Your search keyword '"Alexandre Trapp"' showing total 13 results

1. Epigenetic aging of the demographically non-aging naked mole-rat

Author

Csaba Kerepesi, Margarita V. Meer, Julia Ablaeva, Vince G. Amoroso, Sang-Goo Lee, Bohan Zhang, Maxim V. Gerashchenko, Alexandre Trapp, Sun Hee Yim, Ake T. Lu, Morgan E. Levine, Andrei Seluanov, Steve Horvath, Thomas J. Park, Vera Gorbunova, and Vadim N. Gladyshev

Subjects

Science

Abstract

The exceptionally long-lived naked mole-rat is characterized by the lack of increased mortality with aging. Here the authors perform epigenetic studies to show that naked mole-rats epigenetically age despite their non-increasing mortality rate.

Published

2022

2. ClockBase: a comprehensive platform for biological age profiling in human and mouse

Author

Kejun Ying, Alexander Tyshkovskiy, Alexandre Trapp, Hanna Liu, Mahdi Moqri, Csaba Kerepesi, and Vadim N. Gladyshev

Abstract

Aging represents the greatest risk factor for chronic diseases and mortality, but to understand it we need the ability to measure biological age. In recent years, many machine learning algorithms based on omics data, termed aging clocks, have been developed that can accurately predict the age of biological samples. However, there is currently no resource for systematic profiling of biological age. Here, we describeClockBase, a platform that features biological age estimates based on multiple aging clock models applied to more than 2,000 DNA methylation datasets and nearly 200,000 samples. We further provide an online interface for statistical analyses and visualization of the data. To show how this resource could facilitate the discovery of biological age-modifying factors, we describe a novel anti-aging drug candidate, zebularine, which reduces the biological age estimates based on all aging clock models tested. We also show that pulmonary fibrosis accelerates epigenetic age. Together,ClockBaseprovides a resource for the scientific community to quantify and explore biological ages of samples, thus facilitating discovery of new longevity interventions and age-accelerating conditions.

Published

2023

3. TIME-Seq Enables Highly-Efficient Epigenetic Age Predictions in Large-Scale Human and Mouse Longevity Studies

Author

Patrick Griffin, Alice E. Kane, Alexandre Trapp, Jien Li, Matthew Arnold, Jesse R. Poganik, Ryan J. Conway, Maeve S. McNamara, Margarita Meer, Noah Hoffman, Joao A. Amorim, Xiao Tian, Michael R. MacArthur, Sarah J. Mitchell, Amber L. Mueller, Colleen Carmody, Daniel L. Vera, Csaba Kerepesi, Nicole Noren Hooten, James R. Mitchell, Michele K. Evans, Vadim N. Gladyshev, and David A. Sinclair

Published

2023

4. Characterization of naked mole‐rat hematopoiesis reveals unique stem and progenitor cell patterns and neotenic traits

Author

Stephan Emmrich, Alexandre Trapp, Frances Tolibzoda Zakusilo, Maggie E Straight, Albert K Ying, Alexander Tyshkovskiy, Marco Mariotti, Spencer Gray, Zhihui Zhang, Michael G Drage, Masaki Takasugi, Jan‐Henning Klusmann, Vadim N Gladyshev, Andrei Seluanov, and Vera Gorbunova

Subjects

Adult, Aging, General Immunology and Microbiology, Mole Rats, Stem Cells, General Neuroscience, Articles, Middle Aged, General Biochemistry, Genetics and Molecular Biology, Hematopoiesis, Mice, Phenotype, Animals, Humans, Molecular Biology

Abstract

Naked mole rats (NMRs) are the longest-lived rodents yet their stem cell characteristics remain enigmatic. Here, we comprehensively mapped the NMR hematopoietic landscape and identified unique features likely contributing to longevity. Adult NMRs form red blood cells in spleen and marrow, which comprise a myeloid bias toward granulopoiesis together with decreased B-lymphopoiesis. Remarkably, youthful blood and marrow single-cell transcriptomes and cell compositions are largely maintained until at least middle age. Similar to primates, the primitive stem and progenitor cell (HSPC) compartment is marked by CD34 and THY1. Stem cell polarity is seen for Tubulin but not CDC42, and is not lost until 12 years of age. HSPC respiration rates are as low as in purified human stem cells, in concert with a strong expression signature for fatty acid metabolism. The pool of quiescent stem cells is higher than in mice, and the cell cycle of hematopoietic cells is prolonged. By characterizing the NMR hematopoietic landscape, we identified resilience phenotypes such as an increased quiescent HSPC compartment, absence of age-related decline, and neotenic traits likely geared toward longevity.

