Search

Your search keyword '"Julian, R."' showing total 12,358 results
Start Over Author "Julian, R."

Refine your results

more »

more »

more »

more »

more »

more »

more »
12,358 results on '"Julian, R."'

1. Improvements for lower bounds of mutually orthogonal Latin squares of sizes $54$, $96$ and $108$

Author

Abel, R. Julian R., Janiszczak, Ingo, and Staszewski, Reiner

Subjects
Mathematics - Combinatorics, 05B15
Abstract

We will show that there are at least 8, 10 and 9 mutually orthogonal Latin squares (MOLS) of orders $n=54$, $96$ and $108$. The cases $n=54$ and $96$ are obtained by constructing separable permutation codes consisting of $8 \times 54$ and $10 \times 96$ codeword respectively; in addition, these codes respectively have lengths $54$, $96$ and minimum distances $53$, $95$. Here we will follow exactly the procedure given in \cite{JS2019}. The case $n=108$ is obtained by constructing a $(108,10,1)$ difference matrix. Also, an error in \cite{ACD} for $n=45$ will be corrected., Comment: 12 pages, GAP code in the appendix

Published
2024

4. The Genomic Landscape of Oceania

Author

Quinto-Cortés, Consuelo D., Jonas, Carmina Barberena, Vieyra-Sánchez, Sofía, Oppenheimer, Stephen, González-Buenfil, Ram, Auckland, Kathryn, Robson, Kathryn, Parks, Tom, Moreno-Mayar, J. Víctor, Blanco-Portillo, Javier, Homburger, Julian R., Wojcik, Genevieve L., Severson, Alissa L., Friedlaender, Jonathan S., Friedlaender, Francoise, Allen, Angela, Allen, Stephen, Stoneking, Mark, Hill, Adrian V. S., Aho, George, Koki, George, Pomat, William, Bustamante, Carlos D., Phipps, Maude, Mentzer, Alexander J., Moreno-Estrada, Andrés, and Ioannidis, Alexander G.

Subjects
Quantitative Biology - Populations and Evolution
Abstract

Encompassing regions that were amongst the first inhabited by humans following the out-of-Africa expansion, hosting populations with the highest levels of archaic hominid introgression, and including Pacific islands that are the most isolated inhabited locations on the planet, Oceania has a rich, but understudied, human genomic landscape. Here we describe the first region-wide analysis of genome-wide data from population groups spanning Oceania and its surroundings, from island and peninsular southeast Asia to Papua New Guinea, east across the Pacific through Melanesia, Micronesia, and Polynesia, and west across the Indian Ocean to related island populations in the Andamans and Madagascar. In total we generate and analyze genome-wide data from 981 individuals from 92 different populations, 58 separate islands, and 30 countries, representing the most expansive study of Pacific genetics to date. In each sample we disentangle the Papuan and more recent Austronesian ancestries, which have admixed in various proportions across this region, using ancestry-specific analyses, and characterize the distinct patterns of settlement, migration, and archaic introgression separately in these two ancestries. We also focus on the patterns of clinically relevant genetic variation across Oceania--a landscape rippled with strong founder effects and island-specific genetic drift in allele frequencies--providing an atlas for the development of precision genetic health strategies in this understudied region of the world.

Published
2024

5. Examining the healthy human microbiome concept

Author

Joos, Raphaela, Boucher, Katy, Lavelle, Aonghus, Arumugam, Manimozhiyan, Blaser, Martin J., Claesson, Marcus J., Clarke, Gerard, Cotter, Paul D., De Sordi, Luisa, Dominguez-Bello, Maria G., Dutilh, Bas E., Ehrlich, Stanislav D., Ghosh, Tarini Shankar, Hill, Colin, Junot, Christophe, Lahti, Leo, Lawley, Trevor D., Licht, Tine R., Maguin, Emmanuelle, Makhalanyane, Thulani P., Marchesi, Julian R., Matthijnssens, Jelle, Raes, Jeroen, Ravel, Jacques, Salonen, Anne, Scanlan, Pauline D., Shkoporov, Andrey, Stanton, Catherine, Thiele, Ines, Tolstoy, Igor, Walter, Jens, Yang, Bo, Yutin, Natalia, Zhernakova, Alexandra, Zwart, Hub, Doré, Joël, and Ross, R. Paul

Published
2025
Full Text
View/download PDF

11. Incidences of colorectal adenomas and cancers under colonoscopy surveillance suggest an accelerated “Big Bang” pathway to CRC in three of the four Lynch syndromes

Author

Møller, Pål, Haupt, Saskia, Ahadova, Aysel, Kloor, Matthias, Sampson, Julian R., Sunde, Lone, Seppälä, Toni, Burn, John, Bernstein, Inge, Capella, Gabriel, Evans, D. Gareth, Lindblom, Annika, Winship, Ingrid, Macrae, Finlay, Katz, Lior, Laish, Ido, Vainer, Elez, Monahan, Kevin, Half, Elizabeth, Horisberger, Karoline, da Silva, Leandro Apolinário, Heuveline, Vincent, Therkildsen, Christina, Lautrup, Charlotte, Klarskov, Louise L, Cavestro, Giulia Martina, Möslein, Gabriela, Hovig, Eivind, and Dominguez-Valentin, Mev

Published
2024
Full Text
View/download PDF

14. A cryptic new species of tiger swallowtail (Lepidoptera, Papilionidae) from eastern North America

Author

Charles J. DeRoller, Xi Wang, Julian R. Dupuis, and B. Christian Schmidt

Subjects
Zoology, QL1-991
Abstract

In the eastern Great Lakes region of North America, two tiger swallowtail species have previously been recognized, Papilio glaucus Linnaeus, 1758 and Papilio canadensis Rothschild & Jordan, 1906. A third entity, the Midsummer Tiger Swallowtail, has been treated as a P. glaucus × canadensis hybrid, and exhibits a mosaic of both intermediate and unique morphological and biological traits. Here we demonstrate that rather than being a localized, historically recent hybrid phenomenon, the Midsummer Tiger Swallowtail maintains its morphological and physiological distinctness over a large geographic region in the absence of one or both putative parental species, and was first documented in the literature nearly 150 years ago. Papilio solstitius sp. nov. is physiologically unique in delaying post-diapause development, which results in allochronic isolation between the spring flights of P. glaucus and P. canadensis, and the late summer flight of P. glaucus. Similarly, the geographic range of Papilio solstitius spans the region between the northern terminus of P. glaucus and southern limits of P. canadensis, remaining distinct in areas of sympatry. Defining the taxonomic identity of this unique evolutionary lineage provides an important baseline for further inquiry into what has served as an exemplary species group in evolutionary study.

