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182,221 results on '"Mammals"'

1. Modularity and Development: The Case of Spatial Reorientation.

Author

Hermer, Linda and Spelke, Elizabeth

Abstract

Investigated the development of reorientation abilities in humans in contrast to other mammals. Findings support the domain specificity of human's core cognitive abilities, the conservation of cognitive abilities across related species and over the course of human development, and the developmental processes by which core abilities are extended to permit more flexible, uniquely human kinds of problem solving. (AA)

Published
1996

3. The Concept Map as a Research and Evaluation Tool: Further Evidence of Validity.

Author

Markham, Kimberly M.

Abstract

Describes a study that examines the extent to which differences exist in the concept maps of advanced college biology majors (n=25) and beginning nonmajors (n=25) in the domain of mammals. Results indicate that the concept maps of biology majors are structurally more complex than those of nonmajors. (ZWH)

Published
1994

4. Children's Information Skills: Making Effective Use of Multimedia Sources.

Author

Oliver, Ron and Perzylo, Lesa

Abstract

Describes a study of 12-year-old elementary school students in Western Australia that was conducted to investigate the students' capacity to extract meaningful information from nontext sources when using a hypermedia CD-ROM package in an inquiry activity. (34 references) (LRW)

Published
1994

5. Powdertracking Small Mammals: An Illuminating Exercise for Undergraduates.

Author

Hoagland, Donald B.

Abstract

Describes an easy-to-use, inexpensive field trip/laboratory exercise designed to delineate the home ranges of small animals. Students participate in the design of the exercise; collection, analysis, and interpretation of data; and the presentation of results. Contains 19 references. (DDR)

Published
1993

6. An Investigation of Children's Use of a Multimedia CD-ROM Product for Information Retrieval.

Author

Perzylo, Lisa and Oliver, Ron

Abstract

Examines the efficacy and utility of the National Geographic Society's Mammals Multimedia Encyclopedia, an interactive multimedia CD-ROM, used by 12-year-old elementary students as the principal source for a summary paper. Existing research, project methodology, student information seeking and recording strategies, form of information accessed, and outcomes are covered. (14 references) (KRN)

Published
1992

7. Developmental Changes within the Structure of the Mammal Domain.

Author

Johnson, Kathy E.

Abstract

Judgments of similarity among mammals, including humans, were elicited from 7 and 10 year olds and adults. Results partially supported a consensus model of shared cultural knowledge. Patterns of deviation from the model appeared between children and adults because of the emergence of a primate category after age 10. (BC)

Published
1992

8. Experience as a Component of Normal Development: Evolutionary Considerations.

Author

Greenough, William T.

Abstract

Suggests that experiential canalization is appropriately applied to constraints caused by the behavior of an organism or members of its species. When other aspects of the environment propel the organism to develop in certain ways, this process reflects adaptation to the environment. Conditions for evolution of experience as a guide to development are considered. (BC)

Published
1991

9. A Thematic Literary Unit: Using Literature across the Curriculum in an Elementary Classroom.

Author

North Dakota Univ., Grand Forks. Center for Teaching and Learning. and Vivian, Diane M.

Abstract

"Think Big" is a thematic literary unit, using literature about elephants in a holistic way and attempting to cross the curriculum into the content areas of science and math. It is a way of expanding the basal reading series and providing appropriate and supportive instruction in a cooperative, more interactive learning environment. To assess what students already knew and to stimulate interest, students were informally given an elephant fact test and brainstormed about elephants. After reading non-fiction books about elephants, the factual information was confirmed and reviewed by use of cloze procedure, semantic mapping, and reviewing the initial brainstorming words and phrases. Students participated in literature groups to discuss and retell fiction stories. Students spent time daily in writing workshops which provided for practice and sharing of their written responses to literature. They made up their own stories about elephants and collected elephant jokes and riddles. Students responded to the books about elephants that they read at home in a variety of ways. Math skills were used to generate new meaning for the concepts of size and weight used in the elephant fiction and non-fiction materials. During science, students compared and researched the size of mammals. Reading, writing, and literature were used as a vehicle through which learning occurred. (Three figures showing the cloze procedure, semantic mapping, and fiction discussion sheets are included. Eleven references are included as well as 13 tradebook references used in the thematic unit.) (MG)

Published
1990

10. All about Mammals. Animal Life for Children. [Videotape].

Abstract

In this videotape, students learn more about the characteristics of common warm-blooded mammals and what makes them different from other animals. Children also find out how humans are more advanced in structure than other mammals, but how they still share the same basic traits. This videotape correlates to the following National Science Education Standards for Life Science: characteristics of organisms; life cycles of organisms; and organisms and environments. The videotape is accompanied by a teacher's guide and a hands-on student experiment. (CCM)

Published
2000

11. Mammals. Animal Life in Action[TM]. Schlessinger Science Library. [Videotape].

Abstract

This 23-minute videotape for grades 5-8, presents the myriad of animal life that exists on the planet. Students can view and perform experiments and investigations that help explain animal traits and habits. Students learn about the incredible variety of mammals and how they survive in different environments while discovering which characteristics make these animals more advanced than others. A hands-on experiment in which students simulate how the amazing natural insulation of blubber keeps whales warm in cold water is included. This program is based on the concepts outlined in the National Science Education Standards for Life Science: (1) structure and function in living systems; (2) reproduction and heredity; (3) regulation and behavior; (4) populations and ecosystems; and (5) diversity and adaptations of organisms. A teacher's guide is also included. (ASK)

Published
1999

12. Mammals in Our Lives.

Abstract

Examines how humans have treated mammals throughout history. Identifies both the problems facing animals and the corrective efforts that are currently underway. Student activities include stories, games, a scavenger hunt, a mural, a puzzle, and a survey focusing on mammals. (ML)

Published
1986

13. Appendix.

Abstract

Presents: (1) a list of 23 questions about mammals (with answers); (2) a glossary with mammal-related words; and (3) a bibliography listing reference books, children's books, audiovisual aids, field guides, activity sources, and mammal-related articles appearing in "Ranger Rick" magazine. (ML)

Published
1986

14. Staying Alive and Fitting In.

Abstract

Examines the various adaptations, food-getting strategies, and defense mechanisms that mammals have employed in surviving from one season to the next. Contains exercises in simulating animal movements and in identifying animal tracks and habitats. (ML)

Published
1986

15. Family Life.

Abstract

Focuses on various aspects of mammal family life ranging from ways different species are born to how different mammals are raised. Learning activities include making butter from cream, creating birth announcements for mammals, and playing a password game on family life. (ML)

Published
1986

16. What Makes a Mammal a Mammal?

Abstract

Describes the distinctive characteristics of mammals and compares modern mammals with their prehistoric relatives as well as with other animal groups. Includes activities and ready-to-copy games, illustrations, and diagrams of wolves, vertebrates, and past and present mammals. (ML)

Published
1986

17. Bats.

Abstract

Presents information about bats, including definitions and descriptions of the characteristics of bats. Provides teaching activities such as "Bat and Math,""A Bat Like That,""Bat Party,""Ears in the Dark," and "The Big Bat Mystery." Contains reproducible handouts and quizzes. (TW)