Published

2022

5. Meeting Report: Aging Research and Drug Discovery

Author

Esther Meron, Maria Thaysen, Suzanne Angeli, Adam Antebi, Nir Barzilai, Joseph A. Baur, Simon Bekker-Jensen, Maria Birkisdottir, Evelyne Bischof, Jens Bruening, Anne Brunet, Abigail Buchwalter, Filipe Cabreiro, Shiqing Cai, Brian H. Chen, Maria Ermolaeva, Collin Y. Ewald, Luigi Ferrucci, Maria Carolina Florian, Kristen Fortney, Adam Freund, Anastasia Georgievskaya, Vadim N. Gladyshev, David Glass, Tyler Golato, Vera Gorbunova, Jan Hoejimakers, Riekelt H. Houtkooper, Sibylle Jager, Frank Jaksch, Georges Janssens, Martin Borch Jensen, Matt Kaeberlein, Gerard Karsenty, Peter de Keizer, Brian Kennedy, James L. Kirkland, Michael Kjaer, Guido Kroemer, Kai-Fu Lee, Jean-Marc Lemaitre, David Liaskos, Valter D. Longo, Yu-Xuan Lu, Michael R. MacArthur, Andrea B. Maier, Christina Manakanatas, Sarah J. Mitchell, Alexey Moskalev, Laura Niedernhofer, Ivan Ozerov, Linda Partridge, Emmanuelle Passegué, Michael A. Petr, James Peyer, Dina Radenkovic, Thomas A. Rando, Suresh Rattan, Christian G. Riedel, Lenhard Rudolph, Ruixue Ai, Manuel Serrano, Björn Schumacher, David A. Sinclair, Ryan Smith, Yousin Suh, Pam Taub, Alexandre Trapp, Anne-Ulrike Trendelenburg, Dario Riccardo Valenzano, Kris Verburgh, Eric Verdin, Jan Vijg, Rudi G.J. Westendorp, Alessandra Zonari, Daniela Bakula, Alex Zhavoronkov, Morten Scheibye-Knudsen, Neurosciences, ACS - Diabetes & metabolism, ACS - Heart failure & arrhythmias, Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory for General Clinical Chemistry

Subjects

Aging, Drug discovery, Physiology, Longevity, Oncology and Carcinogenesis, Drugs, Conference, Cell Biology, drug discovery, longevity, Ai, Envelliment, AI, Chronic diseases, Malalties cròniques, Biochemistry and Cell Biology, Medicaments, conference, Developmental Biology

Abstract

Aging is the single largest risk factor for most chronic diseases, and thus possesses large socioeconomic interest to continuously aging societies. Consequently, the field of aging research is expanding alongside a growing focus from the industry and investors in aging research. This year's 8th Annual Aging Research and Drug Discovery (ARDD) meeting was organized as a hybrid meeting from August 30th to September 3rd 2021 with more than 130 attendees participating on-site at the Ceremonial Hall at University of Copenhagen, Denmark, and 1800 engaging online. The conference comprised of presentations from 75 speakers focusing on new research in topics including mechanisms of aging and how these can be modulated as well as the use of AI and new standards of practices within aging research. This year, a longevity workshop was included to build stronger connections with the clinical community., Aging, 14 (2), ISSN:1945-4589

Published

2022

6. Emerging rejuvenation strategies—Reducing the biological age

Author

Bohan Zhang, Alexandre Trapp, Csaba Kerepesi, and Vadim N. Gladyshev

Subjects

Aging, rejuvenation, biomarkers, Humans, Cell Biology, Review, epigenetic clocks

Abstract

Several interventions have recently emerged that were proposed to reverse rather than just attenuate aging, but the criteria for what it takes to achieve rejuvenation remain controversial. Distinguishing potential rejuvenation therapies from other longevity interventions, such as those that slow down aging, is challenging, and these anti‐aging strategies are often referred to interchangeably. We suggest that the prerequisite for a rejuvenation intervention is a robust, sustained, and systemic reduction in biological age, which can be assessed by biomarkers of aging, such as epigenetic clocks. We discuss known and putative rejuvenation interventions and comparatively analyze them to explore underlying mechanisms., Emerging interventions have suggested that biological aging can be reversed rather than just attenuated, but the criteria for what it takes to achieve rejuvenation remain controversial. In this review, we discuss known and putative rejuvenation interventions, exploring their connections within the context of aging biomarkers. We suggest that the prerequisite for classifying an intervention as rejuvenating is a robust and reproducible reduction in biological age, which can be assessed by high‐dimensional trackers of aging such as epigenetic clocks.