Published
2025
Full Text
View/download PDF

15. Colorectal carcinogenesis in the Lynch syndromes and familial adenomatous polyposis: trigger events and downstream consequences

Author

Pål Møller, Aysel Ahadova, Matthias Kloor, Toni T. Seppälä, John Burn, Saskia Haupt, Finlay Macrae, Mev Dominguez-Valentin, Gabriela Möslein, Annika Lindblom, Lone sunde, Ingrid Winship, Gabriel Capella, Kevin Monahan, Daniel D. Buchanan, D. Gareth Evans, Eivind Hovig, and Julian R. Sampson

Subjects
Inherited, Cancer, Colorectal, Lynch syndromes, LS, MSI, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Genetics, QH426-470
Abstract

Abstract Carcinogenesis encompasses processes that lead to increased mutation rates, enhanced cellular division (tumour growth), and invasive growth. Colorectal cancer (CRC) carcinogenesis in carriers of pathogenic APC (path_APC) and pathogenic mismatch repair gene (path_MMR) variants is initiated by a second hit affecting the corresponding wild-type allele. In path_APC carriers, second hits result in the development of multiple adenomas, with CRC typically emerging after an additional 20 years. In path_MLH1 and path_MSH2 carriers, second hits lead to the formation of microscopically detectable, microsatellite unstable (MSI) crypts, from which CRC develops in about half of carriers over their lifetime, often without progressing through a diagnosable adenoma stage. These divergent outcomes reflect the distinct functions of. the APC and MMR genes. In path_MLH1 and path_MSH2 carriers, a direct consequence of stochastic mutations may be the occurrence of invasive growth before tumour expansion, challenging the paradigm that an invasive cancer must always have an non-invasive precursor. In contrast to other path_ MMR carriers, path_PMS2 carriers who receive colonoscopic surveillance exhibit minimal increase in CRC incidence. This is consistent with a hybrid model: the initial mutation may cause an adenoma, and the second hit in the wild-type PMS2 allele may drive the adenoma towards become cancerous with MSI. Since all mutational events are stochastic, interventions aimed at preventing or curing cancer should ideally target the initial mutational events. Interventions focused on downstream events are external factors that influence which tumour clones survive Darwinian selection. In Lynch Syndrome, surveillance colonoscopy to remove adenomas may select for carcinogenetic pathways that bypass the adenoma stage.

Published
2025
Full Text
View/download PDF

16. Group divisible designs with block size 4 and group sizes 4 and 7

Author

Abel, R. Julian R., Britz, Thomas, Bunjamin, Yudhistira A., and Combe, Diana

Subjects
Mathematics - Combinatorics, 05B05
Abstract

In this paper, we consider the existence of group divisible designs (GDDs) with block size $4$ and group sizes $4$ and $7$. We show that there exists a 4-GDD of type $4^t 7^s$ for all but a finite specified set of feasible values for $(t, s)$., Comment: arXiv admin note: substantial text overlap with arXiv:2109.11221

Published
2023

17. What does ChatGPT know about natural science and engineering?

Author

Balhorn, Lukas Schulze, Weber, Jana M., Buijsman, Stefan, Hildebrandt, Julian R., Ziefle, Martina, and Schweidtmann, Artur M.

Subjects
Computer Science - Human-Computer Interaction
Abstract

ChatGPT is a powerful language model from OpenAI that is arguably able to comprehend and generate text. ChatGPT is expected to have a large impact on society, research, and education. An essential step to understand ChatGPT's expected impact is to study its domain-specific answering capabilities. Here, we perform a systematic empirical assessment of its abilities to answer questions across the natural science and engineering domains. We collected 594 questions from 198 faculty members across 5 faculties at Delft University of Technology. After collecting the answers from ChatGPT, the participants assessed the quality of the answers using a systematic scheme. Our results show that the answers from ChatGPT are on average perceived as ``mostly correct''. Two major trends are that the rating of the ChatGPT answers significantly decreases (i) as the complexity level of the question increases and (ii) as we evaluate skills beyond scientific knowledge, e.g., critical attitude.

Published
2023

19. The p97/VCP adaptor UBXD1 drives AAA+ remodeling and ring opening through multi-domain tethered interactions

Author

Braxton, Julian R, Altobelli, Chad R, Tucker, Maxwell R, Tse, Eric, Thwin, Aye C, Arkin, Michelle R, and Southworth, Daniel R

Subjects
Biochemistry and Cell Biology, Biological Sciences, 2.1 Biological and endogenous factors, Humans, Valosin Containing Protein, Protein Binding, Protein Structure, Tertiary, Cell Cycle Proteins, Chemical Sciences, Medical and Health Sciences, Biophysics, Developmental Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences
Abstract

p97, also known as valosin-containing protein, is an essential cytosolic AAA+ (ATPases associated with diverse cellular activities) hexamer that unfolds substrate polypeptides to support protein homeostasis and macromolecular disassembly. Distinct sets of p97 adaptors guide cellular functions but their roles in direct control of the hexamer are unclear. The UBXD1 adaptor localizes with p97 in critical mitochondria and lysosome clearance pathways and contains multiple p97-interacting domains. Here we identify UBXD1 as a potent p97 ATPase inhibitor and report structures of intact human p97-UBXD1 complexes that reveal extensive UBXD1 contacts across p97 and an asymmetric remodeling of the hexamer. Conserved VIM, UBX and PUB domains tether adjacent protomers while a connecting strand forms an N-terminal domain lariat with a helix wedged at the interprotomer interface. An additional VIM-connecting helix binds along the second (D2) AAA+ domain. Together, these contacts split the hexamer into a ring-open conformation. Structures, mutagenesis and comparisons to other adaptors further reveal how adaptors containing conserved p97-remodeling motifs regulate p97 ATPase activity and structure.

Published
2023

20. Homopolymer switches mediate adaptive mutability in mismatch repair-deficient colorectal cancer

Author

Kayhanian, Hamzeh, Cross, William, van der Horst, Suzanne E. M., Barmpoutis, Panagiotis, Lakatos, Eszter, Caravagna, Giulio, Zapata, Luis, Van Hoeck, Arne, Middelkamp, Sjors, Litchfield, Kevin, Steele, Christopher, Waddingham, William, Patel, Dominic, Milite, Salvatore, Jin, Chen, Baker, Ann-Marie, Alexander, Daniel C., Khan, Khurum, Hochhauser, Daniel, Novelli, Marco, Werner, Benjamin, van Boxtel, Ruben, Hageman, Joris H., Buissant des Amorie, Julian R., Linares, Josep, Ligtenberg, Marjolijn J. L., Nagtegaal, Iris D., Laclé, Miangela M., Moons, Leon M. G., Brosens, Lodewijk A. A., Pillay, Nischalan, Sottoriva, Andrea, Graham, Trevor A., Rodriguez-Justo, Manuel, Shiu, Kai-Keen, Snippert, Hugo J. G., and Jansen, Marnix

Published
2024
Full Text
View/download PDF

21. Changing the Odds: Student Achievement after Introduction of a Middle School Math Intervention

Author

Julian R. Betts, Andrew C. Zau, Karen Volz Bachofer, and Dina Polichar

Abstract

The paper evaluates math performance at four high-need middle schools during a four-year intervention, which was designed to help math teachers diagnose students' areas of need and to design lesson plans responsive to those needs. Before the intervention began, the researchers pre-selected four comparison schools by matching based on achievement and also on demographics. A difference-in-difference analysis finds a significant increase of about 0.11 standard deviation in test scores per year for students in the program schools. Supplementary event study and synthetic control analyses to detect year-by-year effects lack precision but are weakly suggestive of a smaller impact in year 1 than later years. A cost analysis considers the affordability of extending similar programs.

