle a high number of sensors in a large capture volume is required.
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Gender-based variations in surgical management of colorectal liver metastases
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BMC Cancer published the paper "Gender-based variations in surgical management of colorectal liver metastases: comprehensive analysis". Authors are Pia F. Koch, Kristina Ludwig, Karl H. Hillebrandt, Hannes Freitag, Moritz Blank, Sebastian Knitter, Dominik P. Modest, Felix Krenzien, Georg Lurje, Wenzel Schöning, Johann Pratschke, Igor M. Sauer, Simon Moosburner, and Nathanael Raschzok.

Colorectal cancer with liver metastasis affects both men and women. However, therapeutic strategies and long-term outcomes could be influenced by patients' sex, due to variations in tumour biology, lifestyle, and dietary habits. By conducting a comprehensive comparative analysis, this study aims to detail differences in tumour characteristics, postoperative complications, recurrence rates, and survival outcomes between sexes.
We performed a Single-centre retrospective analysis between 2010 and 2022 of all patients undergoing liver surgery for colorectal liver metastases (CRLM) at the Department of Surgery, Charité- Universitätsmedizin Berlin. Patients were stratified by sex. Statistical analysis was performed using RV4.2.We analysed 642 patients who underwent hepatic resections for CRLM. Baseline patient characteristics were comparable between sexes: However, significant differences (p < 0.001) were noted in body mass index (BMI), with females exhibiting lower BMIs (median BMI in females: 23.7 kg/m² vs. males: 26.5 kg/m²). Primary tumour locations varied significantly (p = 0.008), with females presenting more sigmoid colon tumours (37%), while males predominantly had rectal tumours (35%). RAS mutation rates were higher in females (54%) than males (34%, p = 0.005). A higher prevalence of bilobar metastases were evident in men (62%, p = 0.011), yet surgical techniques and complications showed comparable distributions. The time for resection was longer in males (median 304 min vs. 290 min in females); however, conversion to open surgery took place more often in females (5.2% vs. 2.3% in males). Postoperative complications and survival rates showed no significant differences by patients' sex.
Distinct sex-related patterns in tumour characteristics and postoperative outcomes in patients with CRLM were observed, emphasizing the need for further investigations to understand and address gender-based disparities for more personalized clinical management in the future.

The paper is available open access here.

Clinical prognosticators and targets in the immune microenvironment of intrahepatic cholangiocarcinoma
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The work on "
200pubmed" target="_blank">Clinical prognosticators and targets in the immune microenvironment of intrahepatic cholangiocarcinoma" has been published by Oncoimmunology. Authors are Isis Lozzi, Alexander Arnold, Matthias Barone, Juliette Claire Johnson, Bruno V. Sinn, Johannes Eschrich, Pimrapat Gebert, Ruonan Wang, Mengwen Hu, Linda Feldbrügge, Anja Schirmeier, Anja Reutzel-Selke, Thomas Malinka, Felix Krenzien, Wenzel Schöning, Dominik P. Modest, Johann Pratschke, Igor M. Sauer, and Matthäus Felsenstein.

Intrahepatic cholangiocarcinoma (ICC) is a disease with poor prognosis and limited therapeutic options. We investigated the tumor immune microenvironment (TIME) to identify predictors of disease outcome and to explore targets for therapeutic modulation. Liver tissue samples were collected during 2008-2019 from patients (n = 139) diagnosed with ICC who underwent curative intent surgery without neoadjuvant chemotherapy. Samples from the discovery cohort (n = 86) were immunohistochemically analyzed on tissue microarrays (TMAs) for the expression of CD68, CD3, CD4, CD8, Foxp3, PD-L1, STAT1, and p-STAT1 in tumor core and stroma areas. Results were digitally analyzed using QuPath software and correlated with clinicopathological characteristics. For validation of TIME-related biomarkers, we performed multiplex imaging mass cytometry (IMC) in a validation cohort (n = 53).