Published

2021

7. Multi-omic rejuvenation and lifespan extension upon exposure to youthful circulation

Author

Alexandre Trapp, Anastasia V. Shindyapina, Lu A, Alexander Tyshkovskiy, David E Lee, L. H. McKay, Gurpreet S. Baht, James P. White, Steve Horvath, Sergey E. Dmitriev, Vadim N. Gladyshev, Csaba Kerepesi, Akshay Bareja, and Bohan Zhang

Subjects

Transcriptome, Parabiosis, Period (gene), Epigenetics, Biology, Omics, Heterochrony, Rejuvenation, Epigenomics, Cell biology

Abstract

SUMMARYHeterochronic parabiosis (HPB) is known for its functional rejuvenation effects across several mouse tissues. However, its impact on the biological age of organisms and their long-term health remains unknown. Here, we performed extended (3-month) HPB, followed by a 2-month detachment period of anastomosed pairs. Old detached mice exhibited improved physiological parameters and lived longer than control isochronic mice. HPB drastically reduced the biological age of blood and liver based on epigenetic analyses across several clock models on two independent platforms; remarkably, this rejuvenation effect persisted even after 2 months of detachment. Transcriptomic and epigenomic profiles of anastomosed mice showed an intermediate phenotype between old and young, suggesting a comprehensive multi-omic rejuvenation effect. In addition, old HPB mice showed transcriptome changes opposite to aging, but akin to several lifespan-extending interventions. Altogether, we reveal that long-term HPB can decrease the biological age of mice, in part through long-lasting epigenetic and transcriptome remodeling, culminating in the extension of lifespan and healthspan.

Published

2021

8. TIME-Seq Enables Scalable and Inexpensive Epigenetic Age Predictions

Author

Patrick T Griffin, Alice E Kane, Alexandre Trapp, Jien Li, Matthew Arnold, Jesse R Poganik, Maeve S McNamara, Margarita V Meer, Noah Hoffman, João Amorim, Xiao Tian, Michael R MacArthur, Sarah J Mitchell, Amber L Mueller, Colleen Carmody, Daniel L Vera, Csaba Kerepesi, Nicole Noren Hooten, James R Mitchell, Michele K Evans, Vadim N Gladyshev, and David A Sinclair

Subjects

Computer science, Scalability, DNA methylation, Epigenetics, Computational biology, Biomarker Analysis

Abstract

Epigenetic “clocks” based on DNA methylation (DNAme) have emerged as the most robust and widely employed aging biomarkers, but conventional methods for applying them are expensive and laborious. Here, we developTagmentation-based Indexing forMethylationSequencing (TIME-Seq), a highly multiplexed and scalable method for low-cost epigenetic clocks. Using TIME-Seq, we applied multi-tissue and tissue-specific epigenetic clocks to over 1,600 mouse DNA samples. We also discovered a novel approach for age prediction from shallow sequencing (e.g., 10,000 reads) by adaptingscAgefor bulk measurements. In benchmarking experiments, TIME-Seq performed favorably against prevailing methods and could quantify the effects of interventions thought to accelerate, slow, and reverse aging in mice. Finally, we built and validated a highly accurate human blood clock from 1,056 demographically representative individuals. Our methods increase the scalability and reduce the cost of epigenetic age predictions by more than 100-fold, enabling accurate aging biomarkers to be applied in more large-scale animal and human studies.