Published
2024
Full Text
View/download PDF

22. Evaluation of intestinal biopsy tissue preservation methods to facilitate large-scale mucosal microbiota researchResearch in context

Author

Nicola J. Wyatt, Hannah Watson, Gregory R. Young, Mary Doona, Ned Tilling, Dean Allerton, Andrea C. Masi, Tariq Ahmad, Jennifer A. Doyle, Katherine Frith, Ailsa Hart, Victoria Hildreth, Peter M. Irving, Claire Jones, Nicholas A. Kennedy, Sarah Lawrence, Charlie W. Lees, Robert Lees, Trevor Liddle, James O. Lindsay, Julian R. Marchesi, Miles Parkes, Nick Powell, Natalie J. Prescott, Tim Raine, Jack Satsangi, Kevin Whelan, Ruth Wood, Andrew King, Luke Jostins-Dean, R. Alexander Speight, Naomi McGregor, Christopher J. Stewart, and Christopher A. Lamb

Subjects
Inflammatory bowel disease, Precision medicine, Gut microbiome, Tissue microbiome, Tissue preservative reagents, Formalin fixed paraffin embedded, Medicine, Medicine (General), R5-920
Abstract

Summary: Background: Large-scale multicentre studies are needed to understand complex relationships between the gut microbiota, health and disease. Interrogating the mucosal microbiota may identify important biology not captured by stool analysis. Gold standard tissue cryopreservation (‘flash freezing’) limits large-scale study feasibility. We aimed to compare gut microbiota in gold standard and pragmatic mucosal biopsy storage conditions. Methods: We collected endoscopic recto-sigmoid biopsies from 20 adults with inflammatory bowel disease. Biopsies were preserved using three methods: (i) flash freezing (most proximal and distal biopsy sites); (ii) nucleic acid preservative reagents (QIAGEN Allprotect®, Invitrogen RNAlater™, and Zymo DNA/RNA Shield™); and (iii) formalin fixation with paraffin embedding (FFPE), which is used to preserve tissue for clinical histopathology within healthcare settings. Microbiota were sequenced on the MiSeq platform (V4 region, 16S rRNA gene). Findings: Tissue microbiota were consistent between most proximal and distal tissue suggesting any within-patient variation observed reflected storage condition, not biopsy location. There was no significant difference in alpha-diversity or microbial community profiles of reagent-preserved versus gold standard tissue. FFPE community structure was significantly dissimilar to other tissue samples, driven by differential relative abundance of obligate gut anaerobes; Faecalibacterium, Anaerostipes and Lachnospiraceae. Despite these differences, tissue microbiota grouped by participant regardless of preservation and storage conditions. Interpretation: Preservative reagents offer a convenient alternative to flash freezing tissue in prospective large-scale mucosal microbiota studies. Whilst less comparable, FFPE provides potential for retrospective microbiota studies using historical samples. Funding: Medical Research Council (MR/T032162/1) and The Leona M. and Harry B. Helmsley Charitable Trust (G-2002-04255).

Published
2025
Full Text
View/download PDF

23. Intestinal Microbiota Transplant Prior to Allogeneic Stem Cell Transplant (MAST) trial: study protocol for a multicentre, double-blinded, placebo-controlled, phase IIa trial

Author

Julian R Marchesi, Emma Nicholson, Benjamin H Mullish, Renuka Palanicawandar, Graham Wheeler, Francesca Kinsella, Andrew J Innes, Lauren A Roberts, Shian Anim-Burton, Lee Webber, Nicholas A Johnson, Rohma Ghani, Pakhshan Farshi, Anjum B Khan, Panagiotis Kottaridis, Pramila Krishnamurthy, Frances Davies, and Jiří Pavlů

Subjects
Medicine
Abstract

Introduction Lower diversity of the gut microbiome prior to allogeneic haematopoietic cell transplantation (HCT) correlates with reduced survival after the intervention. Most patients undergoing HCT for a haematological malignancy have previously received intensive chemotherapy, resulting in prolonged neutropenic episodes requiring broad-spectrum antibiotics; use of these has been linked to reduced microbiome diversity. Intestinal microbiota transplant (IMT) is a novel treatment approach that restores this diversity. We hypothesised that IMT performed prior to initiation of HCT conditioning restores microbiome diversity during the early stages of HCT, leading to decreased frequency of complications and improved outcomes of HCT.Methods and analysis 50 adult patients receiving allogeneic HCT will be recruited into this phase IIa trial and randomised 1:1 to receive capsulised IMT or matched placebo shortly prior to initiation of HCT conditioning and followed for up to 12 months. The primary outcome will be to assess the increase in alpha diversity between pre-IMT and that measured at ~42 days after IMT administration (day +28 of HCT), comparing the difference between patients receiving IMT compared with placebo. Secondary outcomes will include tolerability, the dynamics of gut microbiome diversity metrics and taxonomy over all time points assessed, as well as clinical outcomes (including burden of invasive infections, days of fever, admission to intensive care, development of graft-vs-host disease and mortality).Ethics and dissemination This study was approved by a UK Research Ethics Committee (REC reference: 23/NE/0105). Dissemination of results will be in concert with patient and public involvement group input and is expected to be primarily via abstract presentation at conferences and manuscripts in peer-reviewed journals.Trial registration numbers NCT6355583; EudraCT: 2022-003617-10.