Published
1986

18. Mammals With Hooves.

Abstract

Presents information about mammals that have hooves, including definitions and descriptions of their characteristics. Contains teaching activities such as "Build a Paper Pachyderm,""Do the Funky Trunk Dance,""A Horse of a Different Color," and "Horns and Antlers." A reproducible quiz is also provided. (TW)

Published
1986

19. Creationism and Mammal Origins.

Author

Cain, Joseph Allen

Abstract

Questions a hypothesis from creation science dealing with mammals. Claims that, when tested, the hypothesis fails in two ways. (TW)

Published
1988

20. Our Allotted Lifetimes

Author

Gould, Stephen Jay

Abstract

It is suggested that measured by the internal clock of heartbeats or breathing, all mammals live a similar lifespan. This is based on the fact that mammals, regardless of size, breathe about 200 million times in their lifetime at a rate of 1 breath for every 4 heartbeats. (AJ)

Published
1977

22. Hands-On Science: Cool Ways to Teach about Warm-Blooded Animals.

Author

VanCleave, Janice

Abstract

Presents three activities for teaching elementary students about the built-in mechanisms that help warm-blooded animals maintain constant internal body temperatures. The activities help students understand why humans sweat, why dogs pant, and why blubber keeps whales warm in frigid water. (SM)

Published
1998

23. Crafty Corner.

Abstract

Presents step-by-step procedures for two arts and crafts lessons that focus on mammals. Directions are offered for making mammal-shaped dough magnets and also for creating mammal note cards. Examples of each are illustrated. (ML)

Published
1986

24. The History of Mammals

Author

Brightman, F. H.

Abstract

Briefly discusses the origin and radiation of mammals through the different geologic eras. (PEB)

Published
1973

25. Fundamental equations linking methylation dynamics to maximum lifespan in mammals.

Author

Horvath, Steve, Zhang, Joshua, Haghani, Amin, Lu, Ake, and Fei, Zhe

Subjects
Animals, DNA Methylation, Longevity, Mammals, Dogs, Chromatin, Promoter Regions, Genetic, Aging, Humans
Abstract

We describe a framework that addresses concern that the rate of change in any aging biomarker displays a trivial inverse relation with maximum lifespan. We apply this framework to methylation data from the Mammalian Methylation Consortium. We study the relationship of lifespan with the average rate of change in methylation (AROCM) from two datasets: one with 90 dog breeds and the other with 125 mammalian species. After examining 54 chromatin states, we conclude three key findings: First, a reciprocal relationship exists between the AROCM in bivalent promoter regions and maximum mammalian lifespan: AROCM ∝ 1/MaxLifespan. Second, the correlation between average methylation and age bears no relation to maximum lifespan, Cor(Methyl,Age) ⊥ MaxLifespan. Third, the rate of methylation change in young animals is related to that in old animals: Young animals AROCM ∝ Old AROCM. These findings critically hinge on the chromatin context, as different results emerge in other chromatin contexts.

Published
2024

26. Mammals show faster recovery from capture and tagging in human-disturbed landscapes.

Author

Stiegler, Jonas, Gallagher, Cara, Hering, Robert, Müller, Thomas, Tucker, Marlee, Apollonio, Marco, Arnold, Janosch, Barker, Nancy, Barthel, Leon, Bassano, Bruno, Beest, Floris, Belant, Jerrold, Berger, Anne, Beyer, Dean, Bidner, Laura, Blake, Stephen, Börner, Konstantin, Brivio, Francesca, Brogi, Rudy, Buuveibaatar, Bayarbaatar, Cagnacci, Francesca, Dekker, Jasja, Dentinger, Jane, Duľa, Martin, Duquette, Jarred, Eccard, Jana, Evans, Meaghan, Ferguson, Adam, Fichtel, Claudia, Ford, Adam, Fowler, Nicholas, Gehr, Benedikt, Getz, Wayne, Goheen, Jacob, Goossens, Benoit, Grignolio, Stefano, Haugaard, Lars, Hauptfleisch, Morgan, Heim, Morten, Heurich, Marco, Hewison, Mark, Isbell, Lynne, Janssen, René, Jarnemo, Anders, Jeltsch, Florian, Miloš, Jezek, Kaczensky, Petra, Kamiński, Tomasz, Kappeler, Peter, Kasper, Katharina, Kautz, Todd, Kimmig, Sophia, Kjellander, Petter, Kowalczyk, Rafał, Kramer-Schadt, Stephanie, Kröschel, Max, Krop-Benesch, Anette, Linderoth, Peter, Lobas, Christoph, Lokeny, Peter, Lührs, Mia-Lana, Matsushima, Stephanie, McDonough, Molly, Melzheimer, Jörg, Morellet, Nicolas, Ngatia, Dedan, Obermair, Leopold, Olson, Kirk, Patanant, Kidan, Payne, John, Petroelje, Tyler, Pina, Manuel, Piqué, Josep, Premier, Joseph, Pufelski, Jan, Pyritz, Lennart, Ramanzin, Maurizio, Roeleke, Manuel, Rolandsen, Christer, Saïd, Sonia, Sandfort, Robin, Schmidt, Krzysztof, Schmidt, Niels, Scholz, Carolin, Schubert, Nadine, Selva, Nuria, Sergiel, Agnieszka, Serieys, Laurel, Silovský, Václav, Slotow, Rob, Sönnichsen, Leif, Solberg, Erling, Stelvig, Mikkel, Street, Garrett, Sunde, Peter, Svoboda, Nathan, Thaker, Maria, Tomowski, Maxi, Ullmann, Wiebke, and Vanak, Abi

Subjects
Animals, Humans, Mammals, Ecosystem, Male, Female, Locomotion, Herbivory, Animals, Wild, Behavior, Animal, Species Specificity
Abstract

Wildlife tagging provides critical insights into animal movement ecology, physiology, and behavior amid global ecosystem changes. However, the stress induced by capture, handling, and tagging can impact post-release locomotion and activity and, consequently, the interpretation of study results. Here, we analyze post-tagging effects on 1585 individuals of 42 terrestrial mammal species using collar-collected GPS and accelerometer data. Species-specific displacements and overall dynamic body acceleration, as a proxy for activity, were assessed over 20 days post-release to quantify disturbance intensity, recovery duration, and speed. Differences were evaluated, considering species-specific traits and the human footprint of the study region. Over 70% of the analyzed species exhibited significant behavioral changes following collaring events. Herbivores traveled farther with variable activity reactions, while omnivores and carnivores were initially less active and mobile. Recovery duration proved brief, with alterations diminishing within 4-7 tracking days for most species. Herbivores, particularly males, showed quicker displacement recovery (4 days) but slower activity recovery (7 days). Individuals in high human footprint areas displayed faster recovery, indicating adaptation to human disturbance. Our findings emphasize the necessity of extending tracking periods beyond 1 week and particular caution in remote study areas or herbivore-focused research, specifically in smaller mammals.