CD68+ cells were the predominant immune cell type in the TIME of ICC. CD4+high T cell density correlated with better overall survival (OS). Prediction modeling together with validation cohort confirmed relevance of CD4+ cells, PD-L1 expression by immune cells in the stroma and N-stage on overall disease outcome. In turn, IMC analyses revealed that silent CD3+CD4+ clusters inversely impacted survival. Among annotated immune cell clusters, PD-L1 was most relevantly expressed by CD4+FoxP3+ cells. A subset of tumors with high density of immune cells ("hot" cluster) correlated with PD-L1 expression and could identify a group of candidates for immune checkpoint inhibition (ICI). Ultimately, higher levels of STAT1 expression were associated with higher lymphocyte infiltration and PD-L1 expression.
These results highlight the importance of CD4+ T cells in immune response against ICC. Secondly, a subset of tumors with "hot" TIME represents potential candidates for ICI, while stimulation of STAT1 pathway could be a potential target to turn "cold" into "hot" TIME in ICC.
Cytokine-armed vaccinia virus promotes cytotoxicity towards pancreatic carcinoma cells
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The manuscript "Cytokine-armed vaccinia virus promotes cytotoxicity towards pancreatic carcinoma cells via activation of human intermediary CD56dimCD16dim natural killer cells" by Ruonan Wang, Mengwen Hu, Isis Lozzi, Cao Z.J. Jin, Dou Ma, Katrin Splith, Jörg Mengwasser, Vincent Wolf, Linda Feldbrügge, Peter Tang, Lea Timmermann, Karl H. Hillebrandt, Marieluise Kirchner, Philipp Mertins, Georg Hilfenhaus, Christopher Neumann, Thomas Kammertoens, Johann Pratschke, Thomas Malinka, Igor Sauer, Elfriede Nössner, Zhongsheng Guo and Matthäus Felsenstein is available open access in the International Journal of Cancer.
 
Pancreatic ductal adenocarcinoma (PDAC) remains a particularly aggressive disease with few effective treatments. The PDAC tumor immune microenvironment (TIME) is known to be immune suppressive. Oncolytic viruses can increase tumor immunogenicity via immunogenic cell death(ICD). We focused on tumor-selective (vvDD) and cytokine-armed Western-Reserve vaccinia viruses (vvDD-IL2, vvDD-IL15) and infected carcinoma cell lines as well as patient-derived primary PDAC cells. In co-culture experiments, we investigated the cytotoxic response and the activation of human natural killer cells (NK). Infection and virus replication were assessed by measuring virus encoded YFP. We then analyzed intracellular signaling processes and oncolysis via in-depth proteomic analysis, immunoblotting and TUNEL assay. Following the co-culture of mock or virus infected carcinoma cell lines with allogenic PBMCs or NK cell lines, CD56+ NK cells were analyzed with respect to their activation, cytotoxicity and effector function. Both, dose- and time-dependent release of danger signals following infection was assayed. Viruses effectively entered PDAC cells and emitted YFP signals. Infection resulted in concomitant oncolysis. The proteome showed reprogramming of normally active core signaling pathways in PDAC occurred(e.g. MAPK-ERK signaling). Danger-associated molecular patterns were released upon infection and stimulated co-cultured NK cells for enhanced effector cytotoxicity. NK cell subtyping revealed enhanced numbers and activation of a rare CD56dimCD16dim population. Tumor cell killing was primarily triggered via Fas ligands rather than granule release, resulting in marked apoptosis. Cytokine-armed vaccinia viruses induced NK cell activation and enhanced cytotoxicity towards human PDAC cells in vitro. The cytokine-armed virus targets the carcinoma cells with great potential to modulate the TIME in PDAC.
DFG-funded ExTra Trial
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Prof. Dr. Nathanael Raschzok received a grant of € 1.85 million for the first three years from the German Research Foundation (Deutsche Forschungsgemeinschaft, DFG) for the Pilot, open, prospective, randomized, multicenter trial on expanding the donor pool by quality assessment of liver grafts declined for transplantation by normothermic ex vivo liver perfusion – ExTra. Co-applicants and/or significantly involved in the preparation of the study were Prof. Dr. Johann Pratschke, Prof. Dr. Igor M. Sauer, Prof. Dr. Dominik Modest, and Priv.-Doz. Dr. Simon Moosburner.