Published
2024
Full Text
View/download PDF

24. Dual RNA-seq study of the dynamics of coding and non-coding RNA expression during Clostridioides difficile infection in a mouse model

Author

Victor Kreis, Claire Toffano-Nioche, Cécile Denève-Larrazet, Jean-Christophe Marvaud, Julian R. Garneau, Florent Dumont, Erwin L. van Dijk, Yan Jaszczyszyn, Anaïs Boutserin, Francesca D'Angelo, Daniel Gautheret, Imad Kansau, Claire Janoir, and Olga Soutourina

Subjects
dual RNA-seq, Clostridioides difficile, host-pathogen interactions, non-coding RNA, gut microbiota, Microbiology, QR1-502
Abstract

ABSTRACT Clostridioides difficile is the leading cause of healthcare-associated diarrhea in industrialized countries. Many questions remain to be answered about the mechanisms governing its interaction with the host during infection. Non-coding RNAs (ncRNAs) contribute to shape virulence in many pathogens and modulate host responses; however, their role in C. difficile infection (CDI) has not been explored. To better understand the dynamics of ncRNA expression contributing to C. difficile infectious cycle and host response, we used a dual RNA-seq approach in a conventional murine model. From the pathogen side, this transcriptomic analysis revealed the upregulation of virulence factors, metabolism, and sporulation genes, as well as the identification of 61 ncRNAs differentially expressed during infection that correlated with the analysis of available raw RNA-seq data sets from two independent studies. From these data, we identified 118 potential new transcripts in C. difficile, including 106 new ncRNA genes. From the host side, we observed the induction of several pro-inflammatory pathways, and among the 185 differentially expressed ncRNAs, the overexpression of microRNAs (miRNAs) previously associated to inflammatory responses or unknown long ncRNAs and miRNAs. A particular host gene expression profile could be associated to the symptomatic infection. In accordance, the metatranscriptomic analysis revealed specific microbiota changes accompanying CDI and specific species associated with symptomatic infection in mice. This first adaptation of in vivo dual RNA-seq to C. difficile contributes to unravelling the regulatory networks involved in C. difficile infectious cycle and host response and provides valuable resources for further studies of RNA-based mechanisms during CDI.IMPORTANCEClostridioides difficile is a major cause of nosocomial infections associated with antibiotic therapy classified as an urgent antibiotic resistance threat. This pathogen interacts with host and gut microbial communities during infection, but the mechanisms of these interactions remain largely to be uncovered. Noncoding RNAs contribute to bacterial virulence and host responses, but their expression has not been explored during C. difficile infection. We took advantage of the conventional mouse model of C. difficile infection to look simultaneously to the dynamics of gene expression in pathogen, its host, and gut microbiota composition, providing valuable resources for future studies. We identified a number of ncRNAs that could mediate the adaptation of C. difficile inside the host and the crosstalk with the host immune response. Promising inflammation markers and potential therapeutic targets emerged from this work open new directions for RNA-based and microbiota-modulatory strategies to improve the efficiency of C. difficile infection treatments.

Published
2024
Full Text
View/download PDF

25. EGR1 regulates oral epithelial cell responses to Candida albicans via the EGFR- ERK1/2 pathway

Author

Ruth E. Dickenson, Aize Pellon, Nicole O. Ponde, Olivia Hepworth, Lydia F. Daniels Gatward, Julian R. Naglik, and David L. Moyes

Subjects
EGR1, Candida, epithelial cell, Infectious and parasitic diseases, RC109-216
Abstract

Candida albicans is a fungal pathobiont colonizing mucosal surfaces of the human body, including the oral cavity. Under certain predisposing conditions, C. albicans invades mucosal tissues activating EGFR-MAPK signalling pathways in epithelial cells via the action of its peptide toxin candidalysin. However, our knowledge of the epithelial mechanisms involved during C. albicans colonization is rudimentary. Here, we describe the role of the transcription factor early growth response protein 1 (EGR1) in human oral epithelial cells (OECs) in response to C. albicans. EGR1 expression increases in OECs when exposed to C. albicans independently of fungal viability, morphology, or candidalysin release, suggesting EGR1 is involved in the fundamental recognition of C. albicans, rather than in response to invasion or “pathogenesis.” Upregulation of EGR1 is mediated by EGFR via Raf1, ERK1/2, and NF-κB signalling but not PI3K/mTOR signalling. Notably, EGR1 mRNA silencing impacts on anti-C. albicans immunity, reducing GM-CSF, IL-1α and IL-1β release, and increasing IL-6 and IL-8 production. These findings identify an important role for EGR1 in priming epithelial cells to respond to subsequent invasive infection by C. albicans and elucidate the regulation circuit of this transcription factor after contact.

Published
2024
Full Text
View/download PDF

26. Changes in intestinal permeability and gut microbiota following diet-induced weight loss in patients with metabolic dysfunction-associated steatohepatitis and liver fibrosis

Author

Dimitrios A. Koutoukidis, Sandi Yen, Paula Gomez Castro, Mariya Misheva, Susan A. Jebb, Paul Aveyard, Jeremy W. Tomlinson, Ferenc E. Mozes, Jeremy F. Cobbold, Jethro S. Johnson, and Julian R. Marchesi

Subjects
Diet, weight loss, intestinal permeability, gut microbiota, metabolic dysfunction-associated liver disease, Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Weight loss improves metabolic dysfunction-associated steatohepatitis (MASH). We investigated whether there were associated changes in intestinal permeability, short-chain fatty acids (SCFAs), and gut microbiota, which are implicated in the pathophysiology of MASH. Sixteen adults with MASH, moderate fibrosis, and obesity received a low-energy total diet replacement program for 12 weeks and stepped food re-introduction over the following 12 weeks (ISRCTN12900952). Intestinal permeability, fecal SCFAs, and fecal microbiota were assessed at 0, 12, and 24 weeks. Data were analyzed using mixed-effects linear regression and sparse partial least-squares regression. Fourteen participants completed the trial, lost 15% (95% CI: 11.2–18.6%) of their weight, and 93% had clinically relevant reductions in liver disease severity markers. Serum zonulin concentrations were reduced at both 12 and 24 weeks (152.0 ng/ml, 95% CI: 88.0–217.4, p

Published
2024
Full Text
View/download PDF

27. Faecal (or intestinal) microbiota transplant: a tool for repairing the gut microbiome

Author

Rohma Ghani, Despoina Chrysostomou, Lauren A Roberts, Madhumitha Pandiaraja, Julian R. Marchesi, and Benjamin H. Mullish

Subjects
Faecal microbiota transplant, gut microbiome, metabolome, antibiotic resistance, Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Faecal/intestinal microbiota transplant (FMT/IMT) is an efficacious treatment option for recurrent Clostridioides difficile infection, which has prompted substantial interest in FMT’s potential role in the management of a much broader range of diseases associated with the gut microbiome. Despite its promise, the success rates of FMT in these other settings have been variable. This review critically evaluates the current evidence on the impact of clinical, biological, and procedural factors upon the therapeutic efficacy of FMT, and identifies areas that remain nebulous. Due to some of these factors, the optimal therapeutic approach remains unclear; for example, the preferred timing of FMT administration in a heavily antibiotic-exposed hematopoietic cell transplant recipient is not standardized, with arguments that can be made in alternate directions. We explore how these factors may impact upon more informed selection of donors, potential matching of donors to recipients, and aspects of clinical care of FMT recipients. This includes consideration of how gut microbiome composition and functionality may strategically inform donor selection criteria. Furthermore, we review how the most productive advances within the FMT space are those where clinical and translational outcomes are assessed together, and where this model has been used productively in recent years to better understand the contribution of the gut microbiome to human disease, and start the process toward development of more targeted microbiome therapeutics.