Published
2024

27. Commentary: The International Mouse Phenotyping Consortium: high-throughput in vivo functional annotation of the mammalian genome

Author

Lloyd, KC Kent

Subjects
Biological Sciences, Bioinformatics and Computational Biology, Genetics, Rare Diseases, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Generic health relevance, Good Health and Well Being, Animals, Mice, Knockout, Mammals, Humans, Mice, Phenotype, Genome, Molecular Sequence Annotation, Genetics & Heredity
Abstract

The International Mouse Phenotyping Consortium (IMPC) is a worldwide effort producing and phenotyping knockout mouse lines to expose the pathophysiological roles of all genes in human diseases and make mice and data available and accessible to the global research community. It has created new knowledge on the function of thousands of genes for which little to anything was known. This new knowledge has informed the genetic basis of rare diseases, posited gene product influences on common diseases, influenced research on targeted therapies, revealed functional pleiotropy, essentiality, and sexual dimorphism, and many more insights into the role of genes in health and disease. Its scientific contributions have been many and widespread, however there remain thousands of "dark" genes yet to be illuminated. Nearing the end of its current funding cycle, IMPC is at a crossroads. The vision forward is clear, the path to proceed less so.

Published
2024

28. Mistranslating the genetic code with leucine in yeast and mammalian cells

Author

Davey-Young, Josephine, Hasan, Farah, Tennakoon, Rasangi, Rozik, Peter, Moore, Henry, Hall, Peter, Cozma, Ecaterina, Genereaux, Julie, Hoffman, Kyle S, Chan, Patricia P, Lowe, Todd M, Brandl, Christopher J, and O’Donoghue, Patrick

Subjects
Biological Sciences, Genetics, Animals, Humans, Saccharomyces cerevisiae, Anticodon, Leucine, RNA, Transfer, Leu, Genetic Code, Codon, RNA, Transfer, Amino Acyl-tRNA Synthetases, Alanine, Mammals, Genetic code, mistranslation, neuroblastoma cells, protein synthesis, Transfer RNA, translation fidelity, yeast, Developmental Biology, Biochemistry and cell biology
Abstract

Translation fidelity relies on accurate aminoacylation of transfer RNAs (tRNAs) by aminoacyl-tRNA synthetases (AARSs). AARSs specific for alanine (Ala), leucine (Leu), serine, and pyrrolysine do not recognize the anticodon bases. Single nucleotide anticodon variants in their cognate tRNAs can lead to mistranslation. Human genomes include both rare and more common mistranslating tRNA variants. We investigated three rare human tRNALeu variants that mis-incorporate Leu at phenylalanine or tryptophan codons. Expression of each tRNALeu anticodon variant in neuroblastoma cells caused defects in fluorescent protein production without significantly increased cytotoxicity under normal conditions or in the context of proteasome inhibition. Using tRNA sequencing and mass spectrometry we confirmed that each tRNALeu variant was expressed and generated mistranslation with Leu. To probe the flexibility of the entire genetic code towards Leu mis-incorporation, we created 64 yeast strains to express all possible tRNALeu anticodon variants in a doxycycline-inducible system. While some variants showed mild or no growth defects, many anticodon variants, enriched with G/C at positions 35 and 36, including those replacing Leu for proline, arginine, alanine, or glycine, caused dramatic reductions in growth. Differential phenotypic defects were observed for tRNALeu mutants with synonymous anticodons and for different tRNALeu isoacceptors with the same anticodon. A comparison to tRNAAla anticodon variants demonstrates that Ala mis-incorporation is more tolerable than Leu at nearly every codon. The data show that the nature of the amino acid substitution, the tRNA gene, and the anticodon are each important factors that influence the ability of cells to tolerate mistranslating tRNAs.

Published
2024

30. Conserved and divergent features of trophoblast stem cells.

Author

Sah, Nirvay and Soncin, Francesca

Subjects
epigenetics, epigenomics, placenta, trophoblast stem cells, Mice, Pregnancy, Animals, Female, Cattle, Humans, Placenta, Epigenesis, Genetic, Histones, Trophoblasts, Stem Cells, Cell Differentiation, Mammals
Abstract

Trophoblast stem cells (TSCs) are a proliferative multipotent population derived from the trophectoderm of the blastocyst, which will give rise to all the functional cell types of the trophoblast compartment of the placenta. The isolation and culture of TSCs in vitro represent a robust model to study mechanisms of trophoblast differentiation into mature cells both in successful and diseased pregnancy. Despite the highly conserved functions of the placenta, there is extreme variability in placental morphology, fetal-maternal interface, and development among eutherian mammals. This review aims to summarize the establishment and maintenance of TSCs in mammals such as primates, including human, rodents, and nontraditional animal models with a primary emphasis on epigenetic regulation of their origin while defining gaps in the current literature and areas of further development. FGF signaling is critical for mouse TSCs but dispensable for derivation of TSCs in other species. Human, simian, and bovine TSCs have much more complicated requirements of signaling pathways including activation of WNT and inhibition of TGFβ cascades. Epigenetic features such as DNA and histone methylation as well as histone acetylation are dynamic during development and are expressed in cell- and gestational age-specific pattern in placental trophoblasts. While TSCs from different species seem to recapitulate some select epigenomic features, there is a limitation in the comprehensive understanding of TSCs and how well TSCs retain placental epigenetic marks. Therefore, future studies should be directed at investigating epigenomic features of global and placental-specific gene expression in primary trophoblasts and TSCs.

Published
2024

31. Individual variation in life-history timing: synchronous presence, asynchronous events and phenological compensation in a wild mammal.

Author

Lozano, Raquel, Morris, Patricia, Robinson, Patrick, Keates, Theresa, Favilla, Arina, Kilpatrick, A, Costa, Daniel, Beltran, Roxanne, and Holser, Rachel

Subjects
individual, life history, presence, synchronous, timings, variation, Animals, Female, Birds, Molting, Reproduction, Mammals, Seasons, Seals, Earless
Abstract

Many animals and plants have species-typical annual cycles, but individuals vary in their timing of life-history events. Individual variation in fur replacement (moult) timing is poorly understood in mammals due to the challenge of repeated observations and longitudinal sampling. We examined factors that influence variation in moult duration and timing among elephant seals (Mirounga angustirostris). We quantified the onset and progression of fur loss in 1178 individuals. We found that an exceptionally rapid visible moult (7 days, the shortest of any mammals or birds), and a wide range of moult start dates (spanning 6-10× the event duration) facilitated high asynchrony across individuals (only 20% of individuals in the population moulting at the same time). Some of the variation was due to reproductive state, as reproductively mature females that skipped a breeding season moulted a week earlier than reproductive females. Moreover, individual variation in timing and duration within age-sex categories far outweighed (76-80%) variation among age-sex categories. Individuals arriving at the end of the moult season spent 50% less time on the beach, which allowed them to catch up in their annual cycles and reduce population-level variance during breeding. These findings underscore the importance of individual variation in annual cycles.