Liver transplantation in Germany is severely limited by a critical shortage of acceptable grafts and a high mortality rate on the waiting list. Furthermore, a significant number of organs are declined due to quality concerns. As demonstrated in pilot studies in the UK, Netherlands, Australia, and the United States, declined liver grafts can and should be used for transplantation after quality assessment by normothermic ex vivo liver machine perfusion (NMP).

The ExTra trial is a randomized controlled trial with a specific focus on patients with a model for end-stage liver disease (MELD) score ≤25 that are not eligible for (non)standard MELD exceptions. This cohort of patients faces an unacceptably long wait time for transplantation, which increases their mortality risk while on the waitlist. The ExTra trial aims to demonstrate that the time-to-transplant for these patients is shortened through the use of grafts that were initially declined for transplantation but fulfill specified quality criteria on normothermic ex vivo machine perfusion assessment. A total of 186 patients will be randomized in a 1:1 fashion to the experimental arm, which consists of a 12-month option to receive a liver graft that was declined by all German transplant centers but meets specified quality criteria, in addition to listing for liver transplantation through the standard allocation process. The control arm will consist of patients who are waitlisted for liver transplantation through the standard allocation process. Liver grafts that have been declined for transplantation must meet specific quality criteria. These include a maximum of 60% macrovesicular steatosis, no fibrosis greater than stage F3, and no cirrhosis. In line with previously published viability criteria for initially declined liver grafts, the decision to use or decline the graft will be made at least four hours after the start of perfusion.

The ExTra trial aims to show that by expanding the donor pool to include the ExTra option of non-transplantable organs, which appear to be usable after machine perfusion, patients without a high MELD score can be transplanted significantly faster. The ExTra trial is thus the first study worldwide in which this concept will be investigated in a randomized clinical trial. The study should make an important contribution to expanding the donor pool for liver transplants and thus ultimately help all patients on the waiting list for liver transplantation.

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Deutschlandfunk: AI in the operating theater
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How artificial intelligence supports surgeons: Planning surgical procedures, monitoring patients or predicting complications: there are already many useful applications for AI in the operating theater in research. In hospitals, the technology is still an exception. This is likely to change soon.
A Deutschlandfunk radio show/podcast by Carina Schroeder and Friederike Walch-Nasseri reports on the work in our Digital Surgery Lab (in German).
 
Artificial intelligence is revolutionizing our everyday lives. It translates texts, filters news, analyzes X-ray images and decides who gets a job. In the “KI verstehen (Understanding AI)” podcast, Deutschlandfunk provides answers to questions about dealing with AI every week.

Induced pluripotent stem cell (iPSC) line (EXSURGi001-A) from a patient homozygous for the p.Ala165Thr mutation in the MTARC1 gene
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The paper "Induced pluripotent stem cell (iPSC) line (EXSURGi001-A) from a patient homozygous for the p.Ala165Thr mutation in the MTARC1 gene" in Stem Cell Research is available open access. Authors are Peter Tang, Eriselda Keshi, Silvana Wilken, Louise Wutsdorff, Julienne Mougnekabol, Johann Pratschke, Igor M. Sauer and Nils Haep.

Metabolic dysfunction-associated fatty liver disease (MAFLD), the leading cause of end-stage liver disease in developed countries, is expected to increase over the next decade. Characterized by hepatic steatosis, MAFLD is commonly studied in animal models.
Here, we generated a human induced pluripotent stem cell (iPSC) line from a patient homozygous of the protective MTARC1 gene variant rs2642438:A.
This line displays a normal karyotype and typical pluripotent stem cell morphology and can differentiate into all three germ layers in vitro.
Extracellular NAD+ Response to Post-Hepatectomy Liver Failure: Bridging Preclinical and Clinical Findings
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Our manuscript entitled "Extracellular NAD+ Response to Post-Hepatectomy Liver Failure: Bridging Preclinical and Clinical Findings" has been accepted for publication in Communications Biology. Authors are Can Kamali, Philipp Brunnbauer, Kaan Kamali, Al-Hussein Saqr, Alexander Arnold, Gulcin Harman Kamali, Julia Babigian, Eriselda Keshi, Raphael Mohr, Matthäus Felsenstein, Simon Moosburner, Karl Hillebrandt, Jasmin Bartels, Igor Sauer, Frank Tacke, Moritz Schmelzle, Johann Pratschke, and Felix Krenzien.