Published
2024
Full Text
View/download PDF

28. Philly Building Philly: Identifying Local Government Best Practices for Improving HUD Section 3 Compliance in Philadelphia, Pennsylvania.

Author

Lutz, Julian R.

Subjects
Working poor -- Compensation and benefits -- Laws, regulations and rules, Construction industry -- Recruiting -- Laws, regulations and rules -- Alliances and partnerships, Employee selection -- Methods -- Demographic aspects -- Management, Interagency cooperation -- Laws, regulations and rules -- Methods, Best practices -- Analysis, Community development -- Methods -- Laws, regulations and rules, Low income housing -- Laws, regulations and rules, Workplace multiculturalism -- Management -- Laws, regulations and rules, Housing subsidies -- Laws, regulations and rules, State-city relations -- Management -- Laws, regulations and rules, Philadelphia, Pennsylvania. Housing Authority -- Powers and duties, Government regulation, Industry hiring, Hiring, Company business management, Housing and Urban Development Act of 1968 (12 U.S.C. 1701u)
Abstract

I. INTRODUCTION 448 II. SECTION 3'S HIRING AND CONTRACTING COMMITMENTS 450 A. Section 3 's Contents and Definitions 450 B. The Roots of the Problem: Contracting Requirements, Compliance, and Enforcement [...], This Note gives an overview of Section 3 of the Housing and Urban Development Act of 1968, commonly known as HUD Section 3. Section 3 requires that local governments that receive federal housing funds ensure the jobs and contracts the funds create go to residents of low-income areas. I first discuss HUD Section 3 's contents and legislative history, finding an ambitious mandate to train and contract with residents of low-income areas. Next, I describe HUD's long struggle to monitor and enforce that mandate and low-income residents' efforts to self-organize and claim their mandated benefits. Finding little federal enforcement, this Note studies Section 3 compliance and related local hiring laws in Philadelphia, Pennsylvania. Philadelphia's policies, maintained by the City of Philadelphia and the independent Philadelphia Housing Authority, are ambitious but underdeveloped. To find opportunities to improve them, the Note analyzes various cities' public works local hiring policies and assesses best practices for achieving Section 3 's goals. Finally, the Note argues Philadelphia's agencies have the potential to effectively coordinate a nation-leading Section 3 policy by setting realistic goals and collaborating with each other and with unions.

Published
2024

29. Phylogenomics and the rise of the angiosperms

Author

Zuntini, Alexandre R., Carruthers, Tom, Maurin, Olivier, Bailey, Paul C., Leempoel, Kevin, Brewer, Grace E., Epitawalage, Niroshini, Françoso, Elaine, Gallego-Paramo, Berta, McGinnie, Catherine, Negrão, Raquel, Roy, Shyamali R., Simpson, Lalita, Toledo Romero, Eduardo, Barber, Vanessa M. A., Botigué, Laura, Clarkson, James J., Cowan, Robyn S., Dodsworth, Steven, Johnson, Matthew G., Kim, Jan T., Pokorny, Lisa, Wickett, Norman J., Antar, Guilherme M., DeBolt, Lucinda, Gutierrez, Karime, Hendriks, Kasper P., Hoewener, Alina, Hu, Ai-Qun, Joyce, Elizabeth M., Kikuchi, Izai A. B. S., Larridon, Isabel, Larson, Drew A., de Lírio, Elton John, Liu, Jing-Xia, Malakasi, Panagiota, Przelomska, Natalia A. S., Shah, Toral, Viruel, Juan, Allnutt, Theodore R., Ameka, Gabriel K., Andrew, Rose L., Appelhans, Marc S., Arista, Montserrat, Ariza, María Jesús, Arroyo, Juan, Arthan, Watchara, Bachelier, Julien B., Bailey, C. Donovan, Barnes, Helen F., Barrett, Matthew D., Barrett, Russell L., Bayer, Randall J., Bayly, Michael J., Biffin, Ed, Biggs, Nicky, Birch, Joanne L., Bogarín, Diego, Borosova, Renata, Bowles, Alexander M. C., Boyce, Peter C., Bramley, Gemma L. C., Briggs, Marie, Broadhurst, Linda, Brown, Gillian K., Bruhl, Jeremy J., Bruneau, Anne, Buerki, Sven, Burns, Edie, Byrne, Margaret, Cable, Stuart, Calladine, Ainsley, Callmander, Martin W., Cano, Ángela, Cantrill, David J., Cardinal-McTeague, Warren M., Carlsen, Mónica M., Carruthers, Abigail J. A., de Castro Mateo, Alejandra, Chase, Mark W., Chatrou, Lars W., Cheek, Martin, Chen, Shilin, Christenhusz, Maarten J. M., Christin, Pascal-Antoine, Clements, Mark A., Coffey, Skye C., Conran, John G., Cornejo, Xavier, Couvreur, Thomas L. P., Cowie, Ian D., Csiba, Laszlo, Darbyshire, Iain, Davidse, Gerrit, Davies, Nina M. J., Davis, Aaron P., van Dijk, Kor-jent, Downie, Stephen R., Duretto, Marco F., Duvall, Melvin R., Edwards, Sara L., Eggli, Urs, Erkens, Roy H. J., Escudero, Marcial, de la Estrella, Manuel, Fabriani, Federico, Fay, Michael F., Ferreira, Paola de L., Ficinski, Sarah Z., Fowler, Rachael M., Frisby, Sue, Fu, Lin, Fulcher, Tim, Galbany-Casals, Mercè, Gardner, Elliot M., German, Dmitry A., Giaretta, Augusto, Gibernau, Marc, Gillespie, Lynn J., González, Cynthia C., Goyder, David J., Graham, Sean W., Grall, Aurélie, Green, Laura, Gunn, Bee F., Gutiérrez, Diego G., Hackel, Jan, Haevermans, Thomas, Haigh, Anna, Hall, Jocelyn C., Hall, Tony, Harrison, Melissa J., Hatt, Sebastian A., Hidalgo, Oriane, Hodkinson, Trevor R., Holmes, Gareth D., Hopkins, Helen C. F., Jackson, Christopher J., James, Shelley A., Jobson, Richard W., Kadereit, Gudrun, Kahandawala, Imalka M., Kainulainen, Kent, Kato, Masahiro, Kellogg, Elizabeth A., King, Graham J., Klejevskaja, Beata, Klitgaard, Bente B., Klopper, Ronell R., Knapp, Sandra, Koch, Marcus A., Leebens-Mack, James H., Lens, Frederic, Leon, Christine J., Léveillé-Bourret, Étienne, Lewis, Gwilym P., Li, De-Zhu, Li, Lan, Liede-Schumann, Sigrid, Livshultz, Tatyana, Lorence, David, Lu, Meng, Lu-Irving, Patricia, Luber, Jaquelini, Lucas, Eve J., Luján, Manuel, Lum, Mabel, Macfarlane, Terry D., Magdalena, Carlos, Mansano, Vidal F., Masters, Lizo E., Mayo, Simon J., McColl, Kristina, McDonnell, Angela J., McDougall, Andrew E., McLay, Todd G. B., McPherson, Hannah, Meneses, Rosa I., Merckx, Vincent S. F. T., Michelangeli, Fabián A., Mitchell, John D., Monro, Alexandre K., Moore, Michael J., Mueller, Taryn L., Mummenhoff, Klaus, Munzinger, Jérôme, Muriel, Priscilla, Murphy, Daniel J., Nargar, Katharina, Nauheimer, Lars, Nge, Francis J., Nyffeler, Reto, Orejuela, Andrés, Ortiz, Edgardo M., Palazzesi, Luis, Peixoto, Ariane Luna, Pell, Susan K., Pellicer, Jaume, Penneys, Darin S., Perez-Escobar, Oscar A., Persson, Claes, Pignal, Marc, Pillon, Yohan, Pirani, José R., Plunkett, Gregory M., Powell, Robyn F., Prance, Ghillean T., Puglisi, Carmen, Qin, Ming, Rabeler, Richard K., Rees, Paul E. J., Renner, Matthew, Roalson, Eric H., Rodda, Michele, Rogers, Zachary S., Rokni, Saba, Rutishauser, Rolf, de Salas, Miguel F., Schaefer, Hanno, Schley, Rowan J., Schmidt-Lebuhn, Alexander, Shapcott, Alison, Al-Shehbaz, Ihsan, Shepherd, Kelly A., Simmons, Mark P., Simões, André O., Simões, Ana Rita G., Siros, Michelle, Smidt, Eric C., Smith, James F., Snow, Neil, Soltis, Douglas E., Soltis, Pamela S., Soreng, Robert J., Sothers, Cynthia A., Starr, Julian R., Stevens, Peter F., Straub, Shannon C. K., Struwe, Lena, Taylor, Jennifer M., Telford, Ian R. H., Thornhill, Andrew H., Tooth, Ifeanna, Trias-Blasi, Anna, Udovicic, Frank, Utteridge, Timothy M. A., Del Valle, Jose C., Verboom, G. Anthony, Vonow, Helen P., Vorontsova, Maria S., de Vos, Jurriaan M., Al-Wattar, Noor, Waycott, Michelle, Welker, Cassiano A. D., White, Adam J., Wieringa, Jan J., Williamson, Luis T., Wilson, Trevor C., Wong, Sin Yeng, Woods, Lisa A., Woods, Roseina, Worboys, Stuart, Xanthos, Martin, Yang, Ya, Zhang, Yu-Xiao, Zhou, Meng-Yuan, Zmarzty, Sue, Zuloaga, Fernando O., Antonelli, Alexandre, Bellot, Sidonie, Crayn, Darren M., Grace, Olwen M., Kersey, Paul J., Leitch, Ilia J., Sauquet, Hervé, Smith, Stephen A., Eiserhardt, Wolf L., Forest, Félix, and Baker, William J.