Published
2024

32. Gentrification drives patterns of alpha and beta diversity in cities.

Author

Fidino, Mason, Sander, Heather, Lewis, Jesse, Lehrer, Elizabeth, Rivera, Kimberly, Murray, Maureen, Adams, Henry, Kase, Anna, Flores, Andrea, Stankowich, Theodore, Schell, Christopher, Salsbury, Carmen, Rohnke, Adam, Jordan, Mark, Green, Austin, R Gramza, Ashley, Zellmer, Amanda, Williamson, Jacque, Surasinghe, Thilina, Storm, Hunter, Sparks, Kimberly, Ryan, Travis, Remine, Katie, Pendergast, Mary, Mullen, Kayleigh, Minier, Darren, Middaugh, Christopher, Mertl, Amy, McClung, Maureen, Long, Robert, Larson, Rachel, Kohl, Michel, Harris, Lavendar, Hall, Courtney, Haight, Jeffrey, Drake, David, Davidge, Alyssa, Cheek, Ann, Bloch, Christopher, Biro, Elizabeth, Anthonysamy, Whitney, Angstmann, Julia, Allen, Maximilian, Adalsteinsson, Solny, Short Gianotti, Anne, LaMontagne, Jalene, Gelmi-Candusso, Tiziana, and Magle, Seth

Subjects
alpha diversity, beta diversity, camera trap, gentrification, mammals, Animals, Humans, Cities, Residential Segregation, Biodiversity, Mammals, Animals, Wild, Ecosystem
Abstract

While there is increasing recognition that social processes in cities like gentrification have ecological consequences, we lack nuanced understanding of the ways gentrification affects urban biodiversity. We analyzed a large camera trap dataset of mammals (>500 g) to evaluate how gentrification impacts species richness and community composition across 23 US cities. After controlling for the negative effect of impervious cover, gentrified parts of cities had the highest mammal species richness. Change in community composition was associated with gentrification in a few cities, which were mostly located along the West Coast. At the species level, roughly half (11 of 21 mammals) had higher occupancy in gentrified parts of a city, especially when impervious cover was low. Our results indicate that the impacts of gentrification extend to nonhuman animals, which provides further evidence that some aspects of nature in cities, such as wildlife, are chronically inaccessible to marginalized human populations.

Published
2024

33. Proliferation-driven mechanical compression induces signalling centre formation during mammalian organ development

Author

Shroff, Neha Pincha, Xu, Pengfei, Kim, Sangwoo, Shelton, Elijah R, Gross, Ben J, Liu, Yucen, Gomez, Carlos O, Ye, Qianlin, Drennon, Tingsheng Yu, Hu, Jimmy K, Green, Jeremy BA, Campàs, Otger, and Klein, Ophir D

Subjects
Biochemistry and Cell Biology, Biological Sciences, 2.1 Biological and endogenous factors, Animals, Female, Pregnancy, Signal Transduction, Incisor, Cell Differentiation, Mammals, Cell Proliferation, Stress, Mechanical, Medical and Health Sciences, Developmental Biology, Biochemistry and cell biology
Abstract

Localized sources of morphogens, called signalling centres, play a fundamental role in coordinating tissue growth and cell fate specification during organogenesis. However, how these signalling centres are established in tissues during embryonic development is still unclear. Here we show that the main signalling centre orchestrating development of rodent incisors, the enamel knot (EK), is specified by a cell proliferation-driven buildup in compressive stresses (mechanical pressure) in the tissue. Direct mechanical measurements indicate that the stresses generated by cell proliferation are resisted by the surrounding tissue, creating a circular pattern of mechanical anisotropy with a region of high compressive stress at its centre that becomes the EK. Pharmacological inhibition of proliferation reduces stresses and suppresses EK formation, and application of external pressure in proliferation-inhibited conditions rescues the formation of the EK. Mechanical information is relayed intracellularly through YAP protein localization, which is cytoplasmic in the region of compressive stress that establishes the EK and nuclear in the stretched anisotropic cells that resist the pressure buildup around the EK. Together, our data identify a new role for proliferation-driven mechanical compression in the specification of a model signalling centre during mammalian organ development.

Published
2024

34. The activity of antimicrobial peptoids against multidrug-resistant ocular pathogens

Author

Sara, Manjulatha, Yasir, Muhammad, Kalaiselvan, Parthasarathi, Hui, Alex, Kuppusamy, Rajesh, Kumar, Naresh, Chakraborty, Sudip, Yu, Tsz Tin, Wong, Edgar HH, Molchanova, Natalia, Jenssen, Håvard, Lin, Jennifer S, Barron, Annelise E, and Willcox, Mark

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Antimicrobial Resistance, Emerging Infectious Diseases, Infectious Diseases, Biodefense, Biotechnology, Eye Disease and Disorders of Vision, 5.1 Pharmaceuticals, Infection, Animals, Humans, Peptoids, Methicillin-Resistant Staphylococcus aureus, Microbial Sensitivity Tests, Anti-Infective Agents, Anti-Bacterial Agents, Mammals, Antimicrobial peptoids, Keratitis, Pseudomonas aeruginosa, Staphylococcus aureus, Opthalmology and Optometry, Ophthalmology & Optometry, Ophthalmology and optometry
Abstract

BackgroundOcular infections caused by antibiotic-resistant pathogens can result in partial or complete vision loss. The development of pan-resistant microbial strains poses a significant challenge for clinicians as there are limited antimicrobial options available. Synthetic peptoids, which are sequence-specific oligo-N-substituted glycines, offer potential as alternative antimicrobial agents to target multidrug-resistant bacteria.MethodsThe antimicrobial activity of synthesised peptoids against multidrug-resistant (MDR) ocular pathogens was evaluated using the microbroth dilution method. Hemolytic propensity was assessed using mammalian erythrocytes. Peptoids were also incubated with proteolytic enzymes, after which their minimum inhibitory activity against bacteria was re-evaluated.ResultsSeveral alkylated and brominated peptoids showed good inhibitory activity against multidrug-resistant Pseudomonas aeruginosa strains at concentrations of ≤15 μg mL-1 (≤12 µM). Similarly, most brominated compounds inhibited the growth of methicillin-resistant Staphylococcus aureus at 1.9 to 15 μg mL-1 (12 µM). The N-terminally alkylated peptoids caused less toxicity to erythrocytes. The peptoid denoted as TM5 had a high therapeutic index, being non-toxic to either erythrocytes or corneal epithelial cells, even at 15 to 22 times its MIC. Additionally, the peptoids were resistant to protease activity.ConclusionsPeptoids studied here demonstrated potent activity against various multidrug-resistant ocular pathogens. Their properties make them promising candidates for controlling vision-related morbidity associated with eye infections by antibiotic-resistant strains.

Published
2024

35. Increased enhancer–promoter interactions during developmental enhancer activation in mammals

Author

Chen, Zhuoxin, Snetkova, Valentina, Bower, Grace, Jacinto, Sandra, Clock, Benjamin, Dizehchi, Atrin, Barozzi, Iros, Mannion, Brandon J, Alcaina-Caro, Ana, Lopez-Rios, Javier, Dickel, Diane E, Visel, Axel, Pennacchio, Len A, and Kvon, Evgeny Z

Subjects
Biochemistry and Cell Biology, Biological Sciences, Genetics, Generic health relevance, Animals, Mice, Enhancer Elements, Genetic, Promoter Regions, Genetic, Transcriptional Activation, Mammals, Chromatin, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology
Abstract

Remote enhancers are thought to interact with their target promoters via physical proximity, yet the importance of this proximity for enhancer function remains unclear. Here we investigate the three-dimensional (3D) conformation of enhancers during mammalian development by generating high-resolution tissue-resolved contact maps for nearly a thousand enhancers with characterized in vivo activities in ten murine embryonic tissues. Sixty-one percent of developmental enhancers bypass their neighboring genes, which are often marked by promoter CpG methylation. The majority of enhancers display tissue-specific 3D conformations, and both enhancer-promoter and enhancer-enhancer interactions are moderately but consistently increased upon enhancer activation in vivo. Less than 14% of enhancer-promoter interactions form stably across tissues; however, these invariant interactions form in the absence of the enhancer and are likely mediated by adjacent CTCF binding. Our results highlight the general importance of enhancer-promoter physical proximity for developmental gene activation in mammals.