Liver fibrosis progressing to cirrhosis is a major risk factor for liver cancer, impacting surgical treatment and survival. Our study investigates extracellular Nicotinamide adenine dinucleotide (eNAD+) in liver fibrosis, analyzing patients undergoing surgery and exploring NAD+'s therapeutic potential in a mouse model of extended liver resection and in vitro using 3D hepatocyte spheroids.

eNAD+ correlated with aspartate transaminase (AST) and bilirubin after liver resection (AST: r = 0.2828, p = 0.0087; Bilirubin: r = 0.2584, p = 0.0176). Post-hepatectomy liver failure (PHLF) was associated with higher eNAD+ peaks (n = 10; p = 0.0063). Postoperative eNAD+ levels decreased significantly (p < 0.05), but in advanced liver fibrosis or cirrhosis, this decline diminished or increased. NAD+ biosynthesis enzymes, NAMPT and NMNAT3, were significantly upregulated in higher fibrosis stages (p < 0.0001). NAD+ administration in 3D hepatocyte spheroids rescued hepatocytes from TNFα-induced cell death and improved viability (p < 0.0001). In mice, NAD+ treatment significantly improved survival (p = 0.0155) and liver regeneration (p = 0.0186) after extended liver resection.

eNAD+ is upregulated in PHLF, and NAD+ biosynthesis enzymes show higher expression in liver fibrosis. eNAD+ administration improved survival and hepatocyte viability, offering a potential target for future therapies.

Viscoelastic properties of colorectal liver metastases reflect the tumour cell viability
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Our paper on "Viscoelastic properties of colorectal liver metastases reflect the tumour cell viability" has been accepted for publication in Journal of Translational Medicine.

Colorectal cancer is one of the third most common cancers in the world and up to 50% of the patients develop liver metastases (CRLM) within five years. To improve and personalize therapeutic strategies, new diagnostic tools are urgently needed. An improvement could be achieved by considering biomechanical tumour properties with the implementation of magnetic resonance elastography (MRE). Our main hypothesis is that ex vivo MRE combined with histological evaluation of CRLM could provide the knowledge for using tissue mechanical properties as a diagnostic marker for cell viability in tumours.

We examined 34 CRLM samples from patients who had undergone liver resection at the Charité – Universitätsmedizin Berlin, Department of Surgery. The samples were investigated with an ex vivo MRE.  We employed a frequency range from 500 Hz to 5300 Hz, with increments of 400 Hz. For histological analysis, the samples were stained with H&E for categorization by a board-certified pathologist based on their grade of regression. The radiological response was evaluated using the RECIST-criteria.

Five samples showed major response to chemotherapy, 6 samples partial response, and 23 samples showed no response. Analysis of shear wave speed c significant correlation for frequencies including 2100 Hz and above depending on the grade of regression, indicating that low cell viability in CRLM is associated with higher tumour stiffness. Analysis of frequency-independent values of the SP-model showed a more elastic-solid behaviour at low cell viability. Our results suggest that MRE can be used to characterize the biomechanical properties associated with cell viability in CRLM, showing a higher stiffness and elastic-solid behaviour with high regression. In the future, MRE could help to improve the diagnostic tools to create an individual, tailored therapy plan for patients with CRLM.

Authors are Lisa-Marie Skrip, Simon Moosburner, Peter Tang, Jing Guo, Steffen Görner, Heiko Tzschätzsch, Clarissa Hosse, Uli Fehrenbach, Alexander Arnold, Dominik Modest, Felix Krenzien, Wenzel Schöning, Thomas Malinka, Johann Pratschke, Björn Papke, Josef A. Käs, Ingolf Sack, Igor M. Sauer, and Karl H. Hillebrandt,
Distinctive protein expression in elderly livers in a Sprague-Dawley rat model of normothermic ex vivo liver machine perfusion
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Our manuscript “Distinctive protein expression in elderly livers in a Sprague-Dawley rat model of normothermic ex vivo liver machine perfusion” has been published in the latest issue of the European Journal of Medical Research,
Authors are Maximilian Zimmer, Karl H. Hillebrandt, Nora M. Roschke, Steffen Lippert, Oliver Klein, Grit Nebrich, Joseph M.G.V. Gassner, Felix Strobl, Johann Pratschke, Felix Krenzien, Igor M. Sauer, Nathanael Raschzok, and Simon Moosburner.