Published
2024
Full Text
View/download PDF

30. Secretion of the fungal toxin candidalysin is dependent on conserved precursor peptide sequences

Author

Müller, Rita, König, Annika, Groth, Sabrina, Zarnowski, Robert, Visser, Corissa, Handrianz, Tom, Maufrais, Corinne, Krüger, Thomas, Himmel, Maximilian, Lee, Sejeong, Priest, Emily L., Yildirim, Deniz, Richardson, Jonathan P., Blango, Matthew G., Bougnoux, Marie-Elisabeth, Kniemeyer, Olaf, d’Enfert, Christophe, Brakhage, Axel A., Andes, David R., Trümper, Verena, Nehls, Christian, Kasper, Lydia, Mogavero, Selene, Gutsmann, Thomas, Naglik, Julian R., Allert, Stefanie, and Hube, Bernhard

Published
2024
Full Text
View/download PDF

31. 3D printed rectal swabs for assessing the gut microbiome, metabolome and inflammation

Author

Robert W. Perry, Benjamin H. Mullish, James L. Alexander, Raashi Shah, Nathan P. Danckert, Jesus Miguens Blanco, Lauren Roberts, Zhigang Liu, Despoina Chrysostomou, Shiva T. Radhakrishnan, Sharmili Balarajah, Rachael Barry, Lucy C. Hicks, Horace R. T. Williams, and Julian R. Marchesi

Subjects
Medicine, Science
Abstract

Abstract Investigating the gut microbiome and metabolome frequently requires faecal samples, which can be difficult to obtain. Previous studies have shown that rectal swabs are comparable to faecal samples for analysing gut microbiota composition and key metabolites. In this study, 3D printed rectal swabs were compared with conventional flocked swabs and faecal samples, due to the potential advantages 3D printing as a technique offers for swab production and development. 16S rRNA gene sequencing, qPCR and metabolite profiling (using 1H-NMR spectroscopy) were performed on swab and faecal samples from healthy participants. Faecal calprotectin and total protein analysis were performed on samples from inflammatory bowel disease (IBD) patients. There were no significant differences between both swab types and faecal samples when assessing key measures of alpha and beta diversity, and differences in the abundance of major phyla. There was a strong correlation between both swab types and faecal samples for all combined metabolites detected by NMR. In IBD patients, there was no significant difference in faecal calprotectin and total protein levels between both swab types and faecal samples. These data lead us to conclude that 3D printed swabs are equivalent to flocked swabs for the analysis of the gut microbiome, metabolome and inflammation.