Published

2021

9. Ectopic cervical thymi and no thymic involution until midlife in naked mole rats

Author

Alexandre Trapp, Vera Gorbunova, Andrei Seluanov, Zhengdong Zhang, Xuming Zhou, Stephan Emmrich, Quanwei Zhang, Vadim N. Gladyshev, Ellen M. Irving, Frances Tolibzoda Zakusilo, and Michael G. Drage

Subjects

Male, Aging, medicine.medical_specialty, Longevity, T‐lymphocytes, Thymus Gland, Immune system, thymus, Internal medicine, Mole, medicine, Animals, Cytotoxic T cell, Lymphopoiesis, Naked mole-rat, immunosenescence, Thymic involution, biology, Mole Rats, naked mole rat, lymphopoiesis, Cell Biology, Immunosenescence, biology.organism_classification, Original Papers, Rats, Disease Models, Animal, Endocrinology, CD4‐CD8 Ratio, Original Article, CD8

Abstract

Immunosenescence is a hallmark of aging and manifests as increased susceptibility to infection, autoimmunity, and cancer in the elderly. One component of immunosenescence is thymic involution, age‐associated shrinkage of the thymus, observed in all vertebrates studied to date. The naked mole rat (Heterocephalus glaber) has become an attractive animal model in aging research due to its extreme longevity and resistance to disease. Here, we show that naked mole rats display no thymic involution up to 11 years of age. Furthermore, we found large ectopic cervical thymi in addition to the canonical thoracic thymus, both being identical in their cell composition. The developmental landscape in naked mole rat thymi revealed overt differences from the murine T‐cell compartment, most notably a decrease of CD4+/CD8+ double‐positive cells and lower abundance of cytotoxic effector T cells. Our observations suggest that naked mole rats display a delayed immunosenescence. Therapeutic interventions aimed at reversing thymic aging remain limited, underscoring the importance of understanding the cellular and molecular mechanisms behind a sustained immune function in the naked mole rat., Naked mole‐rats do not display thymic involution by 11 years of age, in contrast to continuous thymus shrinkage in mice. The key markers of youthful thymus function Aire and Foxn1 decrease with age in mice, but are maintained in naked mole‐rats. Characterization of organ integrity and function in >30 year‐old naked mole‐rats could provide a blueprint to naturally maintain a healthy thymus.

Published

2021

10. Ectopic cervical thymi and no thymic involution until midlife in naked mole-rats

Author

Zhengdong Zhang, Andrei Seluanov, Frances Tolibzoda Zakusilo, Michael G. Drage, Alexandre Trapp, Ellen M. Irving, Stephan Emmrich, Quanwei Zhang, Vadim N. Gladyshev, Vera Gorbunova, and Xuming Zhou

Subjects

medicine.medical_specialty, Thymic involution, biology, T cell, Immunosenescence, medicine.disease_cause, biology.organism_classification, Autoimmunity, medicine.anatomical_structure, Immune system, Endocrinology, Internal medicine, medicine, Cytotoxic T cell, CD8, Naked mole-rat

Abstract

Immunosenescence is a hallmark of aging and manifests as increased susceptibility to infection, autoimmunity, and cancer in the elderly. One component of immunosenescence is thymic involution, age-associated shrinkage of the thymus, observed in all vertebrates studied to date. The naked mole-rat (Heterocephalus glaber) has become an attractive animal model in aging research due to its extreme longevity and resistance to disease. Here we show that naked mole rats display no thymic involution up to 11 years of age. Furthermore, we found large ectopic cervical thymi in addition to the canonical thoracic thymus, both being identical in their cell composition. The developmental landscape in naked mole-rat thymi revealed overt differences from the murine T cell compartment, most notably a decrease of CD4+/CD8+ double-positive cells and lower abundance of cytotoxic effector T cells. Our observations suggest that naked mole rats display a delayed immunosenescence. Therapeutic interventions aimed at reversing thymic aging remain limited, underscoring the importance of understanding the cellular and molecular mechanisms behind a sustained immune function in the naked mole rat.

Published

2021

11. Naked Mole-Rat Hematopoietic Stem and Progenitors are Highly Quiescent with an Inherent Myeloid Bias

Author

Zhonghe Ke, Maggie E. Straight, Michael G. Drage, Marco Mariotti, Spencer Gray, Jan-Henning Klusmann, Stephan Emmrich, Frances Tolibzoda Zakusilo, Zhihui Zhang, Alexandre Trapp, Andrei Seluanov, Vadim N. Gladyshev, Vera Gorbunova, and Masaki Takasugi

Subjects

Haematopoiesis, Myeloid, medicine.anatomical_structure, Leukopoiesis, CD34, medicine, Cell cycle, Biology, Progenitor cell, Stem cell, Granulopoiesis, Cell biology