Liver grafts are frequently declined due to high donor age or age mismatch with the recipient. To improve the outcome of marginal grafts, we aimed to characterize the performance of elderly vs. young liver grafts in a standardized rat model of normothermic ex vivo liver machine perfusion (NMP).

Livers from Sprague-Dawley rats aged 3 or 12 months were procured and perfused for 6 h using a rat NMP system or collected as a reference group (n = 6/group). Tissue, bile, and perfusate samples were used for biochemical, and proteomic analyses.

All livers cleared lactate during perfusion and continued to produce bile after 6 h of perfusion (614 mg/h). Peak urea levels in 12-month-old animals were higher than in younger animals. Arterial and portal venous pressure, bile production and pH did not differ between groups. Proteomic analysis identified a total of 1477 proteins with oxidoreductase and catalytic activity dominating the gene ontology analysis. Proteins such as aldehyde dehydrogenase 1A1 and 2-Hydroxyacid oxidase 2 were significantly more present in livers of older age.

Young and elderly liver grafts exhibited similar viability during NMP, though proteomic analyses indicated that older grafts are less resilient to oxidative stress. Our study is limited by the elderly animal age, which corresponds to mature but not elderly human age typically seen in marginal human livers. Nevertheless, reducing oxidative stress could be a promising therapeutic target in the future.
Thrombogenicity assessment of perfusable tissue engineered constructs: a systematic review
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Our systematic review on "Thrombogenicity assessment of perfusable tissue engineered constructs" has been accepted for publication in Tissue Engineering, Part B, and is available online ahead of print.

Vascular surgery faces a critical demand for novel vascular grafts that are biocompatible and thromboresistant. This urgency particularly applies to bypass operations involving small caliber vessels. In the realm of tissue engineering, the development of fully vascularized organs holds great promise as a solution to organ shortage for transplantation. To achieve this, it is imperative to (re-)construct a biocompatible and non-thrombogenic vascular network within these organs. In this systematic review, we identify, classify and discuss basic principles and methods used to perform in vitro/ex vivo dynamic thrombogenicity testing of perfusable tissue engineered organs and tissues. We conducted a pre-registered systematic review of studies published in the last 23 years according to PRISMA-P Guidelines, comprising a systematic data extraction, in-depth analysis and risk of bias assessment of 116 included studies. We identified shaking (n=28), flow loop (n=17), ex vivo (arterio-venous shunt, n=33) and dynamic in vitro models (n=38) as main approaches for thrombogenicity assessment. This comprehensive review unveils a prevalent lack of standardization and serves as a valuable guide in the design of standardized experimental setups.

Authors are Luna M. Haderer, Yijun Zhou, Peter Tang, Assal Daneshgar, Brigitta Globke, Felix Krenzien, Anja Reutzel-Selke, Marie Weinhart, Johann Pratschke, Igor M. Sauer, Karl H. Hillebrandt, and Eriselda Keshi.
Fritz Linder Prize 2024
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At the 141st German Surgical Congress (DCK 2024), Dr. Friederike Martin received the Fritz Linder Prize 2024 of the German Society of Surgery! The Forum Prize is awarded to the first author of the best presentation within the Surgical Forum. Friederike was honored for her work "Aging is transferable: Old Organs Accelerate Aging and Induce Senescence in Young Recipients“.
In Leipzig, she presented the results of her DFG-funded work with the phantastic team in the laboratory of Stefan G. Tullius, MD, PhD, Division of Transplant Surgery, Department of Surgery, Brigham and Women's Hospital, Harvard University Medical School, in Boston. Her exciting results are another example of the fruitful axis between Stefan's laboratory and the Experimental Surgery in Berlin, which is funded by the Einstein Foundation Berlin!

Congratulations!
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© 2025 Prof. Dr. Igor M. Sauer | Charité - Universitätsmedizin Berlin | Disclaimer

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