Published
2024
Full Text
View/download PDF

32. Author Correction: Examining the healthy human microbiome concept

Author

Joos, Raphaela, Boucher, Katy, Lavelle, Aonghus, Arumugam, Manimozhiyan, Blaser, Martin J., Claesson, Marcus J., Clarke, Gerard, Cotter, Paul D., De Sordi, Luisa, Dominguez-Bello, Maria G., Dutilh, Bas E., Ehrlich, Stanislav D., Ghosh, Tarini Shankar, Hill, Colin, Junot, Christophe, Lahti, Leo, Lawley, Trevor D., Licht, Tine R., Maguin, Emmanuelle, Makhalanyane, Thulani P., Marchesi, Julian R., Matthijnssens, Jelle, Raes, Jeroen, Ravel, Jacques, Salonen, Anne, Scanlan, Pauline D., Shkoporov, Andrey, Stanton, Catherine, Thiele, Ines, Tolstoy, Igor, Walter, Jens, Yang, Bo, Yutin, Natalia, Zhernakova, Alexandra, Zwart, Hub, Doré, Joël, and Ross, R. Paul

Published
2025
Full Text
View/download PDF

38. Pigment epithelium derived factor drives melanocyte proliferation and migration in neurofibromatosis café au lait macules

Author

Charlotte Lovatt, Megan Williams, Alex Gibbs, Abdullahi Mukhtar, Huw J. Morgan, Simone Lanfredini, Carlotta Olivero, Gill Spurlock, Sally Davies, Charlotte Philpott, Hannah Tovell, Peter Turnpenny, Dilair Baban, Sam Knight, Hilde Brems, Julian R. Sampson, Eric Legius, Meena Upadhyaya, and Girish K. Patel

Subjects
Dermatology, RL1-803
Abstract

Abstract Background RASopathies, which include neurofibromatosis type 1 (NF1), are defined by Ras/mitogen‐activated protein kinase (Ras/MAPK) pathway activation. They represent a group of clinically related disorders often characterised by multiple Café au Lait Macules (CALMs). Objectives To determine, using in depth transcriptomic analysis of NF1 melanocytes from CALM and unaffected skin, (1) the gene(s) responsible for melanocyte proliferation and migration, and (2) the activated signalling pathway(s) in NF1 melanoma. Methods Classical NF1 (n = 2, who develop tumours) and 3bp deletion NF1 (p. Met992del, who do not develop tumours) (n = 3) patients underwent skin biopsies from CALM and unaffected skin. Melanocytes were isolated and propagated, with five replicates from each tissue sample. DNA and RNA were extracted for mutational analysis and transcriptomic profiling with six replicates per sample. Mechanistic determination was undertaken using melanocyte and melanoma cell lines. Results All CALMs in NF1 were associated with biallelic NF1 loss, resulting in amplification of Ras/MAPK and Wnt pathway signalling. CALMs were also associated with reduced SERPINF1 gene expression (and pigment epithelium‐derived factor (PEDF) levels, the reciprocal protein), a known downstream target of the master regulator of melanocyte differentiation microphthalmia‐associated transcription factor (MITF), leading to increased melanocyte proliferation, migration and invasion. In classical NF1 and melanoma, but not 3bp deletion NF1, there was also activation of the PI3K/AKT pathway. Pigment epithelium‐derived factor was found to reduce cell proliferation and invasion of NF1 melanoma. Conclusions Melanocyte proliferation and migration leading to CALMs in NF1 arises from biallelic NF1 loss, resulting in RAS/MAPK pathway activation, and reduced expression of the tumour suppressor PEDF. Activation of the PI3K/AKT pathway in classical NF1 and NF1 melanoma may facilitate tumour growth.

Published
2024
Full Text
View/download PDF

41. Enabling Dynamic and Intelligent Workflows for HPC, Data Analytics, and AI Convergence

Author

Ejarque, Jorge, Badia, Rosa M., Albertin, Loïc, Aloisio, Giovanni, Baglione, Enrico, Becerra, Yolanda, Boschert, Stefan, Berlin, Julian R., D'Anca, Alessandro, Elia, Donatello, Exertier, François, Fiore, Sandro, Flich, José, Folch, Arnau, Gibbons, Steven J, Koldunov, Nikolay, Lordan, Francesc, Lorito, Stefano, Løvholt, Finn, Macías, Jorge, Marozzo, Fabrizio, Michelini, Alberto, Monterrubio-Velasco, Marisol, Pienkowska, Marta, de la Puente, Josep, Queralt, Anna, Quintana-Ortí, Enrique S., Rodríguez, Juan E., Romano, Fabrizio, Rossi, Riccardo, Rybicki, Jedrzej, Kupczyk, Miroslaw, Selva, Jacopo, Talia, Domenico, Tonini, Roberto, Trunfio, Paolo, and Volp, Manuela

Subjects
Computer Science - Distributed, Parallel, and Cluster Computing
Abstract

The evolution of High-Performance Computing (HPC) platforms enables the design and execution of progressively larger and more complex workflow applications in these systems. The complexity comes not only from the number of elements that compose the workflows but also from the type of computations they perform. While traditional HPC workflows target simulations and modelling of physical phenomena, current needs require in addition data analytics (DA) and artificial intelligence (AI) tasks. However, the development of these workflows is hampered by the lack of proper programming models and environments that support the integration of HPC, DA, and AI, as well as the lack of tools to easily deploy and execute the workflows in HPC systems. To progress in this direction, this paper presents use cases where complex workflows are required and investigates the main issues to be addressed for the HPC/DA/AI convergence. Based on this study, the paper identifies the challenges of a new workflow platform to manage complex workflows. Finally, it proposes a development approach for such a workflow platform addressing these challenges in two directions: first, by defining a software stack that provides the functionalities to manage these complex workflows; and second, by proposing the HPC Workflow as a Service (HPCWaaS) paradigm, which leverages the software stack to facilitate the reusability of complex workflows in federated HPC infrastructures. Proposals presented in this work are subject to study and development as part of the EuroHPC eFlows4HPC project.

Published
2022
Full Text
View/download PDF

43. Novel gastrointestinal tools (GI Tools) for evaluating gut functional capacity in adults with environmental enteropathy in Zambia and Zimbabwe: A cross-sectional study protocol [version 1; peer review: awaiting peer review]

Author

Tracy N. Phiri, James W. Weatherill, Elena Monford-Sanchez, Jose-Ivan Serrano-Contreras, Callum Melvin, Mirriam Kunaka, Ian Chisenga, Perpetual Ngalande, Monica N. Mweetwa, Ellen Besa, Tafhima Haider, Nilanjan Mandal, Alex J. Thompson, Christine A. Edwards, Claire D. Burke, Ruairi C. Robertson, Joram M. Posma, Rosemary Banda, Mulima Mwiinga, Lydia Kazhila, Leolin Katsidzira, Mutsa Bwakura-Dangarembizi, Beatrice Amadi, Isabel Garcia-Perez, Kathryn Maitland, Julian R. Marchesi, Douglas J. Morrison, Gary Frost, and Paul Kelly

Subjects
Study Protocol, Articles, Environmental Enteric Dysfunction, Intestinal Absorption, Intestinal Permeability, Microbiome, Stable Isotopes
Abstract