Published
2024

36. A Pro-Regenerative Supramolecular Prodrug Protects Against and Repairs Colon Damage in Experimental Colitis.

Author

DeFrates, Kelsey, Tong, Elaine, Cheng, Jing, Heber-Katz, Ellen, and Messersmith, Phillip

Subjects
HIF‐1α, inflammatory bowel disease, prolyl hydroxylase inhibitor, regeneration, Mice, Animals, Colitis, Inflammatory Bowel Diseases, Intestinal Mucosa, Disease Models, Animal, Mammals
Abstract

Structural repair of the intestinal epithelium is strongly correlated with disease remission in inflammatory bowel disease (IBD); however, ulcer healing is not addressed by existing therapies. To address this need, this study reports the use of a small molecule prolyl hydroxylase (PHD) inhibitor (DPCA) to upregulate hypoxia-inducible factor one-alpha (HIF-1α) and induce mammalian regeneration. Sustained delivery of DPCA is achieved through subcutaneous injections of a supramolecular hydrogel, formed through the self-assembly of PEG-DPCA conjugates. Pre-treatment of mice with PEG-DPCA is shown to protect mice from epithelial erosion and symptoms of dextran sodium sulfate (DSS)-induced colitis. Surprisingly, a single subcutaneous dose of PEG-DPCA, administered after disease onset, leads to accelerated weight gain and complete restoration of healthy tissue architecture in colitic mice. Rapid DPCA-induced restoration of the intestinal barrier is likely orchestrated by increased expression of HIF-1α and associated targets leading to an epithelial-to-mesenchymal transition. Further investigation of DPCA as a potential adjunctive or stand-alone restorative treatment to combat active IBD is warranted.

Published
2024

37. Targeting host deoxycytidine kinase mitigates Staphylococcus aureus abscess formation.

Author

Winstel, Volker, Abt, Evan, Le, Thuc, and Radu, Caius

Subjects
Staphylococcus aureus, apoptosis, infectious disease, macrophages, microbiology, Animals, Humans, Staphylococcus aureus, Deoxycytidine Kinase, Abscess, Staphylococcal Infections, Anti-Infective Agents, Mammals
Abstract

Host-directed therapy (HDT) is an emerging approach to overcome antimicrobial resistance in pathogenic microorganisms. Specifically, HDT targets host-encoded factors required for pathogen replication and survival without interfering with microbial growth or metabolism, thereby eliminating the risk of resistance development. By applying HDT and a drug repurposing approach, we demonstrate that (R)-DI-87, a clinical-stage anticancer drug and potent inhibitor of mammalian deoxycytidine kinase (dCK), mitigates Staphylococcus aureus abscess formation in organ tissues upon invasive bloodstream infection. Mechanistically, (R)-DI-87 shields phagocytes from staphylococcal death-effector deoxyribonucleosides that target dCK and the mammalian purine salvage pathway-apoptosis axis. In this manner, (R)-DI-87-mediated protection of immune cells amplifies macrophage infiltration into deep-seated abscesses, a phenomenon coupled with enhanced pathogen control, ameliorated immunopathology, and reduced disease severity. Thus, pharmaceutical blockade of dCK represents an advanced anti-infective intervention strategy against which staphylococci cannot develop resistance and may help to fight fatal infectious diseases in hospitalized patients.

Published
2024

38. Site-specific acetylation of polynucleotide kinase 3′-phosphatase regulates its distinct role in DNA repair pathways

Author

Islam, Azharul, Chakraborty, Anirban, Sarker, Altaf H, Aryal, Uma K, Pan, Lang, Sharma, Gulshan, Boldogh, Istvan, and Hazra, Tapas

Subjects
Biochemistry and Cell Biology, Biological Sciences, Genetics, Rare Diseases, Neurosciences, 2.1 Biological and endogenous factors, Underpinning research, Aetiology, 1.1 Normal biological development and functioning, Generic health relevance, Animals, Humans, Mice, Acetylation, DNA Damage, DNA Repair, DNA Repair Enzymes, Mammals, Phosphotransferases (Alcohol Group Acceptor), Polynucleotide 5'-Hydroxyl-Kinase, Environmental Sciences, Information and Computing Sciences, Developmental Biology, Biological sciences, Chemical sciences, Environmental sciences
Abstract

Mammalian polynucleotide kinase 3'-phosphatase (PNKP), a DNA end-processing enzyme with 3'-phosphatase and 5'-kinase activities, is involved in multiple DNA repair pathways, including base excision (BER), single-strand break (SSBR), and double-strand break repair (DSBR). However, little is known as to how PNKP functions in such diverse repair processes. Here we report that PNKP is acetylated at K142 (AcK142) by p300 constitutively but at K226 (AcK226) by CBP, only after DSB induction. Co-immunoprecipitation analysis using AcK142 or AcK226 PNKP-specific antibodies showed that AcK142-PNKP associates only with BER/SSBR, and AcK226 PNKP with DSBR proteins. Despite the modest effect of acetylation on PNKP's enzymatic activity in vitro, cells expressing non-acetylable PNKP (K142R or K226R) accumulated DNA damage in transcribed genes. Intriguingly, in striatal neuronal cells of a Huntington's Disease (HD)-based mouse model, K142, but not K226, was acetylated. This is consistent with the reported degradation of CBP, but not p300, in HD cells. Moreover, transcribed genomes of HD cells progressively accumulated DSBs. Chromatin-immunoprecipitation analysis demonstrated the association of Ac-PNKP with the transcribed genes, consistent with PNKP's role in transcription-coupled repair. Thus, our findings demonstrate that acetylation at two lysine residues, located in different domains of PNKP, regulates its distinct role in BER/SSBR versus DSBR.

Published
2024

39. Weak coupling between energetic status and the timing of reproduction in an Arctic ungulate.

Author

Tyler, N, Post, Eric, and Hazlerigg, D

Subjects
Animals, Seasons, Reproduction, Mammals, Reindeer, Animals, Wild, Climate Change
Abstract

Bioenergetic constraints are the ultimate determinant of the timing of reproduction, and seasonal breeding is consequently a widely observed trait. Consistent with this, attention has focused on plasticity in reproductive phenology conceptualized as a response to concomitant advances in the phenology of the environmental energy supply caused by climate change. Few studies, however, have directly compared timing of reproduction with energetic status in free-living wild animals. Here we demonstrate that neither body mass nor adiposity are strong proximate predictors of date of conception in wild reindeer (Rangifer tarandus). Weak coupling between energetic status and the phenology of reproduction accounts for the increasing discrepancy between the phenology of forage (energy supply) and the phenology of reproduction (energy demand) observed across the last 2-4 decades in two populations of this species. The results emphasise that phenological plasticity is not a passive response to changes in energy supply but derives from the way in which environmental factors interact with the core control mechanisms that govern timing. Central in this respect is integration, within the rheostatic centres of the hypothalamus, of information on nutritional status with the circannual life-history calendar.