Abstract

Naked mole-rats (NMRs) are the longest-lived rodents yet their stem cell characteristics remain enigmatic. Here we comprehensively mapped the NMR hematopoietic landscape and identified unique features likely contributing to longevity. Adult NMRs form red blood cells in spleen and marrow, which is a neotenic trait. A myeloid bias towards granulopoiesis in concert with decreased B-lymphopoiesis defines the marrow composition, resembling fetal leukopoiesis. Very similar to primates, the primitive stem cell compartment is marked by CD34 and THY1. Remarkably, stem and progenitor respiration rates are as low as in human cells, while NMR cells show a strong expression signature for fatty acid metabolism. The pool of quiescent stem cells is higher than in mice, and the cell cycle of hematopoietic cells is prolonged. Our work provides a platform to study immunology and stem cell biology in an animal model of exceptional longevity.TeaserJuvenile features of hematopoiesis shape the blood system of the longest-lived rodent.

Published

2021

12. Epigenetic clocks reveal a rejuvenation event during embryogenesis followed by aging

Author

Bohan Zhang, Csaba Kerepesi, Sang-Goo Lee, Vadim N. Gladyshev, and Alexandre Trapp

Subjects

0303 health sciences, Multidisciplinary, Offspring, Event (relativity), Embryogenesis, SciAdv r-articles, Biology, Prenatal development, Germline, 03 medical and health sciences, 0302 clinical medicine, Evolutionary biology, Genetics, Epigenetics, Induced pluripotent stem cell, 030217 neurology & neurosurgery, Research Articles, Rejuvenation, 030304 developmental biology, Research Article, Developmental Biology

Abstract

Epigenetic clocks reveal a rejuvenation event during embryogenesis followed by aging., The notion that the germ line does not age goes back to the 19th-century ideas of August Weismann. However, being metabolically active, the germ line accumulates damage and other changes over time, i.e., it ages. For new life to begin in the same young state, the germ line must be rejuvenated in the offspring. Here, we developed a multi-tissue epigenetic clock and applied it, together with other aging clocks, to track changes in biological age during mouse and human prenatal development. This analysis revealed a significant decrease in biological age, i.e., rejuvenation, during early stages of embryogenesis, followed by an increase in later stages. We further found that pluripotent stem cells do not age even after extensive passaging and that the examined epigenetic age dynamics is conserved across species. Overall, this study uncovers a natural rejuvenation event during embryogenesis and suggests that the minimal biological age (ground zero) marks the beginning of organismal aging.

Published

2021

13. The hematopoietic landscape at single-cell resolution reveals unexpected stem cell features in naked mole-rats

Author

Maggie E. Straight, Vera Gorbunova, Masaki Takasugi, Alexandre Trapp, Andrei Seluanov, Marco Mariotti, Vadim N. Gladyshev, and Stephan Emmrich

Subjects

medicine.diagnostic_test, Cell, Spleen, Biology, medicine.disease_cause, Cell biology, Flow cytometry, Haematopoiesis, medicine.anatomical_structure, medicine, Erythropoiesis, Involution (medicine), Stem cell, Carcinogenesis

Abstract

SUMMARYNaked mole-rats are the longest-lived rodents endowed with resistance to cancer and age-related diseases, yet their stem cell characteristics remain enigmatic. We profiled the naked mole-rat hematopoietic system down to single-cell resolution, and identified several unique features likely contributing to longevity. In adult naked mole-rats red blood cells are formed in spleen and marrow, a neotenic feature beneficial for hypoxic environments and to prevent anemia. Platelet numbers are lower compared to short-lived mice, which may preclude age-related platelet increase and thrombosis. T cells mature in thymus and lymph nodes, providing a supply of T cells after age-related thymus involution. The pool of quiescent stem cells is higher than in mice, and HSCs overexpress an oxidative phosphorylation signature, revealing a new paradigm of stem cell metabolism to benefit longevity and oppose oncogenesis. Our work provides a platform to study immunology and stem cell biology in an animal model of healthy aging.HIGHLIGHTSFlow cytometry labelling panel to purify viable naked mole-rat HSPCsThe spleen as the major site of erythropoiesis in the naked mole-ratNaked mole-rats show extrathymic T-cell development under homeostatic conditionsNaked mole-rat hematopoietic stem cells (HSCs) have high OXPHOS activity

Published

2019