Background Environmental enteropathy (EE) is a highly prevalent subclinical inflammatory intestinal disorder associated with growth failure, impaired neurocognitive development, poor response to oral vaccines, and micronutrient deficiencies. However, EE research and clinical trials are hampered by the lack of non-invasive tools for measuring intestinal function in detail. This study aims to develop new tools for the measurement of multiple domains of gut functional capacity. Methods The GI TOOLS project is a cross-sectional study that will recruit adults aged 18-65 years with EE in Lusaka, Zambia. Each participant will undergo assessment of gut functional capacity using novel near-point-of-care tools and provide multiple samples for detailed laboratory analyses. Participants will also undergo endoscopy for collection of duodenal biopsies. Novel techniques include stable isotopes approaches to measuring digestion, absorption, and bidirectional transmucosal amino acid flux, a non-invasive fluorescence tool for real-time evaluation of gut permeability, and assessment of reverse permeation of intravenous antibiotics to be carried out separately in Zimbabwe. Stool and duodenal microbiome sequencing using MinION sequencing, metabolome analysis applied to plasma and intestinal fluids, blood immune cell phenotyping, in vitro epithelial barrier models, and duodenal immunohistochemistry will also be used to explore EE in depth. These will all be integrated with gold standard histology and mucosal morphometry, alongside lactulose permeation data, and stool and plasma biomarker analysis. The protocol has been approved by ethics committees and regulators in Zambia, Zimbabwe, and the UK. Participants will give informed consent before they can participate Anticipated outcomes Based on this extensive phenotyping, tests will be developed which can be simplified and refined for use in adults and children with EE, and for clinical trials. Findings from this project will be disseminated through in-person meetings with caregivers and regulatory bodies, presentations at conferences and in peer-reviewed journals.

Published
2024
Full Text
View/download PDF

47. Variations in candidalysin amino acid sequence influence toxicity and host responses

Author

Don N. Wickramasinghe, Claire M. Lyon, Sejeong Lee, Olivia W. Hepworth, Emily L. Priest, Corinne Maufrais, Adam P. Ryan, Emmanuelle Permal, Derek Sullivan, Brenda A. McManus, Bernhard Hube, Geraldine Butler, Christophe d'Enfert, Julian R. Naglik, and Jonathan P. Richardson

Subjects
Candida, candidalysin, fungus, toxin, epithelial, Microbiology, QR1-502
Abstract

ABSTRACT Candida albicans causes millions of mucosal infections in humans annually. Hyphal overgrowth on mucosal surfaces is frequently associated with tissue damage caused by candidalysin, a secreted peptide toxin that destabilizes the plasma membrane of host cells thereby promoting disease and immunopathology. Candidalysin was first identified in C. albicans strain SC5314, but recent investigations have revealed candidalysin “variants” of differing amino acid sequence in isolates of C. albicans, and the related species C. dubliniensis, and C tropicalis, suggesting that sequence variation among candidalysins may be widespread in natural populations of these Candida species. Here, we analyzed ECE1 gene sequences from 182 C. albicans isolates, 10 C. dubliniensis isolates, and 78 C. tropicalis isolates and identified 10, 3, and 2 candidalysin variants in these species, respectively. Application of candidalysin variants to epithelial cells revealed differences in the ability to cause cellular damage, changes in metabolic activity, calcium influx, MAPK signalling, and cytokine secretion, while biophysical analyses indicated that variants exhibited differences in their ability to interact with and permeabilize a membrane. This study identifies candidalysin variants with differences in biological activity that are present in medically relevant Candida species.IMPORTANCEFungal infections are a significant burden to health. Candidalysin is a toxin produced by Candida albicans that damages host tissues, facilitating infection. Previously, we demonstrated that candidalysins exist in the related species C. dubliniensis and C. tropicalis, thereby identifying these molecules as a toxin family. Recent genomic analyses have highlighted the presence of a small number of candidalysin “variant” toxins, which have different amino acid sequences to those originally identified. Here, we screened genome sequences of isolates of C. albicans, C. dubliniensis, and C. tropicalis and identified candidalysin variants in all three species. When applied to epithelial cells, candidalysin variants differed in their ability to cause damage, activate intracellular signaling pathways, and induce innate immune responses, while biophysical analysis revealed differences in the ability of candidalysin variants to interact with lipid bilayers. These findings suggest that intraspecies variation in candidalysin amino acid sequence may influence fungal pathogenicity.

Published
2024
Full Text
View/download PDF

49. Group divisible designs with block size 4 and group sizes 2 and 5

Author

Abel, R. Julian R., Britz, Thomas, Bunjamin, Yudhistira A., and Combe, Diana

Subjects
Mathematics - Combinatorics, 05B05
Abstract

In this paper we provide a $4$-GDD of type $2^2 5^5$, thereby solving the existence question for the last remaining feasible type for a $4$-GDD with no more than $30$ points. We then show that $4$-GDDs of type $2^t 5^s$ exist for all but a finite specified set of feasible pairs $(t,s)$.

Published
2021
Full Text
View/download PDF

50. Gut microbiomes of agropastoral children from the Adadle region of Ethiopia reflect their unique dietary habits

Author

Simon Yersin, Julian R. Garneau, Pierre H. H. Schneeberger, Kadra Ali Osman, Colin Ivano Cercamondi, Abdifatah Muktar Muhummed, Rea Tschopp, Jakob Zinsstag, and Pascale Vonaesch

Subjects
Medicine, Science
Abstract

Abstract The composition and function of the intestinal microbiota are major determinants of human health and are strongly influenced by diet, antibiotic treatment, lifestyle and geography. Nevertheless, we currently have only little data on microbiomes of non-westernized communities. We assess the stool microbiota composition in 59 children aged 2–5 years from the Adadle district of Ethiopia, Somali Regional State. Here, milk and starch-rich food are predominant components of the local diet, where the inhabitants live a remote, traditional agropastoral lifestyle. Microbiota composition, function and the resistome were characterized by both 16S rRNA gene amplicon and shotgun metagenomic sequencing and compared to 1471 publicly available datasets from children living in traditional, transitional, and industrial communities with different subsistence strategies. Samples from the Adadle district are low in Bacteroidaceae, and Prevotellaceae, the main bacterial representatives in the feces of children living in industrialized and non-industrialized communities, respectively. In contrast, they had a higher relative abundance in Streptococcaceae, Bifidobacteriaceae and Erysipelatoclostridiaceae. Further, genes involved in degradation pathways of lactose, d-galactose and simple carbohydrates were enriched. Overall, our study revealed a unique composition of the fecal microbiota of these agropastoral children, highlighting the need to further characterize the fecal bacterial composition of human populations living different lifestyles.

Published
2023
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results