Published
2024

40. Mono-UFMylation promotes misfolding-associated secretion of α-synuclein.

Author

Wang, Lihui, Xu, Yue, Fukushige, Tetsunari, Saidi, Layla, Wang, Xiaorong, Yu, Clinton, Lee, Jin-Gu, Krause, Michael, Ye, Yihong, and Huang, Lan

Subjects
Animals, Humans, alpha-Synuclein, Protein Transport, Endoplasmic Reticulum, Mammals, Endopeptidases
Abstract

Stressed cells secret misfolded proteins lacking signaling sequence via an unconventional protein secretion (UcPS) pathway, but how misfolded proteins are targeted selectively in UcPS is unclear. Here, we report that misfolded UcPS clients are subject to modification by a ubiquitin-like protein named ubiquitin-fold modifier 1 (UFM1). Using α-synuclein (α-Syn) as a UcPS model, we show that mutating the UFMylation sites in α-Syn or genetic inhibition of the UFMylation system mitigates α-Syn secretion, whereas overexpression of UFBP1, a component of the endoplasmic reticulum-associated UFMylation ligase complex, augments α-Syn secretion in mammalian cells and in model organisms. UFM1 itself is cosecreted with α-Syn, and the serum UFM1 level correlates with that of α-Syn. Because UFM1 can be directly recognized by ubiquitin specific peptidase 19 (USP19), a previously established UcPS stimulator known to associate with several chaperoning activities, UFMylation might facilitate substrate engagement by USP19, allowing stringent and regulated selection of misfolded proteins for secretion and proteotoxic stress alleviation.

Published
2024

41. Listeria monocytogenes utilizes glutathione and limited inorganic sulfur compounds as sources of essential cysteine

Author

Berude, John C, Kennouche, Paul, Reniere, Michelle L, and Portnoy, Daniel A

Subjects
Microbiology, Biological Sciences, Biodefense, Infectious Diseases, Foodborne Illness, Emerging Infectious Diseases, Digestive Diseases, Animals, Listeria monocytogenes, Cysteine, Glutathione Disulfide, Sulfur Compounds, Glutathione, Sulfur, Bacterial Proteins, Gene Expression Regulation, Bacterial, Mammals, GSH, GSSG, Ctp, CtaP, Opp, OppABCDF, CysK, thiosulfate, auxotrophy, pathoadaptation, Agricultural and Veterinary Sciences, Medical and Health Sciences, Immunology, Medical microbiology
Abstract

Listeria monocytogenes (Lm) is a Gram-positive facultative intracellular pathogen that leads a biphasic lifecycle, transitioning its metabolism and selectively inducing virulence genes when it encounters mammalian hosts. Virulence gene expression is controlled by the master virulence regulator PrfA, which is allosterically activated by the host- and bacterially derived glutathione (GSH). The amino acid cysteine is the rate-limiting substrate for GSH synthesis in bacteria and is essential for bacterial growth. Unlike many bacteria, Lm is auxotrophic for cysteine and must import exogenous cysteine for growth and virulence. GSH is enriched in the host cytoplasm, and previous work suggests that Lm utilizes exogenous GSH for PrfA activation. Despite these observations, the import mechanism(s) for GSH remains elusive. Analysis of known GSH importers predicted a homologous importer in Lm comprised of the Ctp ABC transporter and the OppDF ATPases of the Opp oligopeptide importer. Here, we demonstrated that the Ctp complex is a high-affinity GSH/GSSG importer that is required for Lm growth at physiologically relevant concentrations. Furthermore, we demonstrated that OppDF is required for GSH/GSSG import in an Opp-independent manner. These data support a model where Ctp and OppDF form a unique complex for GSH/GSSG import that supports growth and pathogenesis. In addition, we show that Lm utilizes the inorganic sulfur sources thiosulfate and H2S for growth in a CysK-dependent manner in the absence of other cysteine sources. These findings suggest a pathoadaptive role for partial cysteine auxotrophy in Lm, where locally high GSH/GSSG or inorganic sulfur concentrations may signal arrival to distinct host niches.

Published
2024

42. Expression and potential regulatory functions of Drosophila octopamine receptors in the female reproductive tract.

Author

Rohrbach, Ethan, Knapp, Elizabeth, Deshpande, Sonali, and Krantz, David

Subjects
egg-laying, octopamine, octopamine receptor, oviposition, spermatheca, Animals, Female, Male, Drosophila, Drosophila melanogaster, Octopamine, Semen, Drosophila Proteins, Mammals, Receptors, Biogenic Amine
Abstract

Aminergic signaling is known to play a critical role in regulating female reproductive processes in both mammals and insects. In Drosophila, the ortholog of noradrenaline, octopamine, is required for ovulation as well as several other female reproductive processes. Two octopamine receptors have already been shown to be expressed in the Drosophila reproductive tract and to be required for egg-laying: OAMB and Octβ2R. The Drosophila genome contains 4 additional octopamine receptors-Octα2R, Octβ1R, Octβ3R, and Oct-TyrR-but their cellular patterns of expression in the reproductive tract and potential contribution(s) to egg-laying are not known. In addition, the mechanisms by which OAMB and Octβ2R regulate reproduction are incompletely understood. Using a panel of MiMIC Gal4 lines, we show that Octα2R, Octβ1R, Octβ3R, and Oct-TyrR receptors are not detectable in either epithelium or muscle but are clearly expressed in neurons within the female fly reproductive tract. Optogenetic activation of neurons that express at least 3 types of octopamine receptors stimulates contractions in the lateral oviduct. We also find that octopamine stimulates calcium transients in the sperm storage organs and that its effects in spermathecal, secretory cells, can be blocked by knock-down of OAMB. These data extend our understanding of the pathways by which octopamine regulates egg-laying in Drosophila and raise the possibility that multiple octopamine receptor subtypes could play a role in this process.

Published
2024

43. Synthetic autophagy receptor

Author

Jiang, Ziwen, Kuo, Yu-Hsuan, and Arkin, Michelle R

Subjects
Biochemistry and Cell Biology, Biological Sciences, Animals, Autophagy, Sequestosome-1 Protein, Proteins, Autophagosomes, Ubiquitin, Carrier Proteins, Mammals, Antibody-fusion protein, autophagy receptor, targeted organelle degradation, targeted protein degradation, proximity-based therapeutics, Biochemistry & Molecular Biology, Biochemistry and cell biology
Abstract

Macroautophagy/autophagy receptors target their substrates to phagophores for subsequent sequestration within autophagosomes. During phagophore membrane expansion in mammalian cells, autophagy receptors simultaneously interact with the ubiquitinated substrates and the LC3/GABARAP proteins on the expanding membrane. In this punctum, we summarize and discuss our recent research progress on synthetic autophagy receptors (AceTACs). The series of AceTACs were designed by engineering the essential interacting domains and motifs of SQSTM1/p62 (sequestosome 1), a major mammalian autophagy receptor. Particularly, we replaced the ubiquitin-associated domain of SQSTM1 with a target-specific antibody, redirecting the bifunctional interactions of wild-type SQSTM1 and directing the degradation target into the autophagy process. We successfully demonstrated the targeted degradation of aggregation-prone proteins using the AceTAC degraders. Moreover, we presented a model system with a guideline to induce targeted degradation of organelles through the autophagy machinery.

Published
2024

44. Cross-family small GTPase ubiquitination by the intracellular pathogen Legionella pneumophila

Author

Steinbach, Adriana, Bhadkamkar, Varun, Jimenez-Morales, David, Stevenson, Erica, Jang, Gwendolyn M, Krogan, Nevan J, Swaney, Danielle L, and Mukherjee, Shaeri

Subjects
Biochemistry and Cell Biology, Biological Sciences, Infectious Diseases, Lung, Pneumonia & Influenza, Pneumonia, Aetiology, 2.1 Biological and endogenous factors, Infection, Generic health relevance, Animals, Legionella pneumophila, Monomeric GTP-Binding Proteins, Bacterial Proteins, Ubiquitination, Ubiquitin, Vacuoles, Ligases, Mammals, Medical and Health Sciences, Developmental Biology, Biochemistry and cell biology
Abstract

The intracellular bacterial pathogen Legionella pneumophila (L.p.) manipulates eukaryotic host ubiquitination machinery to form its replicative vacuole. While nearly 10% of L.p.'s ∼330 secreted effector proteins are ubiquitin ligases or deubiquitinases, a comprehensive measure of temporally resolved changes in the endogenous host ubiquitinome during infection has not been undertaken. To elucidate how L.p. hijacks host cell ubiquitin signaling, we generated a proteome-wide analysis of changes in protein ubiquitination during infection. We discover that L.p. infection increases ubiquitination of host regulators of subcellular trafficking and membrane dynamics, most notably ∼40% of mammalian Ras superfamily small GTPases. We determine that these small GTPases undergo nondegradative ubiquitination at the Legionella-containing vacuole (LCV) membrane. Finally, we find that the bacterial effectors SidC/SdcA play a central role in cross-family small GTPase ubiquitination, and that these effectors function upstream of SidE family ligases in the polyubiquitination and retention of GTPases in the LCV membrane. This work highlights the extensive reconfiguration of host ubiquitin signaling by bacterial effectors during infection and establishes simultaneous ubiquitination of small GTPases across the Ras superfamily as a novel consequence of L.p. infection. Our findings position L.p. as a tool to better understand how small GTPases can be regulated by ubiquitination in uninfected contexts.

Published
2024

45. An extended wave of global mRNA deadenylation sets up a switch in translation regulation across the mammalian oocyte-to-embryo transition.

Author

Lee, Katherine, Cho, Kyucheol, Morey, Robert, and Cook-Andersen, Heidi

Subjects
3′ UTR motif, CP: Developmental biology, CP: Molecular biology, deadenylation, development, mRNA stability, oocyte-to-embryo transition, polyadenylation, post-transcriptional regulation, translation, Animals, Mice, Embryo, Mammalian, Gene Expression Profiling, Oocytes, RNA, Messenger, Mammals
Abstract

Without new transcription, gene expression across the oocyte-to-embryo transition (OET) relies instead on regulation of mRNA poly(A) tails to control translation. However, how tail dynamics shape translation across the OET in mammals remains unclear. We perform long-read RNA sequencing to uncover poly(A) tail lengths across the mouse OET and, incorporating published ribosome profiling data, provide an integrated, transcriptome-wide analysis of poly(A) tails and translation across the entire transition. We uncover an extended wave of global deadenylation during fertilization in which short-tailed, oocyte-deposited mRNAs are translationally activated without polyadenylation through resistance to deadenylation. Subsequently, in the embryo, mRNAs are readenylated and translated in a surge of global polyadenylation. We further identify regulation of poly(A) tail length at the isoform level and stage-specific enrichment of mRNA sequence motifs among regulated transcripts. These data provide insight into the stage-specific mechanisms of poly(A) tail regulation that orchestrate gene expression from oocyte to embryo in mammals.

Published
2024

46. Genome-wide screens identify SEL1L as an intracellular rheostat controlling collagen turnover.

Author

Podolsky, Michael, Kheyfets, Benjamin, Pandey, Monika, Beigh, Afaq, Yang, Christopher, Lizama, Carlos, Datta, Ritwik, Lin, Liangguang, Wang, Zhihong, Wolters, Paul, McManus, Michael, Qi, Ling, and Atabai, Kamran

Subjects
Animals, Humans, Collagen, Extracellular Matrix, Fibrosis, Proteolysis, Lung, Mammals, Proteins
Abstract

Accumulating evidence has implicated impaired extracellular matrix (ECM) clearance as a key factor in fibrotic disease. Despite decades of research elucidating the effectors of ECM clearance, relatively little is understood regarding the upstream regulation of this process. Collagen is the most abundant constituent of normal and fibrotic ECM in mammalian tissues. Its catabolism occurs through extracellular proteolysis and cell-mediated uptake of collagen fragments for intracellular degradation. Given the paucity of information regarding the regulation of this latter process, here we execute unbiased genome-wide screens to understand the molecular underpinnings of cell-mediated collagen clearance. Using this approach, we discover a mechanism through which collagen biosynthesis is sensed by cells internally and directly regulates clearance of extracellular collagen. The sensing mechanism appears to be dependent on endoplasmic reticulum-resident protein SEL1L and occurs via a noncanonical function of this protein. This pathway functions as a homeostatic negative feedback loop that limits collagen accumulation in tissues. In human fibrotic lung disease, the induction of this collagen clearance pathway by collagen synthesis is impaired, thereby contributing to the pathological accumulation of collagen in lung tissue. Thus, we describe cell-autonomous, rheostatic collagen clearance as an important pathway of tissue homeostasis.

Published
2024

47. The bii4africa dataset of faunal and floral population intactness estimates across Africas major land uses.

Author

Clements, Hayley, Do Linh San, Emmanuel, Hempson, Gareth, Linden, Birthe, Maritz, Bryan, Monadjem, Ara, Reynolds, Chevonne, Siebert, Frances, Stevens, Nicola, Biggs, Reinette, De Vos, Alta, Blanchard, Ryan, Child, Matthew, Esler, Karen, Hamann, Maike, Loft, Ty, Reyers, Belinda, Selomane, Odirilwe, Skowno, Andrew, Tshoke, Tshegofatso, Abdoulaye, Diarrassouba, Aebischer, Thierry, Aguirre-Gutiérrez, Jesús, Alexander, Graham, Ali, Abdullahi, Allan, David, Amoako, Esther, Angedakin, Samuel, Aruna, Edward, Avenant, Nico, Badjedjea, Gabriel, Bakayoko, Adama, Bamba-Kaya, Abraham, Bates, Michael, Bates, Paul, Belmain, Steven, Bennitt, Emily, Bradley, James, Brewster, Chris, Brown, Michael, Bryja, Josef, Butynski, Thomas, Carvalho, Filipe, Channing, Alan, Chapman, Colin, Cohen, Callan, Cords, Marina, Cramer, Jennifer, Cronk, Nadine, Cunneyworth, Pamela, Dalerum, Fredrik, Danquah, Emmanuel, Davies-Mostert, Harriet, de Blocq, Andrew, De Jong, Yvonne, Demos, Terrence, Denys, Christiane, Djagoun, Chabi, Doherty-Bone, Thomas, Drouilly, Marine, du Toit, Johan, Ehlers Smith, David, Ehlers Smith, Yvette, Eiseb, Seth, Fashing, Peter, Ferguson, Adam, Fernández-García, José, Finckh, Manfred, Fischer, Claude, Gandiwa, Edson, Gaubert, Philippe, Gaugris, Jerome, Gibbs, Dalton, Gilchrist, Jason, Gil-Sánchez, Jose, Githitho, Anthony, Goodman, Peter, Granjon, Laurent, Grobler, J, Gumbi, Bonginkosi, Gvozdik, Vaclav, Harvey, James, Hauptfleisch, Morgan, Hayder, Firas, Hema, Emmanuel, Herbst, Marna, Houngbédji, Mariano, Huntley, Brian, Hutterer, Rainer, Ivande, Samuel, Jackson, Kate, Jongsma, Gregory, Juste, Javier, Kadjo, Blaise, Kaleme, Prince, Kamugisha, Edwin, Kaplin, Beth, Kato, Humphrey, Kiffner, Christian, and Kimuyu, Duncan

Subjects
Animals, Humans, Ecosystem, Conservation of Natural Resources, Biodiversity, Vertebrates, Mammals
Abstract

Sub-Saharan Africa is under-represented in global biodiversity datasets, particularly regarding the impact of land use on species population abundances. Drawing on recent advances in expert elicitation to ensure data consistency, 200 experts were convened using a modified-Delphi process to estimate intactness scores: the remaining proportion of an intact reference population of a species group in a particular land use, on a scale from 0 (no remaining individuals) to 1 (same abundance as the reference) and, in rare cases, to 2 (populations that thrive in human-modified landscapes). The resulting bii4africa dataset contains intactness scores representing terrestrial vertebrates (tetrapods: ±5,400 amphibians, reptiles, birds, mammals) and vascular plants (±45,000 forbs, graminoids, trees, shrubs) in sub-Saharan Africa across the regions major land uses (urban, cropland, rangeland, plantation, protected, etc.) and intensities (e.g., large-scale vs smallholder cropland). This dataset was co-produced as part of the Biodiversity Intactness Index for Africa Project. Additional uses include assessing ecosystem condition; rectifying geographic/taxonomic biases in global biodiversity indicators and maps; and informing the Red List of Ecosystems.

Published
2024

48. Role of H3K4 monomethylation in gene regulation

Author

Wang, Zhaoning and Ren, Bing

Subjects
Biochemistry and Cell Biology, Biological Sciences, Human Genome, Genetics, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Animals, Histones, Lysine, Methylation, Saccharomyces cerevisiae, Gene Expression Regulation, Mammals, Developmental Biology, Biochemistry and cell biology
Abstract

Methylation of histone H3 on the lysine-4 residue (H3K4me) is found throughout the eukaryotic domain, and its initial discovery as a conserved epigenetic mark of active transcription from yeast to mammalian cells has contributed to the histone code hypothesis. However, recent studies have raised questions on whether the different forms of H3K4me play a direct role in gene regulation or are simply by-products of the transcription process. Here, we review the often-conflicting experimental evidence, focusing on the monomethylation of lysine 4 on histone H3 that has been linked to the transcriptional state of enhancers in metazoans. We suggest that this epigenetic mark acts in a context-dependent manner to directly facilitate the transcriptional output of the genome and the establishment of cellular identity.

Published
2024

49. Deep Conservation and Unexpected Evolutionary History of Neighboring lncRNAs MALAT1 and NEAT1.

Author

Weghorst, Forrest, Torres Marcén, Martí, Faridi, Garrison, Lee, Yuh, and Cramer, Karina

Subjects
Birds, Comparative genomics, Long non-coding RNA, MALAT1, NEAT1, Animals, RNA, Long Noncoding, Phylogeny, Gene Expression Regulation, Biological Evolution, Mammals
Abstract

Long non-coding RNAs (lncRNAs) have begun to receive overdue attention for their regulatory roles in gene expression and other cellular processes. Although most lncRNAs are lowly expressed and tissue-specific, notable exceptions include MALAT1 and its genomic neighbor NEAT1, two highly and ubiquitously expressed oncogenes with roles in transcriptional regulation and RNA splicing. Previous studies have suggested that NEAT1 is found only in mammals, while MALAT1 is present in all gnathostomes (jawed vertebrates) except birds. Here we show that these assertions are incomplete, likely due to the challenges associated with properly identifying these two lncRNAs. Using phylogenetic analysis and structure-aware annotation of publicly available genomic and RNA-seq coverage data, we show that NEAT1 is a common feature of tetrapod genomes except birds and squamates. Conversely, we identify MALAT1 in representative species of all major gnathostome clades, including birds. Our in-depth examination of MALAT1, NEAT1, and their genomic context in a wide range of vertebrate species allows us to reconstruct the series of events that led to the formation of the locus containing these genes in taxa from cartilaginous fish to mammals. This evolutionary history includes the independent loss of NEAT1 in birds and squamates, since NEAT1 is found in the closest living relatives of both clades (crocodilians and tuataras, respectively). These data clarify the origins and relationships of MALAT1 and NEAT1 and highlight an opportunity to study the change and continuity in lncRNA structure and function over deep evolutionary time.

Published
2024

50. Identification of AgRP cells in the murine hindbrain that drive feeding

Author

Bachor, Tomas P, Hwang, Eunsang, Yulyaningsih, Ernie, Attal, Kush, Mifsud, Francois, Pham, Viana, Vagena, Eirini, Huarcaya, Renzo, Valdearcos, Martin, Vaisse, Christian, Williams, Kevin W, Emmerson, Paul J, and Xu, Allison W

Subjects
Biochemistry and Cell Biology, Biological Sciences, Obesity, Neurosciences, Nutrition, Underpinning research, 1.1 Normal biological development and functioning, Mice, Animals, Agouti-Related Protein, Hypothalamus, Mice, Transgenic, Melanocortins, Rhombencephalon, Mammals, AgRP, Hindbrain, Feeding, Physiology, Biochemistry and cell biology
Abstract

ObjectiveThe central melanocortin system is essential for the regulation of food intake and body weight. Agouti-related protein (AgRP) is the sole orexigenic component of the central melanocortin system and is conserved across mammalian species. AgRP is currently known to be expressed exclusively in the mediobasal hypothalamus, and hypothalamic AgRP-expressing neurons are essential for feeding. Here we characterized a previously unknown population of AgRP cells in the mouse hindbrain.MethodsExpression of AgRP in the hindbrain was investigated using gene expression analysis, single-cell RNA sequencing, immunofluorescent analysis and multiple transgenic mice with reporter expressions. Activation of AgRP neurons was achieved by Designer Receptors Exclusively Activated by Designer Drugs (DREADD) and by transcranial focal photo-stimulation using a step-function opsin with ultra-high light sensitivity (SOUL).ResultsAgRP expressing cells were present in the area postrema (AP) and the adjacent subpostrema area (SubP) and commissural nucleus of the solitary tract (cNTS) of the mouse hindbrain (termed AgRPHind herein). AgRPHind cells consisted of locally projecting neurons as well as tanycyte-like cells. Food deprivation stimulated hindbrain Agrp expression as well as neuronal activity of subsets of AgRPHind cells. In adult mice that lacked hypothalamic AgRP neurons, chemogenetic activation of AgRP neurons resulted in hyperphagia and weight gain. In addition, transcranial focal photo-stimulation of hindbrain AgRP cells increased food intake in adult mice with or without hypothalamic AgRP neurons.ConclusionsOur study indicates that the central melanocortin system in the hindbrain possesses an orexigenic component, and that AgRPHind neurons stimulate feeding independently of hypothalamic AgRP neurons.

Published
2024

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